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视黄醇诱导的内皮细胞细胞外基质修饰:其在生长控制中的作用。

Retinol-induced modification of the extracellular matrix of endothelial cells: its role in growth control.

作者信息

Paige K, Palomares M, D'Amore P A, Braunhut S J

机构信息

Department of Ophthalmology, Harvard Medical School, Boston, Massachusetts.

出版信息

In Vitro Cell Dev Biol. 1991 Feb;27A(2):151-7. doi: 10.1007/BF02631002.

Abstract

The growth of the endothelial cell (EC) is tightly regulated throughout the body. Many factors have been implicated in modulating EC growth including diffusible compounds, cell-to-cell interactions, and the extracellular matrix (ECM). Retinol, or vitamin A alcohol, has recently been shown to inhibit the growth of bovine capillary ECs, in vitro. Retinoids are known to modify ECM in other cell systems, and pure ECM components have been shown to effect EC growth rates. We, therefore, examined the role of the matrix in the retinol-induced inhibition of ECs. Cell-free matrices from control and vitamin A-treated ECs were prepared by removing cells with EGTA treatment after 7 d of culture. Matrix proteins were analyzed by solubilizing the matrices in 5 M guanidine-HCl and performing Western blot analysis using specific antibodies to matrix proteins. In isolating the ECM, we observed that retinol-treated cultures of ECs were resistant to EGTA removal; retinol-treated ECs required twice the exposure time to EGTA to detach from their matrix than did controls cells. Western blot analysis of matrix proteins derived from control and retinol-treated EC cultures demonstrated a 1.6-fold increase in laminin beta chains and a 2.5-fold increase in fibronectin in the ECM of retinol-treated EC compared to control cell matrix. Functional properties of these matrices were assessed by plating control and Day 6 retinol-treated ECs onto the matrices and measuring attachment and growth by determining cell numbers at 24, 72, and 144 h. These studies revealed that control cells attached in greatest numbers to a control matrix whereas retinol-treated ECs preferentially attached to a matrix derived from retinol-treated cells. Furthermore, control ECs which grew rapidly on a control matrix were growth inhibited on a retinol-derived matrix. These data indicate that vitamin A treatment of ECs effects both their phenotype and influences the composition and the functional properties of their underlying ECM. These studies also demonstrate that alterations of the matrix are at least in part responsible for the growth inhibition of EC by retinol.

摘要

内皮细胞(EC)的生长在全身受到严格调控。许多因素参与调节内皮细胞的生长,包括可扩散化合物、细胞间相互作用以及细胞外基质(ECM)。视黄醇,即维生素A醇,最近已被证明在体外可抑制牛毛细血管内皮细胞的生长。已知类视黄醇可在其他细胞系统中改变细胞外基质,并且已证明纯细胞外基质成分会影响内皮细胞的生长速率。因此,我们研究了基质在视黄醇诱导的内皮细胞抑制中的作用。在培养7天后,通过用乙二醇双四乙酸(EGTA)处理去除细胞,制备来自对照和维生素A处理的内皮细胞的无细胞基质。通过将基质溶解在5M盐酸胍中并使用针对基质蛋白的特异性抗体进行蛋白质印迹分析来分析基质蛋白。在分离细胞外基质时,我们观察到视黄醇处理的内皮细胞培养物对EGTA去除具有抗性;与对照细胞相比,视黄醇处理的内皮细胞需要两倍的EGTA暴露时间才能从其基质上脱离。对来自对照和视黄醇处理的内皮细胞培养物的基质蛋白进行蛋白质印迹分析表明,与对照细胞基质相比视黄醇处理的内皮细胞的细胞外基质中层粘连蛋白β链增加了1.6倍,纤连蛋白增加了2.5倍。通过将对照和第6天视黄醇处理的内皮细胞接种到基质上,并通过在24、72和144小时测定细胞数量来测量附着和生长,评估这些基质的功能特性。这些研究表明,对照细胞在对照基质上附着的数量最多,而视黄醇处理的内皮细胞优先附着于来自视黄醇处理细胞的基质。此外,在对照基质上快速生长的对照内皮细胞在视黄醇衍生的基质上生长受到抑制。这些数据表明,维生素A处理内皮细胞会影响其表型,并影响其下方细胞外基质的组成和功能特性。这些研究还表明,基质的改变至少部分是视黄醇抑制内皮细胞生长的原因。

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