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卵巢早衰:血管活性肠肽作为纤维炎症和泡沫巨噬细胞生成的关键调节因子。

Ovarian premature aging: VIP as key regulator of fibro-inflammation and foamy macrophages generation.

作者信息

Castagnola Lara, Gallino Lucila, Schafir Ana, Vota Daiana, Grasso Esteban, Gori Soledad, Waschek James, Parborell Fernanda, Pérez Leirós Claudia, Hauk Vanesa, Ramhorst Rosanna

机构信息

Universidad de Buenos Aires - CONICET, Instituto de Química Biológica de La Facultad de Ciencias Exactas y Naturales (IQUIBICEN), Buenos Aires, Argentina.

The David Geffen School of Medicine, University of California, Los Angeles, USA.

出版信息

Mol Cell Endocrinol. 2025 Apr 1;599:112486. doi: 10.1016/j.mce.2025.112486. Epub 2025 Jan 31.

Abstract

Ovarian aging is associated with fibro-inflammation, contributing to the decline in oocyte count and quality. Given the immunomodulatory properties of the vasoactive intestinal peptide (VIP) in the reproductive tract, we investigated its role in maintaining ovarian immune homeostasis and preventing premature aging. We evaluated young VIP knockout (KO) mice, comparing them to young wild type (WT) females, for signs of premature aging. Histological staining revealed aberrant ovarian morphology in VIP KO mice, characterized by increased atretic follicles and decreased ovarian reserve compared to WT controls. Moreover, VIP KO ovaries showed reduced vascularization, increased collagen deposition and elevated ROS and IL-1β levels. Foamy macrophages were significantly predominant, indicating premature aging in young VIP KO ovaries. To determine potential mechanisms behind these pathogenic changes, we conditioned peritoneal macrophages from young WT or VIP KO mice in vitro with ovarian-conditioned media from young WT or VIP KO mice to mimic the respective ovarian microenvironment. When WT or VIP KO peritoneal macrophages were conditioned with ovarian media from their respective genotypes, lipid droplet accumulation increased compared to control medium. In cross-genotype experiments, WT macrophages conditioned with media from VIP KO ovaries selectively accumulated higher levels of lipid droplets, whereas no differences were observed in VIP KO macrophages conditioned with WT ovarian media. This suggests that VIP KO macrophages are uniquely sensitized to the inflammatory environment of VIP KO ovaries, implicating both ovarian factors and macrophage status. These findings highlight the role of VIP in preventing fibro-inflammation, thereby preserving ovarian health and preventing premature aging.

摘要

卵巢衰老与纤维炎症相关,导致卵母细胞数量和质量下降。鉴于血管活性肠肽(VIP)在生殖道中的免疫调节特性,我们研究了其在维持卵巢免疫稳态和预防早衰中的作用。我们评估了年轻的VIP基因敲除(KO)小鼠,并将其与年轻的野生型(WT)雌性小鼠进行比较,以观察早衰迹象。组织学染色显示,与WT对照组相比,VIP KO小鼠的卵巢形态异常,其特征是闭锁卵泡增多,卵巢储备减少。此外,VIP KO卵巢的血管化减少,胶原沉积增加,ROS和IL-1β水平升高。泡沫巨噬细胞明显占优势,表明年轻的VIP KO卵巢出现早衰。为了确定这些致病变化背后的潜在机制,我们在体外使用来自年轻WT或VIP KO小鼠的卵巢条件培养基对年轻WT或VIP KO小鼠的腹腔巨噬细胞进行处理,以模拟各自的卵巢微环境。当WT或VIP KO腹腔巨噬细胞用各自基因型的卵巢培养基处理时,与对照培养基相比,脂滴积累增加。在跨基因型实验中,用VIP KO卵巢培养基处理的WT巨噬细胞选择性地积累了更高水平的脂滴,而用WT卵巢培养基处理的VIP KO巨噬细胞未观察到差异。这表明VIP KO巨噬细胞对VIP KO卵巢的炎症环境具有独特的敏感性,这涉及卵巢因子和巨噬细胞状态。这些发现突出了VIP在预防纤维炎症中的作用,从而维护卵巢健康并预防早衰。

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