首页> 美国卫生研究院文献>American Journal of Human Genetics >A human homologue of the Drosophila melanogaster diaphanous gene is disrupted in a patient with premature ovarian failure: evidence for conserved function in oogenesis and implications for human sterility.
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A human homologue of the Drosophila melanogaster diaphanous gene is disrupted in a patient with premature ovarian failure: evidence for conserved function in oogenesis and implications for human sterility.

机译:卵巢早衰患者的果蝇腹透性基因的人类同源物被破坏:卵子发生中的保守功能及其对人类不育的影响的证据。

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摘要

Premature ovarian failure (POF) is a defect of ovarian development and is characterized by primary or secondary amenorrhea, with elevated levels of serum gonadotropins, or by early menopause. The disorder has been attributed to various causes, including rearrangements of a large "critical region" in the long arm of the X chromosome. Here we report identification, in a family with POF, of a gene that is disrupted by a breakpoint. The gene is the human homologue of the Drosophila melanogaster diaphanous gene; mutated alleles of this gene affect spermatogenesis or oogenesis and lead to sterility. The protein (DIA) encoded by the human gene (DIA) is the first human member of the growing FH1/FH2 protein family. Members of this protein family affect cytokinesis and other actin-mediated morphogenetic processes that are required in early steps of development. We propose that the human DIA gene is one of the genes responsible for POF and that it affects the cell divisions that lead to ovarian follicle formation.
机译:卵巢早衰(POF)是卵巢发育的缺陷,其特征是原发性或继发性闭经,血清促性腺激素水平升高或更年期提前。该疾病归因于各种原因,包括X染色体长臂中的大“关键区域”的重排。在这里,我们报告在一个患有POF的家庭中鉴定出一个被断点破坏的基因。该基因是果蝇腹透性基因的人类同源物;该基因的突变等位基因影响精子发生或卵子发生并导致不育。由人类基因(DIA)编码的蛋白质(DIA)是正在成长的FH1 / FH2蛋白质家族的第一个人类成员。该蛋白家族的成员影响发育早期所需的胞质分裂和其他肌动蛋白介导的形态发生过程。我们建议人类DIA基因是负责POF的基因之一,并且它影响导致卵巢卵泡形成的细胞分裂。

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