Inheritance of Human Muscle Enzyme Adaptation to Isokinetic Strength Training

Thibault, M. C.; Simoneau, J. A.; Côté, Claude H.; Boulay, M. R.; Lagassé, Pierre P.; Marcotte, M.; Bouchard, Claude

doi:10.1159/000153657

Cited by 25 publications

(11 citation statements)

References 12 publications

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“…Here we show that muscle HKII content and hence glucose phosphorylation capacity, is a critical determinant of exercise endurance capacity in C57BL/6J mice. These findings strongly suggest that the exercise training‐induced increase in HKII activity that has been reported previously (Barnard & Peter, 1969; Lamb et al 1969; Bylund et al 1977; Mandroukas et al 1984; Thibault et al 1986; Bigard et al 1991; Greiwe et al 1999) may be important to the increased exercise endurance of trained individuals. This is consistent with the observation that mice selected for increased running capacity have increased muscle hexokinase activity compared to control mice (Houle‐Leroy et al 2000).…”

Section: Discussionsupporting

confidence: 77%

Hexokinase II protein content is a determinant of exercise endurance capacity in the mouse

Fueger¹,

Shearer²,

Krueger³

et al. 2005

The Journal of Physiology

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Hexokinase (HK) II content is elevated in fatigue resistant muscle fibres and exercise trained muscle. The aim of this study was to determine if exercise capacity is dependent on muscle HK protein content. C57Bl/6 mice with a 50% HK knockout (HK +/− ), no genetic manipulation (wild-type, WT) and an ∼3-fold HK overexpression (HK Tg ) were tested. Mice (n = 12/group) completed both a maximal oxygen consumption (V O 2 ,max ) test and an endurance capacity test (run at ∼75%V O 2 ,max ) on an enclosed treadmill equipped to measure gas exchange. Arterial and venous catheters were surgically implanted into separate groups of mice (n = 9-11/group) in order to measure an index of muscle glucose uptake (R g ) during 30 min of treadmill exercise. Maximum work rate (0.95 ± 0.05, 1.00 ± 0.04 and 1.06 ± 0.07 kg m min −1 ),V O 2 ,max (137 ± 3, 141 ± 4 and 141 ± 5 ml kg −1 min −1 ) and maximal respiratory exchange ratio (1.04 ± 0.02, 1.00 ± 0.03 and 1.04 ± 0.04) were similar in HK +/− , WT and HK Tg , respectively. Exercise endurance capacity (measured as time to exhaustion) increased as HK content increased (55 ± 11, 77 ± 5 and 98 ± 9 min) and this was related to R g measured in mice during 30 min of exercise (13 ± 2, 24 ± 5 and 42 ± 5 µmol (100 g) −1 min −1 ). Muscle glycogen in sedentary HK +/− mice and HK +/− mice following 30 min of exercise were significantly lower than in HK Tg and WT mice. However, the net exercise-induced muscle glycogen breakdown was equal in the three genotypes. In summary, HK protein content within the range studied (a) was not associated with a difference in the capacity to perform maximal intensity exercise, (b) was a powerful determinant of the ability to sustain moderate intensity exercise, as reducing HK content impaired endurance and increasing HK content enhanced endurance, and (c) although directly related to exercise endurance, was not a determinant of net muscle glycogen usage during exercise. In conclusion, adaptations that increase HK protein content and/or functional activity such as regular exercise contribute to increased muscular endurance.

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Section: Discussionsupporting

confidence: 77%

Hexokinase II protein content is a determinant of exercise endurance capacity in the mouse

Fueger¹,

Shearer²,

Krueger³

et al. 2005

The Journal of Physiology

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“…Although the heritability of the adaptation of these muscle phenotypes to strength training (ST) has not been well studied, the adaptive response also appears to have a genetic component (26,27 The purpose of the present study was to investigate the association of ACE genotype with muscle phenotypes before and after ST in older men and women. Though the literature is inconclusive, the biological rationale suggests an advantage for the D allele with regard to muscle phenotypes; thus, we hypothesized that the D allele would be associated with higher values for muscle phenotypes before ST, and greater increases in muscle phenotypes in response to ST. As most studies have investigated only men, we investigated men and women to determine possible sex differences.…”

Section: Angiotensin-converting Enzyme; Genetics; Muscle Mass; Musclementioning

confidence: 99%

ACE Genotype and the Muscle Hypertrophic and Strength Responses to Strength Training

Charbonneau

Hanson

Ludlow

et al. 2008

Medicine &Amp; Science in Sports &Amp; Exercise

103

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Purpose-Previous studies have linked an insertion/deletion polymorphism in the angiotensinconverting enzyme (ACE) gene with variability in muscle strength responses to strength training (ST), though conclusions have been inconsistent across investigations. Moreover, most previous studies have not investigated the influence of sex on the association of ACE I/D genotype with muscle phenotypes. The purpose of this study was to investigate the association of ACE genotype with muscle phenotypes before and after ST in older men and women.Methods-Eighty-six inactive men and 139 inactive women, ages 50-85 yr (mean: 62 yr), were studied before and after 10 wk of unilateral knee extensor ST. The one-repetition maximum (1RM) test was used to assess knee extensor muscle strength, and computed tomography was used to measure quadriceps muscle volume (MV). Differences were compared among ACE genotype groups (II vs ID vs DD).Results-Across the entire cohort at baseline, ACE genotype was significantly associated with total lean mass and body weight, with higher values in DD genotype carriers (both P < 0.05). At baseline, DD genotype carriers exhibited significantly greater MV compared with II genotype carriers for both the trained leg (men: 1828 ± 44 vs 1629 ± 70; women: 1299 ± 34 vs 1233 ± 49; P = 0.02) and untrained leg (men: 1801 ± 46 vs 1559 ± 72; women: 1268 ± 36 vs 1189 ± 51; P = 0.01), with no significant genotype × sex interaction. No ACE genotype associations were observed for the 1RM or MV adaptations to ST in either men or women.Conclusions-In the present study, ACE genotype was associated with baseline differences in muscle volume, but it was not associated with the muscle hypertrophic response to ST. Keywords ANGIOTENSIN-CONVERTING ENZYME; GENETICS; MUSCLE MASS; MUSCLE SIZE; SKELETAL MUSCLEMuscle strength and mass are heritable phenotypes, with a heritability range of 14-80% for strength (1,21,28,30) and 20-85% for muscle mass (1,14,24,28). Although the heritability of the adaptation of these muscle phenotypes to strength training (ST) has not been well studied, the adaptive response also appears to have a genetic component (26,27 The purpose of the present study was to investigate the association of ACE genotype with muscle phenotypes before and after ST in older men and women. Though the literature is inconclusive, the biological rationale suggests an advantage for the D allele with regard to muscle phenotypes; thus, we hypothesized that the D allele would be associated with higher values for muscle phenotypes before ST, and greater increases in muscle phenotypes in response to ST. As most studies have investigated only men, we investigated men and women to determine possible sex differences. METHODS SubjectsParticipants in the study consisted of 243 inactive, healthy volunteers between the ages of 50 and 85 yr. For this investigation, "inactive" was operationally defined as a person who performs less than 20 min of vigorous activity per week. Subjects were required to be nonsmokers with no significant car...

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“…Significant genetic influences have also been identified for measures of skeletal muscle strength and performance, including the response of oxoglutarate dehydrogenase activity to training (Thibault et al 1986), muscle adaptation to endurance exercise (Hamel et al 1986), vertical jump height as a measure of explosive power (Maes et al 1996), various measures of muscle strength and their response to training (Thomis et al 1998), anaerobic capacity and explosive power (Calvo et al 2002), average size of type I (slow oxidative) fibres in the sedentary state and maximal activity of energy production enzymes both in the sedentary state and in response to training (Rico-Sanz et al 2003b). The genetic contribution to variation in the relative proportions of skeletal muscle fibre types is estimated as lying between 40% and 50% (Simoneau and Bouchard 1995).…”

Section: Heritability Of Performance-related Traitsmentioning

confidence: 99%

Genes and human elite athletic performance

2005

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Physical fitness is a complex phenotype influenced by a myriad of environmental and genetic factors, and variation in human physical performance and athletic ability has long been recognised as having a strong heritable component. Recently, the development of technology for rapid DNA sequencing and genotyping has allowed the identification of some of the individual genetic variations that contribute to athletic performance. This review will examine the evidence that has accumulated over the last three decades for a strong genetic influence on human physical performance, with an emphasis on two sets of physical traits, viz. cardiorespiratory and skeletal muscle function, which are particularly important for performance in a variety of sports. We will then review recent studies that have identified individual genetic variants associated with variation in these traits and the polymorphisms that have been directly associated with elite athlete status. Finally, we explore the scientific implications of our rapidly growing understanding of the genetic basis of variation in performance.

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Inheritance of Human Muscle Enzyme Adaptation to Isokinetic Strength Training

Cited by 25 publications

References 12 publications

Hexokinase II protein content is a determinant of exercise endurance capacity in the mouse

Hexokinase II protein content is a determinant of exercise endurance capacity in the mouse

ACE Genotype and the Muscle Hypertrophic and Strength Responses to Strength Training

Genes and human elite athletic performance

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