Zhao Mingming, Janas Justyna A, Niki Masaru, Pandolfi Pier Paolo, Van Aelst Linda
Cold Spring Harbor Laboratory, 1 Bungtown Road, Cold Spring Harbor, New York 11724, USA.
Mol Cell Biol. 2006 Apr;26(7):2479-89. doi: 10.1128/MCB.26.7.2479-2489.2006.
The Dok adaptor proteins play key regulatory roles in receptor and non-receptor kinase-initiated signaling pathways. Dok-1, the prototype member of this family, negatively regulates cell proliferation elicited by numerous growth factors, including platelet-derived growth factor (PDGF). However, how Dok-1 exerts its negative effect on mitogenesis has remained elusive. Using Dok-1 knockout cells and Dok-1 mutants deficient in binding to specific Dok-1-interacting proteins, we show that Dok-1 interferes with PDGF-stimulated c-myc induction and Ras/mitogen-activated protein kinase (MAPK) activation by tethering different signaling components to the cell membrane. Specifically, Dok-1 attenuates PDGF-elicited c-myc induction by recruiting Csk to active Src kinases, whereupon their activities and consequent c-myc induction are diminished. On the other hand, Dok-1 negatively regulates PDGF-induced MAPK activation by acting on Ras-GAP and at least one other Dok-1-interacting protein. Importantly, we demonstrate that Dok-1's actions on both of these signaling pathways contribute to its inhibitory effect on mitogenesis. Our data suggest a mechanistic basis for the inhibitory effect of Dok-1 on growth factor-induced mitogenesis and its role as a tumor suppressor.
Dok衔接蛋白在受体和非受体激酶启动的信号通路中发挥关键调节作用。该家族的原型成员Dok-1对包括血小板衍生生长因子(PDGF)在内的多种生长因子引发的细胞增殖具有负调节作用。然而,Dok-1如何对有丝分裂产生负面影响仍不清楚。利用Dok-1基因敲除细胞和缺乏与特定Dok-1相互作用蛋白结合能力的Dok-1突变体,我们发现Dok-1通过将不同的信号成分拴系到细胞膜上,干扰PDGF刺激的c-myc诱导和Ras/丝裂原活化蛋白激酶(MAPK)激活。具体而言,Dok-1通过招募Csk到活性Src激酶,减弱PDGF引发的c-myc诱导,随后它们的活性以及随之而来的c-myc诱导均减弱。另一方面,Dok-1通过作用于Ras-GAP和至少一种其他Dok-1相互作用蛋白,对PDGF诱导的MAPK激活起负调节作用。重要的是,我们证明Dok-1对这两条信号通路的作用均有助于其对有丝分裂的抑制作用。我们的数据为Dok-1对生长因子诱导的有丝分裂的抑制作用及其作为肿瘤抑制因子的作用提供了机制基础。
