vv
Archives of Sports Medicine and
Physiotherapy
DOI CC By
016
Medical Group
Citation: Ulucan K (2017) Is CRISPR a fear Against Sports? Arch Sports Med Physiother 2(1): 016-017.
Editorial
Is CRISPR a fear Against Sports?
Korkut Ulucan1,2
*
1
Marmara University, Faculty of Dentistry,
Department of Medical Biology and Genetics,
Istanbul, Turkey
2
Üsküdar University, Faculty of Engineering and
Natural Sciences, Department of Molecular Biology
and Genetics, Istanbul, Turkey
Dates: Received: 29 May, 2017; Accepted: 01 July,
2017; Published: 03 July, 2017
*Corresponding author: Korkut Ulucan, Marmara
University, Faculty of Dentistry, Department of Medi-
cal Biology and Genetics, Istanbul, Turkey, E-mail:
https://www.peertechz.com
Dear Editor
One of the most worrying applications of molecular
technology in sport is the gene doping, which is an outgrowth
of gene therapy. In gene therapy, the missing or out- functioned
gene or gene fragment is replaced with the functioning one, by
the help of transfectionable devices such as viruses. In gene
doping, the interested region is mostly the genetic material
for enhancing athletic capacity. World Anti- doping Agency
defined gene doping as the “nontherapeutic use of cells, genes,
genetic elements, or modulation of gene expression, having
the capacity to enhance performance”. To date, different
researchers have attempted to inject different types of genes to
model organisms [1,2], but still these approaches are far from
safeness in humans, even in medical area.
A new gene editing strategy gives promise for genome
editing. Many scientists have now an opportunity to edit an
organism genome by clustered, regularly interspaced, short
palindromic repeat (CRISPR) technology. By this technology,
with the help of RNA-guided nucleases, such as CRISPR
Associated Protein 9 (Cas9), it is possible to modify endogenous
genes by using a modified CRISPR-Cas9 system. This modified
system will not only spur the development of novel molecular
therapeutics for medication of diseases, but also perform
targeted, highly efficient alterations of genome sequence and
gene expression [3].
The CRISPR/Cas system is a natural prokaryotic acquired
immune system that are used against some plasmids and
phages [4]. This system is found nearly 40% of sequenced
bacterial genomes and 90% of sequenced archaea, and shows
sequence similarities [5]. This system’s potential to recognize,
metabolize and edit the foreign DNA and RNA let scientists to
consider the application of this system to human cell lines gör
therapeutical reasons. Briefly, site directed enzymes recognizes
the genomic region, and operate the editing process in the
genome, without giving any damage to the genome metabolism.
To date, several laboratories announced their ongoing research
to apply CRISPR to human embryos for medical purposes [6].
to treat genetic diseases. Liang et al. (2015) reported the first
results of applying this methodology to non-viable human
embryos for repairing a mutation responsible for a heritable
genetic disorder, beta thalassemia. The oncologist, Lu You,
from Sichuan University in China, applied this technique to the
isolated immune cells of a patient with aggressive lung cancer,
and these modified cells were delivered back to the patient to
fight against cancer cells [7]. By the end of 2017, scientists hope
to start clinical trials using CRISPR-Cas9 against different
types of diseases, after the completion of funding or needed
approvals.
Sport genomic is branch of science that deals with the genetic
endowmentofathletes.Itinvestigatesthegeneticpredisposition
to exercise, non-contact injuries like tendonopathies, stress
conditions effecting athletic performance and nutrigenomic
biomarkers in sports. Most single nucleotide polymorphisms
(SNPs) have effects on gene regulation, and therefore have
effects on athletic performance. To date, upto 250 SNPs are
considered to be related with athletic performance [8]. Having
information about these SNPs now let us to give optimal advice
for training, or for nutritional approaches. For example one
of the gene coding for actin proteins in muscles is alpha-
actinin-3 (ACTN3). The common form, wild type, of this gene
is expressed in fast switching muscles fibers, allowing athletes
to have a more power phenotype [9]. A polymorphism within
the gene (C>T transition) alter the amino acid number by a
non-sense mutation, and protein structure. Arginine (R) amino
acid changes to a stop codon (X) at position 577. Polymorphic
variant makes the muscles to have more endurance phenotype.
Like in this example, with the help of CRISPR-Cas9 strategy,
it will be possible for cheaters to edit an athlete’s genome for
endurance, or power phenotypes, by giving a way to C or T
allele in the interested region. Not only in ACTN3, but also the
genes responsible for endurance phenotype, like MCT1, IL6,
PPAR-alpha, MSTN, will be all in the scope of gene dopers. And
017
Publications Pvt. Ltd.
Citation: Ulucan K (2017) Is CRISPR a fear Against Sports? Arch Sports Med Physiother 2(1): 016-017.
Copyright: © 2017 Ulucan K. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use,
distribution, and reproduction in any medium, provided the original author and source are credited.
this scientific, but not in sports spirit, approaches will be the
worrying barrier in front of sports. As f today, this technology
cannot complete its evolution in the terms of gene therapy,
and this seems to be the most important limitation against the
applicability. Against these, new strategies should be developed
for detecting CRISPR- edited genomes, although it is a little bit
difficult. But no need to say, the ones who “Dope for hope”
by using this technology will be under stress all over their life,
because of the fact that there will be the time that detectable
diagnostic approaches will be ready to be used. They also will
have the same penalties like chemical dopers, or blood dopers
after being detected.
References
1. Wang XY, Zhang CL, Yu RT, Nelson MC, Corinne RB-Ocampo, et al. (2004)
Regulation of Muscle Fiber Type and Running Endurance by PPARGamma.
PloS Biology. Link: https://goo.gl/reCtkX
2. Barton ER, Morris L, Musaro A, Rosenthal N, Sweeney HL (2002) Muscle-
specific expression of insulin-like growth factor I counters muscle
decline inmdx mice. The Journal of Cell Biology 157: 137-147. Link:
https://goo.gl/E2SjdE
3. Jeffry D Sander & J Keith Joung (2014) CRISPR-Cas systems for editing,
regulating and targeting genomes. Nature Biotechnology 32: 347–355. Link:
https://goo.gl/wyeecz
4. Barrangou R, Fremaux C, Deveau H, Richards M, Boyaval P, et al. (2007)
“CRISPR provides acquired resistance against viruses in prokaryotes”.
Science 315: 1709–1712. Link: https://goo.gl/HszUNZ
5. Grissa I, Vergnaud G, Pourcel C (2007) “The CRISPRdb database and tools to
display CRISPRs and to generate dictionaries of spacers and repeats”. BMC
Bioinformatics. Link: https://goo.gl/VEcWAH
6. Liang P, Xu Y, Zhang X, Ding C, Huang R, et al. (2015) “CRISPR/Cas9-mediated
gene editing in human tripronuclear zygotes”. Protein & Cell 6: 363–372.
Link: https://goo.gl/BNuvop
7. Cyranoski D (2016) CRISPR gene-editing tested in a person for the first time.
Nature. Link: https://goo.gl/xRBfCk
8. Ulucan K (2016) Spor Genetiği Açısından Türk Sporcuların ACTN3
R577X Polimorfizm Literatür Özeti. Clin Exp Health Sci 6: 44-47. Link:
https://goo.gl/cieqjm
9. Ulucan K, Bayyurt GM, Konuk M, Güney AI (2014) Effect of alpha-actinin-3
gene on Turkish trained and untrained middle school children’s sprinting
performance: a pilot study. Biological Rhythm Research 45: 509- 514. Link:
https://goo.gl/EUejWa

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Is CRISPR a fear Against Sports?

  • 1. vv Archives of Sports Medicine and Physiotherapy DOI CC By 016 Medical Group Citation: Ulucan K (2017) Is CRISPR a fear Against Sports? Arch Sports Med Physiother 2(1): 016-017. Editorial Is CRISPR a fear Against Sports? Korkut Ulucan1,2 * 1 Marmara University, Faculty of Dentistry, Department of Medical Biology and Genetics, Istanbul, Turkey 2 Üsküdar University, Faculty of Engineering and Natural Sciences, Department of Molecular Biology and Genetics, Istanbul, Turkey Dates: Received: 29 May, 2017; Accepted: 01 July, 2017; Published: 03 July, 2017 *Corresponding author: Korkut Ulucan, Marmara University, Faculty of Dentistry, Department of Medi- cal Biology and Genetics, Istanbul, Turkey, E-mail: https://www.peertechz.com Dear Editor One of the most worrying applications of molecular technology in sport is the gene doping, which is an outgrowth of gene therapy. In gene therapy, the missing or out- functioned gene or gene fragment is replaced with the functioning one, by the help of transfectionable devices such as viruses. In gene doping, the interested region is mostly the genetic material for enhancing athletic capacity. World Anti- doping Agency defined gene doping as the “nontherapeutic use of cells, genes, genetic elements, or modulation of gene expression, having the capacity to enhance performance”. To date, different researchers have attempted to inject different types of genes to model organisms [1,2], but still these approaches are far from safeness in humans, even in medical area. A new gene editing strategy gives promise for genome editing. Many scientists have now an opportunity to edit an organism genome by clustered, regularly interspaced, short palindromic repeat (CRISPR) technology. By this technology, with the help of RNA-guided nucleases, such as CRISPR Associated Protein 9 (Cas9), it is possible to modify endogenous genes by using a modified CRISPR-Cas9 system. This modified system will not only spur the development of novel molecular therapeutics for medication of diseases, but also perform targeted, highly efficient alterations of genome sequence and gene expression [3]. The CRISPR/Cas system is a natural prokaryotic acquired immune system that are used against some plasmids and phages [4]. This system is found nearly 40% of sequenced bacterial genomes and 90% of sequenced archaea, and shows sequence similarities [5]. This system’s potential to recognize, metabolize and edit the foreign DNA and RNA let scientists to consider the application of this system to human cell lines gör therapeutical reasons. Briefly, site directed enzymes recognizes the genomic region, and operate the editing process in the genome, without giving any damage to the genome metabolism. To date, several laboratories announced their ongoing research to apply CRISPR to human embryos for medical purposes [6]. to treat genetic diseases. Liang et al. (2015) reported the first results of applying this methodology to non-viable human embryos for repairing a mutation responsible for a heritable genetic disorder, beta thalassemia. The oncologist, Lu You, from Sichuan University in China, applied this technique to the isolated immune cells of a patient with aggressive lung cancer, and these modified cells were delivered back to the patient to fight against cancer cells [7]. By the end of 2017, scientists hope to start clinical trials using CRISPR-Cas9 against different types of diseases, after the completion of funding or needed approvals. Sport genomic is branch of science that deals with the genetic endowmentofathletes.Itinvestigatesthegeneticpredisposition to exercise, non-contact injuries like tendonopathies, stress conditions effecting athletic performance and nutrigenomic biomarkers in sports. Most single nucleotide polymorphisms (SNPs) have effects on gene regulation, and therefore have effects on athletic performance. To date, upto 250 SNPs are considered to be related with athletic performance [8]. Having information about these SNPs now let us to give optimal advice for training, or for nutritional approaches. For example one of the gene coding for actin proteins in muscles is alpha- actinin-3 (ACTN3). The common form, wild type, of this gene is expressed in fast switching muscles fibers, allowing athletes to have a more power phenotype [9]. A polymorphism within the gene (C>T transition) alter the amino acid number by a non-sense mutation, and protein structure. Arginine (R) amino acid changes to a stop codon (X) at position 577. Polymorphic variant makes the muscles to have more endurance phenotype. Like in this example, with the help of CRISPR-Cas9 strategy, it will be possible for cheaters to edit an athlete’s genome for endurance, or power phenotypes, by giving a way to C or T allele in the interested region. Not only in ACTN3, but also the genes responsible for endurance phenotype, like MCT1, IL6, PPAR-alpha, MSTN, will be all in the scope of gene dopers. And
  • 2. 017 Publications Pvt. Ltd. Citation: Ulucan K (2017) Is CRISPR a fear Against Sports? Arch Sports Med Physiother 2(1): 016-017. Copyright: © 2017 Ulucan K. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. this scientific, but not in sports spirit, approaches will be the worrying barrier in front of sports. As f today, this technology cannot complete its evolution in the terms of gene therapy, and this seems to be the most important limitation against the applicability. Against these, new strategies should be developed for detecting CRISPR- edited genomes, although it is a little bit difficult. But no need to say, the ones who “Dope for hope” by using this technology will be under stress all over their life, because of the fact that there will be the time that detectable diagnostic approaches will be ready to be used. They also will have the same penalties like chemical dopers, or blood dopers after being detected. References 1. Wang XY, Zhang CL, Yu RT, Nelson MC, Corinne RB-Ocampo, et al. (2004) Regulation of Muscle Fiber Type and Running Endurance by PPARGamma. PloS Biology. Link: https://goo.gl/reCtkX 2. Barton ER, Morris L, Musaro A, Rosenthal N, Sweeney HL (2002) Muscle- specific expression of insulin-like growth factor I counters muscle decline inmdx mice. The Journal of Cell Biology 157: 137-147. Link: https://goo.gl/E2SjdE 3. Jeffry D Sander & J Keith Joung (2014) CRISPR-Cas systems for editing, regulating and targeting genomes. Nature Biotechnology 32: 347–355. Link: https://goo.gl/wyeecz 4. Barrangou R, Fremaux C, Deveau H, Richards M, Boyaval P, et al. (2007) “CRISPR provides acquired resistance against viruses in prokaryotes”. Science 315: 1709–1712. Link: https://goo.gl/HszUNZ 5. Grissa I, Vergnaud G, Pourcel C (2007) “The CRISPRdb database and tools to display CRISPRs and to generate dictionaries of spacers and repeats”. BMC Bioinformatics. Link: https://goo.gl/VEcWAH 6. Liang P, Xu Y, Zhang X, Ding C, Huang R, et al. (2015) “CRISPR/Cas9-mediated gene editing in human tripronuclear zygotes”. Protein & Cell 6: 363–372. Link: https://goo.gl/BNuvop 7. Cyranoski D (2016) CRISPR gene-editing tested in a person for the first time. Nature. Link: https://goo.gl/xRBfCk 8. Ulucan K (2016) Spor Genetiği Açısından Türk Sporcuların ACTN3 R577X Polimorfizm Literatür Özeti. Clin Exp Health Sci 6: 44-47. Link: https://goo.gl/cieqjm 9. Ulucan K, Bayyurt GM, Konuk M, Güney AI (2014) Effect of alpha-actinin-3 gene on Turkish trained and untrained middle school children’s sprinting performance: a pilot study. Biological Rhythm Research 45: 509- 514. Link: https://goo.gl/EUejWa