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Transcriptome analysis of meiotic and post-meiotic spermatogenic cells reveals the potential hub genes of aging on the decline of male fertility

生物 转录组 减数分裂 遗传学 基因 精子 配子 表观遗传学 减数分裂细胞 男科 基因表达 医学
作者
Yiqian Gui,Xixiang Ma,Mengneng Xiong,Yujiao Wen,Congcong Cao,Liang Zhang,Xiaoli Wang,Chunyan Liu,Huiping Zhang,Xunbin Huang,Chengliang Xiong,Feng Pan,Shuiqiao Yuan
出处
期刊:Gene [Elsevier]
卷期号:893: 147883-147883 被引量:1
标识
DOI:10.1016/j.gene.2023.147883
摘要

Genetic and epigenetic changes in sperm caused by male aging may be essential factors affecting semen parameters, but the effects and specific molecular mechanisms of aging on male reproduction have not been fully clarified. In this study, to explore the effect of aging on male fertility and seek the potential molecular etiology, we performed high-throughput RNA-sequencing in isolated spermatogenic cells, including pachytene spermatocytes (marked by the completion of chromosome synapsis) and round spermatids (produced by the separation of sister chromatids) from the elderly and the young men. Functional enrichment analysis of differentially expressed genes (DEGs) in round spermatids between the elderly and young showed that they were significantly enriched in gamete generation, spindle assembly, and cilium movement involved in cell motility. In addition, the expression levels of DEGs in round spermatids (post-meiotic cells) were found to be more susceptible to age. Furthermore, ten genes (AURKA, CCNB1, CDC20, CCNB2, KIF2C, KIAA0101, NR5A1, PLK1, PTTG1, RAD51AP1) were identified to be the hub genes involved in the regulation of sperm quality in the elderly through Protein-Protein Interaction (PPI) network construction and measuring semantic among GO terms and gene products. Our data provide aging-related molecular alterations in meiotic and post-meiotic spermatogenic cells, and the information gained from this study may explain the abnormal aging-related male fertility decline.
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