Literature DB >> 15800845

Quantitative founder-effect analysis of French Canadian families identifies specific loci contributing to metabolic phenotypes of hypertension.

P Hamet1, E Merlo, O Seda, U Broeckel, J Tremblay, M Kaldunski, D Gaudet, G Bouchard, B Deslauriers, F Gagnon, G Antoniol, Z Pausová, M Labuda, M Jomphe, F Gossard, G Tremblay, R Kirova, P Tonellato, S N Orlov, J Pintos, J Platko, T J Hudson, J D Rioux, T A Kotchen, A W Cowley.   

Abstract

The Saguenay-Lac St-Jean population of Quebec is relatively isolated and has genealogical records dating to the 17th-century French founders. In 120 extended families with at least one sib pair affected with early-onset hypertension and/or dyslipidemia, we analyzed the genetic determinants of hypertension and related cardiovascular and metabolic conditions. Variance-components linkage analysis revealed 46 loci after 100,000 permutations. The most prominent clusters of overlapping quantitative-trait loci were on chromosomes 1 and 3, a finding supported by principal-components and bivariate analyses. These genetic determinants were further tested by classifying families by use of LOD score density analysis for each measured phenotype at every 5 cM. Our study showed the founder effect over several generations and classes of living individuals. This quantitative genealogical approach supports the notion of the ancestral causality of traits uniquely present and inherited in distinct family classes. With the founder effect, traits determined within population subsets are measurably and quantitatively transmitted through generational lineage, with a precise component contributing to phenotypic variance. These methods should accelerate the uncovering of causal haplotypes in complex diseases such as hypertension and metabolic syndrome.

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Year:  2005        PMID: 15800845      PMCID: PMC1199371          DOI: 10.1086/430133

Source DB:  PubMed          Journal:  Am J Hum Genet        ISSN: 0002-9297            Impact factor:   11.025


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