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小鼠11号染色体的综合遗传图谱揭示了小鼠和人类之间广泛的连锁保守性。

A comprehensive genetic map of murine chromosome 11 reveals extensive linkage conservation between mouse and human.

作者信息

Buchberg A M, Brownell E, Nagata S, Jenkins N A, Copeland N G

机构信息

Mammalian Genetics Laboratory, NCI-Frederick Cancer Research Facility, Maryland 21701.

出版信息

Genetics. 1989 May;122(1):153-61. doi: 10.1093/genetics/122.1.153.

DOI:10.1093/genetics/122.1.153
PMID:2567264
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1203679/
Abstract

Interspecific backcross animals from a cross between C57BL/6J and Mus spretus mice were used to generate a comprehensive linkage map of mouse chromosome 11. The relative map positions of genes previously assigned to mouse chromosome 11 by somatic cell hybrid or genetic backcross analysis were determined (Erbb, Rel, 11-3, Csfgm, Trp53-1, Evi-2, Erba, Erbb-2, Csfg, Myhs, Cola-1, Myla, Hox-2 and Pkca). We also analyzed genes that we suspected would map to chromosome 11 by virtue of their location in human chromosomes and the known linkage homologies that exist between murine chromosome 11 and human chromosomes (Mpo, Ngfr, Pdgfr and Fms). Two of the latter genes, Mpo and Ngfr, mapped to mouse chromosome 11. Both genes also mapped to human chromosome 17, extending the degree of linkage conservation observed between human chromosome 17 and mouse chromosome 11. Pdgfr and Fms, which are closely linked to II-3 and Csfgm in humans on chromosome 5, mapped to mouse chromosome 18 rather than mouse chromosome 11, thereby defining yet another conserved linkage group between human and mouse chromosomes. The mouse chromosome 11 linkage map generated in these studies substantially extends the framework for identifying homologous genes in the mouse that are involved in human disease, for elucidating the genes responsible for several mouse mutations, and for gaining insights into chromosome evolution and genome organization.

摘要

利用C57BL/6J小鼠和西班牙小鼠杂交产生的种间回交动物,构建了小鼠11号染色体的综合连锁图谱。确定了先前通过体细胞杂交或遗传回交分析定位到小鼠11号染色体上的基因的相对图谱位置(Erbb、Rel、11 - 3、Csfgm、Trp53 - 1、Evi - 2、Erba、Erbb - 2、Csfg、Myhs、Cola - 1、Myla、Hox - 2和Pkca)。我们还分析了一些基因,这些基因由于其在人类染色体上的位置以及小鼠11号染色体与人类染色体之间已知的连锁同源性,我们怀疑它们会定位到11号染色体上(Mpo、Ngfr、Pdgfr和Fms)。后两个基因中的Mpo和Ngfr定位到了小鼠11号染色体上。这两个基因也定位到了人类17号染色体上,扩展了在人类17号染色体和小鼠11号染色体之间观察到的连锁保守程度。在人类中与5号染色体上的II - 3和Csfgm紧密连锁的Pdgfr和Fms,定位到了小鼠18号染色体而不是小鼠11号染色体上,从而确定了人类和小鼠染色体之间的另一个保守连锁群。在这些研究中产生的小鼠11号染色体连锁图谱极大地扩展了用于识别参与人类疾病的小鼠同源基因、阐明导致几种小鼠突变的基因以及深入了解染色体进化和基因组组织的框架。

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