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对121例具有I型蛋白C缺乏症的连续有症状法国患者中的90例进行突变鉴定。法国国家卫生与医学研究所负责蛋白C和蛋白S缺乏症分子异常的网络研究。

Identification of mutations in 90 of 121 consecutive symptomatic French patients with a type I protein C deficiency. The French INSERM Network on Molecular Abnormalities Responsible for Protein C and Protein S deficiencies.

作者信息

Gandrille S, Aiach M

机构信息

INSERM U 428, Unité de Formation et de Recherche (UFR) des Sciences Pharmaceutiques et Biologiques, Paris, France.

出版信息

Blood. 1995 Oct 1;86(7):2598-605.

PMID:7670104
Abstract

By studying the protein C gene of 121 consecutive patients with symptomatic type I protein C deficiency, we detected 55 different candidate mutations in 90 cases. The mutations, 76% of which were missense changes, were distributed throughout the gene. More than half the missense mutations involved Cys, Phe, Pro, or Gly, amino acids known to affect the structure of the polypeptide chain by various mechanisms. Thus, 40% of protein C deficiencies may be caused by polypeptide chain instability rather than a lack of expression of the mutated allele; this may also account for phenotypic heterogeneity. Seventeen of the 55 different mutations were found in apparently unrelated families. Half the French families we studied bore one of these 17 mutations. The wide variety of mutations suggests that both sporadic cases and a founder effect contribute to the spectrum of protein C mutations in a given population. The differences in both unique and recurrent mutations in French and Dutch populations-the only large population samples so far studied-support this hypothesis.

摘要

通过研究121例连续性有症状的I型蛋白C缺乏症患者的蛋白C基因,我们在90例患者中检测到55种不同的候选突变。这些突变分布于整个基因,其中76%为错义突变。超过半数的错义突变涉及半胱氨酸(Cys)、苯丙氨酸(Phe)、脯氨酸(Pro)或甘氨酸(Gly),这些氨基酸已知可通过多种机制影响多肽链的结构。因此,40%的蛋白C缺乏症可能是由多肽链不稳定引起的,而非突变等位基因表达缺失;这也可能解释了表型异质性。55种不同突变中的17种在明显无亲缘关系的家族中被发现。我们研究的法国家族中有一半带有这17种突变中的一种。突变种类繁多表明,散发病例和奠基者效应均对特定人群中蛋白C突变谱有影响。法国和荷兰人群(目前仅有的两个大规模人群样本)中独特突变和复发突变的差异支持了这一假说。

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