Open access peer-reviewed chapter

Pharmacological Actions of Citrus Species

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Flavia Cristina Fernandes Pimenta, Nathália de Alencar Cunha Tavares, Gabriel Chaves Neto, Mateus Alves, Martina Fernandes Pimenta, Juliete Melo Diniz, Arnaldo Correia de Medeiros and Margareth de Fátima Formiga Melo Diniz

Submitted: 21 June 2016 Reviewed: 21 October 2016 Published: 12 April 2017

DOI: 10.5772/66464

From the Edited Volume

Citrus Pathology

Edited by Harsimran Gill and Harsh Garg

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Abstract

The genus Citrus belongs to family Rutaceae, which is characterized by trees and bushes. Citrus species are extensively cultivated throughout the world because of their multiple health benefits for humans and their applications in pharmaceutical and food industries. This chapter is a survey covering in vitro and in vivo studies that demonstrate the pharmacological activities of various Citrus species. The species Citrus aurantium, Citrus sinensis, Citrus limon, and Citrus bergamia are well known and several studies have been carried out to evaluate the pharmacological effects of their extracts, essential oils, and isolated constituents. These studies have found that they possess anxiolytic, anti‐inflammatory, hypoglycemic, anthelmintic, anticancer, and anti‐infective properties.

Keywords

  • Citrus
  • Pharmacology
  • Citrus aurantium
  • Citrus sinensis
  • Citrus limon
  • Citrus bergamia

1. Introduction

The genus Citrus belongs to family Rutaceae, which is characterized by trees and bushes. Fruits of this genus, such as oranges, lemons, and tangerines, are widely cultivated in the tropical and subtropical areas of the world [1].

In medicine, Citrus fruits are used in the treatment of various diseases. Research shows that the intake of Citrus fruits can reduce the incidence of gastric cancer [2]. In addition, some isolated compounds from these fruits have effects on the central nervous system. For example, limonene, which is present in high concentrations in Citrus aurantium, showed a strong anxiolytic effect when tested in both animals and humans [3, 4].

To further understand the therapeutic potential of different Citrus species, we carried out a survey of in vitro and in vivo studies demonstrating their pharmacological actions, and summarized them in this chapter.

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2. Citrus species with pharmacological activity

2.1. Citrus aurantium L

The species C. aurantium L., popularly known as bitter orange, laranjeira‐amarga, or laranjeira‐cavalo, is a native plant of Southeast Asia, a region that corresponds to China and India. It was first introduced to Syria and Egypt by the Arabs and was subsequently brought to Europe [1]. In the medieval times, it was widely used in the Mediterranean region as a cardiac and vascular stimulant, digestive, sedative, tranquilizer, appetite stimulant, general tonic, and antidote against poisons [5]. In traditional Chinese medicine, bitter orange is used as a gastrointestinal stimulant and general tonic [6].

Ethnopharmacological studies in Brazilian communities (documentation of the empirical uses of medicinal plants in traditional communities) describe the popular use of C. aurantium L. fruit peels, flowers, and leaves in the treatment of the central nervous system disorders such as insomnia, anxiety, and hysteria [7, 8]. Another study reports that tea made from the leaves of C. aurantium L. can relieve stomach cramps and constipation, combat stomach acidity, and relieve fever, while tea from the seeds is reported to control diabetes [9].

Studies have focused on the investigation of C. aurantium L. effects on the central nervous system, especially its anxiolytic effect. Several studies on animals and humans have demonstrated the anxiolytic effect of this species. For example, the essential oil obtained from C. aurantium L. peels was found to show an anxiolytic effect on rats after a single dose, denoted by an increase in the residence time in the open arms of the elevated plus maze [10]. In addition, anxiolytic activity was observed in experimental models of generalized anxiety and obsessive‐compulsive disorder. At the same time, the mice did not show any signs of motor impairment, even after 15 consecutive days of treatment [7].

In a study conducted by Leite et al., 12 rats were evaluated in two models of anxiety: elevated plus maze and open field maze models. The rats were previously made to inhale the essential oil from C. aurantium L. at concentrations of 1.0, 2.5, and 5.0% for 7 min in an acrylic box. The authors observed a decrease in the emotional reactivity of the animals in both experimental models, suggesting a possible central action [11]. Moreover, the results of another study strongly suggest the involvement of 5‐HT 1a receptor, a subtype of serotonin receptors, in its anxiolytic activity, suggesting a potential mechanism by which C. aurantium L. affects the central nervous system [12].

Clinical trials testing the anxiolytic effect of C. aurantium have also demonstrated satisfactory results. In a certain study, preoperative patients received distilled C. aurantium L. flower 2 h before the procedure, then the STAI scale was used for anxiety evaluation. In comparison to the control group, the patients from experimental group showed a reduction in preoperative anxiety [13]. In another study, patients with chronic myelogenous leukemia inhaled essential oil of C. aurantium L. before the procedure of medullary material collection. The results indicated that the patients subjected to this intervention showed a decrease in the anxiety levels and remained relaxed during the procedure. In addition, C. aurantium L. oil, even at a single exposure, showed an activity comparable to that of the anxiolytic used as the positive control. This ensures its efficacy in controlling anxiety in patients subjected to unpleasant diagnostic procedures [3].

Its anxiolytic effect was also tested before labor. In a certain study, 18–35‐year‐old primiparous women were subjected to aromatherapy with C. aurantium L. oil during labor, and the results showed a significant reduction in the anxiety during labor in those women. Another clinical trial conducted on 126 primiparous women investigated the effects of aromatherapy with C. aurantium L. on pain during the first stage of labor. The women received 4 ml of C. aurantium L. in distilled water soaked in gauzes every 30 min. The results showed pain relief in the women subjected to this procedure. When asked whether aromatherapy using C. aurantium L. was satisfactory or not, 88.1% of the participants said that they were satisfied with the method applied and 92.1% said that they would use this method in future procedures. These studies show that aromatherapy with C. aurantium L. is a simple, inexpensive, and noninvasive intervention that can be beneficial for pregnant women [14]. However, because vaginal birth is a painful and serious process that is often feared by primiparous women, further studies are still required [15].

Several studies have been conducted to identify other possible actions of C. aurantium L. constituents, other than their effects on the central nervous system. Researchers isolated the flavonoids such as nobiletin, naringin, and hesperidin from C. aurantium L. and evaluated their anti‐inflammatory effect on rat cells in vitro. Results demonstrated the suppression of proinflammatory mediators, which confirms the anti‐inflammatory action of the isolated flavonoids [16]. Flavonoids isolated from C. aurantium L. were also evaluated for possible anticancer activity in murine lung cells. They demonstrated an anticancer effect through the regulation of apoptosis and cell migration, providing scientific support for the use of C. aurantium L. flavonoids in the treatment of human lung cancer [17].

Using a rat model of diabetes, researchers evaluated the possible hypoglycemic effect of neohesperidin derived from C. aurantium L. Treatment with neohesperidin was shown to increase glucose tolerance and insulin sensitivity, and to decrease blood glucose levels in the rats of the experimental group. These results demonstrate its hypoglycemic effect, and thus, its potential application for the prevention of diabetes and its complications [18].

Finally, although C. aurantium L. has been known for millennia, and a large number of studies have been focusing on its effects in the last decade, further research is needed to elucidate new mechanisms of action and therapeutic properties.

2.2. Citrus sinensis

The species C. sinensis, popularly known as sweet orange, also belongs to family Rutaceae. This fruit is of Asian origin, where it has been known for about 4000 years. With the expansion of trade and shipping routes, orange was introduced to various regions of the world for cultivation. Information from 1471 to 1472 reported the presence of sweet orange in Liguria, a region in Italy, before its introduction by the Portuguese to the Iberian Peninsula in 1498. In the eighteenth century, there were reports about varieties of sweet orange in Palestine, possibly introduced by an Armenian monk. In the Americas, Portuguese colonists introduced it to Bahia/BR in the sixteenth and eighteenth centuries, and Jesuits introduced it to California/USA, where they settled and started subsequent plantations [19].

An ethnobotanical survey in a Brazilian community identified the species C.sinensis as the most cited by women in attention to basic health, indicating the use of its leaves prepared in the form of tea as a soft tranquilizer for mild cases of anxiety and insomnia [20]. In addition, the flower and fruit are used by the population as tranquilizers and for relief of headache, migraine, fever, flu, allergy, and cough. We can conclude that sweet orange is among the main species of medicinal plants commonly used by the Brazilian community [21].

The traditional use of C. sinensis as a sedative can be attributed to hesperidin, which was identified in a study as the active principle in this plant responsible for sedation. Hesperidin performs its sedative action through interaction with and stimulation of adenosine receptors. Its effect is opposite to that observed after consumption of coffee and tea, which antagonize the adenosine receptors and thus maintain the wakefulness state [22]. Researchers investigated the properties of hesperidin extracted from C. sinensis through in vitro experiments, revealing its strong cytotoxic activity against human carcinoma cell lines and its antioxidant activity against DPPH free radical. According to these results, hesperidin can be considered a promising future drug. Orange peels are a cheap and available source from which hesperidin can be extracted in an efficient way and with high purity [23].

C. sinensis extracts have shown potent anthelmintic properties in vitro when compared with the positive control, indicating that it is equipotent to conventional anthelmintic drugs. However, in vivo studies should be conducted to establish this efficacy and to identify the active components responsible for the anthelmintic activity [24].

Researchers induced liver cirrhosis in rats for 16 weeks and treated the animals with C. sinensis dried peel extract orally for 9 weeks. After the completion of the treatment, the animals were euthanized to evaluate the biochemical and histopathological changes associated with liver cirrhosis. The histopathological examination of the liver tissue and the biochemical findings demonstrated the curative effect of the extract, suggesting its potential therapeutic application in liver fibrosis and cirrhosis [25].

Another study investigated the effects of the C. sinensis peel extract when administered orally to rats at a concentration of 25 mg/kg and revealed its antidiabetic potential. The researchers administered a single dose of alloxan (120 mg/kg) to the rats, which triggered an increase in serum glucose levels and α‐amylase activity. Then, a group of the rats was administered C. sinensis, which normalized all the adverse changes induced by alloxan. This reinforces the antidiabetic properties of the orange peel extract, which might be applied in the development of therapies for diabetes control [26].

In 2010, Faturi et al. demonstrated that the essential oil from C. sinensis had an anxiolytic effect when inhaled by rats. The animals were subjected to the elevated plus maze test, and the residence time of each rat in the open arms was measured. The possibility that the anxiolytic effect could result from any other inhaled aroma was discarded, since no anxiolytic activity was observed with Melaleuca alternifolia essential oil. The authors also reported that the animals were not previously exposed to the essential oil of sweet orange or any solutions that could contain the essence [27].

In a clinical study conducted on patients waiting for dental care, a group of the patients inhaled sweet orange essential oil in the waiting room, a second group listened to music, and the third group, which was the control group, did not receive any intervention. The results showed that the patients who inhaled the essential oil were calmer and had lower anxiety levels than the patients of the other groups [28].

Results obtained by Goes et al. in 2012 demonstrated the anxiolytic effect of the C. sinensis essential oil on healthy individuals while performing an anxiogenic task. The anxiolytic activity was evidenced by the significant difference in the level of anxiety between the group exposed to C. sinensis and the control group, providing scientific support for the use of this essential oil as a tranquilizer in aromatherapy [29].

The results presented here support the use of C. sinensis as an aid to combat insomnia and anxiety. Research also indicates that the natural constituents of sweet orange can be used in the pharmaceutical industry, as natural cytotoxic agents, anthelmintics, antidiabetic agents, or for the treatment of liver cirrhosis.

2.3. Citrus bergamia

Citrus bergamia, commonly known as bergamot [30], is a plant belonging to family Rutaceae, subfamily Esperidea, and is defined as a hybrid between bitter orange (Citrus aurantium) and lemon (Citrus limon) [31]. The botanical and geographical origins of this plant are still unknown. The name “bergamot” seems to be derived from Berga, a Spanish city from which the plant was transported to Calabria in Southern Italy. C. bergamia is cultivated almost exclusively along the southern coast of Calabria; over 90% of its world production comes from this region. However, it is also cultivated to a lesser extent in other countries, such as Greece, Morocco, Iran, Ivory Coast, Argentina, and Brazil [32].

The fruit of C. bergamia is mainly used for the extraction of its essential oil, which is used in perfumes, drugs, cosmetics, food, and clothing [33]. Throughout the cultivation and the processing of C. bergamia, tons of wastes of low commercial value, but of great industrial potential, are generated. These wastes contain high levels of nutrients, pigments, and bioactive components with low toxicity [34].

There are evidences that C. bergamia contains antibacterial and antifungal active constituents, in addition to its anti‐inflammatory, antiproliferative, neuropsychopharmacological, neuroprotective, and analgesic effects, [35] as well as its cardiovascular properties in rodents [32]. Bergamot juice, which is obtained from the endocarp after the extraction of the essential oil, was found to exhibit hypoglycemic and hypolipidemic activities, as well as anti‐inflammatory [3638] and anticancer properties [39].

The anti‐infective properties of C. bergamia derivatives can be observed from the action of its essential oil against bacteria, mycetes, and larvae, and the action of its juice against Helicobacter pylori. Compounds derived from its fruit peel extract have antimicrobial properties. Studies report that its essential oil has antibacterial and antifungal activities against Campylobacterjejuni, Escherichiacoli O157, Listeriamonocytogenes, Bacilluscereus, Staphylococcusaureus, and dermatophytes. The essential oil of C. bergamia shows in vitro activity against Candida species, which suggests its potential application in the topical treatment of fungal infections by Candida. It also demonstrates in vitro activity against dermatophytes [40].

In addition, favorable results were obtained regarding its pharmacological properties in nervous system disorders. Sometimes, the essential oil from C. bergamia, usually extracted from the peel, is used in aromatherapy to relieve stress and anxiety [41].

In a study carried out on rats to investigate the anxiolytic activity of C. bergamia, the essential oil was administered to the rats at different concentrations and its effects were compared with those of diazepam. The results of this study indicated that C. bergamia showed an anxiolytic action, which was observed when the rats were subjected to the elevated plus maze and hole‐board tests. The researchers observed a reduction in the activity of the hypothalamic‐pituitary‐adrenal axis, reducing corticosterone response to stress [42].

Clinical studies have also reported beneficial effects of C. bergamia essential oil in cardiac control, blood pressure reduction, and stress response management, in addition to its effect on the central nervous system [43]. Although the mechanisms by which the effects on the central nervous system are mediated have not yet been fully elucidated, it has been suggested that this action might be mediated by the release of amino acids that modulate the synaptic plasticity [32].

Some studies demonstrated that the essential oil from C. bergamia also shows anticancer activity. For example, Berliocchi et al. demonstrated in vitro antiproliferative activity of C. bergamia essential oil against SH‐SY5Y human neuroblastoma cells. In this work, the lethal effect of C. bergamia was mediated by activating multiple pathways that lead to cell death by both necrosis and apoptosis [44]. Compounds derived from bergamot oil, such as limonene, monoterpenes related to limonene, alcohol, and perillic acid, were also found to inhibit the proliferation of breast cancer cells, and to show chemopreventive and chemotherapeutic effects in models of mammary tumors [45].

However, the poor water solubility, weak stability, and limited bioavailability of essential oils have prevented their use in cancer therapy. Nevertheless, due to the favorable results regarding the anticancer action of the essential oil from C. bergamia, some attempts have been made to use bergamot in cancer therapy. For example, in 2013, Celia et al. developed liposomes of C. bergamia essential oil, which improved its water solubility and increased its in vitro anticancer activity against SH‐SY5Y human neuroblastoma cells [46].

In order to elucidate the mechanisms by which the essential oil from C. bergamia has anticancer activity, Russo R et al. conducted a study in 2013 to identify the components involved in the cell death process. The results of the study suggested an important role of the combined action of monoterpenes in the process of cell death [35].

Regarding the protective cardiovascular properties, Di Donna et al. established a rat model in 2014 to investigate the hypocholesterolemic effect of 3‐hydroxy‐3‐methyl‐glutaryl flavanones enriched fraction (HMGF), extracted from C. bergamia fruits, in comparison with that of statin (simvastatin). Both HMGF and simvastatin reduced total cholesterol, triglycerides, very low density lipoproteins (VLDL), and low‐density lipoproteins (LDL). However, only HMGF caused an increase in high‐density lipoprotein (HDL). In addition, HMGF showed no genotoxic effects and was cytotoxic only at high concentrations. Thus, the authors concluded that daily supplementation of HMGF in the diet can be very effective against hypercholesterolemia, featuring the cardiovascular protective properties of bergamot [47].

Although all the pharmacological effects of C. bergamia indicate potential clinical applications in the future, only clinical studies investigating its anxiolytic effects in aromatherapy were published heretofore [32].

2.4. Citrus limon

The Latin name of lemon is C. limon (Linnaeus) N. Burman. It belongs to family Rutaceae, and it is sometimes called limoeiro or limoeiro‐azêdo [48]. It originated in Southeast Asia and is believed to have been introduced to Europe by Muslims across the Iberian Peninsula and Sicily [5]. Currently, Spain is considered the main producer country of this genus in the Mediterranean region. Lemon is considered the third most important species of the genus Citrus, as it contains many relevant natural chemical compounds, including citric acid, ascorbic acid, minerals, and flavonoids [49].

Recently, some of the therapeutic properties of C. limon have been recognized in the literature. Studies have found that the use of lemon helps neutralize the acidity of the gastric environment, by stimulating the production of potassium carbonate, indicating its protective effects on the gastric mucosa. It was also found to have analgesic, anti‐anemic, anti‐sclerotic, antipyretic, antiseptic, emollient, and moisturizer properties. The recognized actions of lemon cellulose are that it is anti‐diarrheal, diuretic, intestinal mucosa protector, local hemostatic, vascular stimulant and protector, and vitamin [5].

Production networks of lemon generate large amounts of wastes and by‐products, which are an important source of bioactive compounds with potential applications in animal feeding, processed foods, and health care [49]. Although its health benefits are always attributed to its vitamin C content, recently, it has been found that flavonoids also play an important role [48]. Some authors suggest that flavonoids present in lemon have different biological functions, including antioxidant, anti‐inflammatory, antiallergic, antiviral, antiproliferative, antimutagenic, and anticancer activities [48].

Hesperidin, which is the main flavonoid in C. limon, influences the vascular permeability, increases the capillary resistance, and has analgesic and anti‐inflammatory properties [49]. It is also an effective antioxidant, since it is capable of scavenging free radicals that are involved in cancer. Some studies have shown that flavonoids present in lemon juice also have hypocholesterolemic properties [50].

Trovato et al. conducted a study on rats in 1996 and found that C. limon had a significant effect on the levels of cholesterol and triglycerides, suggesting that the prolonged consumption of its juice might offer significant protection from hypercholesterolemia [51].

Another study investigated the protective effect of the essential oil from C. limon against acute hepatic and renal damage induced by a high dose of aspirin in Wistar albino rats. The data obtained in this study demonstrated that the treatment with C. limon protected the liver and kidney from damages induced by aspirin [52].

Regarding the pharmacological effects on the central nervous system, a recent study conducted by Khan and Riaz evaluated the effects of lemon on the behavior of rats, using three different doses (0.2, 0.4, and 0.6 ml/kg), considered low, moderate, and high doses, respectively. The anxiolytic and antidepressant activities were evaluated twice, for 15 days, using the open field, elevated plus maze, and forced swimming tests. In the open field test, C. limon revealed an increase in the distance traveled, the number of central entries, and the number of rearing at moderate dose, while in the elevated plus maze, the number of open arm entries was found to be increased. Whereas in the forced swimming test, there was a decrease in duration of immobility and an increase in the duration of climbing. Thus, results suggest that C. limon at moderate dose has an anxiolytic effect [53].

It has been noted that disorders such as anxiety and depression can be managed through healthier variations in dietary patterns, since there is evidence that a diet rich in antioxidants and vitamins reduces these symptoms. Accordingly, a study was performed in order to evaluate the behavioral effects of C. limon and Punica granatum in rats. In this study, two combinations of doses were used: 0.4 + 5 ml/kg and 0.2 + 8 ml/kg of C. limon and P. granatum, respectively. As in the previous study, the antidepressant and anxiolytic effects were evaluated twice, for 15 days, using forced swimming, open field, and elevated plus maze tests. In the open field test, the use of C. limon and P. granatum showed an increase in the distance traveled and the number of central entries at the dose combination of 0.4 + 5 ml/kg. In the elevated plus maze test, the number of entries was increased at the highest dose combination (0.2 + 8 ml/kg). In the forced swimming test, there was a decrease in the immobility duration and an increase in the climbing duration at both dose combinations: 0.4 + 5 ml/kg and 0.2 + 8 ml/kg C. limon and P. granatum, respectively. Based on these results, the authors suggested that C. limon and P. granatum, at a combination of 0.4 + 5 ml/kg, show anxiolytic and antidepressant effects [54].

In another study conducted by Riaz et al. in 2014, the effect of C. limon and pomegranate juice on rats’ memory was evaluated. It is known that memory is greatly influenced by factors such as diet, stress, and sleep quality. The results of this study indicated that C. limon contains essential phytochemicals and nutrients that improve the memory, particularly the short‐term memory. They also concluded that flavonoids in these juices could be responsible for this effect [55].

Hesperidin extracted from C. limon was found to play an important vasodilator action. In 2016, Dobias et al. evaluated the effect of hesperidin on vascular responses in normotensive and hypertensive rats. Fifteen‐week‐old healthy Wistar rats and spontaneously hypertensive (SHR) rats were randomly assigned to receive either hesperidin (50 mg/kg/day) or a corresponding volume of water orally for 4 weeks. The vascular responses of isolated femoral arteries were studied using a myograph under control conditions and during the NO‐synthase inhibition. Although hesperidin had no effects on blood pressure, it significantly improved endothelium‐dependent vasodilation in Wistar and SHR rats. The contraction responses were increased in all the groups to a similar extent, but the relaxing responses were significantly attenuated in the SHR group only. The inhibition of the potassium channels (Kv) significantly reduced the endothelium‐dependent vasodilator response only in SHR rats administered hesperidin. This indicates that hesperidin can improve endothelium‐dependent vasodilation during hypertension [56].

Regarding the anti‐inflammatory activities described for C. limon, in 2016, Amorim et al. conducted a study to confirm the hypothesis that essential oil (EO) from C. limon, C. latifolia, C. aurantifolia, and C. limonia have antinociceptive effects. Thus, they were tested each one on the formalin‐induced licking behavior. This model is a widely used pain model in evaluating antinociceptive and anti‐inflammatory drugs. The results of this study suggest that EO from C. limon, C. aurantifolia, and C. limonia have an anti‐inflammatory effect because they reduced the second phase response to formalin. This may occur through a reduction in inflammatory mediator liberation in mice paws or a direct action on one or more mediator receptors [57].

Since C. limon is widely used in traditional medications in India and China, we sought to explore the importance of flavonoids that are abundant in citrus fruits on platelet function. Nobiletin is a highly abundant flavonoid present in these and has been shown to reduce the adhesive properties of platelets. In 2015, Vaiyapuri et al. conducted a study to verify the pharmacological effects of a polymethoxy flavonoid, nobiletin, in the modulation of platelet function. Nobiletin was shown suppress a range of well‐established activatory mechanisms, including platelet aggregation, granule secretion, integrin modulation, calcium mobilization, and thrombus formation. This study provided insight into the underlying molecular mechanisms through which nobiletin modulates hemostasis and thrombus formation. Therefore, nobiletin may represent a potential antithrombotic agent of dietary origins [58].

In conclusion, C. limon presents numerous curative properties, and thus it has been widely used as a traditional medicine for the treatment of various diseases [52]. However, more studies still need to be conducted in order for its application in clinical practice to be established and disseminated [59].

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3. Conclusion

Citrus species are well known and have been commonly used by populations for hundreds of years for various purposes. This knowledge of their therapeutic potential has led to several studies that proved the pharmacological effects of the above‐mentioned species (Table 1). The effect of Citrus species on the central nervous system was highlighted as the study objective in most of the publications. However, research has advanced in seeking other pharmacological actions, especially of isolated constituents of the species.

Citrus speciesPharmacological action
Citrus aurantium L.Gastrointestinal stimulant and general tonic.
Treatment of central nervous system disorders like insomnia, anxiety, and hysteria.
Relieve stomach cramps and constipation, combat stomach acidity.
Hypoglycemic effect.
Anti‐inflammatory.
Anxiolytic effect.
Citrus sinensisSedative action.
Anthelmintic properties.
Treatment of liver cirrhosis.
Antidiabetic properties.
Anxiolytic effect.
Citrus bergamiaAntibacterial. Antifungal. Anti‐inflammatory. Analgesic. Antiproliferative and anticancer properties. Neuropsychopharmacological. Neuroprotective.
Anxiolytic activity.
Hypoglycemic and hypolipidemic activities.
Citrus limonAnalgesic. Anti‐anemic. Anti‐sclerotic. Antipyretic. Antiseptic.
Emollient and moisturizer properties.
Anti‐diarrheal. Diuretic. Intestinal mucosa protector. Local hemostatic.
Vascular stimulant and protector.
Antioxidant. Antiallergic. Antiviral. Anti‐inflammatory. Antiproliferative, antimutagenic, and anticancer activities.

Table 1. 

Pharmacological action of different citrus species (studies in vitro and in vivo).

References

  1. 1. Zou Z, Xi W, Hu Y, Nie C, Zhou Z. Antioxidant activity of Citrus fruits. Food Chem. 2016;196:885–896. Available from: http://dx.doi.org/10.1016/j.foodchem.2015.09.072
  2. 2. González CA, Sala N, Rokkas T. Gastric cancer: Epidemiologic aspects. Helicobacter. 2013;18(S1):34–38.
  3. 3. Pimenta FCF, Alves MF, Pimenta MBF, Melo SAL, Almeida AAF De, Leite JR, et al. Anxiolytic effect of Citrusaurantium L. on patients with chronic myeloid leukemia. Phyther Res. 2016;30(4):613–617.
  4. 4. Alberto C, Ramos F, Cássia R De, Sá S, Alves MF, Salete M, et al. Histopathological and biochemical assessment of d‐limonene‐induced liver injury in rats. Toxicol. Rep. 2015;2:482–488.
  5. 5. Arias B Alvarez, Ramón‐Laca L. Pharmacological properties of Citrus and their ancient and medieval uses in the Mediterranean region. J Ethnopharmacol. 2005;97(1):89–95.
  6. 6. Bouchard NC, Howland MA, Greller HA, Hoffman RS, Nelson LS. Ischemic stroke associated with use of an ephedra‐free dietary supplement containing synephrine. Mayo Clin Proc. 2005;80(4):541–545.
  7. 7. De Moraes Pultrini A, Almeida Galindo L, Costa M. Effects of the essential oil from Citrusaurantium L. in experimental anxiety models in mice. Life Sci. 2006;78(15):1720–1725.
  8. 8. Silva MD, Dreveck S, Zeni ALB. Ethnobotanical study of medicinal plants used by rural population around the Itajaí National Park. Indaial. 2009;10(2):54–64.
  9. 9. Crispim AA, Nogueira CR, Figueira CMB. Comparison between the surveys Ethnobotanical about use of medicinal plants in the municipalities of Passa Vinte/MG and in neighborhood Arthur Cataldi, Barra of Piraí/RJ. Rev episteme transversalis. 2012;3(1):1–16.
  10. 10. Carvalho‐Freitas MIR, Costa M. Anxiolytic and sedative effects of extracts and essential oil from Citrusaurantium L. Biol Pharm Bull. 2002;25(12):1629–1633. Available from: http://www.ncbi.nlm.nih.gov/pubmed/12499653
  11. 11. Leite MP, Fassin J, Baziloni EMF, Almeida RN, Mattei R, Leite JR. Behavioral effects of essential oil of Citrusaurantium L. inhalation in rats. Braz. J Pharmacogn. 2008;18(SUPPL):661–666.
  12. 12. Costa CA, Cury TC, Cassettari BO, Takahira RK, Flório JC, Costa M. Citrusaurantium L. essential oil exhibits anxiolytic‐like activity mediated by 5‐HT(1A)‐receptors and reduces cholesterol after repeated oral treatment. BMC Complement Altern Med. 2013;13:42. Available from: http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=3598547&tool=pmcentrez&rendertype=abstract
  13. 13. Akhlaghi M, Shabanian G, Rafieian‐Kopaei M, Parvin N, Saadat M. Citrus aurantium flower and Preoperative Anxiety. Rev Bras Anestesiol. 2011;61(6):702–712.
  14. 14. Seraj F, Nourani S, Mokhber N, Shakeri MT. Investigating the effects of aromatherapy with Citrusaurantium oil on anxiety during the first stage of labor. Iran J Obstet Gynecol Infertil. 2014;17(111):20–29.
  15. 15. Namazi M, Ali Akbari SA, Mojab F, Talebi A, Majd HA, Jannesari S. Effects of Citrusaurantium (bitter orange) on the severity of first‐stage labor pain. Iran J Pharm Res. 2014;13(3):1011–1018.
  16. 16. Kang SR, Park K Il, Park HS, Lee DH, Kim JA, Nagappan A, et al. Anti‐inflammatory effect of flavonoids isolated from Korean Citrusaurantium L. on lipopolysaccharide‐induced mouse macrophage RAW 264.7 cells by blocking of nuclear factor‐kappa B (NF‐ĸB) and mitogen‐activated protein kinase (MAPK) signalling pathways. Food Chem. 2011;129(4):1721–1728. Available from: http://dx.doi.org/10.1016/j.foodchem.2011.06.039
  17. 17. Park K Il, Park HS, Kim MK, Hong GE, Nagappan A, Lee HJ, et al. Flavonoids identified from Korean Citrusaurantium L. inhibit non‐small cell lung cancer growth in vivo and in vitro. J Funct Foods. 2014;7(1):287–297. Available from: http://dx.doi.org/10.1016/j.jff.2014.01.032
  18. 18. Jia S, Hu Y, Zhang W, Zhao X, Chen Y, Sun C, et al. Hypoglycemic and hypolipidemic effects of neohesperidin derived from Citrusaurantium L. in diabetic KK‐A(y) mice. Food Funct. 2015;6(3):878–886.
  19. 19. Donadio LC. Orange pear. Jaboticabal: FUNEP; 1999.
  20. 20. Nazária MDE, Campelo I, Vieira FJ, Roseli D, Melo F, Orientadora DB, et al. Ethnobotanical survey in the rural community tambaqui. 2011;(1989):30–32.
  21. 21. Ferreira FMC, Lourenço FJDC, Baliza DP. Ethnobotanical survey of medicinal plants in maroon community Carreiros. Mercês ‐ Minas Gerais. 2014;9(3):205–212.
  22. 22. Guzmán‐Gutiérrez SL, Navarrete A. Pharmacological exploration of the sedative mechanism of hesperidin identified as the active principle of Citrussinensis flowers. Planta Med. 2009;75(4):295–301.
  23. 23. Al‐Ashaal HA, El‐Sheltawy ST. Antioxidant capacity of hesperidin from Citrus peel using electron spin resonance and cytotoxic activity against human carcinoma cell lines. Pharm Biol. 2011;49(3):276–282. Available from: http://www.ncbi.nlm.nih.gov/pubmed/21323480
  24. 24. Munne SL, Parwate D V, Ingle VN, Tukadoji R. In‐vitro anthelmintic activity of citrus sinensis seed coats. International Journal of pharmacological research. 2012;2(2):83–85.
  25. 25. Ali S, Prasad R, Naime M, Zafar H, Mahmood A, Routray I, et al. Dried peel fraction of Citrussinensis partially reverses pathological changes in rat model of liver cirrhosis. Med J Nutr Metab. 2011;4(1):57–67.
  26. 26. Parmar HS, Kar A. Antidiabetic potential of Citrussinensis and Punicagranatum peel extracts in alloxan treated male mice. Bio Factors. 2007;31(1):17–24.
  27. 27. Faturi CB, Leite JR, Alves PB, Canton AC, Teixeira‐Silva F. Anxiolytic‐like effect of sweet orange aroma in Wistar rats. Prog Neuro‐Psychopharmacol Biol Psychiatry. 2010;34(4):605–9. Available from: http://dx.doi.org/10.1016/j.pnpbp.2010.02.020
  28. 28. Lehrner J, Marwinski G, Lehr S, Johren P, Deecke L. Ambient odors of orange and lavender reduce anxiety and improve mood in a dental office. Physiol Behav. 2005;86(1–2):92–95.
  29. 29. Goes TC, Antunes FD, Alves PB, Teixeira‐Silva F. Effect of sweet orange aroma on experimental anxiety in humans. J Altern Complement Med. 2012;18(8):798–804.
  30. 30. Cappello AR, Dolce V, Iacopetta D, Martello M, Fiorillo M, Curcio R, et al. Bergamot (Citrusbergamia Risso) flavonoids and their potential benefits in human hyperlipidemia and atherosclerosis: an overview. Mini Rev Med Chem. 2016 [cited 2016 Sep 9];16(8):619–629. Available from: http://www.ncbi.nlm.nih.gov/pubmed/26156545
  31. 31. Cirmi S, Bisignano C, Mandalari G, Navarra M. Anti‐infective potential of Citrusbergamia Risso et Poiteau (bergamot) derivatives: a systematic review. Phytother Res. 2016;30(9):1404–1411 May 24 [cited 2016 Aug 26]; Available from: http://www.ncbi.nlm.nih.gov/pubmed/27218799
  32. 32. Navarra M, Mannucci C, Delbò M, Calapai G. Citrusbergamia essential oil: From basic research to clinical application. Front Pharmacol. 2015;6(MAR):1–7.
  33. 33. Tranchida PQ, Presti M Lo, Costa R, Dugo P, Dugo G, Mondello L. High‐throughput analysis of bergamot essential oil by fast solid‐phase microextraction‐capillary gas chromatography‐flame ionization detection. J Chromatogr A. 2006;1103(1):162–165. Available from: http://www.ncbi.nlm.nih.gov/pubmed/16364343
  34. 34. Navarra M, Ferlazzo N, Cirmi S, Trapasso E, Bramanti P, Lombardo GE, et al. Effects of bergamot essential oil and its extractive fractions on SH‐SY5Y human neuroblastoma cell growth. J Pharm Pharmacol. 2015;67(8):1042–1053. Available from: http://dx.doi.org/10.1016/j.ejca.2015.06.065
  35. 35. Russo R, Ciociaro A, Berliocchi L, Valentina Cassiano MG, Rombolà L, Ragusa S, et al. Implication of limonene and linalyl acetate in cytotoxicity induced by bergamot essential oil in human neuroblastoma cells. Fitoterapia. 2013;89(1):48–57. Available from: http://dx.doi.org/10.1016/j.fitote.2013.05.014
  36. 36. Mollace V, Sacco I, Janda E, Malara C, Ventrice D, Colica C, et al. Hypolipemic and hypoglycaemic activity of bergamot polyphenols: from animal models to human studies. Fitoterapia. 2011;82(3):309–316. Available from: http://www.ncbi.nlm.nih.gov/pubmed/21056640
  37. 37. Impellizzeri D, Bruschetta G, Di Paola R, Ahmad A, Campolo M, Cuzzocrea S, et al. The anti‐inflammatory and antioxidant effects of bergamot juice extract (BJe) in an experimental model of inflammatory bowel disease. Clin Nutr. 2015;34(6):1146–1154. Available from: http://www.ncbi.nlm.nih.gov/pubmed/25491246
  38. 38. Risitano R, Currò M, Cirmi S, Ferlazzo N, Campiglia P, Caccamo D, et al. Flavonoid fraction of Bergamot juice reduces LPS‐induced inflammatory response through SIRT1‐mediated NF‐κB inhibition in THP‐1 monocytes. PLoS One. 2014;9(9):e107431. Available from: http://www.ncbi.nlm.nih.gov/pubmed/25260046
  39. 39. Braakhuis AJ, Campion P, Bishop KS. Reducing breast cancer recurrence: The role of dietary polyphenolics. Nutrients. 2016;8(9). Available from: http://www.ncbi.nlm.nih.gov/pubmed/27608040
  40. 40. Sanguinetti M, Posteraro B, Romano L, Battaglia F, Lopizzo T, De Carolis E, et al. In vitro activity of Citrusbergamia (bergamot) oil against clinical isolates of dermatophytes. J Antimicrob Chemother. 2007;59(2):305–308. Available from: http://www.ncbi.nlm.nih.gov/pubmed/17118937
  41. 41. Bagetta G, Morrone LA, Rombolà L, Amantea D, Russo R, Berliocchi L, et al. Neuropharmacology of the essential oil of bergamot. Fitoterapia. 2010;81(6):453–461. Available from: http://dx.doi.org/10.1016/j.fitote.2010.01.013
  42. 42. Saiyudthong S, Marsden CA. Acute effects of bergamot oil on anxiety‐related behaviour and corticosterone level in rats. Phyther Res. 2011;25(6):858‐62
  43. 43. Rangel‐Huerta OD, Pastor‐Villaescusa B, Aguilera CM, Gil A. A systematic review of the efficacy of bioactive compounds in cardiovascular disease: Phenolic compounds. Nutrients. 2015;7(7):5177–5216. Available from: http://www.ncbi.nlm.nih.gov/pubmed/26132993
  44. 44. Berliocchi L, Ciociaro A, Russo R, Cassiano MGV, Blandini F, Rotiroti D, et al. Toxic profile of bergamot essential oil on survival and proliferation of SH‐SY5Y neuroblastoma cells. Food Chem Toxicol. 2011;49(11):2780–2792. Available from: http://dx.doi.org/10.1016/j.fct.2011.08.017
  45. 45. Ahmadi A, Shadboorestan A, Nabavi SF, Setzer WN, Nabavi SM. The role of hesperidin in cell signal transduction pathway for the prevention or treatment of cancer. Curr Med Chem. 2015;22(30):3462–3471. Available from: http://www.ncbi.nlm.nih.gov/pubmed/26502950
  46. 46. Celia C, Trapasso E, Locatelli M, Navarra M, Ventura CA, Wolfram J, et al. Anticancer activity of liposomal bergamot essential oil (BEO) on human neuroblastoma cells. Colloids Surfaces B Biointerfaces. 2013;112:548–553. Available from: http://dx.doi.org/10.1016/j.colsurfb.2013.09.017
  47. 47. Di Donna L, Iacopetta D, Cappello AR, Gallucci G, Martello E, Fiorillo M, et al. Hypocholesterolaemic activity of 3‐hydroxy‐3‐methyl‐glutaryl flavanones enriched fraction from bergamot fruit (Citrusbergamia): “In vivo” studies. J Funct Foods. 2014;7:558–568. Available from: http://www.sciencedirect.com/science/article/pii/S17564 6461300323X
  48. 48. Del Rio JA, Fuster MD, Gomez P, Porras I, Garcia‐Lidn A, Ortuo A. Citruslimon: A source of flavonoids of pharmaceutical interest. Food Chem. 2004;84(3):457–461.
  49. 49. Gonzalez‐Molina E, Dominguez‐Perles R, Moreno DA, Garcia‐Viguera C. Natural bioactive compounds of Citruslimon for food and health. J Pharm Biomed Anal. 2010;51(2):327–345.
  50. 50. Benavente‐García O, Castillo J. Update on uses and properties of Citrus flavonoids: new findings in anticancer, cardiovascular, and anti‐inflammatory activity. J Agric Food Chem. 2008 Aug 13;56(15):6185–6205. Available from: http://www.ncbi.nlm.nih.gov/pubmed/18593176
  51. 51. Trovato A, Monforte MT, Barbera R, Rossitto A, Galati EM, Forestieri AM. Effects of fruit juices of Citrussinensis L. and Citruslimon L. on experimental hypercholesterolemia in the rat. Phytomedicine. 1996;2(3):221–227.
  52. 52. Bouzenna H, Dhibi S, Samout N, Rjeibi I, Talarmin H, Elfeki A, et al. The protective effect of Citruslimon essential oil on hepatotoxicity and nephrotoxicity induced by aspirin in rats. Biomed Pharmacother. 2016;83:1327–1334. Available from: http://www.ncbi.nlm.nih.gov/pubmed/27571876
  53. 53. Khan RA, Riaz A. Behavioral effects of Citruslimon in rats. Metab Brain Dis. 2015; 30(2):589–596.
  54. 54. Riaz A, Khan RA. Behavioral effects of Citruslimon and Punicagranatum combinations in rats. Metab Brain Dis. 2016; Available from: http://www.ncbi.nlm.nih.gov/pubmed/27510713
  55. 55. Riaz A, Khan RA, Algahtani HA. Memory boosting effect of Citruslimon, Pomegranate and their combinations. Pak J Pharm Sci. 2014;27(6):1837–1840. Available from: http://www.ncbi.nlm.nih.gov/pubmed/25362607
  56. 56. Dobiaš L, Petrová M, Vojtko R, Kristová V. Long‐term treatment with hesperidin improves endothelium‐dependent vasodilation in femoral artery of spontaneously hypertensive rats: The involvement of NO‐synthase and Kv channels. Phytother Res. 2016;30(10):1665–1671; Available from: http://www.ncbi.nlm.nih.gov/pubmed/27363952
  57. 57. Amorim JL, Simas DLR, Pinheiro MMG, Moreno DSA, Alviano CS, da Silva AJR, et al. Anti‐inflammatory properties and chemical characterization of the essential oils of four citrus species. PLoS ONE. 2016;11(4): e0153643. doi:10.1371/journal.pone.0153643
  58. 58. Vaiyapuri S, Roweth H, Ali MS, Unsworth AJ, Stainer AR, Flora GD, et al. Pharmacological actions of nobiletin in the modulation of platelet function. British J. Pharmacol. 2015;(172): 4133–4145
  59. 59. Yavari Kia P, Safajou F, Shahnazi M, Nazemiyeh H. The effect of lemon inhalation aromatherapy on nausea and vomiting of pregnancy: a double‐blinded, randomized, controlled clinical trial. Iran Red Crescent Med J. 2014;16(3):e14360. Available from: http://www.ncbi.nlm.nih.gov/pubmed/24829772

Written By

Flavia Cristina Fernandes Pimenta, Nathália de Alencar Cunha Tavares, Gabriel Chaves Neto, Mateus Alves, Martina Fernandes Pimenta, Juliete Melo Diniz, Arnaldo Correia de Medeiros and Margareth de Fátima Formiga Melo Diniz

Submitted: 21 June 2016 Reviewed: 21 October 2016 Published: 12 April 2017