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Cooper",slug:"robert-d.-cooper"}]},{id:"43671",title:"Ecology of Larval Habitats",slug:"ecology-of-larval-habitats",signatures:"Eliška Rejmánková, John Grieco, Nicole Achee and Donald R.\nRoberts",authors:[{id:"151632",title:"Prof.",name:"Nicole",middleName:null,surname:"Achee",fullName:"Nicole Achee",slug:"nicole-achee"},{id:"152601",title:"Prof.",name:"Eliska",middleName:null,surname:"Rejmankova",fullName:"Eliska Rejmankova",slug:"eliska-rejmankova"},{id:"169016",title:"Dr.",name:"John",middleName:null,surname:"Grieco",fullName:"John Grieco",slug:"john-grieco"}]},{id:"43954",title:"From Anopheles to Spatial Surveillance: A Roadmap Through a Multidisciplinary Challenge",slug:"from-anopheles-to-spatial-surveillance-a-roadmap-through-a-multidisciplinary-challenge",signatures:"Valérie Obsomer, Nicolas Titeux, Christelle Vancustem, Grégory\nDuveiller, Jean-François Pekel, Steve Connor, Pietro Ceccato and\nMarc Coosemans",authors:[{id:"131417",title:"Dr.",name:"Valérie",middleName:null,surname:"Obsomer",fullName:"Valérie Obsomer",slug:"valerie-obsomer"},{id:"152754",title:"Prof.",name:"Marc",middleName:null,surname:"Coosemans",fullName:"Marc Coosemans",slug:"marc-coosemans"},{id:"153949",title:"Dr.",name:"Pietro",middleName:null,surname:"Ceccato",fullName:"Pietro Ceccato",slug:"pietro-ceccato"},{id:"153950",title:"Dr.",name:"Gregory",middleName:null,surname:"Duveiller",fullName:"Gregory Duveiller",slug:"gregory-duveiller"},{id:"153952",title:"Dr.",name:"Christelle",middleName:null,surname:"Vancutsem",fullName:"Christelle Vancutsem",slug:"christelle-vancutsem"},{id:"153980",title:"Dr.",name:"Nicolas",middleName:null,surname:"Titeux",fullName:"Nicolas Titeux",slug:"nicolas-titeux"},{id:"154158",title:"Dr.",name:"Steve J",middleName:null,surname:"Connor",fullName:"Steve J Connor",slug:"steve-j-connor"},{id:"167685",title:"MSc.",name:"Jean-Francois",middleName:null,surname:"Pekel",fullName:"Jean-Francois Pekel",slug:"jean-francois-pekel"}]},{id:"43960",title:"Simian Malaria Parasites: Special Emphasis on Plasmodium knowlesi and Their Anopheles Vectors in Southeast Asia",slug:"simian-malaria-parasites-special-emphasis-on-plasmodium-knowlesi-and-their-anopheles-vectors-in-sout",signatures:"Indra Vythilingam and Jeffery Hii",authors:[{id:"151116",title:"Dr.",name:"Indra",middleName:null,surname:"Vythilingam",fullName:"Indra Vythilingam",slug:"indra-vythilingam"},{id:"169006",title:"Dr.",name:"Jeffery",middleName:null,surname:"Hii",fullName:"Jeffery Hii",slug:"jeffery-hii"}]},{id:"44039",title:"Thermal Stress and Thermoregulation During Feeding in Mosquitoes",slug:"thermal-stress-and-thermoregulation-during-feeding-in-mosquitoes",signatures:"Chloé Lahondère and Claudio R. Lazzari",authors:[{id:"151619",title:"Prof.",name:"Claudio",middleName:null,surname:"R. Lazzari",fullName:"Claudio R. Lazzari",slug:"claudio-r.-lazzari"},{id:"151620",title:"Ms.",name:"Chloé",middleName:null,surname:"Lahondère",fullName:"Chloé Lahondère",slug:"chloe-lahondere"}]},{id:"43955",title:"The Anopheles Mosquito Microbiota and Their Impact on Pathogen Transmission",slug:"the-anopheles-mosquito-microbiota-and-their-impact-on-pathogen-transmission",signatures:"Mathilde Gendrin and George K. Christophides",authors:[{id:"154007",title:"Dr.",name:"Mathilde",middleName:null,surname:"Gendrin",fullName:"Mathilde Gendrin",slug:"mathilde-gendrin"},{id:"154008",title:"Prof.",name:"George",middleName:"K",surname:"Christophides",fullName:"George Christophides",slug:"george-christophides"}]},{id:"43829",title:"Bacterial Biodiversity in Midguts of Anopheles Mosquitoes, Malaria Vectors in Southeast Asia",slug:"bacterial-biodiversity-in-midguts-of-anopheles-mosquitoes-malaria-vectors-in-southeast-asia",signatures:"Sylvie Manguin, Chung Thuy Ngo, Krajana Tainchum, Waraporn\nJuntarajumnong, Theeraphap Chareonviriyaphap, Anne-Laure\nMichon and Estelle Jumas-Bilak",authors:[{id:"50017",title:"Prof.",name:"Sylvie",middleName:null,surname:"Manguin",fullName:"Sylvie Manguin",slug:"sylvie-manguin"},{id:"75315",title:"Prof.",name:"Theeraphap",middleName:null,surname:"Chareonviriyaphap",fullName:"Theeraphap Chareonviriyaphap",slug:"theeraphap-chareonviriyaphap"},{id:"88985",title:"Prof.",name:"Anne-Laure",middleName:null,surname:"Michon",fullName:"Anne-Laure Michon",slug:"anne-laure-michon"},{id:"88986",title:"Prof.",name:"Estelle",middleName:null,surname:"Jumas-Bilak",fullName:"Estelle Jumas-Bilak",slug:"estelle-jumas-bilak"},{id:"156016",title:"MSc.",name:"Chung Thuy",middleName:null,surname:"Ngo",fullName:"Chung Thuy Ngo",slug:"chung-thuy-ngo"},{id:"156018",title:"MSc.",name:"Krajana",middleName:null,surname:"Tainchum",fullName:"Krajana Tainchum",slug:"krajana-tainchum"},{id:"156019",title:"Dr.",name:"Waraporn",middleName:null,surname:"Juntarajumnong",fullName:"Waraporn Juntarajumnong",slug:"waraporn-juntarajumnong"}]},{id:"43899",title:"Distribution, Mechanisms, Impact and Management of Insecticide Resistance in Malaria Vectors: A Pragmatic Review",slug:"distribution-mechanisms-impact-and-management-of-insecticide-resistance-in-malaria-vectors-a-pragmat",signatures:"Vincent Corbel and Raphael N’Guessan",authors:[{id:"152666",title:"Dr.",name:"Vincent",middleName:null,surname:"Corbel",fullName:"Vincent Corbel",slug:"vincent-corbel"},{id:"169017",title:"Dr.",name:"Raphael",middleName:null,surname:"N'Guessan",fullName:"Raphael N'Guessan",slug:"raphael-n'guessan"}]},{id:"43851",title:"Perspectives on Barriers to Control of Anopheles Mosquitoes and Malaria",slug:"perspectives-on-barriers-to-control-of-anopheles-mosquitoes-and-malaria",signatures:"Donald R. Roberts, Richard Tren and Kimberly Hess",authors:[{id:"151439",title:"Prof.",name:"Donald",middleName:null,surname:"R. Roberts",fullName:"Donald R. Roberts",slug:"donald-r.-roberts"},{id:"151656",title:"Mr.",name:"Richard",middleName:null,surname:"Tren",fullName:"Richard Tren",slug:"richard-tren"},{id:"154152",title:"Ms.",name:"Kimberly",middleName:null,surname:"Hess",fullName:"Kimberly Hess",slug:"kimberly-hess"}]},{id:"43874",title:"Residual Transmission of Malaria: An Old Issue for New Approaches",slug:"residual-transmission-of-malaria-an-old-issue-for-new-approaches",signatures:"Lies Durnez and Marc Coosemans",authors:[{id:"152754",title:"Prof.",name:"Marc",middleName:null,surname:"Coosemans",fullName:"Marc Coosemans",slug:"marc-coosemans"},{id:"169018",title:"Dr.",name:"Lies",middleName:null,surname:"Durnez",fullName:"Lies Durnez",slug:"lies-durnez"}]},{id:"44330",title:"Vector Control: Some New Paradigms and Approaches",slug:"vector-control-some-new-paradigms-and-approaches",signatures:"Claire Duchet, Richard Allan and Pierre Carnevale",authors:[{id:"151662",title:"Dr.",name:"Pierre",middleName:null,surname:"Carnevale",fullName:"Pierre Carnevale",slug:"pierre-carnevale"},{id:"169000",title:"Dr.",name:"Richard",middleName:null,surname:"Allan",fullName:"Richard Allan",slug:"richard-allan"},{id:"169008",title:"Dr.",name:"Claire",middleName:null,surname:"Duchet",fullName:"Claire Duchet",slug:"claire-duchet"}]},{id:"43870",title:"New Salivary Biomarkers of Human Exposure to Malaria Vector Bites",slug:"new-salivary-biomarkers-of-human-exposure-to-malaria-vector-bites",signatures:"Papa M. Drame, Anne Poinsignon, Alexandra Marie, Herbert\nNoukpo, Souleymane Doucoure, Sylvie Cornelie and Franck\nRemoue",authors:[{id:"151515",title:"Dr.",name:"Papa Makhtar",middleName:null,surname:"Drame",fullName:"Papa Makhtar Drame",slug:"papa-makhtar-drame"},{id:"151648",title:"Dr.",name:"Franck",middleName:null,surname:"Remoué",fullName:"Franck Remoué",slug:"franck-remoue"},{id:"154034",title:"Dr.",name:"Anne",middleName:null,surname:"Poinsignon",fullName:"Anne Poinsignon",slug:"anne-poinsignon"},{id:"154035",title:"MSc.",name:"Alexandra",middleName:null,surname:"Marie",fullName:"Alexandra Marie",slug:"alexandra-marie"},{id:"154037",title:"Dr.",name:"Souleymane",middleName:null,surname:"Doucoure",fullName:"Souleymane Doucoure",slug:"souleymane-doucoure"},{id:"154038",title:"MSc.",name:"Herbert",middleName:null,surname:"Noukpo",fullName:"Herbert Noukpo",slug:"herbert-noukpo"},{id:"154039",title:"Dr.",name:"Sylvie",middleName:null,surname:"Cornélie",fullName:"Sylvie Cornélie",slug:"sylvie-cornelie"}]},{id:"44149",title:"Transgenic Mosquitoes for Malaria Control: From the Bench to the Public Opinion Survey",slug:"transgenic-mosquitoes-for-malaria-control-from-the-bench-to-the-public-opinion-survey",signatures:"Christophe Boëte and Uli Beisel",authors:[{id:"98400",title:"Dr.",name:"Christophe",middleName:null,surname:"Boëte",fullName:"Christophe Boëte",slug:"christophe-boete"},{id:"167749",title:"Dr.",name:"Uli",middleName:null,surname:"Beisel",fullName:"Uli Beisel",slug:"uli-beisel"}]}]}],publishedBooks:[{type:"book",id:"9114",title:"Vector-Borne Diseases",subtitle:"Recent Developments in Epidemiology and Control",isOpenForSubmission:!1,hash:"97b62d395de991b4cd74bd3148aeb535",slug:"vector-borne-diseases-recent-developments-in-epidemiology-and-control",bookSignature:"David Claborn, Sujit Bhattacharya and Syamal Roy",coverURL:"https://cdn.intechopen.com/books/images_new/9114.jpg",editedByType:"Edited by",editors:[{id:"169536",title:"Dr.",name:"David",surname:"Claborn",slug:"david-claborn",fullName:"David Claborn"}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null,productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}},{type:"book",id:"971",title:"Malaria Parasites",subtitle:null,isOpenForSubmission:!1,hash:"d7a9d672f9988a6d5b059aed14188896",slug:"malaria-parasites",bookSignature:"Omolade O. Okwa",coverURL:"https://cdn.intechopen.com/books/images_new/971.jpg",editedByType:"Edited by",editors:[{id:"99780",title:"Prof.",name:"Omolade",surname:"Okwa",slug:"omolade-okwa",fullName:"Omolade Okwa"}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null,productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}},{type:"book",id:"9133",title:"Hospital Acquired Infection and Legionnaires' Disease",subtitle:null,isOpenForSubmission:!1,hash:"67e9b00ffb1203f7a41d2bb8507367c4",slug:"hospital-acquired-infection-and-legionnaires-disease",bookSignature:"Salim Surani",coverURL:"https://cdn.intechopen.com/books/images_new/9133.jpg",editedByType:"Edited by",editors:[{id:"15654",title:"Dr.",name:"Salim",surname:"Surani",slug:"salim-surani",fullName:"Salim Surani"}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null,productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}},{type:"book",id:"977",title:"Understanding Tuberculosis",subtitle:"Global Experiences and Innovative Approaches to the Diagnosis",isOpenForSubmission:!1,hash:"cb8288ea48f14bd22680c6ae5b13745b",slug:"understanding-tuberculosis-global-experiences-and-innovative-approaches-to-the-diagnosis",bookSignature:"Pere-Joan Cardona",coverURL:"https://cdn.intechopen.com/books/images_new/977.jpg",editedByType:"Edited by",editors:[{id:"78269",title:"Associate Prof.",name:"Pere-Joan",surname:"Cardona",slug:"pere-joan-cardona",fullName:"Pere-Joan Cardona"}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null,productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}},{type:"book",id:"990",title:"Human Respiratory Syncytial Virus Infection",subtitle:null,isOpenForSubmission:!1,hash:"b5d980a120eec6669c7f37a5082f0696",slug:"human-respiratory-syncytial-virus-infection",bookSignature:"Bernhard Resch",coverURL:"https://cdn.intechopen.com/books/images_new/990.jpg",editedByType:"Edited by",editors:[{id:"66173",title:"Prof.",name:"Bernhard",surname:"Resch",slug:"bernhard-resch",fullName:"Bernhard Resch"}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null,productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}}],publishedBooksByAuthor:[]},onlineFirst:{chapter:{type:"chapter",id:"75405",title:"Using of Genome Editing Methods in Plant Breeding",doi:"10.5772/intechopen.96431",slug:"using-of-genome-editing-methods-in-plant-breeding",body:'Currently the world population is about 8 billion people. According to the UN data, the number of people experience moderate or severe food shortages has reached 2 billion or 26.4% of the world population [1]. Huge efforts are being made to eradicate hunger and malnutrition in the world actually. Many of them are associated with scientific breakthrough in the life science and agriculture area [2]. However, despite the achievements of plant breeding, the issue of short term creation of new high-yielding and stress resistant varieties of crops is still actual. All of this is aimed to challenge the such problems as crop losses due to climatic changes, reducing of cultivated areas and spread of more aggressive and resistant pathogens. No less important reason is world population growth [2, 3]. At the moment, this is impossible without the use of biotechnological and genetic engineering approaches.
In the 20th century a classical crop breeding approaches were based on either natural mutations or artificially induced mutagenesis [4]. However, the traditional breeding methods have sufficient disadvantage such as long-term period to create of new varieties with desired agronomic characteristics of any crops. This depends not only on the duration of growing season and reaching of mature stage of plants (especially the long-period growth plants, e.g. trees), as well as is associated with applying of multiple stages of crossing, selection and testing in breeding process. In addition, the following should be mentioned, both natural mutations and conventional methods of chemical and physical mutagenesis do not permit to target the plant genome [4].
At the turn of XXIth century the development and introduction of molecular DNA markers allow to significantly reduce the time required to create new lines and varieties of agricultural crops. In other words, the marker assisted selection approaches were appeared, thus significantly increase the effectiveness of breeding programs to increment in productivity of crops in a wide range of environmental conditions [5, 6]. However, these approaches also do not enable to target the crop genome.
At the same time, advances of next-generation sequencing, multitude of sequenced genomes of major crops and newly identified genes and their functions motivate researchers to pursue targeted breeding of plants. All of this have significantly promoted the development of targeted genome editing (GE) approaches [7, 8, 9, 10]. One of the first GE technologies was RNA interference (RNAi) [4, 11, 12]. Despite the successful application of this technology in functional genomics and plant breeding [15, 16, 17], this method has a number of disadvantages, such as partial gene function suppression and indefinite insertion place of an RNAi construction into the genome [4].
The solution to these breeding problems was the application of GE methods using sequence-specific nucleases (SSN) to introduce targeted mutations in crops with high efficiency and accuracy [7, 8, 9, 10, 12]. Artificially engineered SSNs such as zinc finger nucleases (ZFNs), transcription activator-like effector nucleases (TALENs), and clustered regulatory interspaced short palindromic repeats (CRISPR) associated with the endonuclease Cas (CRISPR/Cas) have been shown to be highly effective in targeting mutagenesis in a wide range of model plants and crops [7, 8, 9, 10, 12]. In addition, oligonucleotide directed mutagenesis (ODM) allows to edit the genome at the single nucleotide level. Moreover, base editors (BEs) have recently been developed to replace A-T base pairs to G-C base pairs [12, 13].
Nowadays GE technologies are widely applied both in functional genomics and in the development of new varieties of crops with new valuable properties and resistant to various biotic and abiotic stresses [7, 8, 9, 10, 12, 13]. Herewith, despite the fact that modern GE technologies are much more accurate than conventional mutagenesis, the legistation of GE crops remains the main bottleneck [13, 14]. A particular difficulty is associated with the biosafety assessment of such crops, the impossibility of determining the subsequent effect of single base mutations after using ODM and BEs [13, 14].
This review discusses GE mechanisms and their use for crop improvement, as well as the problems associated with these approaches.
Currently, there are three main GE methods classified according to the mechanism of action. The most commonly one applied for plant genomics is the targeted generation of double-stranded DNA breaks (DSBs) by SSNs [12, 13]. Whereat this DSBs are recovered by the cell\'s own endogenous repair mechanisms either through non-homologous end joining (NHEJ) or homologous recombination (HDR) [7, 8, 9, 10, 12, 13, 14, 15, 16]. Thereat, the reparation of the target DNA sequence leads to the genesis of single base mutations that changing or shifting of the reading frame and initiating of indels or nucleotide substitutions, as well chromosomal rearrangements [8, 15].
Targeted induction of DSB is possible by programmable nucleases. The prevailing nucleases for GE are zinc finger nucleases (ZFNs), transcription activator-like effector nucleases (TALEN), and clustered regularly interspaced short palindromic repeats (CRISPR) associated with the endonuclease Cas (CRISPR/Cas). These three classes of nucleases are different in structure, activity and action mechanism, that leads to differences in target selection, efficiency, specificity and nature of mutation [7, 8, 9, 10]. Let’s take a closer examine each programmable nucleases types.
Zinc finger nucleases (ZFNs) are the first artificial endonucleases designed for GE [17]. Every ZFN is derived by aggregating of DNA-binding domain containing of a few linked zinc finger (ZF) motifs and the nonspecific endonuclease FokI [12, 17]. Association of ZF motifs promotes to develop ZF proteins (ZFP) consisting of approximately 30 amino acids and having ββα structure stabilized by zinc ions chelation [17]. Combination of ZFP with methylase, FokI and transcription activator/repressor gives rise ZFN [12, 13, 17]. FokI is an endonucleases recognizing of 5-mer non-palindromic sequence 5\'-GGATG-3\' : 5\'-CATCC-3\' and cleaving DNA 9/13 nucleotides downstream of the recognition site [12, 17, 18].
By intersecting with DNA, each ZF motif is capable to bind one triplet of nucleotides inserting an α-helix into the major groove of the DNA double helix [12, 18]. It should be also noted that one ZF has not sufficient specificity for binding to the target genome. However, artificial ZFN usualy contains three or four ZFs, which permit to bind 18-24-mer site after FokI dimerization which is necessary for efficient DNA restriction [17]. During FokI dimerization, two ZFNs can bind both forward and reverse DNA strands respectively, and two target sequences - forward and reverse should be separated by a spacer sequence of 5 to 7 bp [7]. In this case, ZFN acts like dimer and generates DSBs with short 5\'-cohesive overhangs, which are filled by homologous recombination, that gives rise to indels into the genome [7, 8, 9, 10, 12, 17, 18].
It should also be noted that, despite the sufficient binding specificity of ZFNs, they are more likely to make nucleotide mismatch [17]. Heterodimerization of FokI nuclease is used to minimize non-target effects and, accordingly, cellular toxicity of ZFN [19].
According to the first report in 1996, ZFNs have been successfully applied for gene modification in plants [17, 18]. The ZFN technology was used to edit the genome of tobacco and
However, despite the rather successful use of ZFNs, they have not become widespread as a GE tool due to the presence of a number of disadvantages. Main of them is complexity and high cost intensive technology, constructing of protein domains for each specific locus of the genome [18], likelihood of inaccurate cleavage of the target DNA due to single nucleotide substitutions or incorrect interaction between domains [8, 15, 17, 18, 19].
TALENs similar to ZFN are enzymes consisting of specific DNA-binding domains of highly conservative repeats originating from effectors such as transcription activators (TALEs) which associate with FokI [20]. TALEs domains contain 15–30 copies of 33–34 highly conserved amino acid sequences [20]. The exceptions are 12th and 13th amino acid residues, which have high variability (repeat-variable diresidues – RVD) [17, 20]. It permits to establish the recognition code for specific nucleotides using a pair of such amino acids within the repeating peptide chains of a given protein [20]. This code is degenerate, but there is a clearly pronounced preference for some combinations of amino acids [17, 20]. It permit to design recombinant proteins capable of recognizing specific DNA sequences [20]. Activity of TALEN depends on amino acid number between TALE domain and FokI, as well as base number between binding sites [17, 20].
In contrast to ZF each repeat in the TALE domain recognizes one nucleotide [17, 20]. The TALE domains recognize 15-30 nucleotides that is 30-60 nucleotides for each TALEN dimer after FokI dimerization. Moreover, despite the fact that TAL domains have higher binding specificity, they are more likely to allow nucleotide mismatches [12, 13, 17]. As well as ZFN the heterodimerization of FokI is applied to minimize off-target effects by using of TALEN [21].
Analysis of mutations occurred during GE using TALEN shows that deletions are way more than insertions (89% versus 1.6%). The reason is the longer length of the TALEN spacers, which provide more extended protruding ends for the DNA fragments after DSBs [22].
Theoretically, the use of TALEN permit to introduce DSB into any part of the genome. There is one limitation only – the presence of thymidine upstream of the 5\' end of the target sequence is needed for the TALEN nuclease recognition sites. However, variation of the spacer length allows to select restriction sites [20].
CRISPR/Cas technology permits to make different changes in the DNA sequence [12, 13, 14, 15, 16]. Moreover, this GE technology is much cheaper, faster, more efficient and simple in practical application in comparing to ZFN or TALEN [17, 23]. This technology is based on the use of mechanisms of adaptive “immunity” discovered in bacteria – a specific antiviral defense of bacterial cells based on the complementary binding of viral DNA and their follow destruction [7, 8, 9, 10, 12, 13, 14].
In this system small guide RNAs (crRNA) are used for sequence-specific interference of foreign nucleic acids. CRISPR/Cas includes a genetic locus so-called CRISPR containing short repeats separated by unique sequences (spacers) [24, 25, 26, 27, 28, 29]. The CRISPR complex is predated by the AT-enriched leader sequence and flanked by
Depending on the
Currently, CRISPR/Cas type II is most often used for genome editing. This type contains the protein Cas9, which is necessary for interference and bacterial immunity [26]. Let’s a closer look at this genome editing system.
To edit target genes, the CRISPR/Cas9-based GE requires the occurrence of CRISPR-associated protein 9 (Cas9), CRISPR RNA (crRNA), transactivating crRNA (tracrRNA) and ribonuclease III (RNase III) [12, 13, 14]. Thereat the crRNA and tracrRNA coassemble into a single guide RNA (sgRNA) [28].
Cas9 is the endonuclease cleaving a double-stranded DNA (dsDNA) [24, 25, 26, 27]. This nuclease were isolated from various bacteria, such as
Cas9 contains two domains: His-Asn-His (HNH) and RucV-like domains cleaving dsDNA at 3 bp upstream of the motif adjacent to protospacer (PAM) (5′ NGG or 5′-NAG for SpCas9) [24, 25, 29]. The HNH domain cleaves the complementary crRNA strand, while the RucV-like domain - the opposite strand of dsDNA [47]. Then generated DSBs are repaired by NHEJ or HDR [24, 25, 26, 27, 28, 29].
sgRNA is 100-mer synthetic RNA and consists crRNA and tracrRNA. The 5\'-end of sgRNA contains a 20 nucleotide guide sequence to identify the target sequence followed by consensus PAM sequence [27]. 3\'-end of sgRNA has loop structure which permit to fix the guide sequence to the target site and interact with Cas9 forming ribonucleoprotein complex (RNP) which generates DSB at the target DNA region [27, 29].
Efficient DNA cleavage are provided by ribonucleoprotein complex (RNP) [29]. crRNA plays an important role in the recognition of target DNA due to the sequence that directs RNP to a specific locus by base pairing with target DNA with formation of R-loop structure [29]. R-loop generation activates the HNH and RuvC-like endonuclease domains of Cas9, which cleave dsDNA, creating blunt-ended DSB at 3 bp upstream of the PAM site [25]. Thus, CRISPR/Cas9 performs gene editing in three stages. At the first stage Cas9 is expressed, at the second stage – generation of sgRNA which containing 20 nucleotides complementary to the target region. The third stage requires an NGG PAM recognition site located closer to the 3\' end of the target region. The RNP guided by sgRNA generates a blunt-ended DSB at 3 bp upstream of the PAM site [25].
The one limitation of the CRISPR/Cas9 using is the fact that sgRNA design requires the presence of the targeted PAM sequence at the 3\' end [24, 25, 26]. For SpCas9 this sequence is defined as 5\'-NGG-3\' [25]. Frequency of PAM sites in the plant genomes revealed by
ODM is site-directed mutagenesis tool using mutagenic DNA fragments 20-200 nucleotides in length [33]. In this approach, the fragment sequence match with a target sequence in the genome, except of a single base pair, which is a putative mutation introduced into the genome [33, 34].
In eukaryotic cells the oligonucleotide for ODM penetrates into the cytoplasm through the cell membrane, then enters the nucleus and complementarily interacts with the target DNA sequence. Herewith, the mismatched nucleotides contribute to initiate a specific change of the sequence that occur in the target gene due to the errors reparation mechanism in the cell. This is two-stage process initially requires annealing of the specific oligonucleotides with target DNA, and subsequently repair of nucleotide mismatch leading to a directed mutation [33]. This system was first demonstrated on mammalian, after that in plants [35]. However, it should be noted that in plants the oligonucleotide does not integrate into the genome because of modifications of the 5\' and 3\' ends, that prevent DNA ligation, and due to the activity of endonucleases that destroy oligonucleotides [34].
ODM can be accomplished by single-stranded DNA fragments, but their using is limited by a short intracellular half-life [13]. To overcome this disadvantage, the stabilizing modifications for ssODN are necessary. These include chimeraplasts (DNA/RNA duplexes modified by methylation), modification with phosphorothioate, ssODNs with a 5\'-tag Cy3 and modified 3\'idC reverse base [33]. Additionally, it should be noted the rather low efficiency of ODM, that positive correlate with the length of oligonucleotide fragments. It was shown that by increasing of ssODN length to 200 nucleotides it allows to increase accuracy of editing up to 0.05% in
All programmable nucleases generate DSBs that are repaired by either NHEJ or HDR [7, 8, 9, 10]. The common disadvantage of these nucleases is the non-predictable results of DSB repairing due to NHEJ mechanism and the low efficacy of HDR [13]. In this reason it became necessary to develop new methods for the introduction of point mutations excluding of DSBs, which resulted in GE new tools so-called base editors (BE) [38].
BE technologies use nickase Cas9 (nCas9) or functionally inactive Cas9 (dCas9) combined with a cytosine or adenosine deaminase domain, which bring into action transformation bases [39]. For example, cytosine deaminases transform cytosine (C) to uracil (U), which is identified as thymine (T) during following DNA repair and replication, thus providing a C:G to T:A replacement [38, 39]. In the same way, adenine deaminases convert adenine (A) to inosine (I), which polymerases interpreting as guanine (G), creating A:T for G:C replacement [39]. Cytidine deaminase-based BE (CBE) has been used to edit genomes in rice,
In the lack of known adenine deaminases, the substitution of A:T to G:C is a more difficult task than on the contrary [39]. This problem has been solved by bio-engineering of tRNA adenosine deaminases for their adaptation to DNA as a substrate [39, 40, 41].
Initially developed BE had an editor window of for several base pairs only, that led to the appearance of unexpected random mutations. But further improvement of these methods allows to create high-precision Cas9-based BEs that control the length and flexibility of the linker and thus able to selectively edit the bases in direct position with high accuracy, efficiency and simplified PAM requirements [39, 40, 41].
NHEJ- or HDR-mediated repair of DSBs generated by programmed nucleases leads to the appearance of insertions /deletions, which shift the reading frame [7, 8, 9, 10], while the single base changes by ODM [33] or BE [39] promotes targeted replacement of nucleotides. These events lead to changes in the genes activity due to the effects of gene-knockout or gene-knockin, that can be used to reveal their function [17, 29, 34, 42, 43].
Besides gene-knockout and gene-knockin, GE technologies can also be used to regulate gene expression. In this case, genes repression and activation achieved by combining repressors or activators of transcription with the DNA-binding domains of programmed nucleases is most often used [7].
Unlike technologies targeted introducing changes in the DNA nucleotide sequence, gene regulation by GE methods is carried out at the level of transcripts. It allows to reveal the functions of many non-canonical non-coding transcripts without open reading frames [16].
Moreover, the CRISPR/Cas using makes it possible to simultaneously introduce into cells several genetic constructs targeted different regions of the genome [15, 16]. It allows to have an effect on the work of several genes simultaneously and to study intergenic interactions. In this wise, it is possible, for example, to determine the genes involved in the process of crop domestication [29].
In addition, the CRISPR/dCas9 system combined with epigenetic regulatory factors involved in histone acetylation or DNA methylation, can be efficiently used to modulate chromatin activity and gene expression patterns involved in plant development and adaptation to the environment [29].
Nowadays, GE technologies are effectively used to create new varieties of agricultural crops with improved traits, such as increased yield, product quality and resistance to biotic and abiotic stresses. Such traits improvement is often carried out by introducing target mutations into the corresponding regulatory genes that control the development of undesirable traits leading to the suppression of their activity [7, 8, 9, 10].
In this section, we review key advances in crop trait enhancement using GE techniques and discuss their prospects for improving food security.
Productivity is one of the most important economically valuable traits of agricultural crops. At the same time, this trait is also one of the most difficult to improve by conventional breeding methods [44]. It’s explained by the fact that yield is often a quantitative multigenic trait, the development of which is controlled by multiple quantitative trait loci (QTL) [45]. Additionally, traditional yield-based selection is complicated by QTL introgression between different varieties, which is especially pronounced in the case of closely linked loci [44, 45].
In this regard, GE technologies represent a promising tool for the rapid and directed mutagenesis of target genes [7, 8, 9, 10, 13]. Herewith, the most effective way to increase yields using genome editing technologies is to knock out (“turn off”) genes negatively affecting the yield [44]. For example, CRISPR/Cas9-based “turn off” of the functions of yield negative regulators (
Additionally, there is evidence that CRISPR/Cas9-based multiplex knockout of the main negative regulators of rice grain weight (
Also, it was shown that the CRISPR/Cas9-xyr5APOBEC1-mediated single base mutations in two rice genes,
Products quality is another economically valuable trait, the selection of which by traditional methods is accompanied by significant difficulties. Thereat, selection for this trait is complicated both by the difficulty in obtaining targeted mutations by the methods of chemical and physical mutagenesis, and the presence of negative correlations between the traits of quality and yield [11]. GE technologies allow to cope with the deficiencies of chemical and physical mutagenesis due to the ability to introduce targeted mutations into the genome and improve the nutritional properties of crops [7, 8, 9, 10, 44].
Let us consider some examples of the potential application of GE methods for modifying the chemical composition of plants. For example, silencing one of the key genes of phytate biosynthesis
Also, TALEN-based “turn off” of
CRISPR/Cas9-based targeting of conserved regions in the α-gliadin genes has allowed to create wheat lines with reduced gluten immunoreactivity [44]. At the same time, CRISPR/Cas9-mediated multiplex mutagenesis of
In addition, it was reported that CRISPR/Cas9-mediated knockout of genes responsible for amylose biosynthesis:
Herbicides are the class of chemical compounds most widely used in agricultural practice. This is due to the fact that weeds cause significant damage to agriculture, reducing yields from competition with crops for resources [47]. However, despite the success of the herbicide using, their main disadvantage is their non-selective effect. To overcome this disadvantage, herbicide-resistant biotechnological varieties were created using genetic engineering methods. Currently all herbicide-resistant varieties approved for use have been obtained by transgenesis [11]. At the same time, GE methods are an effective tool for creating herbicide-resistant crop lines [7, 8, 9, 10].
The main genes targeted by the GE in creating herbicide-resistant lines are the
Along with this, CRISPR/Cas9-mediated point replacement of two nucleotides in the
Biotic stresses are one of the basic factor of crop losses in agriculture [47]. The main biotic stresses affecting crops include phytopathogens (viruses, bacteria, fungi), insect and pests (phytophagous insects, acari or nematodes). The strategy for dealing with biotic stresses is either in increasing of self defense mechanisms in plants or in introducing into the genome of constructs aimed against the pathogens [47, 48].
The producing of crops lines resistant to pathogens and pests using traditional breeding methods is based on increasing the own defense mechanisms in plants, but the introduction of constructs targeted pathogens into the genome is carried out by genetic engineering. The most of biotechnological crop lines resistant to biotic stresses created to date are obtained by transgenesis or RNA interference (RNAi) methods [47].
Nowadays, GE approaches are widely used to create new resistant lines [7, 8, 9, 10, 44]. Herewith, it should be mentioned these methods makes possible to use both strategies to deal with biotic stresses [44, 47, 48]. Let us to consider some examples of the use several GE technologies to develop lines and varieties of crops resistant to biotic stresses.
Targeting of disease susceptibility factors was also used for creation of virus-resistant crops. As CRISPR/Cas9-based silencing of
To creation of crop lines resistant to biotic stress GE approaches are also used to impact on regulatory elements that can affect the process of pathogen proliferation [49]. So as, TALEN- and CRISPR/Cas9-mediated mutagenesis in effector binding site of promoter region of
Abiotic stresses are the main factors that negatively affect the yield of most crops [52]. In this regard, a creation of resistant to adverse environmental factors crop varieties is the urgent problem. However, the use of traditional breeding methods to develop such varieties is limited by the fact that the traits of resistance to abiotic stress are multigene controlled and have a complex inheritance type [52, 53]. The disadvantages of traditional breeding can be successfully overcome through the use of GE approaches. Herewith, a literature analysis has shown that the GE application in various cultures allowed to increase their resistance to abiotic stresses [7, 44, 53, 54]. Let us consider detailed examples of the GE application to obtain varieties of crops resistant to abiotic stresses.
Summarize the presented data, it should be noted that GE systems are successfully used to modify a wide range of economically valuable traits in main agricultural crops.
One of the main limitation of GE systems is off-target effects, when nucleases, along with target regions, affect other parts of the genome [7, 8, 9, 10, 39, 44]. It stems from the fact that the efficiency of DNA cleavage by nucleases depends both on nuclease activity and the availability of the target site and also the affinity of the DNA-binding domain. Moreover, the designed nucleases specificity largely depends on the binding affinity of the nuclease to DNA. In addition, FokI domain dimerization and interaction of Cas9 with PAM may also play an important role [17, 55, 56].
The preliminary comprehensive bioinformatics analysis to choose of specific sites for the introducing of DBS can minimize the off-target effects of the GE system. When choosing the desired sites, it should avoid regions with repeated sequences, as well as regions with high homology to other regions of the genome [17, 55, 56]. In addition, to minimize off-target effects and cellular toxicity of ZFN and TALEN heterodimerization of FokI nuclease is used [19, 21]. Another effective way to reduce the frequency of unintentional mutations is the use of the sgRNA/aptazyme system (ligand-dependent ribozyme) [56].
The legal and regulatory framework in regard to GE plants in different countries has a great impact on their competitiveness. In most countries, the current biosafety framework is meant to regulate transgenic GMOs. Currently, only Argentina and Brazil have adopted additional legislation for crops obtained using GE techniques [57].
There are two main approaches to defining the regulatory framework for GMOs in global legislation: one is process-based and the other is product-based. In the European Union, a standard is focused on the first approach, while in Canada – on the second. In the United States, a hybrid system is used: the decision on whether a crop belongs to GMOs is based on the first approach, and the risk assessment – on the second. In this case, GE cultures are considered individually [13]. Thus, the same GE culture can be classified in different ways depending on the regulatory framework. For example, in Argentina, crops that are classified as "zero segregants" are not regulated as GMOs [57]. In the EU, GE crops are subject to Directive 2001/18/EC and must undergo a full biosafety assessment procedure, as well as meet the requirements for GMO products [13, 57].
GE tools are considered one of the most promising tools for practical agricultural biotechnology because of their high efficiency, relatively low cost, ease to use and multiplexing ability [7, 8, 9, 10, 14]. Herewith, directed mutagenesis makes it possible to effectively “turn off” or silencing various genes, that helps to determine the functions of genes [17, 29, 34, 42, 43]. Multiplex targeting allow to reveal the role of individual genes and encoded proteins in intracellular signaling pathways and contributes to the engineering of multigenic agronomic traits in crops [7, 8, 9, 10, 44].
Furthermore, CRISPR/Cas9 system may be used for spatial and temporal control of gene expression, as well as tissue-specific regulation of expression [42]. In the furtherance of this goal, influence on the
Epigenomic studies are another promising uses of GE technologies. Herewith, the insertion of transposons into the promoter region due to the NHEJ or HDR mechanisms can affect the epigenetic status and, accordingly, the level of expression of commercially valuable genes [58]. It can be achieved through the using of such dCas9 systems as targeted DNA methylation and demethylation systems [58].
It should also be noted that an advanced uses of GE methods, in particular, CBE and ABE, is the introduction of single base changes into the microRNA (miRNA) binding site of the target gene without alteration of the amino acid sequence of the encoded protein. It will lead to disruption of miRNA/mRNA base pairing and, consequently, to disruption of mRNA cleavage due to the fact that the position and number of mismatches in the miRNA binding site strongly affect the efficiency of miRNA-mediated mRNA cleavage [58]. In turn, such disturbance of miRNA-mediated mRNA cleavage can be used to proper alignment of the target genes expression and, accordingly, can have effect on the development of many agronomical desired trait [58]. In addition, CRISPR/Cas system can be used for NHEJ- or HDR-mediated introduction of translation enhancers into the initiation codon of open reading frames, which provide fine tuning of gene expression at the translation level [58].
Thus, in summary it should be noted that GE systems, especially CRISPR/Cas and BEs, offer great opportunities for crop improvement.
In conclusion, it can be noted that GE technology has enormous potential to create new varieties of crops resistant to biotic and abiotic stresses and improved food value and yield. However, for the effective using of these technologies, it is necessary to resolve issues related to the biosafety assessment, including the revision of regulatory frameworks.
The authors declare no conflict of interest.
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His research interest focuses on computational chemistry and molecular modeling of diverse systems of pharmacological, food, and alternative energy interests by resorting to DFT and Conceptual DFT. He has authored a coauthored more than 255 peer-reviewed papers, 32 book chapters, and 2 edited books. He has delivered speeches at many international and domestic conferences. He serves as a reviewer for more than eighty international journals, books, and research proposals as well as an editor for special issues of renowned scientific journals.",institutionString:"Centro de Investigación en Materiales Avanzados",institution:{name:"Centro de Investigación en Materiales Avanzados",country:{name:"Mexico"}}},{id:"76477",title:"Prof.",name:"Mirza",middleName:null,surname:"Hasanuzzaman",slug:"mirza-hasanuzzaman",fullName:"Mirza Hasanuzzaman",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/76477/images/system/76477.png",biography:"Dr. Mirza Hasanuzzaman is a Professor of Agronomy at Sher-e-Bangla Agricultural University, Bangladesh. He received his Ph.D. in Plant Stress Physiology and Antioxidant Metabolism from Ehime University, Japan, with a scholarship from the Japanese Government (MEXT). Later, he completed his postdoctoral research at the Center of Molecular Biosciences, University of the Ryukyus, Japan, as a recipient of the Japan Society for the Promotion of Science (JSPS) postdoctoral fellowship. He was also the recipient of the Australian Government Endeavour Research Fellowship for postdoctoral research as an adjunct senior researcher at the University of Tasmania, Australia. Dr. Hasanuzzaman’s current work is focused on the physiological and molecular mechanisms of environmental stress tolerance. Dr. Hasanuzzaman has published more than 150 articles in peer-reviewed journals. He has edited ten books and written more than forty book chapters on important aspects of plant physiology, plant stress tolerance, and crop production. According to Scopus, Dr. Hasanuzzaman’s publications have received more than 10,500 citations with an h-index of 53. He has been named a Highly Cited Researcher by Clarivate. He is an editor and reviewer for more than fifty peer-reviewed international journals and was a recipient of the “Publons Peer Review Award” in 2017, 2018, and 2019. He has been honored by different authorities for his outstanding performance in various fields like research and education, and he has received the World Academy of Science Young Scientist Award (2014) and the University Grants Commission (UGC) Award 2018. He is a fellow of the Bangladesh Academy of Sciences (BAS) and the Royal Society of Biology.",institutionString:"Sher-e-Bangla Agricultural University",institution:{name:"Sher-e-Bangla Agricultural University",country:{name:"Bangladesh"}}},{id:"187859",title:"Prof.",name:"Kusal",middleName:"K.",surname:"Das",slug:"kusal-das",fullName:"Kusal Das",position:null,profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bSBDeQAO/Profile_Picture_1623411145568",biography:"Kusal K. Das is a Distinguished Chair Professor of Physiology, Shri B. M. Patil Medical College and Director, Centre for Advanced Medical Research (CAMR), BLDE (Deemed to be University), Vijayapur, Karnataka, India. Dr. Das did his M.S. and Ph.D. in Human Physiology from the University of Calcutta, Kolkata. His area of research is focused on understanding of molecular mechanisms of heavy metal activated low oxygen sensing pathways in vascular pathophysiology. He has invented a new method of estimation of serum vitamin E. His expertise in critical experimental protocols on vascular functions in experimental animals was well documented by his quality of publications. He was a Visiting Professor of Medicine at University of Leeds, United Kingdom (2014-2016) and Tulane University, New Orleans, USA (2017). For his immense contribution in medical research Ministry of Science and Technology, Government of India conferred him 'G.P. Chatterjee Memorial Research Prize-2019” and he is also the recipient of 'Dr.Raja Ramanna State Scientist Award 2015” by Government of Karnataka. He is a Fellow of the Royal Society of Biology (FRSB), London and Honorary Fellow of Karnataka Science and Technology Academy, Department of Science and Technology, Government of Karnataka.",institutionString:"BLDE (Deemed to be University), India",institution:null},{id:"243660",title:"Dr.",name:"Mallanagouda Shivanagouda",middleName:null,surname:"Biradar",slug:"mallanagouda-shivanagouda-biradar",fullName:"Mallanagouda Shivanagouda Biradar",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/243660/images/system/243660.jpeg",biography:"M. S. Biradar is Vice Chancellor and Professor of Medicine of\nBLDE (Deemed to be University), Vijayapura, Karnataka, India.\nHe obtained his MD with a gold medal in General Medicine and\nhas devoted himself to medical teaching, research, and administrations. He has also immensely contributed to medical research\non vascular medicine, which is reflected by his numerous publications including books and book chapters. Professor Biradar was\nalso Visiting Professor at Tulane University School of Medicine, New Orleans, USA.",institutionString:"BLDE (Deemed to be University)",institution:{name:"BLDE University",country:{name:"India"}}},{id:"289796",title:"Dr.",name:"Swastika",middleName:null,surname:"Das",slug:"swastika-das",fullName:"Swastika Das",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/289796/images/system/289796.jpeg",biography:"Swastika N. Das is Professor of Chemistry at the V. P. Dr. P. G.\nHalakatti College of Engineering and Technology, BLDE (Deemed\nto be University), Vijayapura, Karnataka, India. She obtained an\nMSc, MPhil, and PhD in Chemistry from Sambalpur University,\nOdisha, India. Her areas of research interest are medicinal chemistry, chemical kinetics, and free radical chemistry. She is a member\nof the investigators who invented a new modified method of estimation of serum vitamin E. She has authored numerous publications including book\nchapters and is a mentor of doctoral curriculum at her university.",institutionString:"BLDEA’s V.P.Dr.P.G.Halakatti College of Engineering & Technology",institution:{name:"BLDE University",country:{name:"India"}}},{id:"248459",title:"Dr.",name:"Akikazu",middleName:null,surname:"Takada",slug:"akikazu-takada",fullName:"Akikazu Takada",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/248459/images/system/248459.png",biography:"Akikazu Takada was born in Japan, 1935. After graduation from\nKeio University School of Medicine and finishing his post-graduate studies, he worked at Roswell Park Memorial Institute NY,\nUSA. He then took a professorship at Hamamatsu University\nSchool of Medicine. In thrombosis studies, he found the SK\npotentiator that enhances plasminogen activation by streptokinase. He is very much interested in simultaneous measurements\nof fatty acids, amino acids, and tryptophan degradation products. By using fatty\nacid analyses, he indicated that plasma levels of trans-fatty acids of old men were\nfar higher in the US than Japanese men. . He also showed that eicosapentaenoic acid\n(EPA) and docosahexaenoic acid (DHA) levels are higher, and arachidonic acid\nlevels are lower in Japanese than US people. By using simultaneous LC/MS analyses\nof plasma levels of tryptophan metabolites, he recently found that plasma levels of\nserotonin, kynurenine, or 5-HIAA were higher in patients of mono- and bipolar\ndepression, which are significantly different from observations reported before. In\nview of recent reports that plasma tryptophan metabolites are mainly produced by\nmicrobiota. He is now working on the relationships between microbiota and depression or autism.",institutionString:"Hamamatsu University School of Medicine",institution:{name:"Hamamatsu University School of Medicine",country:{name:"Japan"}}},{id:"137240",title:"Prof.",name:"Mohammed",middleName:null,surname:"Khalid",slug:"mohammed-khalid",fullName:"Mohammed Khalid",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/137240/images/system/137240.png",biography:"Mohammed Khalid received his B.S. degree in chemistry in 2000 and Ph.D. degree in physical chemistry in 2007 from the University of Khartoum, Sudan. He moved to School of Chemistry, Faculty of Science, University of Sydney, Australia in 2009 and joined Dr. Ron Clarke as a postdoctoral fellow where he worked on the interaction of ATP with the phosphoenzyme of the Na+/K+-ATPase and dual mechanisms of allosteric acceleration of the Na+/K+-ATPase by ATP; then he went back to Department of Chemistry, University of Khartoum as an assistant professor, and in 2014 he was promoted as an associate professor. In 2011, he joined the staff of Department of Chemistry at Taif University, Saudi Arabia, where he is currently an assistant professor. His research interests include the following: P-Type ATPase enzyme kinetics and mechanisms, kinetics and mechanisms of redox reactions, autocatalytic reactions, computational enzyme kinetics, allosteric acceleration of P-type ATPases by ATP, exploring of allosteric sites of ATPases, and interaction of ATP with ATPases located in cell membranes.",institutionString:"Taif University",institution:{name:"Taif University",country:{name:"Saudi Arabia"}}},{id:"63810",title:"Prof.",name:"Jorge",middleName:null,surname:"Morales-Montor",slug:"jorge-morales-montor",fullName:"Jorge Morales-Montor",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/63810/images/system/63810.png",biography:"Dr. Jorge Morales-Montor was recognized with the Lola and Igo Flisser PUIS Award for best graduate thesis at the national level in the field of parasitology. He received a fellowship from the Fogarty Foundation to perform postdoctoral research stay at the University of Georgia. He has 153 journal articles to his credit. He has also edited several books and published more than fifty-five book chapters. He is a member of the Mexican Academy of Sciences, Latin American Academy of Sciences, and the National Academy of Medicine. He has received more than thirty-five awards and has supervised numerous bachelor’s, master’s, and Ph.D. students. Dr. Morales-Montor is the past president of the Mexican Society of Parasitology.",institutionString:"National Autonomous University of Mexico",institution:{name:"National Autonomous University of Mexico",country:{name:"Mexico"}}},{id:"217215",title:"Dr.",name:"Palash",middleName:null,surname:"Mandal",slug:"palash-mandal",fullName:"Palash Mandal",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/217215/images/system/217215.jpeg",biography:null,institutionString:"Charusat University",institution:null},{id:"49739",title:"Dr.",name:"Leszek",middleName:null,surname:"Szablewski",slug:"leszek-szablewski",fullName:"Leszek Szablewski",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/49739/images/system/49739.jpg",biography:"Leszek Szablewski is a professor of medical sciences. He received his M.S. in the Faculty of Biology from the University of Warsaw and his PhD degree from the Institute of Experimental Biology Polish Academy of Sciences. He habilitated in the Medical University of Warsaw, and he obtained his degree of Professor from the President of Poland. Professor Szablewski is the Head of Chair and Department of General Biology and Parasitology, Medical University of Warsaw. Professor Szablewski has published over 80 peer-reviewed papers in journals such as Journal of Alzheimer’s Disease, Biochim. Biophys. Acta Reviews of Cancer, Biol. Chem., J. Biomed. Sci., and Diabetes/Metabol. Res. Rev, Endocrine. He is the author of two books and four book chapters. He has edited four books, written 15 scripts for students, is the ad hoc reviewer of over 30 peer-reviewed journals, and editorial member of peer-reviewed journals. Prof. Szablewski’s research focuses on cell physiology, genetics, and pathophysiology. He works on the damage caused by lack of glucose homeostasis and changes in the expression and/or function of glucose transporters due to various diseases. He has given lectures, seminars, and exercises for students at the Medical University.",institutionString:"Medical University of Warsaw",institution:{name:"Medical University of Warsaw",country:{name:"Poland"}}},{id:"173123",title:"Dr.",name:"Maitham",middleName:null,surname:"Khajah",slug:"maitham-khajah",fullName:"Maitham Khajah",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/173123/images/system/173123.jpeg",biography:"Dr. Maitham A. Khajah received his degree in Pharmacy from Faculty of Pharmacy, Kuwait University, in 2003 and obtained his PhD degree in December 2009 from the University of Calgary, Canada (Gastrointestinal Science and Immunology). Since January 2010 he has been assistant professor in Kuwait University, Faculty of Pharmacy, Department of Pharmacology and Therapeutics. His research interest are molecular targets for the treatment of inflammatory bowel disease (IBD) and the mechanisms responsible for immune cell chemotaxis. He cosupervised many students for the MSc Molecular Biology Program, College of Graduate Studies, Kuwait University. Ever since joining Kuwait University in 2010, he got various grants as PI and Co-I. He was awarded the Best Young Researcher Award by Kuwait University, Research Sector, for the Year 2013–2014. He was a member in the organizing committee for three conferences organized by Kuwait University, Faculty of Pharmacy, as cochair and a member in the scientific committee (the 3rd, 4th, and 5th Kuwait International Pharmacy Conference).",institutionString:"Kuwait University",institution:{name:"Kuwait University",country:{name:"Kuwait"}}},{id:"195136",title:"Dr.",name:"Aya",middleName:null,surname:"Adel",slug:"aya-adel",fullName:"Aya Adel",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/195136/images/system/195136.jpg",biography:"Dr. Adel works as an Assistant Lecturer in the unit of Phoniatrics, Department of Otolaryngology, Ain Shams University in Cairo, Egypt. Dr. Adel is especially interested in joint attention and its impairment in autism spectrum disorder",institutionString:"Ain Shams University",institution:{name:"Ain Shams University",country:{name:"Egypt"}}},{id:"94911",title:"Dr.",name:"Boulenouar",middleName:null,surname:"Mesraoua",slug:"boulenouar-mesraoua",fullName:"Boulenouar Mesraoua",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/94911/images/system/94911.png",biography:"Dr Boulenouar Mesraoua is the Associate Professor of Clinical Neurology at Weill Cornell Medical College-Qatar and a Consultant Neurologist at Hamad Medical Corporation at the Neuroscience Department; He graduated as a Medical Doctor from the University of Oran, Algeria; he then moved to Belgium, the City of Liege, for a Residency in Internal Medicine and Neurology at Liege University; after getting the Belgian Board of Neurology (with high marks), he went to the National Hospital for Nervous Diseases, Queen Square, London, United Kingdom for a fellowship in Clinical Neurophysiology, under Pr Willison ; Dr Mesraoua had also further training in Epilepsy and Continuous EEG Monitoring for two years (from 2001-2003) in the Neurophysiology department of Zurich University, Switzerland, under late Pr Hans Gregor Wieser ,an internationally known epileptologist expert. \n\nDr B. Mesraoua is the Director of the Neurology Fellowship Program at the Neurology Section and an active member of the newly created Comprehensive Epilepsy Program at Hamad General Hospital, Doha, Qatar; he is also Assistant Director of the Residency Program at the Qatar Medical School. \nDr B. Mesraoua's main interests are Epilepsy, Multiple Sclerosis, and Clinical Neurology; He is the Chairman and the Organizer of the well known Qatar Epilepsy Symposium, he is running yearly for the past 14 years and which is considered a landmark in the Gulf region; He has also started last year , together with other epileptologists from Qatar, the region and elsewhere, a yearly International Epilepsy School Course, which was attended by many neurologists from the Area.\n\nInternationally, Dr Mesraoua is an active and elected member of the Commission on Eastern Mediterranean Region (EMR ) , a regional branch of the International League Against Epilepsy (ILAE), where he represents the Middle East and North Africa(MENA ) and where he holds the position of chief of the Epilepsy Epidemiology Section; Dr Mesraoua is a member of the American Academy of Neurology, the Europeen Academy of Neurology and the American Epilepsy Society.\n\nDr Mesraoua's main objectives are to encourage frequent gathering of the epileptologists/neurologists from the MENA region and the rest of the world, promote Epilepsy Teaching in the MENA Region, and encourage multicenter studies involving neurologists and epileptologists in the MENA region, particularly epilepsy epidemiological studies. \n\nDr. Mesraoua is the recipient of two research Grants, as the Lead Principal Investigator (750.000 USD and 250.000 USD) from the Qatar National Research Fund (QNRF) and the Hamad Hospital Internal Research Grant (IRGC), on the following topics : “Continuous EEG Monitoring in the ICU “ and on “Alpha-lactoalbumin , proof of concept in the treatment of epilepsy” .Dr Mesraoua is a reviewer for the journal \"seizures\" (Europeen Epilepsy Journal ) as well as dove journals ; Dr Mesraoua is the author and co-author of many peer reviewed publications and four book chapters in the field of Epilepsy and Clinical Neurology",institutionString:"Weill Cornell Medical College in Qatar",institution:{name:"Weill Cornell Medical College in Qatar",country:{name:"Qatar"}}},{id:"282429",title:"Prof.",name:"Covanis",middleName:null,surname:"Athanasios",slug:"covanis-athanasios",fullName:"Covanis Athanasios",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/282429/images/system/282429.jpg",biography:null,institutionString:"Neurology-Neurophysiology Department of the Children Hospital Agia Sophia",institution:null},{id:"190980",title:"Prof.",name:"Marwa",middleName:null,surname:"Mahmoud Saleh",slug:"marwa-mahmoud-saleh",fullName:"Marwa Mahmoud Saleh",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/190980/images/system/190980.jpg",biography:"Professor Marwa Mahmoud Saleh is a doctor of medicine and currently works in the unit of Phoniatrics, Department of Otolaryngology, Ain Shams University in Cairo, Egypt. She got her doctoral degree in 1991 and her doctoral thesis was accomplished in the University of Iowa, United States. Her publications covered a multitude of topics as videokymography, cochlear implants, stuttering, and dysphagia. She has lectured Egyptian phonology for many years. Her recent research interest is joint attention in autism.",institutionString:"Ain Shams University",institution:{name:"Ain Shams University",country:{name:"Egypt"}}},{id:"259190",title:"Dr.",name:"Syed Ali Raza",middleName:null,surname:"Naqvi",slug:"syed-ali-raza-naqvi",fullName:"Syed Ali Raza Naqvi",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/259190/images/system/259190.png",biography:"Dr. Naqvi is a radioanalytical chemist and is working as an associate professor of analytical chemistry in the Department of Chemistry, Government College University, Faisalabad, Pakistan. Advance separation techniques, nuclear analytical techniques and radiopharmaceutical analysis are the main courses that he is teaching to graduate and post-graduate students. In the research area, he is focusing on the development of organic- and biomolecule-based radiopharmaceuticals for diagnosis and therapy of infectious and cancerous diseases. Under the supervision of Dr. Naqvi, three students have completed their Ph.D. degrees and 41 students have completed their MS degrees. He has completed three research projects and is currently working on 2 projects entitled “Radiolabeling of fluoroquinolone derivatives for the diagnosis of deep-seated bacterial infections” and “Radiolabeled minigastrin peptides for diagnosis and therapy of NETs”. He has published about 100 research articles in international reputed journals and 7 book chapters. Pakistan Institute of Nuclear Science & Technology (PINSTECH) Islamabad, Punjab Institute of Nuclear Medicine (PINM), Faisalabad and Institute of Nuclear Medicine and Radiology (INOR) Abbottabad are the main collaborating institutes.",institutionString:"Government College University",institution:{name:"Government College University, Faisalabad",country:{name:"Pakistan"}}},{id:"58390",title:"Dr.",name:"Gyula",middleName:null,surname:"Mozsik",slug:"gyula-mozsik",fullName:"Gyula Mozsik",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/58390/images/system/58390.png",biography:"Gyula Mózsik MD, Ph.D., ScD (med), is an emeritus professor of Medicine at the First Department of Medicine, Univesity of Pécs, Hungary. He was head of this department from 1993 to 2003. His specializations are medicine, gastroenterology, clinical pharmacology, clinical nutrition, and dietetics. His research fields are biochemical pharmacological examinations in the human gastrointestinal (GI) mucosa, mechanisms of retinoids, drugs, capsaicin-sensitive afferent nerves, and innovative pharmacological, pharmaceutical, and nutritional (dietary) research in humans. He has published about 360 peer-reviewed papers, 197 book chapters, 692 abstracts, 19 monographs, and has edited 37 books. He has given about 1120 regular and review lectures. He has organized thirty-eight national and international congresses and symposia. He is the founder of the International Conference on Ulcer Research (ICUR); International Union of Pharmacology, Gastrointestinal Section (IUPHAR-GI); Brain-Gut Society symposiums, and gastrointestinal cytoprotective symposiums. He received the Andre Robert Award from IUPHAR-GI in 2014. Fifteen of his students have been appointed as full professors in Egypt, Cuba, and Hungary.",institutionString:"University of Pécs",institution:{name:"University of Pecs",country:{name:"Hungary"}}},{id:"277367",title:"M.Sc.",name:"Daniel",middleName:"Martin",surname:"Márquez López",slug:"daniel-marquez-lopez",fullName:"Daniel Márquez López",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/277367/images/7909_n.jpg",biography:"Msc Daniel Martin Márquez López has a bachelor degree in Industrial Chemical Engineering, a Master of science degree in the same área and he is a PhD candidate for the Instituto Politécnico Nacional. His Works are realted to the Green chemistry field, biolubricants, biodiesel, transesterification reactions for biodiesel production and the manipulation of oils for therapeutic purposes.",institutionString:null,institution:{name:"Instituto Politécnico Nacional",country:{name:"Mexico"}}},{id:"196544",title:"Prof.",name:"Angel",middleName:null,surname:"Catala",slug:"angel-catala",fullName:"Angel Catala",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/196544/images/system/196544.jpg",biography:"Angel Catalá studied chemistry at Universidad Nacional de La Plata, Argentina, where he received a Ph.D. in Chemistry (Biological Branch) in 1965. From 1964 to 1974, he worked as an Assistant in Biochemistry at the School of Medicine at the same university. From 1974 to 1976, he was a fellow of the National Institutes of Health (NIH) at the University of Connecticut, Health Center, USA. From 1985 to 2004, he served as a Full Professor of Biochemistry at the Universidad Nacional de La Plata. He is a member of the National Research Council (CONICET), Argentina, and the Argentine Society for Biochemistry and Molecular Biology (SAIB). His laboratory has been interested for many years in the lipid peroxidation of biological membranes from various tissues and different species. Dr. Catalá has directed twelve doctoral theses, published more than 100 papers in peer-reviewed journals, several chapters in books, and edited twelve books. He received awards at the 40th International Conference Biochemistry of Lipids 1999 in Dijon, France. He is the winner of the Bimbo Pan-American Nutrition, Food Science and Technology Award 2006 and 2012, South America, Human Nutrition, Professional Category. In 2006, he won the Bernardo Houssay award in pharmacology, in recognition of his meritorious works of research. Dr. Catalá belongs to the editorial board of several journals including Journal of Lipids; International Review of Biophysical Chemistry; Frontiers in Membrane Physiology and Biophysics; World Journal of Experimental Medicine and Biochemistry Research International; World Journal of Biological Chemistry, Diabetes, and the Pancreas; International Journal of Chronic Diseases & Therapy; and International Journal of Nutrition. He is the co-editor of The Open Biology Journal and associate editor for Oxidative Medicine and Cellular Longevity.",institutionString:"Universidad Nacional de La Plata",institution:{name:"National University of La Plata",country:{name:"Argentina"}}},{id:"186585",title:"Dr.",name:"Francisco Javier",middleName:null,surname:"Martin-Romero",slug:"francisco-javier-martin-romero",fullName:"Francisco Javier Martin-Romero",position:null,profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bSB3HQAW/Profile_Picture_1631258137641",biography:"Francisco Javier Martín-Romero (Javier) is a Professor of Biochemistry and Molecular Biology at the University of Extremadura, Spain. He is also a group leader at the Biomarkers Institute of Molecular Pathology. Javier received his Ph.D. in 1998 in Biochemistry and Biophysics. At the National Cancer Institute (National Institute of Health, Bethesda, MD) he worked as a research associate on the molecular biology of selenium and its role in health and disease. After postdoctoral collaborations with Carlos Gutierrez-Merino (University of Extremadura, Spain) and Dario Alessi (University of Dundee, UK), he established his own laboratory in 2008. The interest of Javier's lab is the study of cell signaling with a special focus on Ca2+ signaling, and how Ca2+ transport modulates the cytoskeleton, migration, differentiation, cell death, etc. He is especially interested in the study of Ca2+ channels, and the role of STIM1 in the initiation of pathological events.",institutionString:null,institution:{name:"University of Extremadura",country:{name:"Spain"}}},{id:"217323",title:"Prof.",name:"Guang-Jer",middleName:null,surname:"Wu",slug:"guang-jer-wu",fullName:"Guang-Jer Wu",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/217323/images/8027_n.jpg",biography:null,institutionString:null,institution:null},{id:"148546",title:"Dr.",name:"Norma Francenia",middleName:null,surname:"Santos-Sánchez",slug:"norma-francenia-santos-sanchez",fullName:"Norma Francenia Santos-Sánchez",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/148546/images/4640_n.jpg",biography:null,institutionString:null,institution:null},{id:"272889",title:"Dr.",name:"Narendra",middleName:null,surname:"Maddu",slug:"narendra-maddu",fullName:"Narendra Maddu",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/272889/images/10758_n.jpg",biography:null,institutionString:null,institution:null},{id:"242491",title:"Prof.",name:"Angelica",middleName:null,surname:"Rueda",slug:"angelica-rueda",fullName:"Angelica Rueda",position:"Investigador Cinvestav 3B",profilePictureURL:"https://mts.intechopen.com/storage/users/242491/images/6765_n.jpg",biography:null,institutionString:null,institution:null},{id:"88631",title:"Dr.",name:"Ivan",middleName:null,surname:"Petyaev",slug:"ivan-petyaev",fullName:"Ivan Petyaev",position:null,profilePictureURL:"//cdnintech.com/web/frontend/www/assets/author.svg",biography:null,institutionString:null,institution:{name:"Lycotec (United Kingdom)",country:{name:"United Kingdom"}}},{id:"423869",title:"Ms.",name:"Smita",middleName:null,surname:"Rai",slug:"smita-rai",fullName:"Smita Rai",position:null,profilePictureURL:"//cdnintech.com/web/frontend/www/assets/author.svg",biography:null,institutionString:null,institution:{name:"Integral University",country:{name:"India"}}},{id:"424024",title:"Prof.",name:"Swati",middleName:null,surname:"Sharma",slug:"swati-sharma",fullName:"Swati Sharma",position:null,profilePictureURL:"//cdnintech.com/web/frontend/www/assets/author.svg",biography:null,institutionString:null,institution:{name:"Integral University",country:{name:"India"}}},{id:"439112",title:"MSc.",name:"Touseef",middleName:null,surname:"Fatima",slug:"touseef-fatima",fullName:"Touseef Fatima",position:null,profilePictureURL:"//cdnintech.com/web/frontend/www/assets/author.svg",biography:null,institutionString:null,institution:{name:"Integral University",country:{name:"India"}}},{id:"424836",title:"Dr.",name:"Orsolya",middleName:null,surname:"Borsai",slug:"orsolya-borsai",fullName:"Orsolya Borsai",position:null,profilePictureURL:"//cdnintech.com/web/frontend/www/assets/author.svg",biography:null,institutionString:null,institution:{name:"University of Agricultural Sciences and Veterinary Medicine of Cluj-Napoca",country:{name:"Romania"}}},{id:"422262",title:"Ph.D.",name:"Paola Andrea",middleName:null,surname:"Palmeros-Suárez",slug:"paola-andrea-palmeros-suarez",fullName:"Paola Andrea Palmeros-Suárez",position:null,profilePictureURL:"//cdnintech.com/web/frontend/www/assets/author.svg",biography:null,institutionString:null,institution:{name:"University of Guadalajara",country:{name:"Mexico"}}}]}},subseries:{item:{id:"12",type:"subseries",title:"Human Physiology",keywords:"Anatomy, Cells, Organs, Systems, Homeostasis, Functions",scope:"Human physiology is the scientific exploration of the various functions (physical, biochemical, and mechanical properties) of humans, their organs, and their constituent cells. The endocrine and nervous systems play important roles in maintaining homeostasis in the human body. Integration, which is the biological basis of physiology, is achieved through communication between the many overlapping functions of the human body's systems, which takes place through electrical and chemical means. Much of the basis of our knowledge of human physiology has been provided by animal experiments. Because of the close relationship between structure and function, studies in human physiology and anatomy seek to understand the mechanisms that help the human body function. The series on human physiology deals with the various mechanisms of interaction between the various organs, nerves, and cells in the human body.",coverUrl:"https://cdn.intechopen.com/series_topics/covers/12.jpg",hasOnlineFirst:!0,hasPublishedBooks:!0,annualVolume:11408,editor:{id:"195829",title:"Prof.",name:"Kunihiro",middleName:null,surname:"Sakuma",slug:"kunihiro-sakuma",fullName:"Kunihiro Sakuma",profilePictureURL:"https://mts.intechopen.com/storage/users/195829/images/system/195829.jpg",biography:"Professor Kunihiro Sakuma, Ph.D., currently works in the Institute for Liberal Arts at the Tokyo Institute of Technology. He is a physiologist working in the field of skeletal muscle. He was awarded his sports science diploma in 1995 by the University of Tsukuba and began his scientific work at the Department of Physiology, Aichi Human Service Center, focusing on the molecular mechanism of congenital muscular dystrophy and normal muscle regeneration. His interest later turned to the molecular mechanism and attenuating strategy of sarcopenia (age-related muscle atrophy). His opinion is to attenuate sarcopenia by improving autophagic defects using nutrient- and pharmaceutical-based treatments.",institutionString:null,institution:{name:"Tokyo Institute of Technology",institutionURL:null,country:{name:"Japan"}}},editorTwo:null,editorThree:{id:"331519",title:"Dr.",name:"Kotomi",middleName:null,surname:"Sakai",slug:"kotomi-sakai",fullName:"Kotomi Sakai",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0033Y000031QtFXQA0/Profile_Picture_1637053227318",biography:"Senior researcher Kotomi Sakai, Ph.D., MPH, works at the Research Organization of Science and Technology in Ritsumeikan University. She is a researcher in the geriatric rehabilitation and public health field. She received Ph.D. from Nihon University and MPH from St.Luke’s International University. Her main research interest is sarcopenia in older adults, especially its association with nutritional status. Additionally, to understand how to maintain and improve physical function in older adults, to conduct studies about the mechanism of sarcopenia and determine when possible interventions are needed.",institutionString:null,institution:{name:"Ritsumeikan University",institutionURL:null,country:{name:"Japan"}}},series:{id:"10",title:"Physiology",doi:"10.5772/intechopen.72796",issn:"2631-8261"},editorialBoard:[{id:"213786",title:"Dr.",name:"Henrique P.",middleName:null,surname:"Neiva",slug:"henrique-p.-neiva",fullName:"Henrique P. 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