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强直性肌营养不良基因座定位于19q13.2 - 19q13.3及其与19q上12个多态性基因座的关系。

Localisation of the myotonic dystrophy locus to 19q13.2-19q13.3 and its relationship to twelve polymorphic loci on 19q.

作者信息

Harley H G, Walsh K V, Rundle S, Brook J D, Sarfarazi M, Koch M C, Floyd J L, Harper P S, Shaw D J

机构信息

Institute of Medical Genetics, University of Wales College of Medicine, Health Park, Cardiff, UK.

出版信息

Hum Genet. 1991 May;87(1):73-80. doi: 10.1007/BF01213096.

Abstract

The order of fourteen polymorphic markers localised to the long arm of human chromosome 19 has been established by multipoint mapping in a set of 40 CEPH (Centre d'Etude de Polymorphisme Humain, Paris) reference families. We report here the linkage relationship of the myotonic dystrophy (DM) locus to twelve of these markers as studied in 45 families with DM. The resulting genetic map is supported by the localisation of the DNA markers in a panel of somatic cell hybrids. Ten of the twelve markers have been shown to be proximal to the DM gene and two, PRKCG and D19S22, distal but at distances of approximately 25 cM and 15 cM, respectively. The closest proximal markers are APOC2 (apolipoprotein C-II) and CKM (creatine kinase, muscle) approximately 3 cM and 2 cM from the DM gene respectively, in the order APOC2-CKM-DM. The distance between APOC2, CKM and DM (of the order of 2 million base pairs) and their known orientation should permit directional chromosome walking and jumping. The data presented here should enable us to determine whether or not new markers are distal to APOC2/CKM and thus potentially flank the DM gene.

摘要

通过对40个CEPH(巴黎人类多态性研究中心)参考家系进行多点定位,已确定了位于人类19号染色体长臂上的14个多态性标记的顺序。我们在此报告了在45个患有强直性肌营养不良(DM)的家系中研究的DM基因座与其中12个标记之间的连锁关系。所得的遗传图谱得到了一组体细胞杂种中DNA标记定位的支持。12个标记中的10个已显示位于DM基因近端,另外两个,即蛋白激酶Cγ(PRKCG)和D19S22,位于远端,但距离分别约为25厘摩和15厘摩。最接近的近端标记是载脂蛋白C-II(APOC2)和肌酸激酶(肌肉型,CKM),它们与DM基因的距离分别约为3厘摩和2厘摩,顺序为APOC2-CKM-DM。APOC2、CKM与DM之间的距离(约200万个碱基对)及其已知的方向应有助于进行定向染色体步移和跳跃。本文提供的数据应使我们能够确定新标记是否位于APOC2/CKM的远端,从而有可能位于DM基因两侧。

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