4.6 Article

Are 'Endurance' Alleles 'Survival' Alleles? Insights from the ACTN3 R577X Polymorphism

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PLOS ONE
卷 6, 期 3, 页码 -

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PUBLIC LIBRARY SCIENCE
DOI: 10.1371/journal.pone.0017558

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  1. Fondo de Investigaciones Sanitarias (FIS) [PS09/00194]
  2. Swedish Council for Working Life and Social Research (FAS)

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Exercise phenotypes have played a key role for ensuring survival over human evolution. We speculated that some genetic variants that influence exercise phenotypes could be associated with exceptional survival (i.e. reaching >= 100years of age). Owing to its effects on muscle structure/function, a potential candidate is the Arg(R) 577Ter(X) polymorphism (rs1815739) in ACTN3, the structural gene encoding the skeletal muscle protein alpha-actinin-3. We compared the ACTN3 R577X genotype/allele frequencies between the following groups of ethnically-matched (Spanish) individuals: centenarians (cases, n = 64; 57 female; age range: 100-108 years), young healthy controls (n = 283, 67 females, 216 males; 21 +/- 2 years), and humans who are at the two end-points of exercise capacity phenotypes, i.e. muscle endurance (50 male professional road cyclists) and muscle power (63 male jumpers/sprinters). Although there were no differences in genotype/allele frequencies between centenarians (RR: 28.8%; RX: 47.5%; XX:23.7%), and controls (RR: 31.8%; RX: 49.8%; XX:18.4%) or endurance athletes (RR:28.0%; RX:46%; XX:26.0%), we observed a significantly higher frequency of the X allele (P = 0.019) and XX genotype (P = 0.011) in centenarians compared with power athletes (RR:47.6%; RX:36.5%; XX:15.9%). Notably, the frequency of the null XX (alpha-actinin-3 deficient) genotype in centenarians was the highest ever reported in non-athletic Caucasian populations. In conclusion, despite there were no significant differences with the younger, control population, overall the ACTN3 genotype of centenarians resembles that of world-class elite endurance athletes and differs from that of elite power athletes. Our preliminary data would suggest a certain 'survival' advantage brought about by alpha-actinin-3 deficiency and the 'endurance'/oxidative muscle phenotype that is commonly associated with this condition.

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