细胞生物学
生物
干细胞
细胞粘附
整合素
粘附
细胞
信号转导
遗传学
有机化学
化学
作者
Shiyang Chen,Yajuan Zheng,Xiaojuan Ran,Hui Du,Hua Feng,Lei Yang,Yating Wen,Changdong Lin,Shihui Wang,Mengwen Huang,ZhanJun Yan,Dianqing Wu,Hongyan Wang,Gaoxiang Ge,An Zeng,Yi Arial Zeng,Jianfeng Chen
出处
期刊:Cell Research
[Springer Nature]
日期:2021-09-13
卷期号:31 (12): 1291-1307
被引量:24
标识
DOI:10.1038/s41422-021-00561-2
摘要
Intestinal stem cell (ISC) differentiation is regulated precisely by a niche in the crypt, where lymphocytes may interact with stem and transient amplifying (TA) cells. However, whether and how lymphocyte-stem/TA cell contact affects ISC differentiation is largely unknown. Here, we uncover a novel role of T cell-stem/TA cell contact in ISC fate decisions. We show that intestinal lymphocyte depletion results in skewed ISC differentiation in mice, which can be rescued by T cell transfer. Mechanistically, integrin αEβ7 expressed on T cells binds to E-cadherin on ISCs and TA cells, triggering E-cadherin endocytosis and the consequent Wnt and Notch signaling alterations. Blocking αEβ7-E-cadherin adhesion suppresses Wnt signaling and promotes Notch signaling in ISCs and TA cells, leading to defective ISC differentiation. Thus, αEβ7+ T cells regulate ISC differentiation at single-cell level through cell-cell contact-mediated αEβ7-E-cadherin adhesion signaling, highlighting a critical role of the T cell-stem/TA cell contact in maintaining intestinal homeostasis.
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