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Inheritance and Mapping of Compact (Cmpt) a New Mutation Causing Hypermuscularity in Mice

机译:致密基因(Cmpt)的继承与映射致密基因(Cmpt)是一种引起小鼠超肌肉性的新突变

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摘要

During selection for protein content in mice at the Technical University of Berlin, individuals showing high protein content and a compact exterior were noted. Animals showing this ``Compact'' phenotype were separated to form a new line. The present investigations were carried out on a Hungarian subpopulation of this line, selected for maximum expression of the Compact phenotype, and apparently at fixation for the relevant genes. Fertility and viability of the Compact subpopulation was normal. As compared to normal mice, carcass percentage values for male and female Compact mice were 9.4 and 6.8% greater, respectively; and the muscle:bone weight ratio in males was 1.61-fold greater. The Compact phenotype showed variable expressivity and was of intermediate dominance in males, but almost fully recessive in females. The hypothesis that a single gene is solely responsible for the Compact phenotype was rejected by maximum likelihood analysis. Linkage mapping using selective DNA pooling located a single locus (denoted Cmpt) strongly associated with the Compact phenotype on mouse chromosome 1. Fine mapping, using individual selective genotyping and haplotype analysis, located Cmpt to the region between D1Mit375 and D1Mit21, approximately one third of the way to D1Mit21.
机译:在柏林工业大学为小鼠选择蛋白质含量时,注意到个体显示出较高的蛋白质含量和紧凑的外观。显示这种``紧凑''表型的动物被分离以形成新系。目前的研究是针对该品系的匈牙利亚群进行的,选择该基因是为了使致密表型最大化表达,并且显然在固定相关基因的过程中。紧凑型亚群的生育力和生存力是正常的。与正常小鼠相比,雄性和雌性紧凑型小鼠的car体百分比值分别增加了9.4和6.8%。男性的肌肉与骨骼重量比增加了1.61倍。紧密表型表现出可变的表达能力,在男性中处于中等优势地位,但在女性中几乎完全处于隐性地位。最大似然分析拒绝了单个基因完全负责致密表型的假设。使用选择性DNA池进行的连锁作图定位了一个与小鼠染色体1上的紧密表型密切相关的单一基因座(表示为Cmpt)。使用单独的选择性基因分型和单倍型分析,将Cmpt定位于D1Mit375和D1Mit21之间的区域,约占三分之一。通往D1Mit21的方式。

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