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VRK1 signaling pathway in the context of the proliferation phenotype in head and neck squamous cell carcinoma.

机译:头颈部鳞状细胞癌增殖表型中的VRK1信号通路。

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The vaccinia-related kinase (VRK) proteins are a new family with three members in the human kinome. The VRK1 protein phosphorylates several transcription factors and has been postulated to be involved in regulation of cell proliferation. In normal squamous epithelium, VRK1 is expressed in the proliferation area. Because VRK1 can stabilize p53, the expression of the VRK1 protein was analyzed in the context of the p53 pathway and the proliferation phenotype in a series of 73 head and neck squamous cell carcinomas. VRK1 protein level positively correlated with p53 response proteins, particularly hdm2 and p21. The VRK1 protein also correlated positively with several proteins associated with proliferation, such as cyclin-dependent kinase 2 (CDK2), CDK6, cdc2, cyclins B1 and A, topoisomerase II, survivin, and Ki67. The level of VRK1 protein behaves like a proliferation marker in this series of head and neck squamous cell carcinomas. To identify a possible regulatory role for VRK1 and because it regulates gene transcription, the promoters of two genes were studied, CDK2 and SURVIVIN, whose proteins correlated positively with VRK1. VRK1 increases the activity of both the CDK2 and SURVIVIN gene promoters. The expression of VRK1 was analyzed in the context of regulators of the G1-S transition. VRK1 protein levels increase in response to E2F1 and are reduced by retinoblastoma and p16. These data suggest that VRK1 might play a role in cell cycle regulation and is likely to represent the beginning of a new control mechanism of cell cycle, particularly late in the G1-S phase.
机译:牛痘相关激酶(VRK)蛋白是一个新的家族,在人类kinome中具有三个成员。 VRK1蛋白使几种转录因子磷酸化,并被认为参与细胞增殖的调控。在正常的鳞状上皮中,VRK1在增殖区域表达。由于VRK1可以稳定p53,因此在一系列73例头颈部鳞状细胞癌中,通过p53途径和增殖表型分析了VRK1蛋白的表达。 VRK1蛋白水平与p53反应蛋白,尤其是hdm2和p21正相关。 VRK1蛋白还与几种与增殖相关的蛋白正相关,例如细胞周期蛋白依赖性激酶2(CDK2),CDK6,cdc2,细胞周期蛋白B1和A,拓扑异构酶II,survivin和Ki67。在这一系列的头颈部鳞状细胞癌中,VRK1蛋白的水平像增殖标记。为了确定VRK1可能的调节作用,并且因为它调节基因转录,研究了两个基因的启动子CDK2和SURVIVIN,它们的蛋白质与VRK1正相关。 VRK1增加CDK2和SURVIVIN基因启动子的活性。在G1-S过渡的调节子的背景下分析了VRK1的表达。 VRK1蛋白水平响应E2F1而增加,并被成视网膜细胞瘤和p16降低。这些数据表明VRK1可能在细胞周期调控中发挥作用,并且可能代表了细胞周期新控制机制的开始,尤其是在G1-S期后期。

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