Isthmus progenitor cells contribute to homeostatic cellular turnover and support regeneration following intestinal injury

峡部祖细胞有助于维持细胞稳态更新,并支持肠道损伤后的再生。

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作者:Ermanno Malagola ,Alessandro Vasciaveo ,Yosuke Ochiai ,Woosook Kim ,Biyun Zheng ,Luca Zanella ,Alexander L E Wang ,Moritz Middelhoff ,Henrik Nienhüser ,Lu Deng ,Feijing Wu ,Quin T Waterbury ,Bryana Belin ,Jonathan LaBella ,Leah B Zamechek ,Melissa H Wong ,Linheng Li ,Chandan Guha ,Chia-Wei Cheng ,Kelley S Yan ,Andrea Califano ,Timothy C Wang

Abstract

The currently accepted intestinal epithelial cell organization model proposes that Lgr5+ crypt-base columnar (CBC) cells represent the sole intestinal stem cell (ISC) compartment. However, previous studies have indicated that Lgr5+ cells are dispensable for intestinal regeneration, leading to two major hypotheses: one favoring the presence of a quiescent reserve ISC and the other calling for differentiated cell plasticity. To investigate these possibilities, we studied crypt epithelial cells in an unbiased fashion via high-resolution single-cell profiling. These studies, combined with in vivo lineage tracing, show that Lgr5 is not a specific ISC marker and that stemness potential exists beyond the crypt base and resides in the isthmus region, where undifferentiated cells participate in intestinal homeostasis and regeneration following irradiation (IR) injury. Our results provide an alternative model of intestinal epithelial cell organization, suggesting that stemness potential is not restricted to CBC cells, and neither de-differentiation nor reserve ISC are drivers of intestinal regeneration.

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