血管抑制素,即血管抑制性纤连蛋白肽,是溶血磷脂信号传导的选择性抑制剂。
Anastellin, the angiostatic fibronectin peptide, is a selective inhibitor of lysophospholipid signaling.
作者信息
Ambesi Anthony, McKeown-Longo Paula J
机构信息
Center for Cell Biology and Cancer Research (MC-165), Albany Medical College, Albany, NY 12208, USA.
出版信息
Mol Cancer Res. 2009 Feb;7(2):255-65. doi: 10.1158/1541-7786.MCR-08-0195. Epub 2009 Feb 10.
Angiogenesis is regulated by integrin-dependent cell adhesion and the activation of specific cell surface receptors on vascular endothelial cells by angiogenic factors. Lysophosphatidic acid (LPA) and sphingosine-1 phosphate (S1P) are bioactive lysophospholipids that activate G protein-coupled receptors that stimulate phosphatidylinositol 3-kinase (PI3K), Ras, and Rho effector pathways involved in vascular cell survival, proliferation, adhesion, and migration. Previous studies have shown that anastellin, a fragment of the first type III module of fibronectin, functions as an antiangiogenic peptide suppressing tumor growth and metastasis. We have previously shown that anastellin blocks serum-dependent proliferation of microvessel endothelial cells (MVEC) by affecting extracellular signal-regulated kinase (ERK)-dependent G(1)-S transition. However, the mechanism by which anastellin regulates endothelial cell function remains unclear. In the present study, we mapped several lysophospholipid-mediated signaling pathways in MVEC and examined the effects of anastellin on LPA- and S1P-induced MVEC proliferation, migration, and cytoskeletal organization. Both LPA and S1P activated PI3K, Ras/ERK, and Rho/Rho kinase pathways, leading to migration, G(1)-S cell cycle progression, and stress fiber formation, respectively. Stimulation of proliferation by LPA/S1P occurred through a G(i)-dependent Ras/ERK pathway, which was independent of growth factor receptors and PI3K and Rho/Rho kinase signaling. Although LPA and S1P activated both PI3K/Akt and Ras/ERK signaling through G(i), anastellin inhibited only the Ras/ERK pathway. Stress fiber formation in response to LPA was dependent on Rho/Rho kinase but independent of G(i) and unaffected by anastellin. These results suggest that lysophospholipid mediators of G(i) activation leading to PI3K/Akt and Ras/ERK signaling bifurcate downstream of G(i) and that anastellin selectively inhibits the Ras/ERK arm of the pathway.
血管生成受整合素依赖性细胞黏附以及血管生成因子对血管内皮细胞上特定细胞表面受体的激活作用调控。溶血磷脂酸(LPA)和1-磷酸鞘氨醇(S1P)是具有生物活性的溶血磷脂,它们激活G蛋白偶联受体,进而刺激磷脂酰肌醇3激酶(PI3K)、Ras和Rho效应器通路,这些通路参与血管细胞的存活、增殖、黏附和迁移。先前的研究表明,纤连蛋白第一III型模块的片段阿那司他丁可作为一种抗血管生成肽,抑制肿瘤生长和转移。我们之前已经表明,阿那司他丁通过影响细胞外信号调节激酶(ERK)依赖性的G1-S期转换来阻断微血管内皮细胞(MVEC)的血清依赖性增殖。然而,阿那司他丁调节内皮细胞功能的机制仍不清楚。在本研究中,我们绘制了MVEC中几种溶血磷脂介导的信号通路,并研究了阿那司他丁对LPA和S1P诱导的MVEC增殖、迁移和细胞骨架组织的影响。LPA和S1P均激活PI3K、Ras/ERK和Rho/Rho激酶通路,分别导致迁移、G1-S期细胞周期进程和应力纤维形成。LPA/S1P通过G(i)依赖性的Ras/ERK通路刺激增殖,该通路独立于生长因子受体以及PI3K和Rho/Rho激酶信号。尽管LPA和S1P通过G(i)激活PI3K/Akt和Ras/ERK信号,但阿那司他丁仅抑制Ras/ERK通路。对LPA的应激纤维形成依赖于Rho/Rho激酶,但独立于G(i)且不受阿那司他丁影响。这些结果表明,导致PI3K/Akt和Ras/ERK信号的G(i)激活的溶血磷脂介质在G(i)下游发生分支,并且阿那司他丁选择性抑制该通路的Ras/ERK分支。
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