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追踪小鼠胰腺中胰岛特化的细胞基础。

Tracing the cellular basis of islet specification in mouse pancreas.

机构信息

Department of Oncology, University of Cambridge, Hutchison/MRC Research Centre, Cambridge Biomedical Campus, Cambridge, CB2 0XZ, UK.

Wellcome Trust/Medical Research Council Cambridge Stem Cell Institute, University of Cambridge, Tennis Court Road, Cambridge, CB2 1QR, UK.

出版信息

Nat Commun. 2020 Oct 7;11(1):5037. doi: 10.1038/s41467-020-18837-3.

Abstract

Pancreatic islets play an essential role in regulating blood glucose level. Although the molecular pathways underlying islet cell differentiation are beginning to be resolved, the cellular basis of islet morphogenesis and fate allocation remain unclear. By combining unbiased and targeted lineage tracing, we address the events leading to islet formation in the mouse. From the statistical analysis of clones induced at multiple embryonic timepoints, here we show that, during the secondary transition, islet formation involves the aggregation of multiple equipotent endocrine progenitors that transition from a phase of stochastic amplification by cell division into a phase of sublineage restriction and limited islet fission. Together, these results explain quantitatively the heterogeneous size distribution and degree of polyclonality of maturing islets, as well as dispersion of progenitors within and between islets. Further, our results show that, during the secondary transition, α- and β-cells are generated in a contemporary manner. Together, these findings provide insight into the cellular basis of islet development.

摘要

胰岛在调节血糖水平方面发挥着重要作用。尽管胰岛细胞分化的分子途径开始被阐明,但胰岛形态发生和命运分配的细胞基础仍不清楚。通过结合无偏和靶向谱系追踪,我们解决了导致小鼠胰岛形成的事件。通过对多个胚胎时间点诱导的克隆进行统计分析,我们在这里表明,在次级转变过程中,胰岛的形成涉及多个等同的内分泌前体细胞的聚集,这些细胞从前体细胞随机扩增的阶段过渡到亚系限制和有限的胰岛分裂阶段。这些结果共同定量解释了成熟胰岛不均匀的大小分布和多克隆程度,以及祖细胞在胰岛内外的分散。此外,我们的研究结果表明,在次级转变过程中,α 和 β 细胞是同时产生的。这些发现共同为胰岛发育的细胞基础提供了深入的了解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/43c8/7541446/1a0bb90357b2/41467_2020_18837_Fig1_HTML.jpg

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