BMC Medical Genetics (Jul 2011)

A follow-up study for left ventricular mass on chromosome 12p11 identifies potential candidate genes

  • Slifer Susan,
  • McClendon Mark S,
  • Wang Liyong,
  • Rundek Tatjana,
  • Beecham Ashley,
  • Della-Morte David,
  • Blanton Susan H,
  • Di Tullio Marco R,
  • Sacco Ralph L

DOI
https://doi.org/10.1186/1471-2350-12-100
Journal volume & issue
Vol. 12, no. 1
p. 100

Abstract

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Abstract Background Left ventricular mass (LVM) is an important risk factor for cardiovascular disease. Previously we found evidence for linkage to chromosome 12p11 in Dominican families, with a significant increase in a subset of families with high average waist circumference (WC). In the present study, we use association analysis to further study the genetic effect on LVM. Methods Association analysis with LVM was done in the one LOD critical region of the linkage peak in an independent sample of 897 Caribbean Hispanics. Genotype data were available on 7085 SNPs from 23 to 53 MB on chromosome 12p11. Adjustment was made for vascular risk factors and population substructure using an additive genetic model. Subset analysis by WC was performed to test for a difference in genetic effects between the high and low WC subsets. Results In the overall analysis, the most significant association was found to rs10743465, downstream of the SOX5 gene (p = 1.27E-05). Also, 19 additional SNPs had nominal p TMTC1. Twelve additional SNPs in or near 6 genes had p Conclusions The current study supports previously identified evidence by linkage for a genetic effect on LVM on chromosome 12p11 using association analysis in population-based Caribbean Hispanic cohort. SOX5 may play an important role in the regulation of LVM. An interaction of TMTC1 with abdominal obesity may contribute to phenotypic variation of LVM.