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αvβ3和α5β1整合素配体对小动脉平滑肌钙电流的调节作用

Modulation of calcium current in arteriolar smooth muscle by alphav beta3 and alpha5 beta1 integrin ligands.

作者信息

Wu X, Mogford J E, Platts S H, Davis G E, Meininger G A, Davis M J

机构信息

Microcirculation Research Institute and Departments of Medical Physiology, Texas A & M University Health Science Center, College Station, Texas 77843-1114, USA.

出版信息

J Cell Biol. 1998 Oct 5;143(1):241-52. doi: 10.1083/jcb.143.1.241.

Abstract

Vasoactive effects of soluble matrix proteins and integrin-binding peptides on arterioles are mediated by alphav beta3 and alpha5 beta1 integrins. To examine the underlying mechanisms, we measured L-type Ca2+ channel current in arteriolar smooth muscle cells in response to integrin ligands. Whole-cell, inward Ba2+ currents were inhibited after application of soluble cyclic RGD peptide, vitronectin (VN), fibronectin (FN), either of two anti-beta3 integrin antibodies, or monovalent beta3 antibody. With VN or beta3 antibody coated onto microbeads and presented as an insoluble ligand, current was also inhibited. In contrast, beads coated with FN or alpha5 antibody produced significant enhancement of current after bead attachment. Soluble alpha5 antibody had no effect on current but blocked the increase in current evoked by FN-coated beads and enhanced current when applied in combination with an appropriate IgG. The data suggest that alphavbeta3 and alpha5 beta1 integrins are differentially linked through intracellular signaling pathways to the L-type Ca2+ channel and thereby alter control of Ca2+ influx in vascular smooth muscle. This would account for the vasoactive effects of integrin ligands on arterioles and provide a potential mechanism for wound recognition during tissue injury.

摘要

可溶性基质蛋白和整合素结合肽对小动脉的血管活性作用是由αvβ3和α5β1整合素介导的。为了研究其潜在机制,我们测量了小动脉平滑肌细胞中L型钙通道电流对整合素配体的反应。应用可溶性环状RGD肽、玻连蛋白(VN)、纤连蛋白(FN)、两种抗β3整合素抗体中的任何一种或单价β3抗体后,全细胞内向Ba2+电流受到抑制。将VN或β3抗体包被在微珠上并作为不溶性配体呈现时,电流也受到抑制。相比之下,包被有FN或α5抗体的微珠在附着后可使电流显著增强。可溶性α5抗体对电流无影响,但可阻断FN包被微珠引起的电流增加,并在与适当的IgG联合应用时增强电流。数据表明,αvβ3和α5β1整合素通过细胞内信号通路与L型钙通道存在差异连接,从而改变血管平滑肌中Ca2+内流的控制。这可以解释整合素配体对小动脉的血管活性作用,并为组织损伤期间的伤口识别提供潜在机制。

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