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小鼠的数量性状基因座分析与全基因组诱变:剖析复杂性状的互补遗传方法。

QTL analysis and genomewide mutagenesis in mice: complementary genetic approaches to the dissection of complex traits.

作者信息

Belknap J K, Hitzemann R, Crabbe J C, Phillips T J, Buck K J, Williams R W

机构信息

Research Service, Veterans Affairs Medical Center, Portland, Oregon 97201, USA.

出版信息

Behav Genet. 2001 Jan;31(1):5-15. doi: 10.1023/a:1010249607128.

Abstract

Quantitative genetics and quantitative trait locus (QTL) mapping have undergone a revolution in the last decade. Progress in the next decade promises to be at least as rapid, and strategies for fine-mapping QTLs and identifying underlying genes will be radically revised. In this Commentary we address several key issues: first, we revisit a perennial challenge--how to identify individual genes and allelic variants underlying QTLs. We compare current practice and procedures in QTL analysis with novel methods and resources that are just now being introduced. We argue that there is no one standard of proof for showing QTL = gene; rather, evidence from several sources must be carefully assembled until there is only one reasonable conclusion. Second, we compare QTL analysis with whole-genome mutagenesis in mice and point out some of the strengths and weakness of both of these phenotype-driven methods. Finally, we explore the advantages and disadvantages of naturally occurring vs mutagen-induced polymorphisms. We argue that these two complementary genetic methods have much to offer in efforts to highlight genes and pathways most likely to influence the susceptibility and progression of common diseases in human populations.

摘要

在过去十年中,数量遗传学和数量性状基因座(QTL)定位经历了一场变革。未来十年的进展有望同样迅速,精细定位QTL和鉴定潜在基因的策略将被彻底修订。在这篇评论中,我们探讨几个关键问题:首先,我们重新审视一个长期存在的挑战——如何鉴定QTL潜在的单个基因和等位基因变体。我们将QTL分析中的当前实践和程序与刚刚引入的新方法和资源进行比较。我们认为,证明QTL = 基因没有单一的标准;相反,必须仔细整合来自多个来源的证据,直到只有一个合理的结论。其次,我们将QTL分析与小鼠全基因组诱变进行比较,并指出这两种表型驱动方法的一些优缺点。最后,我们探讨自然发生的多态性与诱变诱导的多态性的优缺点。我们认为,这两种互补的遗传方法在突出最有可能影响人类群体常见疾病易感性和进展的基因和途径方面有很大的贡献。

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