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Linkage of myostatin pathway genes with knee strength in humans

2004; American Physical Society; Volume: 17; Issue: 3 Linguagem: Inglês

10.1152/physiolgenomics.00224.2003

1531-2267

Wim Huygens, Martine Thomis, Maarten Peeters, Jeroen Aerssens, Rob Janssen, Robert Vlietinck, Gastón Beunen,

Cardiomyopathy and Myosin Studies

This study was the first to explore the potential role of the myostatin ( GDF8) pathway in relation to muscle strength and estimated muscle cross-sectional area in humans using linkage analysis with a candidate gene approach. In young male sibs ( n = 329) 11 polymorphic markers in or near 10 candidate genes from the myostatin pathway were genotyped. Muscle mass was estimated by anthropometric measurements, and maximal knee strength was evaluated using isokinetic dynamometers (Cybex NORM). Single-point nonparametric variance components and linear quantitative trait locus regression linkage analysis methods were used. Linkage patterns were observed between knee extension and flexion peak torque with markers D2S118 ( GDF8), D6S1051 ( CDKN1A), and D11S4138 ( MYOD1), and a maximum LOD score of 2.63 ( P = 0.0002) was observed with D2S118. The ratios of peak torque over muscle and bone area of the midthigh of the lower contraction velocity (60°/s) showed more frequently significant LOD scores than the torques at high velocity (240°/s). Although myostatin is physiologically more related to muscle mass through possible effects of hyperplasia and hypertrophy than it is to strength, only two estimated muscle cross-sectional areas were marginally linked (LOD 1.06 and 1.07, P = 0.01) with marker D2S118 near GDF8 (2q32.2). The present results gave suggestive evidence that the myostatin pathway might be important for strength phenotypes, and GDF8, CDKN1A, and MYOD1 are potential candidate regions for a further and denser mapping with respect to these phenotypes.