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pp60c-src的肉豆蔻酰化对于与多瘤病毒中T抗原形成复合物并非必需。

Myristylation of pp60c-src is not required for complex formation with polyomavirus middle-T antigen.

作者信息

Wyss A, Kaech S, Ballmer-Hofer K

机构信息

Friedrich Miescher Institute, Basel, Switzerland.

出版信息

J Virol. 1990 Oct;64(10):5163-6. doi: 10.1128/JVI.64.10.5163-5166.1990.

Abstract

Middle-T antigen (middle-T), the transforming gene product of polyomavirus, associates with several cellular tyrosine kinases, such as pp60c-src. Complex formation leads to kinase activation and is essential for cell transformation. Middle-T-associated as well as uncomplexed pp60c-src is predominantly found in the plasma membrane. We transfected mouse 3T3 fibroblasts with a mutated c-src gene (2Ac-src), allowing the expression of a protein containing alanine instead of glycine in position 2 of the primary translation product. Contrary to the wild-type c-src gene product, pp60c-src(2A) was not myristylated and accumulated in the cytoplasm instead of being transferred to cellular membranes. The mutant protein was able to associate with middle-T and was activated similarly to the wild-type c-src gene product. Both wild-type and 2A mutant protein were membrane associated upon complex formation with middle-T. This finding suggests that the putative carboxy-terminal membrane anchor sequence of middle-T is sufficient to hold middle-T-associated pp60c-src(2A) in the plasma membrane.

摘要

中T抗原(Middle-T)是多瘤病毒的转化基因产物,它与多种细胞酪氨酸激酶相关联,如pp60c-src。复合物的形成会导致激酶激活,并且对于细胞转化至关重要。与Middle-T相关以及未形成复合物的pp60c-src主要存在于质膜中。我们用一个突变的c-src基因(2Ac-src)转染小鼠3T3成纤维细胞,该基因允许在初级翻译产物的第2位表达一种含有丙氨酸而非甘氨酸的蛋白质。与野生型c-src基因产物相反,pp60c-src(2A)未被肉豆蔻酰化,而是积累在细胞质中,而不是转移到细胞膜上。突变蛋白能够与Middle-T结合,并且与野生型c-src基因产物一样被激活。野生型和2A突变蛋白在与Middle-T形成复合物后都与膜相关。这一发现表明,Middle-T假定的羧基末端膜锚定序列足以将与Middle-T相关的pp60c-src(2A)保留在质膜中。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cb52/248010/536ef40c9932/jvirol00065-0572-a.jpg

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