Transcriptome analyses reveal key features of mouse seminal vesicle during aging.

IF 2.1 4区 医学 Q3 ANDROLOGY
Peng Luo, Haibin Guo, Baoning Liu, Zhiqiang Zhang, Yun Xie, Jiahui Yao, Xiangping Li, Jun Bian, Jintao Zhuang, Bin Ouyang, Jinhua Wu
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Abstract

Despite the significant morphological changes that occur in the seminal vesicles with aging, the transcriptomic characteristics remain largely unexplored. To address this, we performed bulk RNA sequencing on seminal vesicle samples from mice aged 3, 13, and 21 months to uncover transcriptomic alterations. Our findings reveal that aged seminal vesicles display cystic dilatation, epithelial hypoplasia, disordered muscle layers, fibrosis, and reduced proliferation capability. A comparison between 3-month-old and 21-month-old mice indicated that leukocyte-mediated immunity and leukocyte migration were the most significantly upregulated biological processes among differentially expressed genes (DEGs). Notably, several DEGs associated with "leukocyte migration," such as Vcam1, Cxcl13, and Ccl8, exhibited an increasing trend in transcriptomic and protein expression at three different time points in the seminal vesicles of mice. Additionally, we identified multiple aging-associated DEGs, including P21 and Tnfrsf1b. Two genes (Cd209f and Ccl8) were consistently upregulated across all six regions of the male reproductive glands (testis, epididymis, and seminal vesicle) in the comparison of bulk RNA datasets from 3-month-old and 21-month-old mice. These analyses highlight an enhanced state of immune and inflammatory response in aged seminal vesicles. This study represents the first exploration of the overall transcriptome landscape of seminal vesicles in a murine model of natural aging, offering new insights into the mechanisms underlying aging-related seminal vesicle dysfunction.

转录组分析揭示了小鼠精囊衰老过程中的关键特征。
尽管随着年龄的增长,精囊的形态会发生重大变化,但其转录组特征在很大程度上仍未得到研究。为了解决这个问题,我们对 3 个月、13 个月和 21 个月的小鼠精囊样本进行了大量 RNA 测序,以发现转录组的变化。我们的研究结果表明,老龄精囊显示出囊性扩张、上皮发育不良、肌层紊乱、纤维化和增殖能力下降。对3个月大的小鼠和21个月大的小鼠进行比较后发现,在差异表达基因(DEGs)中,白细胞介导的免疫和白细胞迁移是上调最显著的生物过程。值得注意的是,与 "白细胞迁移 "相关的几个 DEGs,如 Vcam1、Cxcl13 和 Ccl8,在小鼠精囊的三个不同时间点的转录组和蛋白表达量均呈上升趋势。此外,我们还发现了多个与衰老相关的 DEGs,包括 P21 和 Tnfrsf1b。在比较 3 个月大小鼠和 21 个月大小鼠的大量 RNA 数据集时,两个基因(Cd209f 和 Ccl8)在雄性生殖腺(睾丸、附睾和精囊)的所有六个区域中都持续上调。这些分析凸显了老年精囊的免疫和炎症反应状态增强。这项研究首次探索了自然衰老小鼠模型中精囊的整体转录组图谱,为研究与衰老相关的精囊功能障碍的内在机制提供了新的视角。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
4.30
自引率
4.20%
发文量
27
审稿时长
>12 weeks
期刊介绍: Systems Biology in Reproductive Medicine, SBiRM, publishes Research Articles, Communications, Applications Notes that include protocols a Clinical Corner that includes case reports, Review Articles and Hypotheses and Letters to the Editor on human and animal reproduction. The journal will highlight the use of systems approaches including genomic, cellular, proteomic, metabolomic, bioinformatic, molecular, and biochemical, to address fundamental questions in reproductive biology, reproductive medicine, and translational research. The journal publishes research involving human and animal gametes, stem cells, developmental biology and toxicology, and clinical care in reproductive medicine. Specific areas of interest to the journal include: male factor infertility and germ cell biology, reproductive technologies (gamete micro-manipulation and cryopreservation, in vitro fertilization/embryo transfer (IVF/ET) and contraception. Research that is directed towards developing new or enhanced technologies for clinical medicine or scientific research in reproduction is of significant interest to the journal.
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