首页> 美国卫生研究院文献>Biochemical Journal >Signal-transducing protein phosphorylation cascades mediated by Ras/Rho proteins in the mammalian cell: the potential for multiplex signalling.
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Signal-transducing protein phosphorylation cascades mediated by Ras/Rho proteins in the mammalian cell: the potential for multiplex signalling.

机译:Ras / Rho蛋白在哺乳动物细胞中介导的信号转导蛋白磷酸化级联反应:多重信号转导的潜力。

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摘要

The features of three distinct protein phosphorylation cascades in mammalian cells are becoming clear. These signalling pathways link receptor-mediated events at the cell surface or intracellular perturbations such as DNA damage to changes in cytoskeletal structure, vesicle transport and altered transcription factor activity. The best known pathway, the Ras-->Raf-->MEK-->ERK cascade [where ERK is extracellular-signal-regulated kinase and MEK is mitogen-activated protein (MAP) kinase/ERK kinase], is typically stimulated strongly by mitogens and growth factors. The other two pathways, stimulated primarily by assorted cytokines, hormones and various forms of stress, predominantly utilize p21 proteins of the Rho family (Rho, Rac and CDC42), although Ras can also participate. Diagnostic of each pathway is the MAP kinase component, which is phosphorylated by a unique dual-specificity kinase on both tyrosine and threonine in one of three motifs (Thr-Glu-Tyr, Thr-Phe-Tyr or Thr-Gly-Tyr), depending upon the pathway. In addition to activating one or more protein phosphorylation cascades, the initiating stimulus may also mobilize a variety of other signalling molecules (e.g. protein kinase C isoforms, phospholipid kinases, G-protein alpha and beta gamma subunits, phospholipases, intracellular Ca2+). These various signals impact to a greater or lesser extent on multiple downstream effectors. Important concepts are that signal transmission often entails the targeted relocation of specific proteins in the cell, and the reversible formation of protein complexes by means of regulated protein phosphorylation. The signalling circuits may be completed by the phosphorylation of upstream effectors by downstream kinases, resulting in a modulation of the signal. Signalling is terminated and the components returned to the ground state largely by dephosphorylation. There is an indeterminant amount of cross-talk among the pathways, and many of the proteins in the pathways belong to families of closely related proteins. The potential for more than one signal to be conveyed down a pathway simultaneously (multiplex signalling) is discussed. The net effect of a given stimulus on the cell is the result of a complex intracellular integration of the intensity and duration of activation of the individual pathways. The specific outcome depends on the particular signalling molecules expressed by the target cells and on the dynamic balance among the pathways.
机译:哺乳动物细胞中三个不同的蛋白质磷酸化级联的特征正在变得清晰。这些信号通路将受体介导的事件连接到细胞表面或细胞内扰动中,例如DNA损伤以改变细胞骨架结构,囊泡转运和改变的转录因子活性。通常会强烈刺激最著名的途径,即Ras-> Raf-> MEK-> ERK级联[其中ERK是细胞外信号调节激酶,而MEK是丝裂原激活蛋白(MAP)激酶/ ERK激酶]。受促分裂原和生长因子的影响。其他两种途径主要是由各种细胞因子,激素和各种形式的应激刺激,主要利用Rho家族的p21蛋白(Rho,Rac和CDC42),尽管Ras也可以参与。每种激酶的诊断都是MAP激酶成分,该成分在三个基序(Thr-Glu-Tyr,Thr-Phe-Tyr或Thr-Gly-Tyr)之一中,在酪氨酸和苏氨酸上被独特的双特异性激酶磷酸化,取决于路径。除了激活一个或多个蛋白磷酸化级联反应外,启动刺激还可以动员多种其他信号分子(例如蛋白激酶C亚型,磷脂激酶,G蛋白α和βγ亚基,磷脂酶,细胞内Ca2 +)。这些不同的信号或多或少地影响多个下游效应器。重要的概念是,信号传递通常需要特定蛋白质在细胞中的定向转移,以及通过调节的蛋白质磷酸化可逆地形成蛋白质复合物。信号传导电路可通过下游效应子使上游效应子磷酸化而完成,从而导致信号的调制。信号终止,并且组分主要通过去磷酸化返回基态。通路之间的串扰数量不确定,并且通路中的许多蛋白质都属于紧密相关的蛋白质家族。讨论了将一个以上信号同时沿路径传送的可能性(多路信号)。给定刺激对细胞的净效应是单个途径激活的强度和持续时间复杂的细胞内整合的结果。具体的结果取决于靶细胞表达的特定信号分子以及途径之间的动态平衡。

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