Erb L, Liu J, Ockerhausen J, Kong Q, Garrad R C, Griffin K, Neal C, Krugh B, Santiago-Pérez L I, González F A, Gresham H D, Turner J T, Weisman G A
Department of Biochemistry, University of Missouri-Columbia, Columbia, Missouri 65212, USA.
J Cell Biol. 2001 Apr 30;153(3):491-501. doi: 10.1083/jcb.153.3.491.
The P2Y(2) nucleotide receptor (P2Y(2)R) contains the integrin-binding domain arginine-glycine-aspartic acid (RGD) in its first extracellular loop, raising the possibility that this G protein-coupled receptor interacts directly with an integrin. Binding of a peptide corresponding to the first extracellular loop of the P2Y(2)R to K562 erythroleukemia cells was inhibited by antibodies against alpha(V)beta(3)/beta(5) integrins and the integrin-associated thrombospondin receptor, CD47. Immunofluorescence of cells transfected with epitope-tagged P2Y(2)Rs indicated that alpha(V) integrins colocalized 10-fold better with the wild-type P2Y(2)R than with a mutant P2Y(2)R in which the RGD sequence was replaced with RGE. Compared with the wild-type P2Y(2)R, the RGE mutant required 1,000-fold higher agonist concentrations to phosphorylate focal adhesion kinase, activate extracellular signal-regulated kinases, and initiate the PLC-dependent mobilization of intracellular Ca(2+). Furthermore, an anti-alpha(V) integrin antibody partially inhibited these signaling events mediated by the wild-type P2Y(2)R. Pertussis toxin, an inhibitor of G(i/o) proteins, partially inhibited Ca(2+) mobilization mediated by the wild-type P2Y(2)R, but not by the RGE mutant, suggesting that the RGD sequence is required for P2Y(2)R-mediated activation of G(o), but not G(q). Since CD47 has been shown to associate directly with G(i/o) family proteins, these results suggest that interactions between P2Y(2)Rs, integrins, and CD47 may be important for coupling the P2Y(2)R to G(o).
P2Y(2)核苷酸受体(P2Y(2)R)在其第一个细胞外环中含有整合素结合结构域精氨酸-甘氨酸-天冬氨酸(RGD),这增加了这种G蛋白偶联受体与整合素直接相互作用的可能性。与P2Y(2)R第一个细胞外环对应的肽与K562红白血病细胞的结合受到抗α(V)β(3)/β(5)整合素和整合素相关的血小板反应蛋白受体CD47抗体的抑制。用表位标记的P2Y(2)R转染的细胞的免疫荧光表明,α(V)整合素与野生型P2Y(2)R共定位的效果比与RGD序列被RGE取代的突变型P2Y(2)R好10倍。与野生型P2Y(2)R相比,RGE突变体需要高1000倍的激动剂浓度才能使粘着斑激酶磷酸化、激活细胞外信号调节激酶并启动PLC依赖的细胞内Ca(2+)动员。此外,抗α(V)整合素抗体部分抑制了野生型P2Y(2)R介导的这些信号事件。百日咳毒素是一种G(i/o)蛋白抑制剂,它部分抑制了野生型P2Y(2)R介导的Ca(2+)动员,但不抑制RGE突变体介导的Ca(2+)动员,这表明RGD序列是P2Y(2)R介导的G(o)激活所必需的,但不是G(q)激活所必需的。由于已证明CD47可直接与G(i/o)家族蛋白结合,这些结果表明P2Y(2)R、整合素和CD47之间的相互作用可能对P2Y(2)R与G(o)的偶联很重要。
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