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干细胞严格调控死细胞清除以维持组织健康。

Stem cells tightly regulate dead cell clearance to maintain tissue fitness.

作者信息

Stewart Katherine S, Gonzales Kevin Au, Yuan Shaopeng, Tierney Matthew T, Bonny Alain R, Yang Yihao, Infarinato Nicole R, Cowley Christopher J, Levorse John M, Pasolli Hilda Amalia, Ghosh Sourav, Rothlin Carla V, Fuchs Elaine

机构信息

Howard Hughes Medical Institute, Robin Chemers Neustein Laboratory of Mammalian Cell Biology and Development, The Rockefeller University, New York, NY, USA.

Electron Microscopy Resource Center, The Rockefeller University, New York, NY, USA.

出版信息

bioRxiv. 2023 May 22:2023.05.22.541773. doi: 10.1101/2023.05.22.541773.

Abstract

Macrophages and dendritic cells have long been appreciated for their ability to migrate to and engulf dying cells and debris, including some of the billions of cells that are naturally eliminated from our body daily. However, a substantial number of these dying cells are cleared by 'non-professional phagocytes', local epithelial cells that are critical to organismal fitness. How non-professional phagocytes sense and digest nearby apoptotic corpses while still performing their normal tissue functions is unclear. Here, we explore the molecular mechanisms underlying their multifunctionality. Exploiting the cyclical bouts of tissue regeneration and degeneration during the hair cycle, we show that stem cells can transiently become non-professional phagocytes when confronted with dying cells. Adoption of this phagocytic state requires both local lipids produced by apoptotic corpses to activate RXRα, and tissue-specific retinoids for RARγ activation. This dual factor dependency enables tight regulation of the genes requisite to activate phagocytic apoptotic clearance. The tunable phagocytic program we describe here offers an effective mechanism to offset phagocytic duties against the primary stem cell function of replenishing differentiated cells to preserve tissue integrity during homeostasis. Our findings have broad implications for other non-motile stem or progenitor cells which experience cell death in an immune-privileged niche.

摘要

长期以来,巨噬细胞和树突状细胞因能够迁移并吞噬死亡细胞和碎片而受到关注,这些细胞碎片包括我们身体每天自然清除的数十亿细胞中的一部分。然而,相当一部分这些死亡细胞是由“非专职吞噬细胞”清除的,即对机体健康至关重要的局部上皮细胞。非专职吞噬细胞在执行正常组织功能的同时,如何感知并消化附近的凋亡尸体尚不清楚。在这里,我们探索其多功能性背后的分子机制。利用毛囊周期中组织再生和退化的周期性过程,我们发现干细胞在遇到死亡细胞时可以短暂地转变为非专职吞噬细胞。进入这种吞噬状态既需要凋亡尸体产生的局部脂质来激活RXRα,也需要组织特异性视黄酸来激活RARγ。这种双重因子依赖性能够严格调控激活吞噬性凋亡清除所需的基因。我们在此描述的可调节吞噬程序提供了一种有效机制,以平衡吞噬职责与补充分化细胞的主要干细胞功能,从而在体内平衡期间维持组织完整性。我们的发现对其他在免疫特权微环境中经历细胞死亡的非迁移性干细胞或祖细胞具有广泛的意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/85a5/10245816/38c76747164f/nihpp-2023.05.22.541773v1-f0006.jpg

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