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GRTH/DDX25 介导的精子发生中小鼠圆形精子细胞的 miRNA 表达谱:mRNA-miRNA 网络分析。

miRNA Expression Profiles of Mouse Round Spermatids in GRTH/DDX25-Mediated Spermiogenesis: mRNA-miRNA Network Analysis.

机构信息

Section on Molecular Endocrinology, Division of Developmental Biology, Eunice Kennedy Shriver National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, MD 20892, USA.

Bioinformatics and Scientific Programming Core, Eunice Kennedy Shriver National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Cells. 2023 Feb 27;12(5):756. doi: 10.3390/cells12050756.

Abstract

GRTH/DDX25 is a testis-specific DEAD-box family of RNA helicase, which plays an essential role in spermatogenesis and male fertility. There are two forms of GRTH, a 56 kDa non-phosphorylated form and a 61 kDa phosphorylated form (pGRTH). GRTH-KO and GRTH Knock-In (KI) mice with R242H mutation (lack pGRTH) are sterile with a spermatogenic arrest at step 8 of spermiogenesis due to failure of round spermatids (RS) to elongate. We performed mRNA-seq and miRNA-seq analysis on RS of WT, KI, and KO to identify crucial microRNAs (miRNAs) and mRNAs during RS development by establishing a miRNA-mRNA network. We identified increased levels of miRNAs such as miR146, miR122a, miR26a, miR27a, miR150, miR196a, and miR328 that are relevant to spermatogenesis. mRNA-miRNA target analysis on these DE-miRNAs and DE-mRNAs revealed miRNA target genes involved in ubiquitination process (, , ), RS differentiation, and chromatin remodeling/compaction (, , ), reversible protein phosphorylation (, , , , ), and acrosome stability (). Post-transcriptional and translational regulation of some of these germ-cell-specific mRNAs by miRNA-regulated translation arrest and/or decay may lead to spermatogenic arrest in KO and KI mice. Our studies demonstrate the importance of pGRTH in the chromatin compaction and remodeling process, which mediates the differentiation of RS into elongated spermatids through miRNA-mRNA interactions.

摘要

GRTH/DDX25 是一种睾丸特异性 DEAD 框家族 RNA 解旋酶,在精子发生和男性生育力中发挥着重要作用。GRTH 有两种形式,一种是 56 kDa 的非磷酸化形式,另一种是 61 kDa 的磷酸化形式(pGRTH)。由于圆形精子(RS)无法延长,GRTH-KO 和具有 R242H 突变(缺乏 pGRTH)的 GRTH 敲入(KI)小鼠不育,精子发生停滞在精子发生的第 8 步。我们对 WT、KI 和 KO 的 RS 进行了 mRNA-seq 和 miRNA-seq 分析,通过建立 miRNA-mRNA 网络,鉴定 RS 发育过程中的关键 microRNAs(miRNAs)和 mRNAs。我们发现 miR146、miR122a、miR26a、miR27a、miR150、miR196a 和 miR328 等 miRNA 的水平升高,这些 miRNA 与精子发生有关。对这些差异表达 miRNA(DE-miRNA)和差异表达 mRNA(DE-mRNA)的 mRNA-miRNA 靶标分析显示,miRNA 靶基因参与泛素化过程(、、)、RS 分化和染色质重塑/浓缩(、、)、可逆蛋白磷酸化(、、、、)和顶体稳定性()。一些生殖细胞特异性 mRNAs 的转录后和翻译调控可能通过 miRNA 调节的翻译阻滞和/或降解导致 KO 和 KI 小鼠的精子发生停滞。我们的研究表明 pGRTH 在染色质压缩和重塑过程中的重要性,该过程通过 miRNA-mRNA 相互作用介导 RS 向伸长精子的分化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d258/10001410/ffa9e8f07e74/cells-12-00756-g001.jpg

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