生物
长寿
生殖系
利基
干细胞
细胞生物学
粘附
遗传学
生态学
基因
有机化学
化学
作者
Meng Liu,Jiehui Chen,Guizhong Cui,Yumin Dai,Mengjiao Song,Chunyu Zhou,Qingyuan Hu,Qingxia Chen,Hongwei Wang,Wan-Li Chen,Jing‐Dong J. Han,Guangdun Peng,Naihe Jing,Yidong Shen
出处
期刊:The EMBO Journal
[Springer Nature]
日期:2024-07-25
卷期号:43 (18): 4000-4019
被引量:4
标识
DOI:10.1038/s44318-024-00185-3
摘要
Ageing and fertility are intertwined. Germline loss extends the lifespan in various organisms, termed gonadal longevity. However, the original longevity signal from the somatic gonad remains poorly understood. Here, we focused on the interaction between germline stem cells (GSCs) and their niche, the distal tip cells (DTCs), to explore the barely known longevity signal from the somatic gonad in C. elegans. We found that removing germline disrupts the cell adhesions between GSC and DTC, causing a significant transcriptomic change in DTC through hmp-2/β-catenin and two GATA transcription factors, elt-3 and pqm-1 in this niche cell. Inhibiting elt-3 and pqm-1 in DTC suppresses gonadal longevity. Moreover, we further identified the TGF-β ligand, tig-2, as the cytokine from DTC upon the loss of germline, which evokes the downstream gonadal longevity signalling throughout the body. Our findings thus reveal the source of the longevity signalling in response to germline removal, highlighting the stem cell niche as a critical signalling hub in ageing.
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