BMC Medical Genetics (Aug 2007)

PPARα L162V underlies variation in serum triglycerides and subcutaneous fat volume in young males

  • Clarkson Priscilla M,
  • Angelopoulos Theodore J,
  • Price Thomas B,
  • Thompson Paul D,
  • Seip Richard L,
  • Hansen Barbara C,
  • Brandoli Cinzia,
  • Reeves Erica K,
  • Harmon Brennan,
  • Devaney Joseph,
  • Tesi-Rocha Carolina,
  • Bradbury Meg,
  • Gordish-Dressman Heather,
  • Uthurralt Julieta,
  • Moyna Niall M,
  • Pescatello Linda S,
  • Visich Paul S,
  • Zoeller Robert F,
  • Gordon Paul M,
  • Hoffman Eric P

DOI
https://doi.org/10.1186/1471-2350-8-55
Journal volume & issue
Vol. 8, no. 1
p. 55

Abstract

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Abstract Background Of the five sub-phenotypes defining metabolic syndrome, all are known to have strong genetic components (typically 50–80% of population variation). Studies defining genetic predispositions have typically focused on older populations with metabolic syndrome and/or type 2 diabetes. We hypothesized that the study of younger populations would mitigate many confounding variables, and allow us to better define genetic predisposition loci for metabolic syndrome. Methods We studied 610 young adult volunteers (average age 24 yrs) for metabolic syndrome markers, and volumetric MRI of upper arm muscle, bone, and fat pre- and post-unilateral resistance training. Results We found the PPARα L162V polymorphism to be a strong determinant of serum triglyceride levels in young White males, where carriers of the V allele showed 78% increase in triglycerides relative to L homozygotes (LL = 116 ± 11 mg/dL, LV = 208 ± 30 mg/dL; p = 0.004). Men with the V allele showed lower HDL (LL = 42 ± 1 mg/dL, LV = 34 ± 2 mg/dL; p = 0.001), but women did not. Subcutaneous fat volume was higher in males carrying the V allele, however, exercise training increased fat volume of the untrained arm in V carriers, while LL genotypes significantly decreased in fat volume (LL = -1,707 ± 21 mm3, LV = 17,617 ± 58 mm3 ; p = 0.002), indicating a systemic effect of the V allele on adiposity after unilateral training. Our study suggests that the primary effect of PPARα L162V is on serum triglycerides, with downstream effects on adiposity and response to training. Conclusion Our results on association of PPARα and triglycerides in males showed a much larger effect of the V allele than previously reported in older and less healthy populations. Specifically, we showed the V allele to increase triglycerides by 78% (p = 0.004), and this single polymorphism accounted for 3.8% of all variation in serum triglycerides in males (p = 0.0037).