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成纤维细胞在 3D 胶原基质上的形态发生:细胞聚集和细胞迁移之间的平衡。

Fibroblast morphogenesis on 3D collagen matrices: the balance between cell clustering and cell migration.

机构信息

Department of Cell Biology, UT Southwestern Medical Center, 5323 Harry Hines Blvd, Dallas, TX 75390-9039, USA.

出版信息

Exp Cell Res. 2013 Oct 1;319(16):2440-6. doi: 10.1016/j.yexcr.2013.05.003. Epub 2013 May 9.

DOI:10.1016/j.yexcr.2013.05.003
PMID:23664837
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3773009/
Abstract

Fibroblast clusters have been observed in tissues under a variety of circumstances: in fibrosis and scar, in the formation of hair follicle dermal papilla, and as part of the general process of mesenchymal condensation that takes place during development. Cell clustering has been shown to depend on features of the extracellular matrix, growth factor environment, and mechanisms to stabilize cell-cell interactions. In vitro studies have shown that increasing the potential for cell-cell adhesion relative to cell-substrate adhesion promotes cell clustering. Experimental models to study fibroblast clustering have utilized centrifugation, hanging drops, and substrata with poorly adhesive, soft and mechanically unstable properties. In this review, we summarize work on a new, highly tractable, cell clustering research model in which human fibroblasts are incubated on the surfaces of collagen matrices. Fibroblast clustering occurs under procontractile growth factor conditions (e.g., serum or the serum lipid agonist lysophosphatidic acid) but not under promigratory growth factor conditions (e.g., platelet-derived growth factor) and can be reversed by switching growth factor environments. Cell contraction plays a dual role in clustering to bring cells closer together and to stimulate cells to organize fibronectin into a fibrillar matrix. Binding of fibroblasts to a shared fibronectin fibrillar matrix stabilizes clusters, and fragmentation of the fibrillar matrix occurs when growth factor conditions are switched to promote cell dispersal.

摘要

成纤维细胞簇已在多种情况下的组织中观察到

在纤维化和瘢痕组织中、在毛囊真皮乳头形成过程中、以及在发育过程中发生的一般间充质凝聚过程中。已经表明细胞簇集依赖于细胞外基质的特征、生长因子环境以及稳定细胞间相互作用的机制。体外研究表明,相对于细胞-基底相互作用,增加细胞-细胞黏附的潜力可促进细胞簇集。用于研究成纤维细胞簇集的实验模型利用了离心、悬滴和具有较差黏附性、柔软和机械不稳定特性的底物。在这篇综述中,我们总结了一种新的、高度可行的细胞簇集研究模型的工作,其中人成纤维细胞在胶原基质的表面上孵育。成纤维细胞在促收缩生长因子条件(例如血清或血清脂质激动剂溶血磷脂酸)下发生簇集,但不在促迁移生长因子条件(例如血小板衍生生长因子)下发生,并且可以通过切换生长因子环境来逆转。细胞收缩在簇集过程中起双重作用,使细胞更紧密地聚集,并刺激细胞将纤维连接蛋白组织成纤维状基质。成纤维细胞与共享纤维连接蛋白纤维状基质的结合稳定了簇集,并且当生长因子条件切换以促进细胞分散时,纤维状基质会发生碎裂。

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