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亚砷酸盐及其甲基化三价代谢物的体外暴露改变了小鼠精子细胞中的基因转录。

Ex vivo exposures to arsenite and its methylated trivalent metabolites alter gene transcription in mouse sperm cells.

机构信息

Department of Nutrition, Gillings School of Global Public Health, The University of North Carolina at Chapel Hill, USA.

Department of Nutrition, Gillings School of Global Public Health, The University of North Carolina at Chapel Hill, USA; Department of Environmental Science and Engineering, Gillings School of Global Public Health, The University of North Carolina at Chapel Hill, USA.

出版信息

Toxicol Appl Pharmacol. 2022 Nov 15;455:116266. doi: 10.1016/j.taap.2022.116266. Epub 2022 Oct 7.

Abstract

We have previously reported that preconception exposure to iAs may contribute to the development of diabetes in mouse offspring by altering gene expressions in paternal sperm. However, the individual contributions of iAs and its methylated metabolites, monomethylated arsenic (MAs) and dimethylated arsenic (DMAs), to changes in the sperm transcriptome could not be determined because all three As species are present in sperm after in vivo iAs exposure. The goal of the present study was to assess As species-specific effects using an ex vivo model. We exposed freshly isolated mouse sperm to either 0.1 or 1 μM arsenite (iAs) or the methylated trivalent arsenicals, MAs and DMAs, and used RNA-sequencing to identify differentially expressed genes, enriched pathways, and associated protein networks. For all arsenicals tested, the exposures to 0.1 μM concentrations had greater effects on gene expression than 1 μM exposures. Transcription factor AP-1 and B cell receptor complexes were the most significantly enriched pathways in sperm exposed to 0.1 μM iAs. The Mre11 complex and Antigen processing were top pathways targeted by exposure to 0.1 μM MAs and DMAs, respectively. While there was no overlap between gene transcripts altered by ex vivo exposures in the present study and those altered by in vivo exposure in our prior work, several pathways were shared, including PI3K-Akt signaling, Focal adhesion, and Extracellular matrix receptor interaction pathways. Notably, the protein networks associated with these pathways included those with known roles in diabetes. This study is the first to assess the As species-specific effects on sperm transcriptome, linking these effects to the diabetogenic effects of iAs exposure.

摘要

我们之前曾报道过,亲代精子中基因表达的改变可能导致受孕前 iAs 的暴露导致后代小鼠发生糖尿病。然而,由于在体内 iAs 暴露后精子中存在三种 As 物种,因此无法确定 iAs 及其甲基化代谢物单甲基砷(MAs)和二甲基砷(DMAs)对精子转录组变化的个体贡献。本研究的目的是使用离体模型评估 As 物种特异性的影响。我们将新鲜分离的小鼠精子暴露于 0.1 或 1μM 亚砷酸盐(iAs)或甲基化三价砷化合物 MAs 和 DMAs 中,然后使用 RNA 测序来鉴定差异表达基因、富集途径和相关蛋白质网络。对于所有测试的砷化合物,0.1μM 浓度的暴露比 1μM 浓度的暴露对基因表达的影响更大。在 0.1μM iAs 暴露的精子中,AP-1 转录因子和 B 细胞受体复合物是最显著富集的途径。Mre11 复合物和抗原处理分别是 0.1μM MAs 和 DMAs 暴露的最重要途径。虽然本研究中离体暴露改变的基因转录本与我们之前研究中体内暴露改变的基因转录本之间没有重叠,但有几个途径是共享的,包括 PI3K-Akt 信号通路、黏附斑和细胞外基质受体相互作用途径。值得注意的是,与这些途径相关的蛋白质网络包括已知在糖尿病中起作用的那些。这项研究首次评估了 As 物种对精子转录组的特异性影响,将这些影响与 iAs 暴露的致糖尿病作用联系起来。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6de4/9753555/cc7709cad8e5/nihms-1850641-f0001.jpg

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