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血管生成素调节内皮细胞衍生的肝素结合表皮生长因子样生长因子对血管平滑肌细胞的募集作用。

Angiopoietin-regulated recruitment of vascular smooth muscle cells by endothelial-derived heparin binding EGF-like growth factor.

作者信息

Iivanainen Erika, Nelimarkka Lassi, Elenius Varpu, Heikkinen Satu-Maria, Junttila Teemu T, Sihombing Laura, Sundvall Maria, Maatta Jorma A, Laine V Jukka O, Yla-Herttuala Seppo, Higashiyama Shigeki, Alitalo Kari, Elenius Klaus

机构信息

Medicity Research Laboratories, Department of Medical Biochemistry and Molecular Biology, University of Turku, FIN-20520 Turku, Finland.

出版信息

FASEB J. 2003 Sep;17(12):1609-21. doi: 10.1096/fj.02-0939com.

DOI:10.1096/fj.02-0939com
PMID:12958167
Abstract

Recruitment of vascular smooth muscle cells (SMC) by endothelial cells (EC) is essential for angiogenesis. Endothelial-derived heparin binding EGF-like growth factor (HB-EGF) was shown to mediate this process by signaling via ErbB1 and ErbB2 receptors in SMCs. 1) Analysis of ErbB-ligands demonstrated that primary ECs expressed only HB-EGF and neuregulin-1. 2) Primary SMCs expressed ErbB1 and ErbB2, but not ErbB3 or ErbB4. 3) Consistent with their known receptor specificities, recombinant HB-EGF, but not neuregulin-1, stimulated tyrosine phosphorylation of ErbB1 and ErbB2 and migration in SMCs. 4) Neutralization of HB-EGF or inhibition of ErbB1 or ErbB2 blocked 70-90% of the potential of ECs to stimulate SMC migration. Moreover, 5) angiopoietin-1, an EC effector with a role in recruitment of SMC-like cells to vascular structures in vivo, enhanced EC-stimulated SMC migration by a mechanism involving up-regulation of endothelial HB-EGF. Finally, 6) immunohistochemical analysis of developing human tissues demonstrated that HB-EGF was expressed in vivo in ECs associated with SMCs or pericytes but not in ECs of the hyaloid vessels not associated with SMCs. These results suggest an important role for HB-EGF and ErbB receptors in the recruitment of SMCs by ECs and elaborate on the mechanism by which angiopoietins exert their vascular effects.

摘要

内皮细胞(EC)募集血管平滑肌细胞(SMC)对血管生成至关重要。内皮细胞衍生的肝素结合表皮生长因子(HB-EGF)已被证明可通过SMC中的ErbB1和ErbB2受体信号传导来介导这一过程。1)对ErbB配体的分析表明,原代EC仅表达HB-EGF和神经调节蛋白-1。2)原代SMC表达ErbB1和ErbB2,但不表达ErbB3或ErbB4。3)与它们已知的受体特异性一致,重组HB-EGF而非神经调节蛋白-1刺激了SMC中ErbB1和ErbB2的酪氨酸磷酸化及迁移。4)中和HB-EGF或抑制ErbB1或ErbB2可阻断70 - 90%的EC刺激SMC迁移的潜能。此外,5)血管生成素-1是一种在体内将SMC样细胞募集到血管结构中起作用的EC效应因子,它通过涉及上调内皮HB-EGF的机制增强了EC刺激的SMC迁移。最后,6)对发育中的人体组织的免疫组织化学分析表明,HB-EGF在体内与SMC或周细胞相关的EC中表达,但在与SMC不相关的玻璃体血管的EC中不表达。这些结果表明HB-EGF和ErbB受体在EC募集SMC中起重要作用,并阐述了血管生成素发挥其血管效应的机制。

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