2019
DOI: 10.1016/j.ajhg.2019.10.014
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Genome-wide Associations Reveal Human-Mouse Genetic Convergence and Modifiers of Myogenesis, CPNE1 and STC2

Abstract: Muscle bulk in adult healthy humans is highly variable even after accounting for height, age and sex. Low muscle mass, due to fewer and/or smaller constituent muscle fibers, would exacerbate the impact of muscle loss occurring in aging or disease. Genetic variability substantially influences muscle mass differences, but causative genes remain largely unknown. In a genome-wide association study (GWAS) on appendicular lean mass (ALM) in a population of 85,750 middle-age (38-49 years) individuals from the UK Biob… Show more

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Cited by 47 publications
(33 citation statements)
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“…Of the 152 genes implicated by both the gene mapping and gene-based analyses, 78 remained significantly associated with self-reported walking pace following BMI adjustment. These genes included GDF5 , ACBD4 , H1FX , PTPN9 , FAM83C and UQCC1 which have previously been associated with height 17 20 ; MMP24 , NCOA6 , PIGU , GSS and PLCD3 , associated with lean body mass 21 , 22 ; MAPT , TRPC4AP , DCAKD , GGT7 and PROCR , associated with heel bone mineral density 23 , and several genes linked to educational attainment 24 and cognitive function 25 ( SDCCAG8 , BTN3A2 , TCF4 , HIST1H4H , ABT1 , TXNL1 , NYAP2 and ZNF322 ).…”
Section: Resultsmentioning
confidence: 99%
“…Of the 152 genes implicated by both the gene mapping and gene-based analyses, 78 remained significantly associated with self-reported walking pace following BMI adjustment. These genes included GDF5 , ACBD4 , H1FX , PTPN9 , FAM83C and UQCC1 which have previously been associated with height 17 20 ; MMP24 , NCOA6 , PIGU , GSS and PLCD3 , associated with lean body mass 21 , 22 ; MAPT , TRPC4AP , DCAKD , GGT7 and PROCR , associated with heel bone mineral density 23 , and several genes linked to educational attainment 24 and cognitive function 25 ( SDCCAG8 , BTN3A2 , TCF4 , HIST1H4H , ABT1 , TXNL1 , NYAP2 and ZNF322 ).…”
Section: Resultsmentioning
confidence: 99%
“…Moreover, a recent GWAS by Hernandez-Cordero et al [80] evaluated genetic contribution to ALM in the UK Biobank dataset, comparing middle-aged (38-49 years) and elderly (60-74 years) individuals. A total of 182 genome-wide significant regions, many with multiple variants within them, were associated with ALM in middle-aged individuals.…”
Section: Genome-wide Studiesmentioning
confidence: 99%
“…Historically, many candidate gene studies have been statistically underpowered, the replication of findings has been problematic and there has been a suspected bias against publication of negative results, which may lead to conflicting findings [130]. Many of these issues have been overcome by GWAS in large, well characterised cohorts [80,[131][132][133]. Therefore, future GWAS may help to further illuminate the genetic basis of aging muscle phenotypes.…”
Section: Strengths and Limitationsmentioning
confidence: 99%
“…In a more recent study, a GWAS of ALM was conducted in a population of 85,750 middle-aged (aged 38–49 years) individuals from the UK Biobank (UKB) 15 . A total of 182 loci were identified, 78% of which were replicated in a population of 181,862 elderly (aged 60–74 years) individuals from the same UKB cohort.…”
Section: Introductionmentioning
confidence: 99%