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日本杜兴氏和贝克氏肌肉营养不良患者的基因缺失

Gene deletions in Japanese patients with Duchenne and Becker muscular dystrophy.

作者信息

Asano J, Tomatsu S, Sukegawa K, Yamaguchi S, Ikedo Y, Minami R, Iida M, Nishimura M, Nakagawa M, Ohshiro M

机构信息

Department of Pediatrics, Gifu University, School of Medicine, Japan.

出版信息

Jinrui Idengaku Zasshi. 1990 Jun;35(2):159-68. doi: 10.1007/BF01876461.

Abstract

Thirty-eight unrelated Japanese patients with Duchenne and Becker muscular dystrophy (DMD and BMD) have been investigated with the DMD cDNA probes. The 14-kb DMD cDNA was subdivided into 6 subclones and HindIII-digested DNAs were analyzed by Southern blotting. Out of 38 unrelated patients, 14 showed a deletion of one or several of the exon-containing HindIII fragments (36.8%). These corresponded to 50% (9/18) of BMD patients and 25% (5/20) of DMD patients, and the position and extent of deletions were mapped and proved to be more heterogeneous in DMD than in BMD. Both ends of deletions detected in probe 1-2a were common to all six BMD patients without the maintenance of reading frame of messenger RNA, and 5' ends of deletions in probe 5b-7 were also common but maintained in frame in three BMD patients. The phenotypic-specific deletion in Japanese BMD patients has existed in the 5' end of the DMD gene, although its apparently similar deletion produced a wide range of clinical courses (BMD phenotype). There was no tight correlation between clinical severity and presence or absence of deletion in DMD or BMD.

摘要

我们使用杜兴肌营养不良症(DMD)cDNA探针,对38名无亲缘关系的日本杜兴和贝克型肌营养不良症(DMD和BMD)患者进行了研究。14kb的DMD cDNA被细分为6个亚克隆,并通过Southern印迹法分析经HindIII酶切的DNA。在38名无亲缘关系的患者中,14名患者(36.8%)显示出一个或几个含外显子的HindIII片段缺失。这些缺失对应于50%(9/18)的BMD患者和25%(5/20)的DMD患者,并且缺失的位置和范围已被定位,结果表明DMD中的缺失比BMD中的缺失更具异质性。在探针1-2a中检测到的缺失两端在所有6名信使RNA读码框未维持的BMD患者中是相同的,在探针5b-7中缺失的5'端在3名BMD患者中也是相同的,但读码框得以维持。日本BMD患者的表型特异性缺失存在于DMD基因的5'端,尽管其明显相似的缺失导致了广泛的临床病程(BMD表型)。DMD或BMD的临床严重程度与缺失的有无之间没有紧密的相关性。

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