自噬通过控制嘌呤核苷信号发挥抑制肥胖相关纤维化的作用

Klara Piletic, Amir H Kayvanjoo, Felix Clemens Richter, Mariana Borsa, Ana Victoria Lechuga-Vieco, Oliver Popp, Sacha Grenet, Jacky Ka Long Ko, Kristina Zec, Maria Kyriazi, Lada Koneva, Stephen Sansom, Philipp Mertins, Fiona Powrie, Ghada Alsaleh, Anna Katharina Simon
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引用次数: 0

摘要

肥胖症的特征之一是白色脂肪组织(WAT)病理性扩张,并伴有明显的组织功能障碍和纤维化。自噬可促进脂肪细胞分化和脂质稳态,但其在肥胖脂肪细胞和脂肪组织功能障碍中的作用仍不完全清楚。在这里,我们证明自噬是饮食诱导肥胖中 WAT 重塑的一个关键组织特异性调节因子。重要的是,脂肪细胞自噬功能的丧失大大加剧了内脏 WAT 的细胞周围纤维化。内脏脂肪细胞结构的变化与具有组织修复和纤维化特征的巨噬细胞浸润增加有关。我们发现自噬调节肥胖脂肪细胞的嘌呤核苷代谢,防止嘌呤代谢产物黄嘌呤和次黄嘌呤的过度释放。嘌呤通过驱动巨噬细胞向组织修复表型极化,在细胞外发出纤维化信号。我们的研究结果揭示了脂肪细胞自噬在调节组织嘌呤核苷代谢中的新作用,从而限制肥胖相关的纤维化并维持内脏脂肪的功能完整性。嘌呤信号可作为纤维化疾病的关键平衡检查点和治疗靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Autophagy acts as a brake on obesity-related fibrosis by controlling purine nucleoside signalling
A hallmark of obesity is a pathological expansion of white adipose tissue (WAT), accompanied by marked tissue dysfunction and fibrosis. Autophagy promotes adipocyte differentiation and lipid homeostasis, but its role in obese adipocytes and adipose tissue dysfunction remains incompletely understood. Here, we demonstrate that autophagy is a key tissue-specific regulator of WAT remodelling in diet-induced obesity. Importantly, loss of adipocyte autophagy substantially exacerbates pericellular fibrosis in visceral WAT. Change in WAT architecture correlates with increased infiltration of macrophages with tissue-reparative, fibrotic features. We uncover that autophagy regulates purine nucleoside metabolism in obese adipocytes, preventing excessive release of the purine catabolites xanthine and hypoxanthine. Purines signal cell-extrinsically for fibrosis by driving macrophage polarisation towards a tissue reparative phenotype. Our findings reveal a novel role for adipocyte autophagy in regulating tissue purine nucleoside metabolism, thereby limiting obesity-associated fibrosis and maintaining the functional integrity of visceral WAT. Purine signals may serve as a critical balance checkpoint and therapeutic target in fibrotic diseases.
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