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Intestinal crypt homeostasis results from neutral competition between symmetrically dividing Lgr5 stem cells

机译:肠隐窝稳态是由对称分裂的Lgr5干细胞之间的中性竞争导致的

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摘要

Intestinal stem cells, characterized by high Lgr5 expression, reside between Paneth cells at the small intestinal crypt base and divide every day. We have carried out fate mapping of individual stem cells by generating a multicolor Cre-reporter. As a population, Lgr5~(hi) stem cells persist life-long, yet crypts drift toward clonality within a period of 1-6 months. We have collected short- and long-term clonal tracing data of individual Lgr5~(hi) cells. These reveal that most Lgr5~(hi) cell divisions occur symmetrically and do not support a model in which two daughter cells resulting from an Lgr5~(hi) cell division adopt divergent fates (i.e., one Lgr5~(hi) cell and one transit-amplifying [TA] cell per division). The cellular dynamics are consistent with a model in which the resident stem cells double their numbers each day and stochastically adopt stem or TA fates. Quantitative analysis shows that stem cell turnover follows a pattern of neutral drift dynamics.
机译:以Lgr5高表达为特征的肠道干细胞位于小肠隐窝底部的Paneth细胞之间,并且每天分裂。我们已经通过生成多色Cre报告基因对单个干细胞进行了命运定位。作为一个种群,Lgr5〜(hi)干细胞可以终生存在,但是隐窝会在1-6个月内向克隆性漂移。我们已经收集了单个Lgr5〜(hi)细胞的短期和长期克隆追踪数据。这些表明大多数Lgr5〜(hi)细胞分裂是对称发生的,并且不支持其中Lgr5〜(hi)细胞分裂产生的两个子细胞采用发散命运的模型(即,一个Lgr5〜(hi)细胞一次转运)。 -每格扩增[TA]细胞)。细胞动力学与常驻干细胞每天增加一倍,并随机采用干或TA命运的模型是一致的。定量分析表明,干细胞更新遵循中性漂移动力学模式。

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