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调控 STUB1 表达及其在小鼠睾丸支持细胞中的生物学意义。

Regulation of STUB1 expression and its biological significance in mouse Sertoli cells.

机构信息

Reproductive Center, Baoji Maternal and Child Health Hospital, Baoji, P. R. China.

Department of Urology, Baoji Center Hospital, Baoji, P. R. China.

出版信息

Syst Biol Reprod Med. 2022 Aug;68(4):298-313. doi: 10.1080/19396368.2022.2027554. Epub 2022 Mar 26.

DOI:10.1080/19396368.2022.2027554
PMID:35343345
Abstract

STIP1 Homology and U-Box Containing Protein 1 (STUB1), a ubiquitin E3 ligase initially involved in immune responses, has recently emerged as a pleiotropic regulator of different biological systems, including skeletal and male reproduction systems. On the latter, a homozygous mutation in the gene has been identified in patients with hypogonadism. However, the pattern of expression and biological actions of STUB1 in testis remains so far unexplored. Herein, we report analyses on the testicular expression of STUB1 in human testes with impaired spermatogenesis and paracrine regulation of STUB1 expression in mouse testis development and the direct effects of ablation STUB1 on Sertoli cell (SC) functions. STUB1 was expressed abundantly in pachytene spermatocytes and SCs, and weakly in spermatogonia and differentiating spermatids in normal human testis. In contrast, Sertoli-specific expression of STUB1 was significantly decreased in the human testes with impaired spermatogenesis. Throughout postnatal development of mouse testis, however, STUB1 was expressed exclusively in the nuclei of the functionally mature SCs. The adjacent germ cell (GC)-derived IL-1α overtly regulated STUB1 expression through promoting the ETS domain transcription factor Elk-1 (ELK1)-mediated transactivation. Importantly, ablation of endogenous STUB1 caused lipid accumulation and senescence in GC co-incubated SCs. Together with previous reports on the stimulatory effects of IL-1α on cell senescence, our findings suggest that STUB1 may serve as an important negative feedback signaling to modulate the magnitude of GCs-derived IL-1α, which is normally maintained at low levels within testis.

摘要

STIP1 同源和泛素连接酶 E3(STUB1),最初参与免疫反应的泛素连接酶,最近作为不同生物系统的多效调节剂出现,包括骨骼和男性生殖系统。在后一种系统中,已经在性腺功能减退症患者中鉴定出 基因的纯合突变。然而,STUB1 在睾丸中的表达模式和生物学作用迄今为止仍未得到探索。在此,我们报告了对具有受损精子发生的人类睾丸中 STUB1 的睾丸表达以及小鼠睾丸发育中 STUB1 表达的旁分泌调节和直接消融 STUB1 对支持细胞 (SC) 功能的影响的分析。STUB1 在人正常睾丸的粗线期精母细胞和 SC 中大量表达,在精原细胞和分化的精细胞中弱表达。相比之下,在具有受损精子发生的人类睾丸中,Sertoli 特异性表达的 STUB1 显著降低。然而,在小鼠睾丸的出生后发育过程中,STUB1 仅在功能成熟的 SC 的核中表达。相邻的生殖细胞 (GC) 衍生的 IL-1α 通过促进 ETS 结构域转录因子 Elk-1 (ELK1) 介导的反式激活来明显调节 STUB1 的表达。重要的是,内源性 STUB1 的消融导致与 GC 共孵育的 SC 中的脂质积累和衰老。结合之前关于 IL-1α 对细胞衰老的刺激作用的报道,我们的发现表明 STUB1 可能作为一种重要的负反馈信号,调节 GC 衍生的 IL-1α 的大小,IL-1α 通常在睾丸内维持在低水平。

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