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胚胎肾解离后的自我组织是通过输尿管上皮细胞的选择性黏附来驱动的。

Self-organisation after embryonic kidney dissociation is driven via selective adhesion of ureteric epithelial cells.

作者信息

Lefevre James G, Chiu Han S, Combes Alexander N, Vanslambrouck Jessica M, Ju Ali, Hamilton Nicholas A, Little Melissa H

机构信息

Institute for Molecular Bioscience, The University of Queensland, St. Lucia, Brisbane 4072, Australia

Institute for Molecular Bioscience, The University of Queensland, St. Lucia, Brisbane 4072, Australia.

出版信息

Development. 2017 Mar 15;144(6):1087-1096. doi: 10.1242/dev.140228. Epub 2017 Feb 7.

Abstract

Human pluripotent stem cells, after directed differentiation , can spontaneously generate complex tissues via self-organisation of the component cells. Self-organisation can also reform embryonic organ structure after tissue disruption. It has previously been demonstrated that dissociated embryonic kidneys can recreate component epithelial and mesenchymal relationships sufficient to allow continued kidney morphogenesis. Here, we investigate the timing and underlying mechanisms driving self-organisation after dissociation of the embryonic kidney using time-lapse imaging, high-resolution confocal analyses and mathematical modelling. Organotypic self-organisation sufficient for nephron initiation was observed within a 24 h period. This involved cell movement, with structure emerging after the clustering of ureteric epithelial cells, a process consistent with models of random cell movement with preferential cell adhesion. Ureteric epithelialisation rapidly followed the formation of ureteric cell clusters with the reformation of nephron-forming niches representing a later event. Disruption of P-cadherin interactions was seen to impair this ureteric epithelial cell clustering without affecting epithelial maturation. This understanding could facilitate improved regulation of patterning within organoids and facilitate kidney engineering approaches guided by cell-cell self-organisation.

摘要

人类多能干细胞在定向分化后,可通过组成细胞的自我组织自发形成复杂组织。自我组织还能在组织破坏后重塑胚胎器官结构。此前已有研究表明,解离后的胚胎肾脏能够重新建立足以支持肾脏持续形态发生的组成性上皮和间充质关系。在此,我们利用延时成像、高分辨率共聚焦分析和数学建模,研究胚胎肾脏解离后驱动自我组织的时间和潜在机制。在24小时内观察到了足以启动肾单位形成的器官型自我组织。这涉及细胞运动,输尿管上皮细胞聚集后形成结构,这一过程与具有优先细胞黏附的随机细胞运动模型一致。输尿管细胞簇形成后迅速发生输尿管上皮化,而肾单位形成龛的重塑则是较晚发生的事件。P-钙黏蛋白相互作用的破坏会损害这种输尿管上皮细胞的聚集,但不影响上皮成熟。这一认识有助于改善类器官内模式形成的调控,并促进以细胞-细胞自我组织为导向的肾脏工程方法。

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