Love D R, England S B, Speer A, Marsden R F, Bloomfield J F, Roche A L, Cross G S, Mountford R C, Smith T J, Davies K E
Molecular Genetics Group, John Radcliffe Hospital, Headington, England.
Genomics. 1991 May;10(1):57-67. doi: 10.1016/0888-7543(91)90484-v.
The Duchenne muscular dystrophy locus is remarkable in that it shows a high mutation rate and the majority of mutations found are deletions. These deletions are generated as meiotic as well as mitotic events and occur preferentially in the central region of the gene. Nothing is known so far about the mechanisms involved. This paper reports the first sequencing of deletion junctions in the dystrophin gene. The data from a study of two patients with deletions in the central region of dystrophin show the breakpoints to lie in regions of introns in which stretches of dA-dT are seen. The relationship between these observations and possible mechanisms for the mutations is discussed.
杜氏肌营养不良基因座很显著,因为它显示出高突变率,并且所发现的大多数突变都是缺失突变。这些缺失突变是在减数分裂以及有丝分裂事件中产生的,并且优先发生在该基因的中央区域。到目前为止,对于其中涉及的机制尚一无所知。本文报道了肌营养不良蛋白基因中缺失连接点的首次测序。对两名在肌营养不良蛋白中央区域有缺失的患者的研究数据表明,断点位于内含子中可见dA-dT序列的区域。本文讨论了这些观察结果与可能的突变机制之间的关系。
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