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猿猴病毒40转化细胞中病毒功能的调控。

Regulation of viral functions in simian virus 40-transformed cells.

作者信息

Zouzias D, Basilico C

出版信息

Natl Cancer Inst Monogr. 1978 May(48):239-44.

PMID:219356
Abstract

To define the relationship between simian virus 40 (SV40)-specific T-antigen and cell growth and to look for regulatory mechanisms that might control T-antigen synthesis in transformed cells, we studied the expression of T-antigen and the viral transcription in SV40-transformed cells that were exponentially growing or arrested in the G1-phase of the cell cycle. We took advantage of the behavior of two lines of SV40-transformed mouse 3T3 cells (ts SV3T3), which, although transformed by wild-type SV40, are temperature sensitive for the expression of the transformed phenotype. At 32 degrees C, ts SV3T3 cells behave like standard transformants, whereas at 39 degrees C, they become arrested in G1 after reaching saturatio n density or under serum starvation. At 32 degrees C or growing at 39 degrees C, ts SV3T3 were 100% T-antigen positive and contained virus-specific mRNA. However, after G1 arrest at 39 degrees C, most of the cells became T-antigen negative. This seems to be caused by a lack of transcription of the integrated viral DNA, since these cells contain no appreciable amounts of SV40-specific RNA. Induction of proliferation in resting, T-antigen-negative ts SV3T3 cultures results in the reappearance of T-antigen a few hours before the cells enter DNA synthesis. These results suggest that transcription of the viral genome and T-antigen expression in SV40-transformed cells is subjected to a cell cycle control.

摘要

为了确定猿猴病毒40(SV40)特异性T抗原与细胞生长之间的关系,并寻找可能控制转化细胞中T抗原合成的调控机制,我们研究了处于指数生长期或停滞在细胞周期G1期的SV40转化细胞中T抗原的表达和病毒转录情况。我们利用了两株SV40转化的小鼠3T3细胞系(ts SV3T3)的特性,这两株细胞虽然由野生型SV40转化而来,但对转化表型的表达具有温度敏感性。在32℃时,ts SV3T3细胞表现得像标准转化细胞,而在39℃时,它们在达到饱和密度或血清饥饿状态下会停滞在G1期。在32℃或在39℃生长时,ts SV3T3细胞100%为T抗原阳性,并含有病毒特异性mRNA。然而,在39℃停滞在G1期后,大多数细胞变为T抗原阴性。这似乎是由于整合的病毒DNA缺乏转录所致,因为这些细胞不含可观数量的SV40特异性RNA。在静止的、T抗原阴性的ts SV3T3培养物中诱导增殖会导致在细胞进入DNA合成前几小时T抗原重新出现。这些结果表明,SV40转化细胞中病毒基因组的转录和T抗原的表达受到细胞周期的控制。

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