Dependency of neck-of-the-flow
\r\n\tDigital images can be easily distorted by noise during the acquisition, processing, and transmission. Noise level is an important parameter to consider in image processing algorithms, including denoising, compression, feature extraction, motion estimation, optical flow, segmentation, super-resolution, and image quality assessment. Their performance depends on the accuracy of the noise level estimate.
\r\n\r\n\tImage denoising is an important stage to improve the accuracy of many image processing techniques, such as image segmentation and recognition. Image segmentation is another important stage in computer vision applications. Many methodologies utilize both stages in a unique algorithm to solve the problem of the segmentation of noisy images to provide better classification and recognition compared to algorithms that independently use these two stages.
\r\n\tThe goal of this book will be to collect original research chapters that develop or apply new theories and/or hardware or software to process the acquired noisy images to solve the problem of Segmentation of noisy images in the field of medical imaging, remote sensing, engineering, and other research applications.
Relativity theory plays a key role in the operation of the Global Positioning System (GPS). It relies on Einstein’s second postulate of the special theory of relativity (STR) [1] that states that the speed of light in free space is a constant (c), independent of the state of motion of both the source and the observer. As a result, it becomes possible to measure distances using atomic clocks. Indeed, the modern-day definition of the meter is the distance travelled by a light pulse in c-1 s [2]. The value of the speed of light in free space is simply defined to have a fixed value of c=2.99792458 x 108 ms-1. As a consequence, the distance Δr between two fixed points is therefore obtained by measuring the elapsed time Δt for light to traverse it and multiplying this value with c, i.e., Δr = c Δt.
A key objective in the GPS methodology is to accurately measure the distance between an orbiting satellite and a given object. This type of basic information for a series of satellites can then be used to accurately determine the location of the object [3]. The measurement of the elapsed time for light to pass between two points requires communication between atomic clocks located at each position. The problem that needs to be overcome in the GPS methodology is that the rates of the clocks carried onboard satellites are not the same as those that are stationary on the Earth’s surface. For this reason it is imperative that we have a quantitative understanding of how the rates of clocks vary with their state of motion and position in a gravitational field. This topic will be covered in the next section of this chapter.
It also must be recognized that the speed of light only remains constant as it moves through free space and also remains at the same gravitational potential. This is an important distinction that has significant practical consequences when the light pulses must pass through regions in which space-weather events are occurring.
Experimental and theoretical studies of the state of the ionosphere and physicochemical processes that occur in it are caused by the necessity of reliable functioning of communication channels in different frequency bands. In recent years, most attention is paid to the improvement of satellite communication and navigation systems that use transionospheric communication channels. The reliability of communication and navigation systems using ionospheric communication channels depends mainly on the knowledge of the ionosphere behavior both in quiet and perturbed conditions. This determines the situation when not only ionospheric plasma perturbations related to the dynamics of the atmosphere but also processes related to electromagnetic wave interaction with neutral atoms and molecules of the medium in which the wave propagates should be treated as inhomogeneities. On the other hand, an analysis of disturbances and failures of operation of space communication systems that use the decimeter wave range and the development of theoretical concepts of physical processes responsible for these phenomena gives new information about the state of the medium and provides the opportunities for further improvement of communication systems. This led to the necessity of the development of special experimental techniques for studying the ionosphere in order to determine the physical reasons for GPS signal delays. In the second part of this Chapter the role of Rydberg atoms and molecules of neutral ionospheric plasma components excited in collisions with electrons in the formation of UHF and infrared radiations of the E – and D– layers of Earth’s ionosphere is discussed. A new physical mechanism of satellite signal delay due to a cascade of re-emissions on Rydberg states in the decimeter range is suggested.
One of the key results of Maxwell’s theory of electromagnetism introduced in 1864 was the finding that the speed of light waves has a constant value that is given by the relation:
Maxwell’s equations are not invariant to the Galilean transformation and therefore seemed to be inconsistent with the relativity principle (RP). Voigt [4] was the first [5] to give a different space-time transformation that did accomplish this objective. It differed by a constant factor in all of its equations from what is now known as the Lorentz transformation (LT). In 1899 Lorentz wrote down a general version of this transformation [6]:
The space-time coordinates (
The form of the above equations suggested that the Newtonian concept of absolute time needed to be altered in order to be consistent with Maxwell’s electromagnetic theory and corresponding experimental observations. Unlike the simple
In 1905 Einstein’s paper [1] on what he later referred to as the special theory of relativity (STR) became the focus of attention, although at least a decade passed before his ideas gained wide acceptance among his fellow physicists. He came out strongly against the necessity of there being an aether which serves as the medium in which light is carried. He argued instead that such a concept is superfluous, and likewise that there is no space in absolute rest and no “velocity vector associated with a point of empty space in which electromagnetic processes take place” [11]. He formulated his version of electromagnetic theory on the basis of two well-defined postulates, the RP and the constancy of the speed of light in free space independent of the state of motion of the detector/observer or the source of the light. Starting from this basis, Einstein went on to derive a version of the relativistic space-time transformation that leaves Maxwell’s equations invariant. It is exactly the same transformation that Larmor [8] had reported five years earlier and has ever since been referred to as the Lorentz transformation (LT), i.e. with a value of
One of the most interesting features of Einstein’s derivation of the LT is that it contains a different justification for choosing a value of unity for
Einstein proposed a number of intriguing experiments to test STR, many of which involved the phenomenon of time dilation. The relationship between the time intervals
whereby Δx is the distance between the locations of the clock in S at the times the measurements are made there. If one has the normal situation in which the two measurements are made at exactly the same location in S, i.e. with
This equation corresponds to time dilation in the rest frame of the observer in S. It states that the observer in
The corresponding relation between time intervals thus becomes
when one makes the standard assumption that the measurements are carried out at the same location in
The same type of symmetry arises for length measurements, in which case analogous manipulations of eq. (1b) and its inverse lead to both:
which are the FLC predictions in the direction parallel to the relative velocity of the two observers. The orthodox interpretation is that length contraction and time dilation occur together in both rest frames, i.e. eq. (5) goes with eq. (6), whereas eq. (3) goes with eq. (7). In other words, lengths on the moving object contract in the parallel direction at the same time (and by the same factor) that the rates of its clocks slow down. There is no difference in the length measurements in directions that are perpendicular to the relative velocity of the two rest frames according to STR [1], as is easily seen from eqs. (1c-d) using the value of
It is important see that the above symmetry in the predicted results of the two observers represents a stark departure from the long-held belief in the
Einstein’s belief in the above symmetry principle was by no means absolute, however. In the same paper [1], he includes a discussion of a clock that moves from its original rest position and returns via a closed path at some later time. The conclusion is that the rate of the moving clock is decreased during its journey, so that upon return to the point of origin it shows a smaller value for the elapsed time than an identical clock that remained stationary there. The symmetry is broken by the fact that it is possible to distinguish which clock remained at rest in the original inertial system and which did not [1,16]. Einstein ends the discussion by concluding that a clock located at the Equator should run slower by a factor of
The answers to the above questions could only be determined by experiments which were not yet available in 1905. For example, Einstein pointed out that time dilation should produce a transverse (second-order) Doppler effect not expected from the classical theory of light propagation. Eqs. (3) and (5) indicate that a moving light source should emit a lower frequency (greater period) of radiation for a given observer than that of an identical stationary source in his laboratory. The symmetry principle derived from the LT indicates that two observers exchanging light signals should each measure a
Two years later [17], Einstein used the results of his 1905 paper to derive the Equivalence Principle (EP) between kinematic acceleration and gravity. His analysis of electromagnetic interactions at different gravitational potentials led him to make several more revolutionary predictions on the basis of the EP. First of all, he concluded that the light-speed postulate did not have universal validity. He claimed instead that it should increase with the altitude of the light source. At the same time, he determined that the frequency of light waves should increase as the source moves to a higher gravitational potential. Consequently, light emanating from the Sun should be detected on the Earth’s surface with a lower frequency than for an identical source located there. This effect has since been verified many times and in general is referred to as the
The first significant test of Einstein’s time-dilation theory was carried out by Ives and Stilwell in 1938 [18]. The object of this experiment is to measure the wavelength
(
The accuracy of the Ives-Stilwell experiment was gradually improved. It was later estimated that the actual experimental uncertainty in the original investigation lay in the 10-15% range, although the experimental points could be fitted to a curve with as little as 2-3% deviation. Mandelberg and Witten [19] made substantial improvements in the overall procedure, using hydrogen ion velocities of up to 0.0093 c. Their results indicate that the exponent in the
In spite of the generally good agreement between theory and experiment with regard to the time-dilation effect, there is still a loose end that has been almost universally ignored in the ensuing discussion. It is clear that the predicted slowing down of clocks in the transverse Doppler investigations is accompanied by an increase in wavelength, not the
Shortly after the first Ives-Stilwell investigation, Rossi and coworkers [20] reported on their measurements of the transition rate of cosmic-ray muons and other mesons traveling at different speeds relative to the Earth’s atmosphere. The effect of time dilation is much greater in this experiment since the particles are observed to move with speeds exceeding
In the original studies of meson decays in the atmosphere [20], the quantity which was determined experimentally is the average range before decay L. It was assumed that the value of L is proportional to both the speed v of the particles and their lifetime
The above two experiments were in quantitative agreement with Einstein’s predictions about the amount of time dilation [1], but neither one of them provided a test for the truly revolutionary conclusion that measurement is
Hay et al. [25] carried out x-ray frequency measurements employing the Mössbauer effect that had the potential of resolving this question. Both the light source and the absorber/detector were mounted on an ultracentrifuge that attained rotational speeds of up to 500 revolutions per second. The authors thereby eliminated the angular dependence in eq. (8) by ensuring that the relative motion of the source to the detector was almost perfectly transverse (
According to Einstein’s LT [1], the above distinction should have no bearing on the outcome of the experiment. This point is borne out by Will’s analysis of the transverse Doppler effect [26] in which he expresses the expected result as follows [see his eq. (6)]:
where
In describing their experimental results, Hay et al. [25] state that the “expected shift can be calculated in two ways.” By this they mean either by treating the acceleration of the rotor as an effective gravitational field (Einstein’s EP) or by “using the time dilatation of special relativity.” However, the empirical formula they report for the expected fractional shift in both the energy and frequency of the gamma rays is not consistent with eq. (9) since it is proportional to
The rotor experiments were also carried out later by Kündig [28] and by Champeney et al. [29]. The latter authors report their results in terms of the speeds va and vs of the absorber and the x-ray source, respectively:
This result makes several additional points clear: a) there is a shift to higher frequency (to the blue) if the absorber is rotating faster than the source and b) the magnitude of the shift is consistent with a higher-order formula:
If the x-ray source is at rest in the laboratory (
where
It is important to see that the alternative derivation [29] of the empirical formula for frequency shifts given in eq. (10) that makes use of Einstein’s EP [17] also corresponds to an objective theory of measurement. Accordingly, one assumes the relationship for the gravitational red shift [30]:
where the centrifugal field of force corresponds to a radial gravitational field strength of
The gravitational red shift derived in Einstein’s Jahrbuch review [17] is expressed in the equation below [cf. eq. (13)]:
In this formula, νX is the frequency of light emitted from a source that is at rest at a given gravitational potential, whereas νD is the corresponding value of the frequency detected by an observer who is not in relative motion to the source but is located at some other position in the gravitational field. The potential energy difference
The same proportionality factor occurs [17,34] in the relationship between the light speeds measured at the same two positions in the gravitational field, where
As a result, it is clear that according to the EP, both the frequency and the speed of light increase as the light source moves to a higher gravitational potential. Moreover, the fractional amount of the change is the same in both cases. As will be discussed in the following, there is ample experimental evidence to indicate that both of these relations are correct.
Terrestrial confirmation of the gravitational red shift first became possible with the advent of the Mössbauer technique for detecting changes in x-ray frequencies. Pound and Snider [35] placed a 57Fe source at a distance h of 22.5 m above an absorber. According to eq. (14), the fractional change in the x-ray frequency (3.47x1018 Hz) should have a value of ghc-2=2.45x10-15. The authors employed the EP directly to obtain their results. By imparting a downward velocity of
The observed results were found to be within expectations by a factor of 0.9990±0.0076 [35].
The interpretation of the above experiment is nonetheless a matter of some confusion. Pound and Snider [35] basically avoided a theoretical discussion of the ramifications of their work vis-à-vis the general theory of relativity (GTR [36]), but they noted that “the description of the effect as an ‘apparent weight’ of photons is suggestive. The velocity difference predicted is identical to that which a material object would acquire in free fall for a time equal to the time of flight.” The latter value is assumed to be
The above discussion raises another question, however, namely what happens to the speed of light as it descends from the source? According to eq. (15) and Einstein’s EP [17,34], the answer is clearly that it decreases, and by the same fractional amount as for the associated frequency red shift given in eq. (14). To be specific for the Pound-Snider example, the speed of light must have a value of c at ground level for an observer located there, whereas the same observer measures the value at the light source to be ghc-2 times larger. In other words, the speed of light actually
There is another important question that needs to be considered in the present discussion, however, namely what happens to the
It is important in general to recognize that in each of eqs. (14,15,17), the same quantity is the object of measurement for two different observers. The only reason why these observers do not obtain the same result in each case
It is useful to employ the above concepts to follow the course of the light pulses in the Pound-Snider experiment [35]. The analysis of two events is sufficient to illustrate the main points in this discussion, namely the initial emission of the x-rays at the higher gravitational potential (I) and their subsequent arrival at the absorber (II). It is important to use the same set of units in comparing the corresponding measured results. In terms of the units at the x-ray source, the observer X there measures the following values for event I:
The observer D located at the absorber measures generally different values for the same two events, not because he is considering fundamentally different processes, but rather because he bases his numerical results on a different system of physical units (PRM). He therefore finds for event II:
In absolute terms what has happened as a result of the downward passage of the x-rays between source and absorber/detector is that the light frequency has remained constant throughout the entire process, exactly as Einstein demanded in his Jahrbuch review [17]. On the other hand, both the light speed and the corresponding wavelength of the radiation have deceased by a factor of S. This is in agreement with Einstein’s second postulate of STR [1], namely that the observer at the absorber must find that the speed of light when it arrives there has a value of c in his units because it is at the same gravitational potential as the observer at that point in time.
Before closing this section, it is worthwhile to mention how the units of other physical properties vary/scale with gravitational potential. To begin with, energy E satisfies the same proportionality relationship as for frequency and light speed [see eqs. (14,15)]:
Indeed, one can derive this equation to a suitable approximation using Newton’s gravitational theory and the definition of gravitational potential energy as
Einstein also stated in his Jahrbuch article [17] that the above dependence of energy on gravitational potential implies that there is a position-dependent component corresponding to an inertial mass m equal to E/c2 [40]. Because E and c [i.e. the generic speed of light of eq. (15)] both vary as S, it follows that the unit of inertial mass scales as S-1, the same as time. Values of linear momentum
Despite the progress that had been made in carrying out experiments that verify various aspects of Einstein’s STR [1], there was still considerable uncertainty as to how to predict the results of future investigations of the time-dilation effect by the time the next significant advance was made in 1971. At that time, Hafele and Keating [43-44] carried out tests of cesium atomic clocks located onboard circumnavigating airplanes that traveled in opposite directions around the globe. In their introductory remarks, the authors noted that the “relativistic clock paradox” was still a subject of “the most enduring scientific debates of this century.” The first paper presents some predictions of the expected time differences for clocks located on each airplane as well as at the origin of their respective flights. Their calculations are clearly based on an
All speeds to be inserted into eq. (12) must therefore be computed relative to the Earth’s non-rotating polar axis, or more simply, relative to the gravitational midpoint of the Earth itself. The latter therefore serves the same purpose as the rotor axis in the Hay et al. experiments [25] discussed in Sect. III.C. In short, the rotational speed RΩ
The interesting conclusion is that a clock traveling in the westerly direction with the same ground speed (
The latter expression does not include the effect of the gravitational red shift discussed in Sect. III.D. If the altitude of the airplane relative to the ground is h, the ratio becomes:
The gravitational increase in clock rate on the airplane was typically somewhat smaller than the time-dilation effect for the clock traveling eastward, so that the overall effect was still a decrease in its rate relative to the clock at the airport. The two effects reinforce each other for the airplane traveling in the westerly direction.
The predicted effects were mirrored in the experimental data [44]. The observed time difference between the ground and easterly traveling clocks was -40 ± 23 ns as compared to the predicted value of -59 ± 10 ns. The corresponding values for the westward traveling clock were +275 ± 21 ns vs. 273 ± 7 ns. The main sources of error were due to instabilities in the cesium clock rates and uncertainties in the actual flight path of the airplanes.
The transverse Doppler effect was again used to study the effects of motion and gravity on clock rates in an experiment carried out in 1976 by Vessot and Levine [45]. The frequency of a hydrogen-maser oscillator system carried onboard a rocket was measured as it moved up and down in the Earth’s gravitational field. The first-order Doppler effect was eliminated by using a transponder system on the rocket, leaving only the second-order transverse Doppler effect and the gravitational red shifts as the cause of the observed frequency shifts. The flight lasted for nearly two hours and carried the rocket to a maximum altitude of 10000 km.
The speed of the rocket was monitored as a function of altitude and the amount of the frequency shift was predicted on the basis of eq. (20) except that one took into account the variation of g with altitude to obtain the desired accuracy and also consider the effect of the centrifugal acceleration of the ground station [see eq. (1) of Ref. 45]. The position and velocity of both the rocket and the ground station were measured in an Earth-centered inertial frame, consistent with the assumptions of the Hafele-Keating analysis [43] of their data for circumnavigating airplanes. It was also necessary to take account of the refractive index of the ionosphere as the rocket passed through this region of space. The Doppler-canceling feature of the experiment was also successful in removing the gross effects of such variations.
The authors concluded that the rocket experiment was consistent with Einstein’s EP to a suitably high level of accuracy. By assuming the validity of the EP, they were also able to place an upper bound on the ratio of the one-way and two-way velocity of light. The corresponding Δc/c values ranged from 1.9x10-8 to -5.6x10-8 during various parts of the rocket’s trajectory.
The experiments described in the preceding question provide the necessary empirical data to enable the accurate prediction of how the rates of clocks vary as they are carried onboard rockets and satellites. This information is critical for the success of the Global Positioning System because of the need to measure the elapsed times of light signals to pass between its satellites and the Earth’s surface.
Before considering how to make the desired predictions based on the above experience, it is interesting to examine how Einstein’s original theory of clock rate variations [1] has held up in the light of actual experiments. There has been unanimity in the theoretical discussions accompanying these experiments in claiming that their results mirror perfectly Einstein’s predictions. This is particularly true of the authors of the transverse Doppler experiments using high-speed rotors [25,28-29] as well as for Hafele and Keating in their investigations of the rates of atomic clocks onboard circumnavigating airplanes [43,44].
Such an evaluation overlooks the basic point discussed in Sect. II, however, namely that Einstein had two clearly distinguishable conclusions regarding the question of which of two identical clocks in relative motion runs slower in a given experiment [1]. One set of predictions was based on the LT and the conclusion that all inertial systems are equivalent by virtue of the RP. This is a thoroughly
There is no doubt which of Einstein’s two conclusions is meant by the various authors when they assert that their results are perfectly consistent with relativity theory. This point was made quite clear in Sherwin’s analysis [31] of the rotor experiments, which he referred to as a demonstration of “the transverse Doppler effect for accelerating systems.” It is the
A simpler alternative view is that the Earth’s center of mass (ECM) plays the same role for clock rates as for falling bodies. The only way to change the direction in which free fall occurs is to somehow escape the gravitational pull of the Earth. This has been most notably accomplished with the NASA expeditions to the Moon, in which case there is a definite point in the journey where the rocket tends to fall away from planet Earth and towards its satellite instead. It also occurs in a more conventional fashion when a body undergoes sufficient centrifugal acceleration in a parallel direction to the Earth’s surface. In this view, the ORS [46] for computing time dilation is always the same as the reference point for free fall, and thus is subject to change in exactly the same manner. The current speed of the Earth relative to the Sun is therefore irrelevant for the quantitative prediction of clock rates for the applications at hand.
There is a far less subtle point to be considered in the present discussion, however. The conclusion that an accelerated clock always runs slower than one that remains at its original rest location has very definite consequences as far as relativity theory is concerned. It shows unequivocally that Einstein’s symmetry principle [1] is violated, and therefore that the LT is contradicted by the experimental findings. Discussions in the literature [30-32] always emphasize that the acceleration effect was predicted by Einstein in his original paper [1] and that it is also entirely consistent with his EP [17], but there is never any mention of the conflict with the LT, which is after all the essential cornerstone of STR from which many long-accepted conclusions follow. The latter include most especially the FLC and remote non-simultaneity. Showing that the LT fails in one of its most basic predictions, the ambiguity in the ordering of local clock rates for two moving observers [31], necessarily raises equally critical questions about the validity of all its other conclusions. For example, does Lorentz invariance hold for the space and time variables under these experimental conditions? Are two events that occur at exactly the same time for one observer not simultaneous for someone else who happens to be moving relative to him? The latter question is particularly important for the GPS methodology since it relies on the assumption that the time of emission of a light signal is the same on the ground as on an orbiting satellite as long as one corrects for differences in clock rates at the respective locations. We will return to these questions in Sect. V, but first attention will be focused on the way in which the available experimental data on clock rate variations can be applied in practice.
There are two causes of clock-rate variations in terrestrial experiments. Both of them involve the ECM, one depending exclusively on the speed of a given clock relative to that position and the other on the corresponding difference in gravitational potential. As a result, in comparing different clocks on the Earth’s surface, it is necessary to know both the latitude
According to eq. (12), this ratio tells us how much slower (if
where r is the distance of the clock to the ECM. This ratio tells us how much faster (
It is possible to obtain the above ratios without having any communication between the laboratories that house the respective clocks. The necessary synchronization can begin by sending a light signal directly from the position of the clock A lying closest to the standard clock S. The corresponding distance can be determined to as high an accuracy as possible using GPS. Division by c then gives the elapsed time for the one-way travel of the signal based on the standard clock S. The time of arrival on the standard clock is then adjusted backward by this amount to give the time of emission TS0(A) for the signal, again based on the standard clock. The corresponding time of the initial emission read from the local clock is also stored with the value T0(A). In principle, all subsequent timings can be determined by subtracting T0(A) from the current reading on clock A to obtain
where R and S are the specific values of the ratios computed above for clock A.
Once the above procedure has been applied to clock A, it attains equivalent status as a standard. The next step therefore can be applied to the clock which is nearest either to clock A or clock S. In this way the network of standard clocks can be extended indefinitely across the globe. Making use of the “secondary” standard (A) naturally implies that all timings there are based on its adjusted readings. It is important to understand that no physical adjustments need to be made to the secondary clock, rather its direct readings are simply combined with the R and S factors in eq. (24) to obtain the timing results for a hypothetical standard. A discussion of this general point has been given earlier by Van Flandern [47]. The situation is entirely analogous to having a clock in one’s household that runs systematically slower than the standard rate. One can nonetheless obtain accurate timings by multiplying the readings from the faulty clock by an appropriate factor and keeping track of the time that has elapsed since it was last set to the correct time. The key word in this discussion is “systematic.” If the error is always of quantitatively reliable magnitude, the faulty clock can replace the standard without making any repairs.
The same principles used to standardize clock rates on the Earth’s surface can also be applied for adjusting satellite clocks. Assume that the clock is running at the standard rate prior to launch and is perfectly synchronized with the standard clock (i.e. as adjusted at the local position). In order to illustrate the principles involved, the gravitational effects of other objects in the neighborhood of the satellite are neglected in the following discussion, as well as inhomogeneous characteristics of the Earth’s gravitational field.
The main difference relative to the previous example is that the R and S factors needed to make the adjustment from local to standard clock rate using eqs. (23-24) are no longer constant. Their computation requires a precise knowledge of the trajectory of the satellite, specifically the current value of its speed v and altitude r relative to the ECM. The acceleration due to gravity changes in flight and so the ratio S also has to be computed in a more fundamental way. For this purpose, it is helpful to define the following quantity connected with the gravitational potential, which is a generalization of the quantity in parentheses in eq. (18):
where G is the universal gravitational constant (6.670x10-11 Nm2/kg2) and ME is the gravitational mass of the Earth (5.975x1024 kg). The value of S is therefore given as the ratio of the A values for the satellite and the standard clock:
which simplifies to eq. (22) near the Earth’s surface (with
The corresponding value of the R ratio is at least simple in form:
Note that the latitude
In this application the underlying principle is to adjust the satellite clock rate to the corresponding standard value over the entire flight, including the period after orbit has been achieved. The correction is made continuously in small intervals by using eq. (23) and the current values of R and S in each step. The result is tantamount to having the standard clock running at its normal rate on the satellite. This above procedure super-cedes the “pre-correction” technique commonly discussed in the literature [3] according to which the satellite clock is
Although the relativistic principles for adjusting the rates of moving clocks are well understood, there is still an open question about how this all fits in with Einstein’s STR [1]. The standard argument, starting with the high-speed rotor experiments of Hay et al. [25], has been that one only needs to know the speed of the clock relative to some specific inertial system in order to compute the decrease in its rate using eq. (12). While this is true, the procedure itself cannot be said to be consistent with the basic subjectivity of Einstein’s original theory. As discussed in the beginning of Sect. IV, one has to disregard the predictions of the LT in order to have a theory which unambiguously states which of two clocks is running slower, namely the one that is accelerated by the greater amount relative to the aforementioned inertial system [28,31]. The consequences of ignoring the predictions of the LT in this situation are generally avoided in theoretical discussions of clock rates, with authors [16, 30-32] preferring instead to explain how correct predictions can be obtained by assuming that the amount of time dilation is proportional to the
The standard procedure for addressing such problems is to find a way to amend the theory that removes the contradiction at hand, namely in the present case, the prediction of STR that two clocks can both be running slower than the other at the same time [1], while still retaining the capability of making all the other hitherto successful predictions of the theory without further modification. In previous work [48-50] it has been shown that the following space-time transformation accomplishes this objective by making a different choice for the function
In this set of equations,
The alternative Lorentz transformation (ALT) in eqs. (28a-d) satisfies both of Einstein’s postulates [1] because of its direct relation to the general equations in eqs. (1a-d), and it is also consistent with the same velocity transformation (VT) that is an integral part of STR:
It is more than an
This contradiction has been referred to as the “clock riddle” in earlier work [50-51], as opposed to the “clock paradox” frequently discussed in the literature. In fact, the
The ALT is the centerpiece of a thoroughly objective version of relativity theory. It subscribes to the Principle of Rational Measurement (PRM), whereby two observers must always agree in principle on the ratio of physical quantities of the same type [42]. There is never any question about which clock is running slower or which distance is shorter, unlike the case for Einstein’s STR. The new theory [48,49] does this by restating the RP: The laws of physics are the same in all inertial systems,
At the same time, the ALT insists on remote simultaneity by virtue of eq. (28a), since it is no longer possible for
The relativistic and gravitational effects discussed above are observed at sufficiently large distances from GPS satellites to the E-layer of the atmosphere. In accordance with existing experimental data these effects lead to positioning errors which do not exceed 3 m on the Earth’s surface. The next largest sources of error may be due to satellite geometry with respect to the GPS receiver, as well as orbit deformation due to the influence of gravity and the uneven distribution of this field.
We consider below another key aspect of the process of point-location determination by GPS. It is based on the fact that the distance can be determined using information from the atomic clock, and the assumption that the light pulses are always moving with the same speed through space. Then, to determine the appropriate distance it is sufficient to multiply this speed by the time of passage of the light pulse between two points in space. Use of this simple approach leads to problems in GPS positioning that arise from the possibility of light pulse propagation at different speeds through free space. This becomes particularly evident during periods of solar activity and the occurrence of magnetic storms, when the positioning errors are quite large. If one takes the generally accepted view that associates the distortion of GPS signals with wave optics, the positioning errors that occur during these periods correspond to an increase in the optical length of the signal propagation. Allowance for refraction in the scattering of waves on the plasma-type seals like blobs and bubbles with refractive index
With increasing solar activity the time of the GPS signal passage from satellite to the Earth rises, which leads to positioning error enlargement. And it can be realized both in a short period of time (with duration 5-20 min) and for a long period (lasting several hours). In the first case, it occurs under the influence of the radiation coming from the solar flare. In the second case, it takes place in 30-35 hours after the flare under the influence of the solar wind. A concrete example is the time-dependence of the violations of the GPS satellite system during periods of solar activity which was published on the website of Cornell University [54]. According to measurements carried out in real-time monitoring stations of Arecibo Observatory (Puerto Rico) daily from August 30 to September 02, 2011 between 03.00 and 04.00 on the Coordinated Universal Time (UTC), there was a 20-minute failure of GPS. The horizontal positioning error here reached 50 m and more.
More powerful geomagnetic disturbances lead to the complete disappearance of the signal at the GPS receiver for a sufficiently long period of time [55]. Thus, the data obtained at the Sao Luis Observatory (Brazil) on September 15-16, 2011 showed that the loss of GPS signal occurred several times during the day. The signal at the receiver sporadically disappeared five times for 5-30 minutes each between 16.00 UTC September 15 to 01.00 UTC September 16, 2011. Moreover, the horizontal positioning error during these days greatly exceeded the value of 50 m.
It was shown in [56] that during solar flares of different power there was a certain sequence of decreasing carrier/noise ratio for the frequencies L1=1.57542 GHz and L2=1.22760 GHz. During the solar flare of X-1 level (22.15 UTC, December 14, 2006) the carrier/noise ratio for the frequency L1 had become worse. At the same time, the carrier/noise ratio for the L2 frequency remained unchanged. The flare of the X-3 level (02.40 UTC, December 13, 2006) led to a simultaneous deterioration of the carrier/noise ratio for both frequencies. The duration of the phenomena observed in both cases was about 30 minutes.
The next phenomenon that deserves attention is the increasing power of the signal received by GPS receiver during the period of strong solar activity. The time-dependence of the power of the GPS signal, and an integral number of failures at the receiver during a geomagnetic disturbance on July 15, 2000 was published in [57]. There was an increase of about three times in the intensity of the signal at the receiver with respect to satellite signal power. The integral number of failures grew with increasing intensity of the received signal. The authors did not give an explanation for the growth of intensity.
The observations show that a significant increase of high-frequency (UHF) radiation from the upper atmosphere is a result of solar flares. The intensity of UHF radiation in such events in 40 or more times higher than typical levels of solar microwave bursts [58]. In particular, such events were observed during periods of geomagnetic disturbances, such as observations at wavelengths in the 3-50 cm range [59]. The observations were made simultaneously at several points within the project SETI. The intensities were not given in this paper. The corresponding graphical dependences were normalized to the maximum value. Analysis of different possibilities to generate the observed UHF radiation has shown that the largest contribution to the resulting picture of the spectrum is made by transitions between Rydberg levels of neutral components of the non-equilibrium two-temperature plasma. They are excited by the action of solar radiation flux or a stream of electrons emitted from the upper ionosphere in a collision with electrons [55].
Highly excited states of atoms and molecules are called
Harpoon mechanism of the quenching scheme.
The optical transitions between split and degenerate states of quasimolecule
Rydberg states of the particles
where
The increased solar activity leads to the formation of two types of non-equilibrium plasma in the D- and E-layers of the ionosphere. They are
leading to the formation of an intermediate negative ion.
The second type corresponds to a photoionization plasma in which the population of Rydberg states occurs under the action of the light flux coming from the solar flare. In this case, the quantity of the Rydberg states is determined by the intensity of incident radiation. Here, in contrast to the recombination plasma, the low-lying Rydberg states are also populated, which leads to production of the infrared radiation.
Let us consider the effect of molecules
Energy scheme for neck-of-flow location.
Assuming that the electron flow is stationary and their concentration
Passage of the electrons through the neck of the flow on the energy scale is the slowest stage of the process that determines the kinetics of non-equilibrium plasma. The energy
(here concentration of electrons
The Rydberg state perturbations by the neutral particles are reduced to the splitting of degenerate levels of the highly excited
The states with small momenta
where quantum defects induced by the field of the molecule M are equal to
\n\t | \n|||
101\n\t | \n\t77 | \n\t91 | \n\t101 | \n
102\n\t | \n\t58 | \n\t69 | \n\t76 | \n
103\n\t | \n\t43 | \n\t52 | \n\t57 | \n
104\n\t | \n\t33 | \n\t39 | \n\t43 | \n
105\n\t | \n\t25 | \n\t29 | \n\t32 | \n
106\n\t | \n\t19 | \n\t22 | \n\t24 | \n
107\n\t | \n\t14 | \n\t17 | \n\t18 | \n
108\n\t | \n\t11 | \n\t13 | \n\t14 | \n
109\n\t | \n\t8 | \n\t10 | \n\t11 | \n
1010\n\t | \n\t6 | \n\t7 | \n\t8 | \n
1011\n\t | \n\t5 | \n\t6 | \n\t6 | \n
1012\n\t | \n\t4 | \n\t4 | \n\t5 | \n
Dependency of neck-of-the-flow
Potential energy curves of the quasimolecule
Here
Figure 3 shows the energy diagram of the potential energy curves of quantum
Radiation intensities of photon energy emission per unit time for
where
(
The coefficient
The lifetime of degenerate Rydberg states of the quasimolecule characterized by the time of spontaneous emission in the infrared
(i.e.
where the maximum is achieved at a frequency
Here
(x is the exponent that characterizes the medium concentration which in these conditions varies from 12 to 16). Note, that according to (10) the position of the Rydberg state population maximum
\n\t\t\t | \n\t\t\n\t | \n||
1.60 [70] | \n10.6 [73] | \n||
0.75 [71] | \n11.1 [74] | \n
Scattering lengths
*) Because the contribution of the second term in square brackets in (3) is small, we do not give
The intensity of the UHF radiation per unit volume is written as follows:
The
The shift in frequency of these limits for
The optical thickness of the radiating layer
Figure 4 shows the dependence of the frequency of the emission lines for A**N2 and A**O2 quasimolecules on the principal quantum number n for the transitions
\n\t\t\t | \n\n\t | \n|||
1012\n\t | \n\t79 | \n\t74 | \n\t71 | \n\t69 | \n
1013\n\t | \n\t58 | \n\t54 | \n\t52 | \n\t50 | \n
1014\n\t | \n\t42 | \n\t40 | \n\t38 | \n\t37 | \n
1015\n\t | \n\t31 | \n\t29 | \n\t28 | \n\t27 | \n
1016\n\t | \n\t23 | \n\t21 | \n\t20 | \n\t20 | \n
Dependency of the position of maximum population
UHF radiation lines of the A**N2 and A**O2 quasimolecules.
It is seen that the frequency shift for the
The intensities of incoherent UHF radiation for the excited medium calculated by the formula (11) in the 0.8-1.8 GHz range are presented in Fig.5 and Fig.6 as functions of frequency for quiet and disturbed ionosphere states. It is shown that the profile of UHF radiation is a non-monotonic function of the radiation frequency and increases sharply near the right edge of the range.
The spectrum of UHF radiation for a quiet ionosphere. Curve (1) corresponds to electron temperature Te=1000 K and medium concentration
The spectrum of UHF radiation for a disturbed ionosphere. Curve (1) corresponds to electron temperature Te=2000 K, and neutral medium concentration
With increase in electron concentration
The photoionization plasma is formed during 20-30 minutes under the influence of wideband radiation coming into the atmosphere after a solar flare has occurred. This process is caused by multi-quantum excitation of the electronic states of nitrogen and oxygen atoms and molecules. In this case the spin-forbidden character of the corresponding radiative transitions is removed due to interaction of excited particles with ambient molecules
Under these conditions, spontaneous decimeter radiation (which fits to
77 | \n52 | \n36 | \n24 | \n16 | \n11 | \n
Dependence of principal quantum number
This phenomenon should lead to the population emptying of the low-lying molecular Rydberg states as a result of predissociation [68]. In reality, it is necessary that
which depends on the concentration of the medium
The success of the GPS methodology rests on an objective theory of measurement which denies Einstein’s symmetry principle derived on the basis of the LT. There is never any ambiguity in principle as to which of two clocks in relative motion runs slower. The goal of relativity theory is to quantitatively predict relative rates of clocks on the basis of information regarding their respective states of motion and positions in a gravitational field. For this purpose it is necessary to designate a specific rest frame (ORS) to act as reference in determining the speeds of the clocks to be used to compute the amount of time dilation. The Earth’s center of mass (ECM) serves as the ORS for computing the rates of clocks located on orbiting satellites as well as on the Earth’s surface. The effects of gravity on the relative rates can then also be computed from knowledge of their respective positions in space relative to the ECM. To the surprise of many, it was found that the transverse Doppler effect was
In considering this point it has been noted that Einstein made an undeclared assumption,
The difference between the impacts of photoionization and recombination plasma on the distortion of the GPS satellite signals is clearly manifested in the observed dependence of the positioning errors with respect to time. In the first case, there is sharp and narrow (up to 20 min) peak with a positioning error of more than 50 m. The second case corresponds to the formation of a bell-shaped dependence of the error with a typical width of several hours and positioning errors of 15-20 m.
During periods of solar activity, characteristic IR radiation should be formed, which is indicative of Rydberg states having been formed in the D-layer of the Earth’s ionosphere. The integrated intensity close to the IR radiation maximum gives information about the population of Rydberg states at altitudes of 50-60 km. These results can be used as a starting point for the corresponding kinetic calculations. The slope on the left side of the frequency profile contains information about the magnitude of the light flux.
An independent line of the research may be a systematic analysis of the long-wave IR spectrum of radiation (for
In conclusion, it should be noted that two physical factors play key roles during the propagation of GPS satellite signals. The first is the absorption and subsequent stimulated emission of electromagnetic waves on Rydberg states of the A**N2 and A**O2 quasimolecules with a time delay of 10-5-10-6 seconds in a single scattering process. The second is due to incoherent plasma radiation. These processes are applied independently of each other. The increase in two to three times in the envelope of the resonance intensity profile and the formation of a phase shift are the most characteristic features for the resonance absorption of electromagnetic waves with subsequent re-emission. These two processes alone can explain the power growth and the disappearance of GPS signal observed in [57]. This means that the frequencies of the signals emitted by the satellite and subsequently received on the ground may differ substantially from one other.
Thus, the physical cause of the time delay and phase shift of the GPS satellite signal during periods of strong solar activity is associated with a cascade of resonant re-emission of Rydberg states of the A**N2 and A**O2 quasimolecules in the E-and D-layers of the ionosphere, i.e. they are determined by quantum properties of the propagating medium.
Physical exercise is recognized as a highly effective non-pharmaceutical intervention for a range of health conditions in humans. In the first instance, systematic review evidence (comprising millions of participants) has indicated that engagement in regular physical exercise is associated with a reduced risk for all-cause mortality, and in a dose-response manner [1]. Furthermore, it also has important benefits in the prevention and treatment of a range of chronic metabolic conditions [1], such as cardiovascular disease [2], diabetes [3], and cancer [4]. The benefits of regular physical exercise are not restricted solely to metabolic diseases, however. The whole-body homeostatic perturbations brought about by exercise-induced stress also encompass the central nervous system, skeletal muscle, skin, oxygen transport processes, and hepatic function [5]. An important observation is that the relationships between physical activity and health outcomes tend to be curvilinear, in that clinically relevant health benefits can be obtained from relatively little amounts of physical activity [1].
Despite its wide-ranging, multifaceted, and complex health benefits, almost one third of the global population over 15 years of age fails to meet the minimum prescription of physical exercise to obtain worthwhile health benefits [6]. In the United States, 8.3% (95% confidence interval: 6.4–10.2) of deaths have been attributed to inadequate levels of physical activity [7], a sobering statistic when considering the modifiable nature of this risk factor [8]. Yet more worrisome is the growing trend towards increasing sedentary behaviors (i.e., sitting time, computer use) over the previous decade [9, 10]; a fact made all the more severe by the ongoing COVID-19 pandemic and its associated government-mandated lockdown measures to protect public health [11]. Despite the seemingly global trend towards increased sedentariness and inadequate physical activity, impracticalities exist with regards to mandating an entire community, country, and/or global population to optimize their exercise habits [12]. It must also be noted that certain populations may not be able to engage in physical exercise due to injury, disease, or age-associated frailty, and thus would benefit from alternative solutions [13].
The potent effects of regular physical exercise on numerous important domains of human health have given rise to the notion of pharmacological compounds that mimic, or enhance, these effects. Such ‘exercise mimetics’ or ‘exercise pills’ have been touted as a potential, but not entirely probable, therapeutic solution [12, 14] for an otherwise challenging and ongoing public health problem. Although exercise brings about a range of physiological benefits to human health, compliance is often low and in certain groups may not be possible [15]. In recent decades, our understanding of the molecular determinants and physiological processes involved in exercise has improved at an alarming rate. This work has led to the emergence of chemical interventions that can induce the beneficial aspects of exercise, without necessitating actual skeletal muscle activity [15]. Such pharmacologic interventions may represent a viable strategy for addressing metabolic diseases associated with physical inactivity [16] or serve as an intermediary treatment for the morbidly obese or people recovering from serious injury [17]. The mechanistic basis for this supposition, and the opportunities and difficulties associated with such a strategy are the focal considerations of this chapter.
Skeletal muscle is the most abundant tissue in the human body, accounting for around 40% of total body weight, and is the most robustly activated organ in response to physical exercise [13]. In recent years, the effects of physical exercise on several molecular pathways and cellular targets in skeletal muscle have received significant attention. This investigative work has yielded numerous potential factors with relevance for ‘exercise mimetic’ applications in human health.
The repeated muscular contractions brought about during physical exercise activate numerous signaling pathways in skeletal muscle, one of which is the AMPK-SIRT1-PGC1α axis that plays a key role in skeletal muscle energy metabolism and mitochondrial biogenesis [13].
AMPK, or AMP-activated protein kinase, is a master regulator of energy homeostasis and metabolism within the cell. It is a heterotrimeric protein complex that comprises a catalytic subunit (α) and two regulatory subunits (β and γ) of which numerous isoforms exist [18]. AMPK integrates important signals from metabolic pathways and balances nutrient availability with energy demand. During exercise, muscle contractions deplete adenosine triphosphate (ATP), which reduces the ATP:AMP and ATP:ADP ratios within the cell, subsequently activating AMPK [19]. In skeletal muscle, the activation of AMPK induces a switch from anabolic cellular metabolism to a catabolic state of metabolism, blocking energy-consuming activities and promoting the synthesis of ATP from fatty acid oxidation, glycosylation, and glucose uptake [13]. These effects are mediated acutely by direct phosphorylation of metabolic targets, whereas a more chronic effect is brought about by gene transcription [13]. Inactivation of AMPK in skeletal muscle leads to the loss of oxidative fibers, suppressed fat metabolism, and impaired mitochondrial biogenesis [20].
Exercise is perhaps the most prominent physiological activator of AMPK in skeletal muscle. Acutely, exercise intensities above 60% of maximal aerobic capacity can induce AMPK activation, as can lower intensities of a prolonged duration [21]. Given its ‘global’ role as a regulator of cellular energy stress in response to environmental factors such as caloric restriction, physical exercise, and metabolic disease [22], AMPK has garnered substantial attention. It continues to represent a promising potential target for pharmaceutical intervention, particularly when considering its interactions with other effectors.
Sirtuin 1 (SIRT1) is a central regulator of metabolic processes in response to energy availability, and is primarily localized in the nucleus [23]. It is responsive to NAD+ to NADH concentrations, and thus cellular energy availability, through its activation by AMPK [20], and it also senses changes in intracellular redox state [13, 23]. The activation of SIRT1 deacetylates and activates peroxisome proliferator-activated gamma coactivator 1-alpha (PGC1-α), upregulating its specific activity as a transcription factor on genes related to mitochondrial respiration and fatty acid metabolism [13, 24]. In conditions of overexpression or knock-out however, there is evidence to suggest that SIRT1 can also serve as a PGC1-α inhibitor, thus reducing mitochondrial activity [13]. In addition, during low nutrient availability, SIRT1 induces a shift in cellular metabolism towards fatty acid oxidation due to the scarcity of glucose [23]. SIRT1 helps to support cellular energy balance by inducing catabolic processes while inhibiting anabolic processes, thus maintaining energy homeostasis [23].
Physical exercise, specifically high-intensity interval training, has been shown to elevate SIRT1 activity in human skeletal muscle, and this was also associated with mitochondrial biogenesis [25]. Moreover, chronic exercise results in systemic adaptations that increase the levels of SIRT1 expression in the kidney, liver and brain in patients with neurodegenerative diseases, normalizing cellular processes and decreasing disease severity [26]. Defects in the pathways mediated in part by SIRT1 are known to lead to numerous metabolic disorders. Therefore, given the potential benefits of exercise-associated activation of SIRT1 for health and disease, the pharmacological manipulation of this target might elicit multiple benefits, and as such remains an area of focused attention.
PGC1-α plays an integral role in cellular metabolism, serving as a co-activator of a vast range of downstream transcriptional factors and effectors involved in fatty acid oxidation and mitochondrial biogenesis [13]. In skeletal muscle, PGC1-α is activated by endurance exercise-mediated stimulation of p38 mitogen-activated protein kinase (MAPK) [13], subsequently enhancing mitochondrial biogenesis. Importantly, both acute and chronic physical exercise robustly increase the mRNA expression of PGC1-α in rodent muscle, therefore underscoring its importance in exercise training adaptations [20]. PGC1-α mediates the remodeling of skeletal muscle towards a more metabolically oxidative and less glycolytic fiber-type composition [27]. In muscle-specific PGC1-α knock-out models, impaired endurance, abnormal fiber composition, and inconsistent mitochondrial gene regulation have been documented [13], thus reinforcing the indispensable role of PGC1-α in exercise-mediated adaptations. It has also been posited that PGC1-α is a key factor in metabolic disorders, such as diabetes, obesity, and cardiomyopathy. These notions, allied to its regulatory action in lipid metabolism, make PGC1-α a potentially attractive target for pharmacological intervention [27].
Peroxisome proliferator-activated receptor delta (PPARδ) is a nuclear hormone receptor that transcriptionally regulates over 100 genes, playing a vital role in many biological processes [13], particularly those relating to energy balance [28] and fatty acid oxidation [29]. Although expressed abundantly in a range of metabolically active tissues, in skeletal muscle PPARδ is predominantly expressed in oxidative slow-twitch as opposed to glycolytic fast-twitch fibers. This expression is further induced by endurance-type exercise activity known to trigger an oxidative and/or slow-twitch phenotype [20]. Its role in skeletal muscle includes the regulation of slow/fast-twitch fibers, lipid metabolism, oxidative processes, mitochondrial biogenesis, weight reduction, impairment of liver gluconeogenesis, and management of inflammatory processes [13, 20]. In rodent models, muscle-specific activation of PPARδ has demonstrated ‘exercise-like’ effects, such as increasing running endurance and guarding against diet-induced obesity and type II diabetes [30]. Furthermore, ablation of PPARδ in skeletal muscle induces an age-dependent loss of oxidative muscle fibers, running endurance, and insulin sensitivity [31], thus further reinforcing the role of PPARδ in fiber type remodeling. The weight of this evidence has led to the assumption that PPARδ is a central transcriptional regulator of oxidative metabolism the slow-twitch phenotype [20] thus representing a major ‘exercise mimetic’ target of interest.
Estrogen-related receptors (ERRs) are key nuclear regulators in mitochondrial energy metabolism [29], with their transcriptional activity determined by co-factors such as PGC-1α. ERRα is expressed in a range of tissues with high energy turnover, including skeletal muscle. ERRγ has a similar expression pattern but is selectively expressed in tissues with high rates of oxidation such as brain, heart, and muscle [29]. When PGC-1α is induced, ERRα plays a major role in controlling the mitochondrial biogenic gene network; in its absence, the ability of PGC-1α to enhance the expression of mitochondrial genes is drastically reduced [29].
In skeletal muscle, ERRα is expressed in oxidative and glycolytic fibers, whereas ERRγ is expressed in oxidative fibers only [29, 32]. Notably, ERRγ regulates oxidative metabolism not just in skeletal muscle, but in other tissues as well [33], and is a key determinant of the oxidative muscle fiber phenotype [15]. As such, it is highly expressed in type I skeletal muscle fibers. In rodent models, when ERRγ is transgenically expressed in type II fibers, it induces metabolic and vascular adaptations, in the absence of exercise [32]. These adaptations include prominent vascularization, the secretion of proangiogenic factors, and an alarming increase in endurance performance of 100% [32]. Given these characteristics, ERRγ is a prominent target for exercise mimetics because of its direct regulation of genes associated with mitochondrial oxidation, however there is a paucity of research on the topic [12]. When applied ectopically in glycolytic fibers, ERRγ instigates a shift in fiber type from glycolytic to oxidative, inducing mitochondrial biogenesis and bring about increased vascularization [29].
The nuclear receptor REV-ERBα (also known as nuclear receptor subfamily 1 group D member 1 (NR1D1), is highly conserved across species and plays important roles in circadian rhythm and metabolism [33]. In skeletal muscle, REV-ERBα are prominently involved in the regulation of mitochondrial biogenesis, mitophagy, the promotion of an oxidative fiber type, and the processes underpinning a higher endurance capacity [34]. In rodents, muscle-specific ablation of REV-ERBα was shown to blunt the AMPK-SIRT1-PGC-1α signaling pathway, decrease mitochondrial density, reduce oxidative phosphorylation activity, and downregulate genes associated with fatty acid metabolism [34]. Conversely, overexpression of REV-ERBα in C2C12 cells activated these regulators of training adaptations, increased mitochondrial biogenesis and induced fatty acid metabolism genes [35]. REV-ERBα also appears to play a role in modulating muscle mass, with its deficiency leading to increased expression of atrophy genes, and overexpression leading to diminished atrophy genes and increased fiber size [36]. Therefore, REV-ERBα has been identified as a promising pharmacological target for exercise mimetic applications.
The attractive properties of physical exercise for human health have garnered fervent interest from the pharmaceutical industry in recent years, likely due to the large and untapped market of sedentary individuals that, for varying reasons, do not engage in sufficient physical exercise [37]. Chiefly, the development of novel therapeutic approaches to replicate an exercise-training phenotype [38] by activating selected molecular targets—so-called ‘exercise pills’ [15] or ‘exercise mimetics’—remains an area of substantial investment and effort. In using natural or synthetic compounds, it is possible to induce exercise-mimicking effects even in sedentary test animals [12], by activating molecular targets and genomic regulators such as those previously described. The foremost of these therapeutic approaches will now be discussed.
AICAR, or 5-aminoimidazole-4-carboxamide-1-β-D-ribofuranoside, is at the forefront of several ‘exercise-mimetic’ compounds developed to target AMPK, a master regulator of cellular and organismal metabolism [39]. It is a well-known adenosine analog that is intracellularly converted into ZMP, which directly associates with and allosterically stimulates AMPK [12, 22] in a time- and dose-dependent manner [40]. Acutely, AICAR activates AMPK to bring about an increase in fatty acid oxidation, whereas chronic AICAR treatment promotes skeletal muscle fiber type transition from fast- to slow-twitch, and increases the expression of enzymes associated with aerobic respiration [20]. This fiber type reorganization, in concert with mitochondrial biogenesis, has been shown to significantly increase exercise performance (by an unexpected 44%) in sedentary mice following AICAR administration alone [39]. AICAR also induces skeletal muscle glucose uptake by effecting the translocation of the GLUT4 receptor to the sarcolemma [22]. These findings highlight the potential of AICAR as a potential agent to address the insulin resistance seen in type II diabetes.
Metformin is a drug of the biguanide class known to function in an AMPK-dependent manner, and is one of the most broadly available antidiabetic agents presently available [22]. It represents a first line medication used to treat type II diabetes, and activates AMPK in the liver through inhibition of mitochondrial complex I, which concomitantly reduces cellular ATP generation [12]. The glucose-lowering action of metformin is at least partly mediated by the activation of AMPK [38]. Although the mode of activation is different, metformin activates AMPK in a similar manner to AICAR, and they both have similar roles in hepatic glucose production [13]. In diabetic patients, metformin can reduce blood pressure and also improve multiple cardiovascular risk factors in obese individuals [13]. It may also possess anti-inflammatory properties, the specifics of which are still being explored.
Resveratrol, a naturally occurring plant-derived polyphenol, is recognized as an activator of SIRT1 and AMPK [13, 22], but has multiple biological targets [20]. In yeast it has been shown to promote longevity, whereas in rodents this capacity is uncertain [33]. Although abundant in the human diet, resveratrol is perhaps most notably consumed in the seeds and skin of grapes [13]. It is highly lipophilic but has scarce bioavailability; nevertheless it is capable of extracellular, intracellular, and nuclear interactions [13]. Its role on the SIRT1-AMPK axis, as well as PGC1-α [38, 41], has received interest as a potential metabolism-regulating, ‘exercise mimetic’ compound. However, evidence in rodents is conflicting and it has been postulated that resveratrol might actually improve performance when used in synergy with exercise, rather than as a substitute [13]. In human clinical trials, resveratrol was shown to induce the expression of SIRT1 and AMPK in skeletal muscle, albeit in obese type II diabetic males [42]. From the perspective of exercise performance, resveratrol administration suppressed exercise-dependent improvements in aerobic respiration in aged inactive males, thus blunting the beneficial effects of training [43]. Therefore, further research is needed to cogently understand the mechanisms of action and optimal dose before it can be recommended in ‘exercise mimetic’ applications. It should also be noted that novel, more potent synthetic activators of SIRT1, such as SRT1720, have been developed that might represent promising candidates for application in a clinical setting [33], although research on these compounds is still in its infancy.
The compound GW501516 is a selective agonist of PPARδ, and was initially developed for possible beneficial applications in metabolic and cardiovascular diseases [13]. However, pre-clinical work in animals highlighted its carcinogenic effects in multiple organs and the compound was subsequently abandoned [44]. Nevertheless, numerous studies from the past decade have linked this drug with potential ‘exercise mimetic’ effects [39]. For instance, a metabolomic study in mice showed that GW501516 treatment enhanced exhaustive running endurance in both trained and untrained animals, by increasing the specific consumption of fatty acids and sparing blood glucose [45]. The expression of genes regulated by PPARδ, including PGC1-α and pyruvate dehydrogenase kinase 4 (PDK4) were also significantly increased following treatment, as were other markers of fatty acid metabolism in skeletal muscle. Importantly, in untrained mice the administration of GW501516 alone was sufficient to increase running endurance, even following just 1 week of provision. Similar findings have been previously reported, albeit without any benefits to endurance capacity, demonstrating that GW501516 establishes an endurance gene signature, sharing 50% of the gene expression pattern with exercise [39]. Elsewhere, GW501516 administration improved endurance function in a mouse model of myocardial infarction when compared to placebo, and preserved oxidative capacity and fatty acid metabolism [46]. Collectively, these findings suggest that the activation of PPARδ at least partially mimics the effects of exercise.
GSK4716 is a synthetic ERRγ agonist that can activate the receptor with a similar potency to that of its ligand PGC-1α [15, 47]. It robustly activates genes involved in mitochondrial biogenesis, fatty acid oxidation, and the tricarboxylic acid cycle (TCA) when used to treat primary muscle cells [12], and promotes an endurance-trained phenotype in mice [32]. However, there is a discrepancy between acute and chronic activation of ERRγ in ligand-treated primary muscle cells and transgenic animals, respectively [33]. Although GSK4716 has been heralded as a candidate ‘exercise pill’ [15], the aforementioned ‘exercise-mimicking’ effects have not been established
The synthetic REV-ERBα agonist SR9009 was developed at the Scripps Research Institute in 2012 and has been identified as an ‘exercise pill’ of promise [15]. A single injection of SR9009 brought about ‘exercise-like’ effects in rodents, such as enhanced mitochondrial activity and the induction of genes associated with fatty acid metabolism [34]. After 12 days, energy consumption was enhanced without changing the respiratory exchange ratio, and after 30 days mouse running performance was significantly prolonged. Despite these positive findings, REV-ERB independent effects on cell proliferation, metabolism and gene expression have been found in a double-ablation model [48]. Therefore, positive outcomes with respect to the physiological and molecular effects of exercise should be interpreted with a degree of caution. More importantly, SR9009 has not been approved for human use at the time of writing, however tests have been devised against its surreptitious use [49].
A pharmacological method of replicating the multifaceted and complex effects of physical exercise would no doubt be of value to populations that for whatever reason cannot engage in physical activity, such as people with disabilities, disease, frailty, or injury. For example, it might serve as an avenue towards reengaging with physical exercise after a severe injury, or a ‘stepping stone’ for individuals that are morbidly obese. However, there are several important considerations that need to be addressed.
There are inherent dangers in a ‘reductionist’ approach to exercise mimetics, as rodent knockout models have shown that no single ‘exercise gene’ or signaling pathway exists [37]. Even though PGC-1α has, for example, been described as the ‘master regulator’ of endurance exercise adaptations, evidence suggests that it may not be a prerequisite for exercise training-induced mitochondrial adaptations [37]. The biological responses to acute and chronic physical exercise in humans are characterized by a high degree of physiological redundancy at the molecular, cellular, organ-system, and whole-body levels [50]. Furthermore, the exercise-induced skeletal muscle phenotype is independent of a chosen few genes, proteins, and signaling pathways [51, 52]. Therefore, irrespective of the promising research findings discussed above, it is extremely unlikely that the emergence of a single pharmaceutical compound will be able to deliver the myriad and complex physiological, metabolic, and homeostatic disruptions brought about by exercise [5]. The multiplicity of responses, at a macro, ‘system-wide’ level [37], have been described as too diverse for a single pharmaceutical approach to address, and therefore a ‘one size fits all’ panacea is unlikely to come forward. It appears then that there is no true replacement for actual exercise, at least at present, due to the distinct and multifaceted metabolic responses that take place, especially in skeletal muscle. Despite these reservations, ‘exercise mimetics’ might represent an avenue to obtain at least some of the important benefits in those unable to achieve adequate amounts of physical exercise [12]. However, it could be argued that improving adherence to existing evidence-based exercise guidelines and pharmaceutical strategies (e.g., statins for cardiovascular disease) would be a more fruitful and productive objective for the promotion of human health.
From the perspective of performance sport, ‘exercise mimetics’ raise important and challenging questions. PPARδ agonists were added to the WADA Prohibited List that became effective in 2009, with AICAR also banned in the same year. In 2012, both GW501516 and AICAR were moved to class S4 (hormone and metabolic modulators) [53], and at the time of writing, this is still the case. Both of these compounds have received significant media attention over the last decade. For example, in 2012 members of the Spanish cycling team, including the team doctor, were arrested in connection with an international network supplying AICAR, due to its effectiveness on performance [12]. Despite this, it must be emphasized that AICAR is not approved for therapeutic use anywhere in the world, given its status as an experimental compound. In a separate instance, Russian race walker Elena Lashmanova tested positive for GW501516 in 2014 and was subsequently sanctioned. A very stable drug, GW501516 possesses a long half-life and is therefore easily detected in blood and urine samples [12], which poses major consequences for athletes seeking to obtain this compound for performance enhancement. By way of comparison, resveratrol is a natural, albeit weak, compound that has been shown to improve endurance performance in animals, yet it is not a prohibited substance. This is likely due to its low bioavailability and lack of consistently beneficial effects in humans [12]. Therefore, due care and attention must be observed when selecting compounds in pursuit of performance enhancement to ensure compliance with the WADA Prohibited List and mitigate the risk of compromising one’s career.
The constant activation of metabolic pathways by pharmaceutical means, so-called ‘metabolic overdrive’, could have undesirable health effects [37, 54]. For example, the chronic activation of AMPK (i.e., via AICAR) and concomitant inhibition of the mechanistic target of rapamycin (mTOR; a central regulator of protein synthesis and anabolism) could bring about a state of chronic catabolism, or breakdown [37]. This problem would be exacerbated if multiple exercise mimetics or pills, targeting diverse pathways, were consumed. More specifically, and with relevance to the exercise mimetics discussed above, GW501516 demonstrated serious toxicity and multi-organ carcinogenicity in rodent studies, whereas human clinical trials reported no adverse effects, likely due to the short duration and low dose administered [53]. Even the naturally occurring compound resveratrol has been associated with side effects in humans, albeit to a lesser extent than the synthetic compounds previously discussed. In
There do exist non-pharmacological alternatives to ‘exercise pills’ that can potentially be applied to mimic the characteristics of exercise training. For example, neuromuscular electrical stimulation (NMES) has been used to induce involuntary muscle contractions and support the maintenance of muscle mass in injured athletes [57]. This can potentially serve as a surrogate for physical activity, as it has been shown to stimulate muscle protein synthesis rates in older men, and can ameliorate the muscle atrophy associated with limb immobilization to a certain extent [57]. In contrast to the pharmacological methods described above, NMES can maintain muscle mass without safety concerns or appreciable side effects [58], thus representing a potential strategy for mimicking, at least in part, the metabolic effects of physical exercise. These findings may have the most utility in clinical populations observing periods of bed rest or immobilization, by reintroducing a degree of muscle contraction. This activity can enhance muscle protein synthesis in the fasted and fed states, which might support muscle health during short-term periods of disuse in a clinical setting [59].
Acute passive heating has demonstrated some exercise mimetic properties in humans, namely type II diabetics, when implemented in proximity to an oral glucose tolerance test (OGTT) [60]. One-hour of passive heating in water at 40°C either 30 min before or 30 min after commencing an OGTT increased extracellular heat shock protein 70 in the blood and increased heart rate and total energy expenditure (via increased fat oxidation) [60]. However, passive heating did not affect blood glucose concentrations or insulin sensitivity compared with a control group. In skeletal muscle, there is preliminary evidence that chronic passive heating can promote hypertrophy in animal and human models, alongside augmented voluntary and involuntary strength [61]. With further study, passive heating might be a worthwhile non-pharmacologic and exercise mimetic strategy for people that are unable to complete sufficient exercise.
Exercise mimetics remains an area of considerable effort and inquiry but is not without its challenges and controversies. Although early clinical research has identified numerous promising molecular targets for pharmaceutical intervention, there is a lack of human clinical data to support their implementation. This, allied to the multifaceted nature of the human physiological response to exercise, and the redundancy inherent in such a response, suggests that a ‘one size fits all’ approach will be unlikely to manifest. As such, efforts should be focused on increasing adherence to existing evidence-based exercise guidelines and pharmaceutical interventions for the promotion of human health. Notwithstanding, it is possible that multiple pharmaceutical approaches could emerge in the future that target specific molecular pathways for cumulative benefit. These strategies may offer substantial value for populations unable, or unwilling, to engage in actual physical exercise. Nonetheless, the implications of exercise pills for doping in elite sport, and the potential side effects associated with the administration of these compounds for human health, are areas of cautious consideration for the next decade and beyond.
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The author declares no conflict of interest.
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Saleh and Amal I. Hassan",coverURL:"https://cdn.intechopen.com/books/images_new/11139.jpg",editedByType:"Edited by",publishedDate:"August 17th 2022",editors:[{id:"144691",title:"Prof.",name:"Hosam M.",middleName:null,surname:"Saleh",slug:"hosam-m.-saleh",fullName:"Hosam M. Saleh"}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null,productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}}]},subject:{topic:{id:"909",title:"Parasitology",slug:"parasitology",parent:{id:"151",title:"Pure Microbiology",slug:"pure-microbiology"},numberOfBooks:6,numberOfSeries:0,numberOfAuthorsAndEditors:182,numberOfWosCitations:88,numberOfCrossrefCitations:103,numberOfDimensionsCitations:196,videoUrl:null,fallbackUrl:null,description:null},booksByTopicFilter:{topicId:"909",sort:"-publishedDate",limit:12,offset:0},booksByTopicCollection:[{type:"book",id:"9025",title:"Parasitology and Microbiology Research",subtitle:null,isOpenForSubmission:!1,hash:"d9a211396d44f07d2748e147786a2c8b",slug:"parasitology-and-microbiology-research",bookSignature:"Gilberto Antonio Bastidas Pacheco and Asghar Ali Kamboh",coverURL:"https://cdn.intechopen.com/books/images_new/9025.jpg",editedByType:"Edited by",editors:[{id:"238219",title:"Dr.",name:"Gilberto Antonio",middleName:null,surname:"Bastidas Pacheco",slug:"gilberto-antonio-bastidas-pacheco",fullName:"Gilberto Antonio Bastidas Pacheco"}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null,productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}},{type:"book",id:"8806",title:"Biology of Trypanosoma cruzi",subtitle:null,isOpenForSubmission:!1,hash:"514ab85661e01a47575e845792ef5bdc",slug:"biology-of-em-trypanosoma-cruzi-em-",bookSignature:"Wanderley De Souza",coverURL:"https://cdn.intechopen.com/books/images_new/8806.jpg",editedByType:"Edited by",editors:[{id:"161922",title:"Dr.",name:"Wanderley",middleName:null,surname:"De Souza",slug:"wanderley-de-souza",fullName:"Wanderley De Souza"}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null,productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}},{type:"book",id:"6979",title:"Parasites and Parasitic Diseases",subtitle:null,isOpenForSubmission:!1,hash:"f55304c8bd1d92268e33689c368f9e33",slug:"parasites-and-parasitic-diseases",bookSignature:"Gilberto Bastidas",coverURL:"https://cdn.intechopen.com/books/images_new/6979.jpg",editedByType:"Edited by",editors:[{id:"238219",title:"Dr.",name:"Gilberto Antonio",middleName:null,surname:"Bastidas Pacheco",slug:"gilberto-antonio-bastidas-pacheco",fullName:"Gilberto Antonio Bastidas Pacheco"}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null,productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}},{type:"book",id:"8122",title:"Vectors and Vector-Borne Zoonotic Diseases",subtitle:null,isOpenForSubmission:!1,hash:"5a088c3ab82e499c8d5d2f8ceec6a601",slug:"vectors-and-vector-borne-zoonotic-diseases",bookSignature:"Sara Savić",coverURL:"https://cdn.intechopen.com/books/images_new/8122.jpg",editedByType:"Edited by",editors:[{id:"92185",title:"Dr.",name:"Sara",middleName:null,surname:"Savic",slug:"sara-savic",fullName:"Sara Savic"}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null,productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}},{type:"book",id:"5527",title:"Natural Remedies in the Fight Against Parasites",subtitle:null,isOpenForSubmission:!1,hash:"d705be119e74a50305952521b2b5ece0",slug:"natural-remedies-in-the-fight-against-parasites",bookSignature:"Hanem Khater, M. Govindarajan and Giovanni Benelli",coverURL:"https://cdn.intechopen.com/books/images_new/5527.jpg",editedByType:"Edited by",editors:[{id:"71812",title:"Prof.",name:"Hanem Fathy",middleName:"Fathy",surname:"Khater",slug:"hanem-fathy-khater",fullName:"Hanem Fathy Khater"}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null,productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}},{type:"book",id:"1692",title:"Parasitology",subtitle:null,isOpenForSubmission:!1,hash:"b2110e81c765897e4ffdfbd340495e25",slug:"parasitology",bookSignature:"Mohammad Manjur Shah",coverURL:"https://cdn.intechopen.com/books/images_new/1692.jpg",editedByType:"Edited by",editors:[{id:"94128",title:"Dr.",name:"Mohammad Manjur",middleName:null,surname:"Shah",slug:"mohammad-manjur-shah",fullName:"Mohammad Manjur Shah"}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null,productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}}],booksByTopicTotal:6,seriesByTopicCollection:[],seriesByTopicTotal:0,mostCitedChapters:[{id:"31812",doi:"10.5772/32521",title:"Soft Ticks as Pathogen Vectors: Distribution, Surveillance and Control",slug:"soft-ticks-as-pathogen-vectors-distribution-surveillance-and-control-",totalDownloads:6458,totalCrossrefCites:18,totalDimensionsCites:42,abstract:null,book:{id:"1692",slug:"parasitology",title:"Parasitology",fullTitle:"Parasitology"},signatures:"Raúl Manzano-Román, Verónica Díaz-Martín, José de la Fuente and Ricardo Pérez-Sánchez",authors:[{id:"91813",title:"Dr.",name:"Ricardo",middleName:null,surname:"Pérez-Sánchez",slug:"ricardo-perez-sanchez",fullName:"Ricardo Pérez-Sánchez"},{id:"120373",title:"Dr.",name:"Raúl",middleName:null,surname:"Manzano-Román",slug:"raul-manzano-roman",fullName:"Raúl Manzano-Román"},{id:"120375",title:"Ms.",name:"Verónica",middleName:null,surname:"Díaz-Martín",slug:"veronica-diaz-martin",fullName:"Verónica Díaz-Martín"},{id:"120378",title:"Dr.",name:"José",middleName:null,surname:"De La Fuente",slug:"jose-de-la-fuente",fullName:"José De La Fuente"}]},{id:"69898",doi:"10.5772/intechopen.89634",title:"Gut Microbiome: A New Organ System in Body",slug:"gut-microbiome-a-new-organ-system-in-body",totalDownloads:1157,totalCrossrefCites:8,totalDimensionsCites:15,abstract:"The gut microbiome is comprised of various types of bacteria, fungi, protozoa, and viruses naturally occurring in humans and animals as normal microflora. Gut microorganisms are typically host specific, and their number and type vary according to different host species and environment. Gut microbes contribute directly and/or indirectly to various physiological processes including immune modulation, regulation of various neurotransmitter, and hormones, as well as production of many antioxidants and metabolites. They also play a role as antibiotic, anti-inflammatory, anti-diabetic, and anti-carcinogenic agents. Moreover, the ability of gut microbes to attenuate various systemic diseases like coronary heart disease, irritable bowel syndrome, metabolic diseases like diabetes mellitus, and infectious diseases like diarrhea has recently been reported. Current research findings have enough evidence to suggest that gut microbiome is a new organ system mainly due to the microorganisms’ specific biochemical interaction with their hosts and their systemic integration into the host biology. Investigations into the potential ability of gut microbiome to influence metabolism inside their host via biochemical interaction with antibiotics and other drugs has recently been initiated. This chapter specifically focuses on the importance of gut microorganisms as a new organ system.",book:{id:"9025",slug:"parasitology-and-microbiology-research",title:"Parasitology and Microbiology Research",fullTitle:"Parasitology and Microbiology Research"},signatures:"Haseeb Anwar, Shahzad Irfan, Ghulam Hussain, Muhammad Naeem Faisal, Humaira Muzaffar, Imtiaz Mustafa, Imran Mukhtar, Saima Malik and Muhammad Irfan Ullah",authors:[{id:"240684",title:"Dr.",name:"Haseeb",middleName:null,surname:"Anwar",slug:"haseeb-anwar",fullName:"Haseeb Anwar"},{id:"244522",title:"Dr.",name:"Ghulam",middleName:null,surname:"Hussain",slug:"ghulam-hussain",fullName:"Ghulam Hussain"},{id:"244524",title:"Mr.",name:"Imtiaz",middleName:null,surname:"Mustafa",slug:"imtiaz-mustafa",fullName:"Imtiaz Mustafa"},{id:"310200",title:"Dr.",name:"Shahzad",middleName:null,surname:"Irfan",slug:"shahzad-irfan",fullName:"Shahzad Irfan"},{id:"310201",title:"Dr.",name:"Humaira",middleName:null,surname:"Muzaffar",slug:"humaira-muzaffar",fullName:"Humaira Muzaffar"},{id:"310202",title:"Dr.",name:"Imran",middleName:null,surname:"Mukhtar",slug:"imran-mukhtar",fullName:"Imran Mukhtar"},{id:"310203",title:"Ms.",name:"Saima",middleName:null,surname:"Malik",slug:"saima-malik",fullName:"Saima Malik"},{id:"310204",title:"Dr.",name:"Muhammad",middleName:null,surname:"Irfan Ullah",slug:"muhammad-irfan-ullah",fullName:"Muhammad Irfan Ullah"},{id:"311357",title:"Dr.",name:"Muhammad Naeem",middleName:null,surname:"Faisal",slug:"muhammad-naeem-faisal",fullName:"Muhammad Naeem Faisal"}]},{id:"54514",doi:"10.5772/67668",title:"Plant-Derived Compounds as an Alternative Treatment Against Parasites in Fish Farming: A Review",slug:"plant-derived-compounds-as-an-alternative-treatment-against-parasites-in-fish-farming-a-review",totalDownloads:2795,totalCrossrefCites:11,totalDimensionsCites:12,abstract:"Aquaculture has grown rapidly for food production around the world. However, outbreaks of infectious diseases have also increased in aquaculture, causing serious economic losses. For many years, fish farmers have applied conventional treatments such as anti‐parasitics and chemical treatments to control fish parasites. However, previous studies have revealed an accumulation of these chemical residues in fish tissues, and a negative environmental impact from farms to aquatic organisms. As an alternative to conventional methods, many plant‐derived compounds such as essential oils (e.g. Origanum sp. and Lippia spp.) and plant extracts (e.g. Allium sativum and Mentha spp.) have been used as an efficient treatment to control parasites in freshwater, brackishwater and marine aquaculture systems. Our objective with this review is to highlight the advantages of the use of plant extracts as an alternative treatment against parasites in aquaculture (e.g. protozoans, myxozoans and monogeneans) and to show the possible negative environmental impacts of conventional treatments used in fish farming systems. Finally, we also highlight the potential of discovering new plant‐derived bioactive compounds that have been increased in the last year due to the use of new tools such as the application of nanotechnology and microencapsulation to control diseases in fish farming.",book:{id:"5527",slug:"natural-remedies-in-the-fight-against-parasites",title:"Natural Remedies in the Fight Against Parasites",fullTitle:"Natural Remedies in the Fight Against Parasites"},signatures:"Alison Carlos Wunderlich, Érica de Oliveira Penha Zica, Vanessa\nFarias dos Santos Ayres, Anderson Cavalcante Guimarães and\nRenata Takeara",authors:[{id:"124356",title:"Dr.",name:"Erica O.P.",middleName:null,surname:"Zica",slug:"erica-o.p.-zica",fullName:"Erica O.P. Zica"},{id:"192845",title:"Dr.",name:"Alison",middleName:null,surname:"Wunderlich",slug:"alison-wunderlich",fullName:"Alison Wunderlich"},{id:"193541",title:"Dr.",name:"Renata",middleName:null,surname:"Takeara",slug:"renata-takeara",fullName:"Renata Takeara"},{id:"193600",title:"BSc.",name:"Vanessa F. S.",middleName:null,surname:"Ayres",slug:"vanessa-f.-s.-ayres",fullName:"Vanessa F. S. Ayres"},{id:"193601",title:"Prof.",name:"Anderson C.",middleName:null,surname:"Guimarães",slug:"anderson-c.-guimaraes",fullName:"Anderson C. Guimarães"}]},{id:"54617",doi:"10.5772/67554",title:"Introductory Chapter: Back to the Future - Solutions for Parasitic Problems as Old as the Pyramids",slug:"introductory-chapter-back-to-the-future-solutions-for-parasitic-problems-as-old-as-the-pyramids",totalDownloads:1899,totalCrossrefCites:8,totalDimensionsCites:12,abstract:null,book:{id:"5527",slug:"natural-remedies-in-the-fight-against-parasites",title:"Natural Remedies in the Fight Against Parasites",fullTitle:"Natural Remedies in the Fight Against Parasites"},signatures:"Hanem Fathy Khater",authors:[{id:"71812",title:"Prof.",name:"Hanem Fathy",middleName:"Fathy",surname:"Khater",slug:"hanem-fathy-khater",fullName:"Hanem Fathy Khater"}]},{id:"63554",doi:"10.5772/intechopen.80372",title:"Current Aspects in Trichinellosis",slug:"current-aspects-in-trichinellosis",totalDownloads:1395,totalCrossrefCites:2,totalDimensionsCites:9,abstract:"Currently, it is estimated that more than 11 million humans in the world are infected by helminth parasites of Trichinella species, mainly by Trichinella spiralis (T. spiralis), responsible for causing Trichinellosis disease in both animals and humans. Trichinellosis is a cosmopolitan parasitic zoonotic disease, which has direct relevance to human and animal health, because it presents a constant and important challenge to the host’s immune system, especially through the intestinal tract. Currently, there is an intense investigation of new strategies in pharmacotherapy and immunotherapy against infection by Trichinella spiralis. In this chapter, we will present the most current aspects of biology, epidemiology, immunology, clinicopathology, pharmacotherapy and immunotherapy in Trichinellosis.",book:{id:"6979",slug:"parasites-and-parasitic-diseases",title:"Parasites and Parasitic Diseases",fullTitle:"Parasites and Parasitic Diseases"},signatures:"José Luis Muñoz-Carrillo, Claudia Maldonado-Tapia, Argelia López-\nLuna, José Jesús Muñoz-Escobedo, Juan Armando Flores-De La\nTorre and Alejandra Moreno-García",authors:[{id:"214236",title:"Dr.",name:"Jose Luis",middleName:null,surname:"Muñoz-Carrillo",slug:"jose-luis-munoz-carrillo",fullName:"Jose Luis Muñoz-Carrillo"},{id:"216080",title:"Dr.",name:"Alejandra",middleName:null,surname:"Moreno-García",slug:"alejandra-moreno-garcia",fullName:"Alejandra Moreno-García"},{id:"254888",title:"Dr.",name:"Juan Armando",middleName:null,surname:"Flores-De La Torre",slug:"juan-armando-flores-de-la-torre",fullName:"Juan Armando Flores-De La Torre"},{id:"254889",title:"Dr.",name:"José Jesús",middleName:null,surname:"Muñoz-Escobedo",slug:"jose-jesus-munoz-escobedo",fullName:"José Jesús Muñoz-Escobedo"},{id:"254890",title:"Dr.",name:"Argelia",middleName:null,surname:"López-Luna",slug:"argelia-lopez-luna",fullName:"Argelia López-Luna"},{id:"254891",title:"Dr.",name:"Claudia",middleName:null,surname:"Maldonado-Tapia",slug:"claudia-maldonado-tapia",fullName:"Claudia Maldonado-Tapia"}]}],mostDownloadedChaptersLast30Days:[{id:"65773",title:"Life Cycle of Trypanosoma cruzi in the Invertebrate and the Vertebrate Hosts",slug:"life-cycle-of-em-trypanosoma-cruzi-em-in-the-invertebrate-and-the-vertebrate-hosts",totalDownloads:1506,totalCrossrefCites:4,totalDimensionsCites:7,abstract:"Trypanosoma cruzi (T. cruzi) is a protozoan parasite that causes Chagas disease, a zoonotic disease that can be transmitted to humans by blood-sucking triatomine bugs. T. cruzi is a single-celled eukaryote with a complex life cycle alternating between reduviid bug invertebrate vectors and vertebrate hosts. This article will look at the developmental stages of T. cruzi in the invertebrate vector and the vertebrate hosts, the different surface membrane proteins involved in different life cycle stages of T. cruzi, roles of different amino acids in the life cycle, carbon and energy sources and gene expression in the life cycle of T. cruzi. The author will also look at extracellular vesicles (EV) and its role in the dissemination and survival of T. cruzi in mammalian host.",book:{id:"8806",slug:"biology-of-em-trypanosoma-cruzi-em-",title:"Biology of Trypanosoma cruzi",fullTitle:"Biology of Trypanosoma cruzi"},signatures:"Kenechukwu C. Onyekwelu",authors:[{id:"245368",title:"Dr.",name:"Kenechukwu C.",middleName:null,surname:"Onyekwelu",slug:"kenechukwu-c.-onyekwelu",fullName:"Kenechukwu C. Onyekwelu"}]},{id:"55437",title:"Biological Control of Parasites",slug:"biological-control-of-parasites-2017-07",totalDownloads:4349,totalCrossrefCites:7,totalDimensionsCites:7,abstract:"Parasites (ectoparasites or endoparasites) are a major cause of diseases in man, his livestock and crops, leading to poor yield and great economic loss. To overcome some of the major limitations of chemical control methods such as rising resistance, environmental and health risks, and the adverse effect on non‐target organisms, biological control (biocontrol) is now at the forefront of parasite (pests) control. Biocontrol is now a core component of the integrated pest management. Biocontrol is defined as “the study and uses of parasites, predators and pathogens for the regulation of host (pest) densities”. Considerable successes have been achieved in the implementation of biocontrol strategies in the past. This chapter presents a review of the history of biocontrol, its advantages and disadvantages; the different types of biological control agents (BCAs) including predators, parasites (parasitoids) and pathogens (fungi, bacteria, viruses and virus‐like particles, protozoa and nematodes); the effect of biocontrol on native biodiversity; a few case studies of the successful implementation of biocontrol methods and the challenges encountered with the implementation of biocontrol and future perspectives.",book:{id:"5527",slug:"natural-remedies-in-the-fight-against-parasites",title:"Natural Remedies in the Fight Against Parasites",fullTitle:"Natural Remedies in the Fight Against Parasites"},signatures:"Tebit Emmanuel Kwenti",authors:[{id:"191763",title:"Dr.",name:"Tebit Emmanuel",middleName:null,surname:"Kwenti",slug:"tebit-emmanuel-kwenti",fullName:"Tebit Emmanuel Kwenti"}]},{id:"54084",title:"Can the Cure for Chagas’ Disease be Found in Nature?",slug:"can-the-cure-for-chagas-disease-be-found-in-nature-",totalDownloads:1831,totalCrossrefCites:2,totalDimensionsCites:3,abstract:"Nature is a skilled factory that produces a wide variety of secondary metabolites known as natural products. Those compounds synthesized by living organisms are usually related to their vital processes. Many drugs used nowadays, had its origins in medicinal plants and other organisms such as herbs, fungi and sponges. Hence, those sources constitute a viable alternative to conventional medicine in many developing countries. In other hand, protozoan diseases like Chagas, represent a health threat causing mortality to populations around the world. The classic treatment for Chagas’ disease is chemotherapic and includes benznidazole and nifurtimox, although, the search for new drugs still remains. Triatomines that may spread Chagas can also be controlled making use of the insecticide property of certain plants. After literature survey it was found, classes of natural products, plant extracts, essential oils, and other natural sources that have shown activity against T. cruzi. In this context, many substances were tested in vitro and in vivo assays to verify trypanocidal efficacy. Promising results were published regarding to compounds arising from plants and sponges that showed high toxicity on different forms of the parasite with low toxicity on mammalian cells, although few were clinically tested on Chagas’ disease.",book:{id:"5527",slug:"natural-remedies-in-the-fight-against-parasites",title:"Natural Remedies in the Fight Against Parasites",fullTitle:"Natural Remedies in the Fight Against Parasites"},signatures:"Nelissa Pacheco Vaz",authors:[{id:"192870",title:"Dr.",name:"Nelissa",middleName:null,surname:"P. Vaz",slug:"nelissa-p.-vaz",fullName:"Nelissa P. Vaz"}]},{id:"62896",title:"Malaria Pathophysiology as a Syndrome: Focus on Glucose Homeostasis in Severe Malaria and Phytotherapeutics Management of the Disease",slug:"malaria-pathophysiology-as-a-syndrome-focus-on-glucose-homeostasis-in-severe-malaria-and-phytotherap",totalDownloads:1283,totalCrossrefCites:3,totalDimensionsCites:5,abstract:"Severe malaria presents with varied pathophysiological manifestations to include derangement in glucose homeostasis. The changes in glucose management by the infected human host emanate from both Plasmodium parasitic and host factors and/or influences which are aimed at creating a proliferative advantage to the parasite. This also includes morphological changes that that take place to both infected and uninfected cells as structural alterations occur on the cell membranes to allow for increased nutrients (glucose) transportation into the cells. Without the availability, effective and efficient intervention there is a high cost incurred by the human host. Hyperglycaemia, hypoglycaemia and hyperinsulinemia are critical aspects displayed in severe malaria. Conventional treatment to malaria renders itself hostile to the host with negative glucose metabolism changes experiences in the young, pregnant women and malaria naïve individuals. In malaria, therefore, host effects, parasite imperatives and treatment regimens play a pivotal role in the return to wellness of the patient. Phytotherapeutics are emerging as treatment alternatives that ameliorate glucose homeostasis alternations as well as combat malaria parasitaemia. 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He also obtained an MSc in Molecular and Genetic Medicine, and a Ph.D. in Clinical Immunology and Human Genetics from the University of Sheffield, UK. He also completed a short-term fellowship in Pediatric Clinical Immunology and Bone Marrow Transplantation at Newcastle General Hospital, England. Dr. Rezaei is a Full Professor of Immunology and Vice Dean of International Affairs and Research, at the School of Medicine, Tehran University of Medical Sciences, and the co-founder and head of the Research Center for Immunodeficiencies. He is also the founding president of the Universal Scientific Education and Research Network (USERN). Dr. Rezaei has directed more than 100 research projects and has designed and participated in several international collaborative projects. He is an editor, editorial assistant, or editorial board member of more than forty international journals. He has edited more than 50 international books, presented more than 500 lectures/posters in congresses/meetings, and published more than 1,100 scientific papers in international journals.",institutionString:"Tehran University of Medical Sciences",institution:{name:"Tehran University of Medical Sciences",country:{name:"Iran"}}},{id:"180733",title:"Dr.",name:"Jean",middleName:null,surname:"Engohang-Ndong",slug:"jean-engohang-ndong",fullName:"Jean Engohang-Ndong",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/180733/images/system/180733.png",biography:"Dr. Jean Engohang-Ndong was born and raised in Gabon. After obtaining his Associate Degree of Science at the University of Science and Technology of Masuku, Gabon, he continued his education in France where he obtained his BS, MS, and Ph.D. in Medical Microbiology. He worked as a post-doctoral fellow at the Public Health Research Institute (PHRI), Newark, NJ for four years before accepting a three-year faculty position at Brigham Young University-Hawaii. Dr. Engohang-Ndong is a tenured faculty member with the academic rank of Full Professor at Kent State University, Ohio, where he teaches a wide range of biological science courses and pursues his research in medical and environmental microbiology. Recently, he expanded his research interest to epidemiology and biostatistics of chronic diseases in Gabon.",institutionString:"Kent State University",institution:{name:"Kent State University",country:{name:"United States of America"}}},{id:"188773",title:"Prof.",name:"Emmanuel",middleName:null,surname:"Drouet",slug:"emmanuel-drouet",fullName:"Emmanuel Drouet",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/188773/images/system/188773.png",biography:"Emmanuel Drouet, PharmD, is a Professor of Virology at the Faculty of Pharmacy, the University Grenoble-Alpes, France. As a head scientist at the Institute of Structural Biology in Grenoble, Dr. Drouet’s research investigates persisting viruses in humans (RNA and DNA viruses) and the balance with our host immune system. He focuses on these viruses’ effects on humans (both their impact on pathology and their symbiotic relationships in humans). He has an excellent track record in the herpesvirus field, and his group is engaged in clinical research in the field of Epstein-Barr virus diseases. He is the editor of the online Encyclopedia of Environment and he coordinates the Universal Health Coverage education program for the BioHealth Computing Schools of the European Institute of Science.",institutionString:null,institution:{name:"Grenoble Alpes University",country:{name:"France"}}},{id:"131400",title:"Prof.",name:"Alfonso J.",middleName:null,surname:"Rodriguez-Morales",slug:"alfonso-j.-rodriguez-morales",fullName:"Alfonso J. Rodriguez-Morales",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/131400/images/system/131400.png",biography:"Dr. Rodriguez-Morales is an expert in tropical and emerging diseases, particularly zoonotic and vector-borne diseases (especially arboviral diseases). He is the president of the Travel Medicine Committee of the Pan-American Infectious Diseases Association (API), as well as the president of the Colombian Association of Infectious Diseases (ACIN). He is a member of the Committee on Tropical Medicine, Zoonoses, and Travel Medicine of ACIN. He is a vice-president of the Latin American Society for Travel Medicine (SLAMVI) and a Member of the Council of the International Society for Infectious Diseases (ISID). Since 2014, he has been recognized as a Senior Researcher, at the Ministry of Science of Colombia. He is a professor at the Faculty of Medicine of the Fundacion Universitaria Autonoma de las Americas, in Pereira, Risaralda, Colombia. He is an External Professor, Master in Research on Tropical Medicine and International Health, Universitat de Barcelona, Spain. He is also a professor at the Master in Clinical Epidemiology and Biostatistics, Universidad Científica del Sur, Lima, Peru. In 2021 he has been awarded the “Raul Isturiz Award” Medal of the API. Also, in 2021, he was awarded with the “Jose Felix Patiño” Asclepius Staff Medal of the Colombian Medical College, due to his scientific contributions to COVID-19 during the pandemic. He is currently the Editor in Chief of the journal Travel Medicine and Infectious Diseases. His Scopus H index is 47 (Google Scholar H index, 68).",institutionString:"Institución Universitaria Visión de las Américas, Colombia",institution:null},{id:"332819",title:"Dr.",name:"Chukwudi Michael",middleName:"Michael",surname:"Egbuche",slug:"chukwudi-michael-egbuche",fullName:"Chukwudi Michael Egbuche",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/332819/images/14624_n.jpg",biography:"I an Dr. Chukwudi Michael Egbuche. I am a Senior Lecturer in the Department of Parasitology and Entomology, Nnamdi Azikiwe University, Awka.",institutionString:null,institution:{name:"Nnamdi Azikiwe University",country:{name:"Nigeria"}}},{id:"284232",title:"Mr.",name:"Nikunj",middleName:"U",surname:"Tandel",slug:"nikunj-tandel",fullName:"Nikunj Tandel",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/284232/images/8275_n.jpg",biography:'Mr. Nikunj Tandel has completed his Master\'s degree in Biotechnology from VIT University, India in the year of 2012. He is having 8 years of research experience especially in the field of malaria epidemiology, immunology, and nanoparticle-based drug delivery system against the infectious diseases, autoimmune disorders and cancer. He has worked for the NIH funded-International Center of Excellence in Malaria Research project "Center for the study of complex malaria in India (CSCMi)" in collaboration with New York University. The preliminary objectives of the study are to understand and develop the evidence-based tools and interventions for the control and prevention of malaria in different sites of the INDIA. Alongside, with the help of next-generation genomics study, the team has studied the antimalarial drug resistance in India. Further, he has extended his research in the development of Humanized mice for the study of liver-stage malaria and identification of molecular marker(s) for the Artemisinin resistance. At present, his research focuses on understanding the role of B cells in the activation of CD8+ T cells in malaria. Received the CSIR-SRF (Senior Research Fellow) award-2018, FIMSA (Federation of Immunological Societies of Asia-Oceania) Travel Bursary award to attend the IUIS-IIS-FIMSA Immunology course-2019',institutionString:"Nirma University",institution:{name:"Nirma University",country:{name:"India"}}},{id:"334383",title:"Ph.D.",name:"Simone",middleName:"Ulrich",surname:"Ulrich Picoli",slug:"simone-ulrich-picoli",fullName:"Simone Ulrich Picoli",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/334383/images/15919_n.jpg",biography:"Graduated in Pharmacy from Universidade Luterana do Brasil (1999), Master in Agricultural and Environmental Microbiology from Federal University of Rio Grande do Sul (2002), Specialization in Clinical Microbiology from Universidade de São Paulo, USP (2007) and PhD in Sciences in Gastroenterology and Hepatology (2012). She is currently an Adjunct Professor at Feevale University in Medicine and Biomedicine courses and a permanent professor of the Academic Master\\'s Degree in Virology. She has experience in the field of Microbiology, with an emphasis on Bacteriology, working mainly on the following topics: bacteriophages, bacterial resistance, clinical microbiology and food microbiology.",institutionString:null,institution:{name:"Universidade Feevale",country:{name:"Brazil"}}},{id:"229220",title:"Dr.",name:"Amjad",middleName:"Islam",surname:"Aqib",slug:"amjad-aqib",fullName:"Amjad Aqib",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/229220/images/system/229220.png",biography:"Dr. Amjad Islam Aqib obtained a DVM and MSc (Hons) from University of Agriculture Faisalabad (UAF), Pakistan, and a PhD from the University of Veterinary and Animal Sciences Lahore, Pakistan. Dr. Aqib joined the Department of Clinical Medicine and Surgery at UAF for one year as an assistant professor where he developed a research laboratory designated for pathogenic bacteria. Since 2018, he has been Assistant Professor/Officer in-charge, Department of Medicine, Manager Research Operations and Development-ORIC, and President One Health Club at Cholistan University of Veterinary and Animal Sciences, Bahawalpur, Pakistan. He has nearly 100 publications to his credit. His research interests include epidemiological patterns and molecular analysis of antimicrobial resistance and modulation and vaccine development against animal pathogens of public health concern.",institutionString:"Cholistan University of Veterinary and Animal Sciences",institution:{name:"University of Agriculture Faisalabad",country:{name:"Pakistan"}}},{id:"333753",title:"Dr.",name:"Rais",middleName:null,surname:"Ahmed",slug:"rais-ahmed",fullName:"Rais Ahmed",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/333753/images/20168_n.jpg",biography:null,institutionString:null,institution:{name:"University of Agriculture Faisalabad",country:{name:"Pakistan"}}},{id:"62900",title:"Prof.",name:"Fethi",middleName:null,surname:"Derbel",slug:"fethi-derbel",fullName:"Fethi Derbel",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/62900/images/system/62900.jpeg",biography:"Professor Fethi Derbel was born in 1960 in Tunisia. He received his medical degree from the Sousse Faculty of Medicine at Sousse, University of Sousse, Tunisia. He completed his surgical residency in General Surgery at the University Hospital Farhat Hached of Sousse and was a member of the Unit of Liver Transplantation in the University of Rennes, France. He then worked in the Department of Surgery at the Sahloul University Hospital in Sousse. Professor Derbel is presently working at the Clinique les Oliviers, Sousse, Tunisia. His hospital activities are mostly concerned with laparoscopic, colorectal, pancreatic, hepatobiliary, and gastric surgery. He is also very interested in hernia surgery and performs ventral hernia repairs and inguinal hernia repairs. He has been a member of the GREPA and Tunisian Hernia Society (THS). During his residency, he managed patients suffering from diabetic foot, and he was very interested in this pathology. For this reason, he decided to coordinate a book project dealing with the diabetic foot. Professor Derbel has published many articles in journals and collaborates intensively with IntechOpen Access Publisher as an editor.",institutionString:"Clinique les Oliviers",institution:null},{id:"300144",title:"Dr.",name:"Meriem",middleName:null,surname:"Braiki",slug:"meriem-braiki",fullName:"Meriem Braiki",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/300144/images/system/300144.jpg",biography:"Dr. Meriem Braiki is a specialist in pediatric surgeon from Tunisia. She was born in 1985. She received her medical degree from the University of Medicine at Sousse, Tunisia. She achieved her surgical residency training periods in Pediatric Surgery departments at University Hospitals in Monastir, Tunis and France.\r\nShe is currently working at the Pediatric surgery department, Sidi Bouzid Hospital, Tunisia. Her hospital activities are mostly concerned with laparoscopic, parietal, urological and digestive surgery. She has published several articles in diffrent journals.",institutionString:"Sidi Bouzid Regional Hospital",institution:null},{id:"229481",title:"Dr.",name:"Erika M.",middleName:"Martins",surname:"de Carvalho",slug:"erika-m.-de-carvalho",fullName:"Erika M. de Carvalho",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/229481/images/6397_n.jpg",biography:null,institutionString:null,institution:{name:"Oswaldo Cruz Foundation",country:{name:"Brazil"}}},{id:"186537",title:"Prof.",name:"Tonay",middleName:null,surname:"Inceboz",slug:"tonay-inceboz",fullName:"Tonay Inceboz",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/186537/images/system/186537.jfif",biography:"I was graduated from Ege University of Medical Faculty (Turkey) in 1988 and completed his Med. PhD degree in Medical Parasitology at the same university. I became an Associate Professor in 2008 and Professor in 2014. I am currently working as a Professor at the Department of Medical Parasitology at Dokuz Eylul University, Izmir, Turkey.\n\nI have given many lectures, presentations in different academic meetings. I have more than 60 articles in peer-reviewed journals, 18 book chapters, 1 book editorship.\n\nMy research interests are Echinococcus granulosus, Echinococcus multilocularis (diagnosis, life cycle, in vitro and in vivo cultivation), and Trichomonas vaginalis (diagnosis, PCR, and in vitro cultivation).",institutionString:"Dokuz Eylül University",institution:{name:"Dokuz Eylül University",country:{name:"Turkey"}}},{id:"71812",title:"Prof.",name:"Hanem Fathy",middleName:"Fathy",surname:"Khater",slug:"hanem-fathy-khater",fullName:"Hanem Fathy Khater",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/71812/images/1167_n.jpg",biography:"Prof. Khater is a Professor of Parasitology at Benha University, Egypt. She studied for her doctoral degree, at the Department of Entomology, College of Agriculture, Food and Natural Resources, University of Missouri, Columbia, USA. She has completed her Ph.D. degrees in Parasitology in Egypt, from where she got the award for “the best scientific Ph.D. dissertation”. She worked at the School of Biological Sciences, Bristol, England, the UK in controlling insects of medical and veterinary importance as a grant from Newton Mosharafa, the British Council. Her research is focused on searching of pesticides against mosquitoes, house flies, lice, green bottle fly, camel nasal botfly, soft and hard ticks, mites, and the diamondback moth as well as control of several parasites using safe and natural materials to avoid drug resistances and environmental contamination.",institutionString:null,institution:{name:"Banha University",country:{name:"Egypt"}}},{id:"99780",title:"Prof.",name:"Omolade",middleName:"Olayinka",surname:"Okwa",slug:"omolade-okwa",fullName:"Omolade Okwa",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/99780/images/system/99780.jpg",biography:"Omolade Olayinka Okwa is presently a Professor of Parasitology at Lagos State University, Nigeria. She has a PhD in Parasitology (1997), an MSc in Cellular Parasitology (1992), and a BSc (Hons) Zoology (1990) all from the University of Ibadan, Nigeria. She teaches parasitology at the undergraduate and postgraduate levels. She was a recipient of a Commonwealth fellowship supported by British Council tenable at the Centre for Entomology and Parasitology (CAEP), Keele University, United Kingdom between 2004 and 2005. She was awarded an Honorary Visiting Research Fellow at the same university from 2005 to 2007. \nShe has been an external examiner to the Department of Veterinary Microbiology and Parasitology, University of Ibadan, MSc programme between 2010 and 2012. She is a member of the Nigerian Society of Experimental Biology (NISEB), Parasitology and Public Health Society of Nigeria (PPSN), Science Association of Nigeria (SAN), Zoological Society of Nigeria (ZSN), and is Vice Chairperson of the Organisation of Women in Science (OWSG), LASU chapter. She served as Head of Department of Zoology and Environmental Biology, Lagos State University from 2007 to 2010 and 2014 to 2016. She is a reviewer for several local and international journals such as Unilag Journal of Science, Libyan Journal of Medicine, Journal of Medicine and Medical Sciences, and Annual Research and Review in Science. \nShe has authored 45 scientific research publications in local and international journals, 8 scientific reviews, 4 books, and 3 book chapters, which includes the books “Malaria Parasites” and “Malaria” which are IntechOpen access publications.",institutionString:"Lagos State University",institution:{name:"Lagos State University",country:{name:"Nigeria"}}},{id:"273100",title:"Dr.",name:"Vijay",middleName:null,surname:"Gayam",slug:"vijay-gayam",fullName:"Vijay Gayam",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/273100/images/system/273100.jpeg",biography:"Dr. Vijay Bhaskar Reddy Gayam is currently practicing as an internist at Interfaith Medical Center in Brooklyn, New York, USA. He is also a Clinical Assistant Professor at the SUNY Downstate University Hospital and Adjunct Professor of Medicine at the American University of Antigua. He is a holder of an M.B.B.S. degree bestowed to him by Osmania Medical College and received his M.D. at Interfaith Medical Center. His career goals thus far have heavily focused on direct patient care, medical education, and clinical research. He currently serves in two leadership capacities; Assistant Program Director of Medicine at Interfaith Medical Center and as a Councilor for the American\r\nFederation for Medical Research. As a true academician and researcher, he has more than 50 papers indexed in international peer-reviewed journals. He has also presented numerous papers in multiple national and international scientific conferences. His areas of research interest include general internal medicine, gastroenterology and hepatology. He serves as an editor, editorial board member and reviewer for multiple international journals. His research on Hepatitis C has been very successful and has led to multiple research awards, including the 'Equity in Prevention and Treatment Award” from the New York Department of Health Viral Hepatitis Symposium (2018) and the 'Presidential Poster Award” awarded to him by the American College of Gastroenterology (2018). He was also awarded 'Outstanding Clinician in General Medicine” by Venus International Foundation for his extensive research expertise and services, perform over and above the standard expected in the advancement of healthcare, patient safety and quality of care.",institutionString:"Interfaith Medical Center",institution:{name:"Interfaith Medical Center",country:{name:"United States of America"}}},{id:"93517",title:"Dr.",name:"Clement",middleName:"Adebajo",surname:"Meseko",slug:"clement-meseko",fullName:"Clement Meseko",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/93517/images/system/93517.jpg",biography:"Dr. Clement Meseko obtained DVM and PhD degree in Veterinary Medicine and Virology respectively. He has worked for over 20 years in both private and public sectors including the academia, contributing to knowledge and control of infectious disease. Through the application of epidemiological skill, classical and molecular virological skills, he investigates viruses of economic and public health importance for the mitigation of the negative impact on people, animal and the environment in the context of Onehealth. \r\nDr. Meseko’s field experience on animal and zoonotic diseases and pathogen dynamics at the human-animal interface over the years shaped his carrier in research and scientific inquiries. He has been part of the investigation of Highly Pathogenic Avian Influenza incursions in sub Saharan Africa and monitors swine Influenza (Pandemic influenza Virus) agro-ecology and potential for interspecies transmission. He has authored and reviewed a number of journal articles and book chapters.",institutionString:"National Veterinary Research Institute",institution:{name:"National Veterinary Research Institute",country:{name:"Nigeria"}}},{id:"158026",title:"Prof.",name:"Shailendra K.",middleName:null,surname:"Saxena",slug:"shailendra-k.-saxena",fullName:"Shailendra K. Saxena",position:null,profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bRET3QAO/Profile_Picture_2022-05-10T10:10:26.jpeg",biography:"Professor Dr. Shailendra K. Saxena is a vice dean and professor at King George's Medical University, Lucknow, India. His research interests involve understanding the molecular mechanisms of host defense during human viral infections and developing new predictive, preventive, and therapeutic strategies for them using Japanese encephalitis virus (JEV), HIV, and emerging viruses as a model via stem cell and cell culture technologies. His research work has been published in various high-impact factor journals (Science, PNAS, Nature Medicine) with a high number of citations. He has received many awards and honors in India and abroad including various Young Scientist Awards, BBSRC India Partnering Award, and Dr. JC Bose National Award of Department of Biotechnology, Min. of Science and Technology, Govt. of India. Dr. Saxena is a fellow of various international societies/academies including the Royal College of Pathologists, United Kingdom; Royal Society of Medicine, London; Royal Society of Biology, United Kingdom; Royal Society of Chemistry, London; and Academy of Translational Medicine Professionals, Austria. He was named a Global Leader in Science by The Scientist. 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