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猿猴病毒40型回复突变增强子在增强子功能方面表现出受限的宿主范围。

Simian virus 40 revertant enhancers exhibit restricted host ranges for enhancer function.

作者信息

Shepard A, Clarke J, Herr W

机构信息

Cold Spring Harbor Laboratory, New York 11724.

出版信息

J Virol. 1988 Sep;62(9):3364-70. doi: 10.1128/JVI.62.9.3364-3370.1988.

Abstract

We have assayed the cell-specific activity of a matched set of four enhancers found in viral revertants derived from simian virus 40 (SV40) enhancer mutants. These enhancers all contain 71-base-pair duplications that span identical regions or, in one case, the same region shifted by 2 nucleotides. The four enhancers differ, however, in that each one either carries a different wild-type pair of the genetically defined SV40 enhancer A, B, or C elements, with the other two elements mutated, or carries all three elements mutated. The three enhancers carrying two copies of a wild-type element effectively enhance transcription in CV-1 and HeLa cells, but only the enhancer containing a duplicated wild-type C element exhibits activity in NIH 3T3 cells. These results show that the ability of the A, B, and C elements to compensate for one another is cell specific and that selection for enhancer function in one cell type can generate enhancers with different cell-specific activities. These results are consistent with the hypothesis that tandem duplication of multiple distinct enhancer elements, as in wild-type strains of SV40 (e.g., the 72-base-pair repeat), has the property of expanding the host range of an enhancer.

摘要

我们分析了一组匹配的四个增强子的细胞特异性活性,这些增强子存在于源自猴病毒40(SV40)增强子突变体的病毒回复体中。这些增强子都含有71个碱基对的重复序列,它们跨越相同区域,或者在一种情况下,相同区域偏移了2个核苷酸。然而,这四个增强子的不同之处在于,每个增强子要么携带一对不同的、经基因定义的野生型SV40增强子A、B或C元件,另外两个元件发生突变,要么携带所有三个元件均发生突变。携带两个野生型元件拷贝的三个增强子能有效增强CV-1和HeLa细胞中的转录,但只有含有重复野生型C元件的增强子在NIH 3T3细胞中表现出活性。这些结果表明,A、B和C元件相互补偿的能力具有细胞特异性,并且在一种细胞类型中对增强子功能的选择可以产生具有不同细胞特异性活性的增强子。这些结果与以下假设一致,即如SV40野生型菌株(例如72个碱基对的重复序列)中那样,多个不同增强子元件的串联重复具有扩大增强子宿主范围的特性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ee38/253459/83368383732e/jvirol00088-0305-a.jpg

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