腺病毒E3 10.4K和14.5K蛋白定位于质膜,其功能是防止肿瘤坏死因子引起的细胞溶解并下调表皮生长因子受体。
The adenovirus E3 10.4K and 14.5K proteins, which function to prevent cytolysis by tumor necrosis factor and to down-regulate the epidermal growth factor receptor, are localized in the plasma membrane.
作者信息
Stewart A R, Tollefson A E, Krajcsi P, Yei S P, Wold W S
机构信息
Department of Molecular Microbiology and Immunology, St. Louis University School of Medicine, Missouri 63104.
出版信息
J Virol. 1995 Jan;69(1):172-81. doi: 10.1128/JVI.69.1.172-181.1995.
Abstract
The adenovirus type 2 and 5 E3 10,400- and 14,500-molecular-weight (10.4K and 14.5K) proteins are both required to protect some cell lines from lysis by tumor necrosis factor and to down-regulate the epidermal growth factor receptor. We have shown previously that both 10.4K and 14.5K are integral membrane proteins and that 14.5K is phosphorylated and O glycosylated. The 10.4K protein coimmunoprecipitates with 14.5K, indicating that the two proteins function as a complex. Here we show, using immunofluorescence and two different cell surface-labeling techniques, that both proteins are localized in the plasma membrane. In addition, we show that trafficking of each protein to the plasma membrane depends on concomitant expression of the other protein. Finally, neither protein could be immunoprecipitated from conditioned media, indicating that neither is secreted. Taken together, these results suggest that the plasma membrane is the site at which 10.4K and 14.5K function to inhibit cytolysis by tumor necrosis factor and to down-regulate the epidermal growth factor receptor.
摘要
腺病毒2型和5型的E3 10400和14500分子量(10.4K和14.5K)蛋白对于保护某些细胞系免受肿瘤坏死因子介导的裂解以及下调表皮生长因子受体均是必需的。我们之前已经表明,10.4K和14.5K均为整合膜蛋白,且14.5K被磷酸化并进行了O-糖基化修饰。10.4K蛋白与14.5K共同免疫沉淀,表明这两种蛋白作为一个复合物发挥功能。在此我们利用免疫荧光和两种不同的细胞表面标记技术表明,这两种蛋白均定位于质膜。此外,我们表明每种蛋白向质膜的转运均依赖于另一种蛋白的共表达。最后,两种蛋白均不能从条件培养基中免疫沉淀出来,表明二者均不分泌。综上所述,这些结果提示质膜是10.4K和14.5K发挥功能以抑制肿瘤坏死因子介导的细胞溶解和下调表皮生长因子受体的位点。
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