神经酸通过诱导线粒体氧化应激激活NLRP3/ IL-1β通路引发卵巢炎症。

Xiangzhou Zeng, Xinyin Fan, Haitao Yu, Shuang Cai, Liangrui Zhou, Huanwen Wu, Zhiwen Zhang, Shuang Quan, Siyu Li, Xinyu Wang, Bangxin Xue, Lu Liu, Shiyan Qiao, Xiangfang Zeng
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引用次数: 0

摘要

导言代谢综合征是全球严重的公共健康问题。然而,与代谢综合征相关的生育力下降的典型代谢物和机制仍然难以捉摸:本研究旨在探索代谢综合征导致生育能力下降的典型代谢物及其机制:方法:利用代谢组学对繁殖性能高和繁殖性能低的母猪各种组织中的脂肪酸组成进行比较分析。此外,还研究了高脂饮食(HFD)诱导的代谢综合征模型(肥胖小鼠)的血清脂肪酸组成,以阐明与代谢综合征相关的脂质代谢物。此外,还利用啮齿类动物模型(大鼠和小鼠)研究了神经酸(NA)对卵巢功能的影响。通过转录组学、CUT&Tag 和蛋白质翻译后修饰分析等生物技术,利用猪、人和小鼠的卵巢颗粒细胞模型,进一步阐明了 NA 介导的卵巢炎症的分子机制。最后,在确诊为多囊卵巢综合征患者的卵巢上进行了验证:体外靶向血清脂质体分析表明,胚胎存活率低的母猪表现出异常的脂质代谢,其特征是 NA 在肝脏、卵巢和脂肪组织中的异常积累。此外,NA 水平升高会引发卵巢炎症,导致母猪和大鼠卵巢功能失调。从机理上讲,NA通过抑制呼吸链蛋白CYTB和NDFUB8诱导线粒体氧化应激,从而激活NLRP3炎症小体,引发procaspase-1转化为活性caspase-1,并在卵巢颗粒细胞中将细胞因子前体pro-IL-1β转化为具有生物活性的IL-1β。值得注意的是,我们发现NA通过增加IL-1β启动子区域的H3K9ac修饰水平和调节转录因子AP-1的表达来促进IL-1β的活性。最后,我们发现卵巢中CerS2的表达减少和趋化因子CXCL14水平的升高可能是NA异常积累的原因。令人惊讶的是,多囊卵巢综合征、肥胖、非酒精性脂肪肝或妊娠糖尿病患者的血清NA水平较高:总之,我们目前的研究表明,NA是代谢综合征的一种典型代谢产物,它对卵巢功能和胚胎存活有很大影响,同时也表明干扰线粒体ROS的产生是靶向解决NA异常积累的一种潜在有力策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Nervonic acid triggered ovarian inflammation by inducing mitochondrial oxidative stress to activate NLRP3/ IL-1β pathway.

Introduction: Metabolic syndrome is a serious public health concern across the globe. However, the typical metabolites and mechanisms underlying the decreased fertility related to metabolic syndrome is still elusive.

Objectives: The aim of the present study was to explore the typical metabolites and mechanisms underlying the decreased fertility related with metabolic syndrome.

Methods: Utilizing metabolomics, a comparative analysis was conducted on fatty acid compositions in various tissues of sows with high and low reproductive performance. Additionally, serum fatty acid compositions in a metabolic syndrome model (obese mice) induced by a high-fat diet (HFD) were investigated to elucidate the lipid metabolites associated with metabolic syndrome. Furthermore, the impact of nervonic acid (NA) on ovarian function was examined using rodent animal models (rats and mice). Through biological techniques such as transcriptomics, CUT&Tag, and analysis of post-translational protein modifications, the molecular mechanisms underlying NA mediated ovarian inflammation were further elucidated based on models utilizing ovarian granulosa cells from pigs, humans, and mice. Finally, validation was performed on ovaries from patients diagnosed with polycystic ovary syndrome.

Results: In vitro, targeted serum lipidomic analysis revealed that sows with low embryo survival rates exhibited abnormal lipid metabolism characterized by abnormal accumulation of NA in the liver, ovary, and adipose tissue. Additionally, elevated NA levels trigger ovarian inflammation to cause ovarian dysfunction in both sows and rats. Mechanistically, NA induce mitochondrial oxidative stress through inhibiting respiratory chain proteins CYTB and NDFUB8 to activate NLRP3 inflammasome, which triggers procaspase-1 into active caspase-1, and convert the cytokine precursors pro-IL-1β into biologically active IL-1β in ovarian granulosa cells. Notably, we evidenced that NA promotes IL-1β activities by increasing H3K9ac modification level of IL-1β promoter regions and regulating the expression of the transcription factor AP-1. Finally, we found that the decreased expression of CerS2 in ovaries and the increased level of chemokine CXCL14 may be the cause of abnormal NA accumulation. Surprisingly, individuals with polycystic ovary syndrome, obesity, non-alcoholic fatty liver or gestational diabetes mellitus exhibit a high level of serum NA.

Conclusion: Collectively, our current study suggests that NA is a typical metabolite of metabolic syndrome, which strongly influences the ovarian function and embryo survival and also provides that interfering with mitochondrial ROS production is a potential strong strategy for target solving abnormal NA accumulation.

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