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生长因子诱导的DNA合成和钙动员由Gq和Gi2介导。

Mediation of growth factor induced DNA synthesis and calcium mobilization by Gq and Gi2.

作者信息

LaMorte V J, Harootunian A T, Spiegel A M, Tsien R Y, Feramisco J R

机构信息

Department of Medicine, University of California, San Diego, La Jolla 92093.

出版信息

J Cell Biol. 1993 Apr;121(1):91-9. doi: 10.1083/jcb.121.1.91.

Abstract

A newly identified subclass of the heterotrimeric GTP binding regulatory protein family, Gq, has been found to be expressed in a diverse range of cell types. We investigated the potential role of this protein in growth factor signal transduction pathways and its potential relationship to the function of other G alpha subclasses. Recent biochemical studies have suggested that Gq regulates the beta 1 isozyme of phospholipase C (PLC beta 1), an effector for some growth factors. By microinjection of inhibitory antibodies specific to distinct G alpha subunits into living cells, we have determined that G alpha q transduces bradykinin- and thrombin-stimulated intracellular calcium transients which are likely to be mediated by PLC beta 1. Moreover, we found that G alpha q function is required for the mitogenic action of both of these growth factors. These results indicate that both thrombin and bradykinin utilize Gq to couple to increases in intracellular calcium, and that Gq is a necessary component of the mitogenic action of these factors. While microinjection of antibodies against G alpha i2 did not abolish calcium transients stimulated by either of these factors, such microinjection prevented DNA synthesis in response to thrombin but not to bradykinin. These data suggest that thrombin-induced mitogenesis requires both Gq and Gi2, whereas bradykinin needs only the former. Thus, different growth factors operating upon the same cell type use overlapping yet distinct sets of G alpha subtypes in mitogenic signal transduction pathways. The direct identification of the coupling of both a pertussis toxin sensitive and insensitive G protein subtype in the mitogenic pathways utilized by thrombin offers an in vivo biochemical clarification of previous results obtained by pharmacologic studies.

摘要

异三聚体GTP结合调节蛋白家族的一个新发现的亚类Gq,已被发现在多种细胞类型中表达。我们研究了这种蛋白在生长因子信号转导途径中的潜在作用及其与其他Gα亚类功能的潜在关系。最近的生化研究表明,Gq调节磷脂酶C(PLCβ1)的β1同工酶,PLCβ1是一些生长因子的效应器。通过将针对不同Gα亚基的抑制性抗体显微注射到活细胞中,我们确定Gαq转导缓激肽和凝血酶刺激的细胞内钙瞬变,这可能由PLCβ1介导。此外,我们发现这两种生长因子的促有丝分裂作用都需要Gαq发挥功能。这些结果表明,凝血酶和缓激肽都利用Gq来介导细胞内钙的增加,并且Gq是这些因子促有丝分裂作用的必要组成部分。虽然显微注射针对Gαi2的抗体并没有消除这两种因子刺激的钙瞬变,但这种显微注射阻止了凝血酶诱导的DNA合成,而对缓激肽诱导的DNA合成没有影响。这些数据表明,凝血酶诱导的有丝分裂需要Gq和Gi2,而缓激肽只需要前者。因此,作用于同一细胞类型的不同生长因子在有丝分裂信号转导途径中使用重叠但不同的Gα亚型组合。在凝血酶利用的有丝分裂途径中直接鉴定出一种对百日咳毒素敏感和不敏感的G蛋白亚型的偶联,为以前通过药理学研究获得的结果提供了体内生化解释。

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