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黄曲霉毒素 B1 对牛精子蛋白质组和胚胎转录组的影响。

Effect of aflatoxin B1 on bovine spermatozoa's proteome and embryo's transcriptome.

机构信息

The Hebrew University of Jerusalem, Robert H. Smith Faculty of Agriculture, Food and Environment, Rehovot, Israel.

Animal Sperm Research Center, Robert H. Smith Faculty of Agriculture, Food and Environment, Rehovot, Israel.

出版信息

Reproduction. 2020 Nov;160(5):709-723. doi: 10.1530/REP-20-0286.

Abstract

This study aims to evaluate the deleterious effect of the mycotoxin aflatoxin B1 (AFB1) on bull spermatozoa and the carryver effect on the developing embryo. Proteomic analysis of AFB1-treated spermatozoa revealed differential expression of proteins associated with biological processes and cellular pathways that involved in spermatozoon function, fertilization competence and embryonic development. Therefore, we assume that factors delivered by the spermatozoa, regardless of DNA fragmentation, are also involved. To confirm this hypothesis, we have used the annexin V (AV) kit to separate the spermatozoa into apoptotic (AV+) and non-apoptotic (AV-) subpopulations which were found to correlate with high- and low DNA fragmentation, respectively. Fertilization with AV+ AFB1-treated spermatozoa, resulted in no blastocyst formation, whereas fertilization with AV- spermatozoa resulted in reduced cleavage rate and formation of genetically altered blastocysts (POU5F1 and SOX2). Microarray analysis of blastocysts derived from 10 µM AFB1-treated spermatozoa revealed differential expression of 345 genes that involved in cellular pathways such as embryo and placenta development, cell cycle, DNA repair and histone modification, and in signaling pathways, especially calcium signaling pathway. This is the first report on deleterious carrying over effects of AFB1 from the bovine spermatozoa to the formed embryo. Our findings suggest that aside from the damage caused by AFB1 to spermatozoa's DNA integrity, additional damage mechanisms are involved.

摘要

本研究旨在评估真菌毒素黄曲霉毒素 B1(AFB1)对公牛精子的有害影响及其对胚胎发育的载体作用。AFB1 处理后的精子的蛋白质组分析揭示了与精子功能、受精能力和胚胎发育相关的生物过程和细胞途径相关的蛋白质的差异表达。因此,我们假设精子传递的因素,无论是否存在 DNA 碎片化,也可能参与其中。为了证实这一假设,我们使用 Annexin V(AV)试剂盒将精子分离为凋亡(AV+)和非凋亡(AV-)亚群,发现它们分别与高和低 DNA 碎片化相关。用 AV+AFB1 处理的精子进行受精,导致没有囊胚形成,而用 AV-精子进行受精则导致胚胎分裂率降低和形成遗传改变的囊胚(POU5F1 和 SOX2)。对来自 10µM AFB1 处理精子的囊胚进行的微阵列分析显示,345 个基因的表达存在差异,这些基因涉及胚胎和胎盘发育、细胞周期、DNA 修复和组蛋白修饰等细胞途径,以及钙信号通路等信号通路。这是关于 AFB1 从牛精子到形成的胚胎的有害传递作用的首次报道。我们的研究结果表明,除了 AFB1 对精子 DNA 完整性造成的损害外,还涉及其他损伤机制。

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