A global perspective on genetic variation at the ADH genes reveals unusual patterns of linkage disequilibrium and diversity

Michael V. Osier, Andrew J. Pakstis, Himla Soodyall, David Comas, David Goldman, Adekunle Odunsi, Friday Okonofua, Josef Parnas, Leslie O. Schulz, Jaume Bertranpetit, Batsheva Bonne-Tamir, Ru Band Lu, Judith R. Kidd, Kenneth K. Kidd

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230 引文 斯高帕斯(Scopus)

摘要

Variants of different Class I alcohol dehydrogenase (ADH) genes have been shown to be associated with an effect that is protective against alcoholism. Previous work from our laboratory has shown that the two sites showing the association are in linkage disequilibrium and has identified the ADH1B Arg47His site as causative, with the ADH1C Ile349Val site showing association only because of the disequilibrium. Here, we describe an initial study of the nature of linkage disequilibrium and genetic variation, in population samples from different regions of the world, in a larger segment of the ADH cluster (including the three Class I ADH genes and ADH7). Linkage disequilibrium across ∼40 kb of the Class I ADH cluster is moderate to strong in all population samples that we studied. We observed nominally significant pairwise linkage disequilibrium, in some populations, between the ADH7 site and some Class I ADH sites, at moderate values and at a molecular distance as great as 100 kb. Our data indicate (1) that most ADH-alcoholism association studies have failed to consider many sites in the ADH cluster that may harbor etiologically significant alleles and (2) that the relevance of the various ADH sites will be population dependent. Some individual sites in the Class I ADH cluster show Fst values that are among the highest seen among several dozen unlinked sites that were studied in the same subset of populations. The high Fst values can be attributed to the discrepant frequencies of specific alleles in eastern Asia relative to those in other regions of the world. These alleles are part of a single haplotype that exists at high (>65%) frequency only in the eastern-Asian samples. It seems unlikely that this haplotype, which is rare or unobserved in other populations, reached such high frequency because of random genetic drift alone.

原文English
頁(從 - 到)84-99
頁數16
期刊American Journal of Human Genetics
71
發行號1
DOIs
出版狀態Published - 2002

All Science Journal Classification (ASJC) codes

  • 遺傳學
  • 遺傳學(臨床)

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