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在胶原凝胶中,鸡晶状体上皮向间充质转化过程中β1整合素的表达发生变化。

Expression of beta 1 integrins changes during transformation of avian lens epithelium to mesenchyme in collagen gels.

作者信息

Zuk A, Hay E D

机构信息

Department of Anatomy and Cellular Biology, Harvard Medical School, Boston, Massachusetts 02115.

出版信息

Dev Dyn. 1994 Dec;201(4):378-93. doi: 10.1002/aja.1002010409.

Abstract

Remarkably, a number of definitive epithelia, such as that of the anterior lens, give rise when suspended within 3D gels of type I collagen, to elongate, bipolar shaped cells that exhibit the ultrastructure, polarity, and migratory ability of mesenchymal cells. They begin producing type I collagen and stop producing crystallins, type IV collagen, and laminin. Here, we investigated changes in beta 1 integrins and their extracellular matrix (ECM) ligands during this transdifferentiation. The former free surface of the lens epithelium that is now in contact with collagen begins within a day to stain intensely for beta 1 and it is this surface rather than the surface facing the basement membrane that gives rise to mesenchymal cells. Immunoprecipitation experiments reveal a large increase in the beta 1 integrin subunit on mesenchymal cells as compared to the epithelium of origin. The alpha 5 integrin subunit, which is barely detectable in the lens, increases in the mesenchymal cells and alpha 3 continues to be expressed at about the same level as in the epithelium. alpha 6, the epithelial integrin subunit, and laminin, its ECM ligand, are not detected immunohistochemically or biochemically in the mesenchyme. Rather, the mesenchymal cells secrete abundant fibronectin, the major ECM ligand for alpha 5 beta 1. RGD peptides do not inhibit the transformation but antibodies to beta 1 do perturb the emigration of mesenchymal cells from the lens apical surface. We conclude that the beta 1 integrins newly expressed on the apical epithelial surface interact with the surrounding 3D collagen gel to help bring about this unusual epithelial-mesenchymal transition.

摘要

值得注意的是,一些明确的上皮组织,如晶状体前上皮,当悬浮于I型胶原蛋白的三维凝胶中时,会产生伸长的、双极形状的细胞,这些细胞表现出间充质细胞的超微结构、极性和迁移能力。它们开始产生I型胶原蛋白,并停止产生晶状体蛋白、IV型胶原蛋白和层粘连蛋白。在此,我们研究了这种转分化过程中β1整合素及其细胞外基质(ECM)配体的变化。晶状体上皮细胞先前的自由表面现在与胶原蛋白接触,在一天内开始强烈染色β1,正是这个表面而非面向基底膜的表面产生了间充质细胞。免疫沉淀实验表明,与起源上皮相比,间充质细胞上的β1整合素亚基大幅增加。在晶状体中几乎检测不到的α5整合素亚基,在间充质细胞中增加,而α3继续以与上皮中大致相同的水平表达。α6,上皮整合素亚基及其ECM配体层粘连蛋白,在间充质中未通过免疫组织化学或生物化学方法检测到。相反,间充质细胞分泌丰富的纤连蛋白,它是α5β1的主要ECM配体。RGD肽不抑制这种转化,但β1抗体确实会干扰间充质细胞从晶状体顶端表面的迁出。我们得出结论,顶端上皮表面新表达的β1整合素与周围的三维胶原蛋白凝胶相互作用,有助于实现这种不寻常上皮-间充质转化。

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