GENETIC, EVOLUTIONARY, AND PHYLOGENETIC ANALYSIS OF HUMAN ALLELES
人类等位基因的遗传、进化和系统发育分析
基本信息
- 批准号:6100848
- 负责人:
- 金额:--
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:
- 资助国家:美国
- 起止时间:至
- 项目状态:未结题
- 来源:
- 关键词:
项目摘要
We are currently involved in several projects intended to resolve
patterns of recombination, linkage disequilibrium, and molecular
evolution of interesting human loci, especially the major
histocompatibility complex (MHC) region. A principal result of these
studies should be the ability to refine many of the current disease
associations with large genomic regions, such as the MHC, into the
constituent disease locus or loci. The first of these concerns the CCR5-
delta32 allele, which our lab has previously shown to be related both
to AIDS resistance and postponement of AIDS. We have now estimated that
this allele is approximately 4300 years old, and is unique to Caucasians
and populations that have admixed with Caucasians. In the course of this
work we developed a new method for estimating the age of alleles.
Furthermore, the CCR5-delta32 allele is one of several alleles we are
studying that is largely unique to Caucasians. Such "Caucasian" alleles
that are segregating in the African-American population define regions
that will be especially useful for mapping by admixture linkage
disequilibrium (Z01 BC 05681-07 LGD).
The molecular evolution of the MHC is something of a paradox regarding
recombination, in that the well-documented linkage disequilibrium that
extends across the entire MHC suggests a reduced level of recombination,
yet phylogenetic analyses of constituent alleles (e.g., HLAB, DPB1)
suggest extensive inter-allelic recombination as a major source of
allelic diversity. A primary focus of this project is the improvement
of existing population genetic and evolutionary theories, especially
with regard to interpretation of patterns of linkage disequilibrium
under moderate levels of recombination. This includes improvement of the
existing algorithms for detecting recombination, and their application
to allelic sequences from MHC and other loci. We are currently studying
HLAA, -B, -C, and DPB1, with plans to address DRB1, DQA1, and DQB1. For
many MHC loci, the collection of alleles can be described as a series
of mosaic combinations of variable motifs. In this sense, each allele
is a haplotype, which makes linkage disequilibrium theory relevant as
well. We are starting to encounter the types of data exemplified by the
MHC (allele and haplotype frequencies, large numbers of alternative DNA
sequences) from other genomic regions, and these will require a more
rigorous approach to understanding their natural history. The immediate
challenge is that the analysis of such moderate to long range
"haplotypes" of variants embodies coalescence theory, linkage
disequilibrium, and phylogenetics. An underlying objective of these
studies is to be able to determine whether observed genic or allelic
associations are truly functional (e.g., disease related) or simply a
consequence of historic population genetic or evolutionary processes.
我们目前参与的几个项目打算解决
项目成果
期刊论文数量(0)
专著数量(0)
科研奖励数量(0)
会议论文数量(0)
专利数量(0)
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J C STEPHENS其他文献
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{{ truncateString('J C STEPHENS', 18)}}的其他基金
THEORETICAL INVESTIGATIONS OF GENETIC IDENTITY AND DISEQUILIBRIA
遗传同一性和不平衡的理论研究
- 批准号:
3774891 - 财政年份:
- 资助金额:
-- - 项目类别:
THEORETICAL INVESTIGATIONS OF GENETIC IDENTITY AND DISEQUILIBRIA
遗传同一性和不平衡的理论研究
- 批准号:
3838464 - 财政年份:
- 资助金额:
-- - 项目类别:
GENETIC, EVOLUTIONARY, AND PHYLOGENETIC ANALYSIS OF HUMAN ALLELES
人类等位基因的遗传、进化和系统发育分析
- 批准号:
2463671 - 财政年份:
- 资助金额:
-- - 项目类别:
INVESTIGATIONS OF GENETIC DISEQUILIBRIA AS GENE MAPPING STRATEGIES
作为基因图谱策略的遗传不平衡研究
- 批准号:
3752729 - 财政年份:
- 资助金额:
-- - 项目类别:
GENETIC, EVOLUTIONARY, AND PHYLOGENETIC ANALYSIS OF HUMAN ALLELES
人类等位基因的遗传、进化和系统发育分析
- 批准号:
5201542 - 财政年份:
- 资助金额:
-- - 项目类别:
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