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人类染色体19q13区域的远距离限制酶切图谱:肌酸激酶M亚基(CKMM)与ERCC1和ERCC2基因之间紧密的物理连锁关系。

A long-range restriction map of the human chromosome 19q13 region: close physical linkage between CKMM and the ERCC1 and ERCC2 genes.

作者信息

Smeets H, Bachinski L, Coerwinkel M, Schepens J, Hoeijmakers J, van Duin M, Grzeschik K H, Weber C A, de Jong P, Siciliano M J

机构信息

Department of Human Genetics, University of Nijmegen, The Netherlands.

出版信息

Am J Hum Genet. 1990 Mar;46(3):492-501.

Abstract

We report on the physical ordering of genes in a relatively small area of chromosome 19, segment q13, containing the locus for myotonic dystrophy (DM), the most frequent heritable muscular dystrophy of adulthood in man. DNAs from somatic cell hybrids with der 19q products that carry a breakpoint across the muscle-specific creatine kinase (CKMM) gene were analyzed by Southern blotting using probes for CKMM, APOC2, and the repair genes ERCC1 and ERCC2. Results were combined with data from CHEF and field inversion-gel-electrophoresis separation of large-sized DNA restriction fragments to establish a map localizing both DNA-repair genes and the CKMM gene within the same 250 kb of DNA, the order being cen-CKMM-ERCC2-ERCC1-ter, with APOC2 being at more than 260 kb proximal to CKMM. Transcriptional start sites of the CKMM and DNA-repair genes are all on the telomeric side of the genes. Our results provide a framework for the construction of a larger physical map of the area, which will facilitate the search for the DM gene.

摘要

我们报道了19号染色体相对较小区域q13片段中基因的物理排序,该区域包含强直性肌营养不良(DM)的基因座,DM是人类成年期最常见的遗传性肌营养不良。利用肌肉特异性肌酸激酶(CKMM)基因、载脂蛋白C2(APOC2)以及修复基因ERCC1和ERCC2的探针,通过Southern印迹法分析了来自携带横跨CKMM基因断点的der 19q产物的体细胞杂种的DNA。结果与脉冲场凝胶电泳(CHEF)和场反转凝胶电泳分离大尺寸DNA限制片段的数据相结合,以建立一个定位DNA修复基因和CKMM基因于同一250kb DNA区域内的图谱,顺序为着丝粒-CKMM-ERCC2-ERCC1-端粒,APOC2位于CKMM近端超过260kb处。CKMM和DNA修复基因的转录起始位点均在基因的端粒侧。我们的结果为构建该区域更大的物理图谱提供了框架,这将有助于寻找DM基因。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8e0e/1683630/e45ae1242809/ajhg00100-0093-a.jpg

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