首页> 美国卫生研究院文献>The EMBO Journal >Detection of a high frequency RsaI polymorphism in the human pro alpha 2(I) collagen gene which is linked to an autosomal dominant form of osteogenesis imperfecta.
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Detection of a high frequency RsaI polymorphism in the human pro alpha 2(I) collagen gene which is linked to an autosomal dominant form of osteogenesis imperfecta.

机译:检测人类亲α2(I)胶原基因中的高频RsaI多态性该基因与成骨不全症的常染色体显性形式有关。

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摘要

Screening of the pro alpha 2(I) collagen genes of Southern African populations for restriction fragment length polymorphisms (RFLPs) has revealed a locus polymorphic for the restriction enzyme RsaI. The frequency of the RFLP was 0.38 in Afrikaners, but much lower in indigenous Southern African populations, which suggests that it is of European origin. The polymorphism was used to study 19 affected and non-affected individuals in a four generation family with the autosomal dominant disorder, osteogenesis imperfecta (OI) type I. Co-inheritance of the loss of the RsaI site and the OI phenotype was observed with a lod score of 3.91 at a recombination fraction (theta) of zero, indicating strong linkage. This suggests that the defect in this family is caused by a structural mutation within or close to the pro alpha 2(I) collagen gene. The use of this high frequency RFLP together with other recently described polymorphisms at this locus will facilitate the analysis of the role of this gene in OI and other inherited disorders of connective tissue.
机译:南部非洲人群的亲α2(I)胶原基因的限制性片段长度多态性(RFLP)的筛选已显示出限制性酶RsaI的基因座多态性。在南非荷兰语中,RFLP的频率为0.38,但在南部非洲土著人口中较低,这表明它起源于欧洲。该多态性用于研究四代家庭中常染色体显性遗传疾病(I型成骨不全症(OI))的19个患病和未患病个体。观察到RsaI位点缺失和OI表型的共同遗传在重组分数(theta)为零的情况下,lod得分为3.91,表明有很强的联系。这表明该家族中的缺陷是由pro alpha 2(I)胶原基因内部或附近的结构突变引起的。在此基因座处使用这种高频RFLP以及其他最近描述的多态性将有助于分析该基因在OI和其他遗传性结缔组织疾病中的作用。

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