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用于分析酒精相关多基因多效性的选择性育种、同类系以及其他经典遗传学方法。

Selective breeding, congenic strains, and other classical genetic approaches to the analysis of alcohol-related polygenic pleiotropisms.

作者信息

Dudek B C, Underwood K A

机构信息

Department of Psychology, SUNY, Albany 12222.

出版信息

Behav Genet. 1993 Mar;23(2):179-89. doi: 10.1007/BF01067423.

Abstract

Dimensions of behavioral sensitivities to alcohol in mice are under control of polygenic systems of relatively small size. The mode of inheritance of these phenotypes is frequently additive, with no evidence of dominance, epistasis, or sex linkage. The utility of classical breeding methodologies, such as selection, for assessment of genetic correlations is reviewed. A distinction is drawn between pleiotropisms in these polygenic systems, and the statistical concept of a genetic correlation. Development of congenic strains is argued to be a powerful alternative methodology, heretofore unused in alcohol pharmacogenetics. Using the phenotype of behavioral activation produced by a low dose of ethanol, we describe the production of an activated congenic strain on the non-activated background of the C57BL/6 mouse strain. Through five generations of repeated backcrossing, from a genetically heterogenous stock, "activational" alleles are being successfully transferred to the C57BL/6 background. Theoretical issues in the creation of congenic strains in potentially polygenic systems are covered, including number of effective loci and heritability.

摘要

小鼠对酒精行为敏感性的维度受相对较小的多基因系统控制。这些表型的遗传模式通常是累加的,没有显性、上位性或性连锁的证据。本文综述了经典育种方法(如选择)在评估遗传相关性方面的效用。区分了这些多基因系统中的多效性与遗传相关性的统计概念。有人认为,近交系的培育是一种强大的替代方法,此前在酒精药物遗传学中未被使用。利用低剂量乙醇产生的行为激活表型,我们描述了在C57BL/6小鼠品系的非激活背景上产生激活近交系的过程。通过五代重复回交,从遗传异质群体中,“激活”等位基因成功转移到C57BL/6背景中。文中涵盖了在潜在多基因系统中创建近交系的理论问题,包括有效基因座的数量和遗传力。

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