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首页> 美国卫生研究院文献>Elsevier Sponsored Documents >Analysis of LIN28A in early human ovary development and as a candidate gene for primary ovarian insufficiency
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Analysis of LIN28A in early human ovary development and as a candidate gene for primary ovarian insufficiency

机译:LIN28A在人类早期卵巢发育中的分析以及作为原发性卵巢功能不全的候选基因的分析

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Lin28 proteins are emerging as important regulators of microRNAs in endocrine systems. Lin28a regulates primordial germ cell development and puberty timing in mice, whereas the related protein LIN28B is associated with age at menarche in genome-wide association studies in humans. Here, we studied expression of LIN28A and LIN28B in early human gonad development. LIN28A increased in the developing ovary between 6 and 9 weeks post conception, but not in the developing testis. Immunohistochemistry demonstrated LIN28A in peripheral germ cells. LIN28B was expressed at lower levels in both tissues and did not increase with time. As disruption of Lin28a affects germ cell development in mice, LIN28A was considered a candidate gene for primary ovarian insufficiency (POI) in humans. However, no significant changes were found in 50 women studied. These findings show LIN28A is strongly expressed in germ cells during early human ovary development, but disruption of LIN28A is not a common cause of POI.
机译:Lin28蛋白正在成为内分泌系统中microRNA的重要调节剂。 Lin28a调节小鼠原始生殖细胞的发育和青春期,而在人类的全基因组关联研究中,相关蛋白LIN28B与初潮的年龄有关。在这里,我们研究了LIN28A和LIN28B在早期人类性腺发育中的表达。 LIN28A在受孕后6至9周内在发育中的卵巢中增加,但在发育中的睾丸中则没有。免疫组织化学证明外周血生殖细胞中有LIN28A。 LIN28B在两个组织中均以较低的水平表达,并且不随时间增加。由于Lin28a的破坏影响小鼠生殖细胞的发育,因此LIN28A被认为是人类原发性卵巢功能不全(POI)的候选基因。但是,在研究的50名女性中,没有发现明显的变化。这些发现表明,LIN28A在人类早期卵巢发育过程中在生殖细胞中强烈表达,但LIN28A的破坏并不是POI的常见原因。

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