少有人走过的路:从果蝇和人类的基因型到表现型。

Robert R H Anholt, Trudy F C Mackay
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引用次数: 25

摘要

了解基因组变异如何引起表型变异,对于阐明适应性进化、动植物育种和精准医学的机制至关重要。然而,在人类群体中,由于基因组中大量的连锁不平衡以及异质性的发育历史、生活方式、社会和物理环境,确定DNA序列变异和表型变异之间的因果关系是具有挑战性的。黑腹果蝇提供了一个强大的遗传模型,因为连锁不平衡迅速消退,促进了与表型变异相关的多态性的因果关系分配,并且可以在确定的环境条件下,经济地,不受监管限制地饲养大量个体。黑腹果蝇遗传参考小组(DGRP)是一个由205只测序的近交野生果蝇组成的种群,它使形态学、生理、行为和生活史性状的全基因组关联研究成为可能,并证明了复杂性状的遗传结构具有高度的多基因性、两性二态性和背景依赖性,具有广泛的性别、环境和遗传背景(上位性)效应。这些特征与转录组的模块化组织一起说明了复杂性状的动态整合遗传结构。果蝇复杂性状遗传结构的复杂性为人类群体遗传研究的解释提供了重要的警告。复杂性状的遗传基础方面可以表示为简化的基因网络,在此网络上可以叠加人类同源物,为随后对人类种群中类似性状的研究提供蓝图。果蝇复杂性状遗传结构的基本原理可能适用于从DGRP到人类种群的所有门。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The road less traveled: from genotype to phenotype in flies and humans.

Understanding how genomic variation gives rise to phenotypic variation is essential for elucidating mechanisms of adaptive evolution, plant and animal breeding, and precision medicine. However, identifying causal links between DNA sequence variants and variation in phenotypes is challenging in human populations, due to large blocks of linkage disequilibrium in the genome and heterogeneous developmental histories, lifestyles, and social and physical environments. Drosophila melanogaster presents a powerful genetic model, since linkage disequilibrium decays rapidly, facilitating assignment of causality to polymorphisms associated with phenotypic variation, and large numbers of individuals can be reared under defined environmental conditions, economically, and without regulatory restrictions. The D. melanogaster Genetic Reference Panel (DGRP), a population of 205 sequenced, inbred wild-derived flies, has enabled genome-wide association studies of morphological, physiological, behavioral, and life history traits, and demonstrated that genetic architectures of complex traits are highly polygenic, sexually dimorphic, and context dependent with extensive sex-, environment-, and genetic background (epistatic) effects. These features together with a modular organization of the transcriptome illustrate a dynamic integrative genetic architecture for complex traits. The complexity of the genetic architectures for complex traits in Drosophila provides important caveats for the interpretation of genetic studies in human populations. Aspects of the genetic underpinnings of complex traits can be represented as simplified gene networks on which human orthologues can be superimposed to provide blueprints for subsequent studies on analogous traits in human populations. Fundamental principles of the genetic architectures of Drosophila complex traits are likely applicable across phyla, from the DGRP to human populations.

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