Rbbp6-Mediated Bmal1 Ubiquitination Inhibits YAP1 Signaling Pathway to Promote Ferroptosis in Diabetes-Induced Testicular Damage.

IF 6.8 2区 医学 Q1 ENDOCRINOLOGY & METABOLISM Diabetes & Metabolism Journal Pub Date : 2024-11-06 DOI:10.4093/dmj.2024.0099
Yuan Tian, Zhiqiang Zhu, Jun Qiao, Bei Liu, Yuehai Xiao
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Abstract

Background: Diabetes-induced testicular damage (DITD) is a common complication of diabetes. We investigated underlying mechanism of retinoblastoma-binding protein 6 (Rbbp6)-mediated brain and muscle ARNT-like 1 (Bmal1) ubiquitination in modulating ferroptosis in DITD.

Methods: Spermatogenic cell apoptosis and viability were measured by flow cytometry and cell counting kit 8 (CCK-8), respectively. The impact of Rbbp6 and Bmal1 on ferroptosis was assessed by determining expression of ferroptosis markers glutathione peroxidase 4 (GPX4) and solute carrier family 7 member 11 (SLC7A11), and levels of malondialdehyde (MDA), glutathione (GSH), iron, and lipid peroxidation. Co-immunoprecipitation was performed to determine the interaction between Rbbp6 and Bmal1, as well as the ubiquitination level of Bmal1. The expression levels of Rbbp6, Bmal1, Yes-associated protein 1 (YAP1), ferroptosis markers, and testicular steroidogenic enzymes were tested by Western blot.

Results: Bmal1 protein expression was significantly downregulated, while Rbbp6 was upregulated in DITD mouse model and high glucose (HG)-induced GC-1 spg cells. Overexpression of Bmal1 improved testicular injury in diabetic mice, reduced 4-hydroxynonenal (4-HNE), MDA, iron levels, and increased expression levels of GPX4, SLC7A11, GSH, as well as testicular steroidogenic enzymes. Rbbp6 decreased Bmal1 level through promoting its ubiquitination. Meanwhile, Rbbp6 knockdown inhibited the ferroptosis of HG-induced GC-1 spg cells, which were abolished by silencing Bmal1. In addition, knockdown of YAP1 or treatment with ferroptosis inducer erastin blocked the above effects caused by Bmal1 overexpression.

Conclusion: Rbbp6-mediated Bmal1 ubiquitination suppressed YAP1 pathway, promoting ferroptosis in DITD. This study highlighted Rbbp6/Bmal1/YAP1 axis as a potential therapeutic target for mitigating DITD.

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Rbbp6介导的Bmal1泛素化抑制YAP1信号通路,促进糖尿病诱导的睾丸损伤中的铁卟啉酶活性
背景:糖尿病诱导的睾丸损伤(DITD)是糖尿病的一种常见并发症。我们研究了视网膜母细胞瘤结合蛋白6(Rbbp6)介导的脑和肌肉ARNT样1(Bmal1)泛素化在DITD中调节铁凋亡的潜在机制:方法:采用流式细胞术和细胞计数试剂盒8(CCK-8)分别测定生精细胞的凋亡和存活率。Rbbp6和Bmal1对铁变态反应的影响是通过测定铁变态反应标志物谷胱甘肽过氧化物酶4(GPX4)和溶质运载家族7成员11(SLC7A11)的表达以及丙二醛(MDA)、谷胱甘肽(GSH)、铁和脂质过氧化物的水平来评估的。为了确定 Rbbp6 和 Bmal1 之间的相互作用以及 Bmal1 的泛素化水平,进行了共免疫沉淀。Western blot检测了Rbbp6、Bmal1、Yes-associated protein 1 (YAP1)、铁突变标志物和睾丸类固醇生成酶的表达水平:结果:在DITD小鼠模型和高糖(HG)诱导的GC-1 spg细胞中,Bmal1蛋白表达明显下调,而Rbbp6蛋白表达上调。过表达 Bmal1 可改善糖尿病小鼠的睾丸损伤,降低 4-羟基壬烯醛(4-HNE)、MDA 和铁水平,增加 GPX4、SLC7A11、GSH 以及睾丸类固醇生成酶的表达水平。Rbbp6通过促进Bmal1的泛素化来降低其水平。同时,敲除 Rbbp6 可抑制 HG 诱导的 GC-1 spg 细胞的铁突变,而沉默 Bmal1 则可抑制铁突变。此外,敲除YAP1或用铁突变诱导剂erastin处理可阻断Bmal1过表达引起的上述效应:结论:Rbbp6介导的Bmal1泛素化抑制了YAP1通路,促进了DITD中的铁变态反应。本研究强调了Rbbp6/Bmal1/YAP1轴是缓解DITD的潜在治疗靶点。
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
Diabetes & Metabolism Journal
Diabetes & Metabolism Journal Medicine-Endocrinology, Diabetes and Metabolism
CiteScore
10.40
自引率
6.80%
发文量
92
审稿时长
52 weeks
期刊介绍: The aims of the Diabetes & Metabolism Journal are to contribute to the cure of and education about diabetes mellitus, and the advancement of diabetology through the sharing of scientific information on the latest developments in diabetology among members of the Korean Diabetes Association and other international societies. The Journal publishes articles on basic and clinical studies, focusing on areas such as metabolism, epidemiology, pathogenesis, complications, and treatments relevant to diabetes mellitus. It also publishes articles covering obesity and cardiovascular disease. Articles on translational research and timely issues including ubiquitous care or new technology in the management of diabetes and metabolic disorders are welcome. In addition, genome research, meta-analysis, and randomized controlled studies are welcome for publication. The editorial board invites articles from international research or clinical study groups. Publication is determined by the editors and peer reviewers, who are experts in their specific fields of diabetology.
期刊最新文献
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