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参与UTP诱导大鼠动脉平滑肌细胞迁移的核苷酸受体。

Nucleotide receptors involved in UTP-induced rat arterial smooth muscle cell migration.

作者信息

Pillois Xavier, Chaulet Hervé, Belloc Isabelle, Dupuch Françoise, Desgranges Claude, Gadeau Alain-Pierre

机构信息

INSERM U441, Pessac, France.

出版信息

Circ Res. 2002 Apr 5;90(6):678-81. doi: 10.1161/01.res.0000013700.98464.8e.

DOI:10.1161/01.res.0000013700.98464.8e
PMID:11934835
Abstract

Many factors have been shown to be involved in the development of hyperplasic lesions of vessels, but the role of extracellular nucleotides remains largely unknown. The presence of P2Y and P2X nucleotide receptors on arterial endothelial and smooth muscle cells suggests a potential role for nucleotides in the vessel pathophysiology. Although the role of P2X in physiology of vessels is well documented, that of P2Y is not completely understood. We recently demonstrated that extracellular nucleotides, and particularly UTP, induced migration of cultured arterial smooth muscle cells (ASMCs). This migration is dependent on osteopontin expression and involves the Rho and mitogen-activated protein (MAP) kinase pathways. An important question is to determine the specific role of the different P2Y receptors of rat ASMCs in the UTP-induced migration process. Therefore, we first quantified mRNA levels of P2Y(2), P2Y(4), and P2Y(6) nucleotide receptors in cultured rat ASMCs by a competitive RT-PCR approach and demonstrated that P2Y(2) is the most highly expressed among these receptors potentially involved in the UTP-mediated response. In addition to UTP, UDP also induced ASMC migration even when UTP regeneration was inhibited, suggesting the involvement of UDP receptor P2Y(6). Moreover, suramin, a specific antagonist of rat P2Y(2) receptor, acted as an inhibitor of UTP-induced migration. Taken together, these results suggest a prominent role for the UTP receptor, P2Y(2), and for the UDP receptor, P2Y(6), in UTP-induced rat ASMC migration.

摘要

许多因素已被证明与血管增生性病变的发生有关,但细胞外核苷酸的作用在很大程度上仍不清楚。动脉内皮细胞和平滑肌细胞上存在P2Y和P2X核苷酸受体,这表明核苷酸在血管病理生理学中可能发挥作用。尽管P2X在血管生理学中的作用已有充分记录,但P2Y的作用尚未完全明确。我们最近证明,细胞外核苷酸,尤其是UTP,可诱导培养的动脉平滑肌细胞(ASMCs)迁移。这种迁移依赖于骨桥蛋白的表达,并涉及Rho和丝裂原活化蛋白(MAP)激酶途径。一个重要的问题是确定大鼠ASMCs不同P2Y受体在UTP诱导的迁移过程中的具体作用。因此,我们首先通过竞争性RT-PCR方法定量培养的大鼠ASMCs中P2Y(2)、P2Y(4)和P2Y(6)核苷酸受体的mRNA水平,并证明P2Y(2)是这些可能参与UTP介导反应的受体中表达最高的。除了UTP,UDP即使在UTP再生受到抑制时也能诱导ASMC迁移,这表明UDP受体P2Y(6)参与其中。此外,苏拉明是大鼠P2Y(2)受体的特异性拮抗剂,可作为UTP诱导迁移的抑制剂。综上所述,这些结果表明UTP受体P2Y(2)和UDP受体P2Y(6)在UTP诱导的大鼠ASMC迁移中起重要作用。

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