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新生仔鼠接触双酚 A 后精子中 Igf2-H19 印迹控制区异常的 DNA 甲基化及其与植入后丢失的关系。

Aberrant DNA methylation at Igf2-H19 imprinting control region in spermatozoa upon neonatal exposure to bisphenol A and its association with post implantation loss.

机构信息

National Center for Preclinical Reproductive and Genetic Toxicology, National Institute for Research in Reproductive Health (ICMR), J M Street, Parel, Mumbai, 400012, Maharashtra, India.

出版信息

Mol Biol Rep. 2013 Aug;40(8):4747-57. doi: 10.1007/s11033-013-2571-x. Epub 2013 May 8.

Abstract

Bisphenol A (BPA) is an estrogenic compound commonly used in manufacture of various consumer products. Earlier studies from our group have demonstrated that neonatal exposure of male rats to BPA causes decrease in sperm count and motility, increase in post implantation loss, ultimately leading to subfertility during adulthood. One of the factors contributing for post implantation loss is altered methylation pattern of imprinted genes. The present study was undertaken to investigate the molecular effects of neonatal exposure of male rats to BPA (2.4 μg/pup) (F0) on the methylation of H19 imprinting control region (ICR) in resorbed embryo (F1) and compared with spermatozoa of their respective sires (F0). We observed a significant down regulation in the transcript expression of Igf2 and H19 genes in BPA resorbed embryo (F1) as compared to control viable embryo. A significant hypomethylation was observed at the H19 ICR in the spermatozoa as well as in resorbed embryo sired by rats exposed neonatally to BPA. These results indicated that the aberrant methylation at ICR in spermatozoa was inherited by embryo which causes perturbation in the expression of Igf2 and H19, ultimately leading to post implantation loss. This could be one of the possible mechanisms of BPA induced adverse epigenetic effects on male fertility.

摘要

双酚 A(BPA)是一种常用于制造各种消费品的雌激素化合物。我们小组的早期研究表明,新生雄性大鼠暴露于 BPA 会导致精子数量和活力下降、着床后损失增加,最终导致成年后不育。导致着床后损失的因素之一是印迹基因的甲基化模式改变。本研究旨在研究新生雄性大鼠暴露于 BPA(2.4μg/幼仔)(F0)对吸收胚胎(F1)中 H19 印迹控制区(ICR)甲基化的分子影响,并与各自亲代精子进行比较(F0)。我们观察到 BPA 吸收胚胎(F1)中 Igf2 和 H19 基因的转录表达水平明显下调,与对照存活胚胎相比。在经 BPA 新生暴露的大鼠的精子和吸收胚胎中,在 H19 ICR 处观察到明显的低甲基化。这些结果表明,精子中 ICR 的异常甲基化被胚胎继承,导致 Igf2 和 H19 的表达失调,最终导致着床后损失。这可能是 BPA 对雄性生育力产生不利表观遗传影响的可能机制之一。

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