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首页> 外文期刊>Srpski Arhiv za Celokupno Lekarstvo >Duchenne's/Becker's muscular dystrophy: Analysis of genotype-feno-type correlation in 28 patients
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Duchenne's/Becker's muscular dystrophy: Analysis of genotype-feno-type correlation in 28 patients

机译:Duchenne / Becker肌营养不良症:28例患者的基因型-feno型相关性分析

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Duchenne's and Becker's muscular dystrophy (DMD & BMD) is a X linked disease caused by mutations in the dystrophic gene. DMD is the malign form of the disease, which significantly shortens the lifetime of the patient, while BMD has late onset with slow progression. Sixty five percent of DMD and BMD cases are caused by deletion of one or more exons in the dystrophic gene, while duplications cause these diseases in 6 to 7% of the cases. There are two hot spots for deletions and duplications. These are exons in the proximal part of the gene (3rd to 18th) and exons of a distal part of the gene (45th to 52nd). The remaining 30% of DMD and BMD cases are caused by point mutations, small deletions or inversions in the dystrophic gene. The correlation between School of Medicine, University of Belgrade, Belgrade the severity of the disease and the position of deletion shows that most of the out of frame deletions cause DMD phenotype, while in frame deletions result in BMD pheno-type. We report on the results of 28 non-related DMD and BMD patients. In 57% of cases deletions were detected and all were found in the distal hot spot of the gene. These results suggest that in most of the cases, out of frame deletions produce DMD phenotype while in frame deletions result in BMD phenotype. This is in compliance with data from literature.
机译:杜兴氏和贝克氏肌营养不良症(DMD&BMD)是由营养不良性基因突变引起的X连锁疾病。 DMD是该疾病的恶性形式,大大缩短了患者的生命,而BMD起病较晚,进展缓慢。百分之六十五的DMD和BMD病例是由于营养不良基因中一个或多个外显子的缺失而引起的,而重复则在6%至7%的病例中引起这些疾病。删除和重复有两个热点。这些是基因近端部分(第3至18位)的外显子和基因远端部分(第45至52位)的外显子。其余30%的DMD和BMD病例是由营养不良基因的点突变,微小缺失或倒位引起的。贝尔格莱德大学医学院的疾病严重程度与缺失位置之间的相关性表明,大多数无框缺失导致DMD表型,而在框内缺失则导致BMD表型。我们报告了28名非相关DMD和BMD患者的结果。在57%的病例中,检测到缺失,并且全部在基因的远端热点中发现。这些结果表明,在大多数情况下,框外缺失产生DMD表型,而框内缺失导致BMD表型。这符合文献数据。

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