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在缺乏E1B的情况下,腺病毒E1A 12S增强细胞增殖、生长因子诱导及永生化。

Enhanced proliferation, growth factor induction and immortalization by adenovirus E1A 12S in the absence of E1B.

作者信息

Quinlan M P

机构信息

Department of Microbiology and Immunology, University of Tennessee, Memphis 38163.

出版信息

Oncogene. 1994 Sep;9(9):2639-47.

PMID:8058328
Abstract

Immortalization and transformation of primary epithelial cells requires expression of the adenovirus E1A and E1B genes, respectively. The E1A gene is involved in growth stimulatory processes. Little is known about the mechanism utilized by E1B, however, roles in growth stimulatory processes have also been implied. To determine whether there are any functional interactions between E1A 12S and the E1B 55K and 19K polypeptides, primary epithelial cells were infected with 12S viruses with different E1B regions. In the absence of both E1B proteins, there was an increase in 12S expression. This resulted in increased levels of DNA synthesis, entry into S-phase of the cell cycle and increased levels of proliferation, in the presence or absence of serum. There was also a higher induction of growth factor activity. In the presence of the 55K and absence of the 19K protein, there was a decrease in 12S expression. However, the highest induction of proliferative responses was observed. This suggests that expression of the 19K polypeptide inhibits 12S function directly. The lack of 19K expression also enabled the epithelial cells to have a much higher plating efficiency, achieve a greater cell density and reach the immortalized state faster. Although some modest differences in p53 expression were observed when compared to mock, they could not be correlated with any phenotype.

摘要

原代上皮细胞的永生化和转化分别需要腺病毒E1A和E1B基因的表达。E1A基因参与生长刺激过程。然而,对于E1B所利用的机制知之甚少,不过也有人暗示它在生长刺激过程中发挥作用。为了确定E1A 12S与E1B 55K和19K多肽之间是否存在任何功能相互作用,用具有不同E1B区域的12S病毒感染原代上皮细胞。在两种E1B蛋白均不存在的情况下,12S表达增加。这导致DNA合成水平提高、进入细胞周期的S期以及增殖水平提高,无论有无血清。生长因子活性的诱导也更高。在有55K而没有19K蛋白的情况下,12S表达降低。然而,观察到增殖反应的诱导最高。这表明19K多肽的表达直接抑制12S功能。缺乏19K表达还使上皮细胞具有更高的接种效率、达到更高的细胞密度并更快地达到永生化状态。尽管与 mock 相比观察到p53表达有一些适度差异,但它们与任何表型均无关联。

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