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β型转化生长因子决定血管平滑肌细胞培养中的组织行为。

Beta-type transforming growth factor specifies organizational behavior in vascular smooth muscle cell cultures.

作者信息

Majack R A

出版信息

J Cell Biol. 1987 Jul;105(1):465-71. doi: 10.1083/jcb.105.1.465.

Abstract

In culture, vascular smooth muscle cells (SMC) grow in a "hill-and-valley" (multilayered) pattern of organization. We have studied the growth, behavioral organization, and biosynthetic phenotype of rat aortic SMC exposed to purified platelet-derived growth regulatory molecules. We show that multilayered growth is not a constitutive feature of cultured SMC, and that beta-type transforming growth factor (TGF-beta) is the primary determinant of multilayered growth and the hill-and-valley pattern of organization diagnostic for SMC in culture. TGF-beta inhibited, in a dose-dependent manner, the serum- or platelet-derived growth factor-mediated proliferation of these cells in two-dimensional culture, but only when cells were plated at subconfluent densities. The ability of TGF-beta to inhibit SMC growth was inversely correlated to plating cell density. When SMC were plated at monolayer density (5 X 10(4) cells/cm2) to allow maximal cell-to-cell contact, TGF-beta potentiated cell growth. This differential response of SMC to TGF-beta may contribute to the hill-and-valley pattern of organization. Unlike its effect on other cell types, TGF-beta did not enhance the synthesis of fibronectin or its incorporation into the extracellular matrix. However, the synthesis of a number of other secreted proteins was altered by TGF-beta treatment. SMC treated with TGF-beta for 4 or 8 h secreted markedly enhanced amounts of an Mr 38,000-D protein doublet whose synthesis is known to be increased by heparin (another inhibitor of SMC growth), suggesting metabolic similarities between heparin- and TGF-beta-mediated SMC growth inhibition. The data suggest that TGF-beta may play an important and complex regulatory role in SMC proliferation and organization during development and after vascular injury.

摘要

在培养过程中,血管平滑肌细胞(SMC)以“峰谷”(多层)模式生长。我们研究了暴露于纯化的血小板衍生生长调节分子的大鼠主动脉SMC的生长、行为组织和生物合成表型。我们发现多层生长不是培养的SMC的固有特征,β型转化生长因子(TGF-β)是多层生长以及培养中SMC特有的峰谷组织模式的主要决定因素。TGF-β以剂量依赖的方式抑制二维培养中这些细胞由血清或血小板衍生生长因子介导的增殖,但仅在细胞以亚汇合密度接种时才会出现这种情况。TGF-β抑制SMC生长的能力与接种细胞密度呈负相关。当SMC以单层密度(5×10⁴个细胞/cm²)接种以实现最大细胞间接触时,TGF-β会促进细胞生长。SMC对TGF-β的这种差异反应可能有助于形成峰谷组织模式。与它对其他细胞类型的作用不同,TGF-β不会增强纤连蛋白的合成或其整合到细胞外基质中的过程。然而,TGF-β处理会改变许多其他分泌蛋白的合成。用TGF-β处理4或8小时的SMC分泌的一种分子量为38,000-D的蛋白双峰明显增加,已知肝素(另一种SMC生长抑制剂)会增加该蛋白的合成,这表明肝素和TGF-β介导的SMC生长抑制在代谢方面具有相似性。这些数据表明,TGF-β可能在发育过程中和血管损伤后SMC的增殖和组织中发挥重要而复杂的调节作用。

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