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干扰素通过一个5'干扰素共有序列增加主要组织相容性复合体I类基因的转录。

Interferons increase transcription of a major histocompatibility class I gene via a 5' interferon consensus sequence.

作者信息

Sugita K, Miyazaki J, Appella E, Ozato K

出版信息

Mol Cell Biol. 1987 Jul;7(7):2625-30. doi: 10.1128/mcb.7.7.2625-2630.1987.

Abstract

Interferons (IFNs) augment expression of major histocompatibility class I genes in many cells. To study the effect of IFNs on transcription of class I genes, we prepared and tested activity of chloramphenicol acetyltransferase (CAT) hybrid genes in which the cat gene is under the control of the 5' flanking region of the murine H-2Ld gene. NIH 3T3 cells transiently transfected with a cat construct having the sequence from position -210 to -134 showed a four- to fivefold increase in CAT activity when treated with IFN-alpha/beta. This sequence contains the IFN consensus sequence (ICS) shared among IFN-inducible genes, as well as the class I regulatory element (CRE) that controls up and down regulation of class I gene expression. To determine the precise sequence requirement for the IFN action, the ICS and CRE were independently placed upstream of the class I or a heterologous simian virus 40 promoter, and CAT activity was tested. The ICS, but not the CRE, enhanced activity of both promoters by about twofold upon exposure to IFN-alpha/beta, although greater responses were noted when the ICS and CRE were combined. These results demonstrate that the ICS alone is capable of enhancing promoter activity in response to IFN-alpha/beta treatment and that the CRE exerts a synergistic effect. Further, we show that the ICS functions as an inducible enhancer since it acts regardless of its orientation and distance in the simian virus 40 promoter.

摘要

干扰素(IFNs)可增强许多细胞中主要组织相容性复合体I类基因的表达。为了研究IFNs对I类基因转录的影响,我们制备并测试了氯霉素乙酰转移酶(CAT)杂交基因的活性,其中cat基因受鼠H-2Ld基因5'侧翼区域的控制。用具有从-210到-134位置序列的cat构建体瞬时转染的NIH 3T3细胞,在用IFN-α/β处理时,CAT活性增加了4到5倍。该序列包含IFN诱导基因共有的IFN共有序列(ICS),以及控制I类基因表达上调和下调的I类调节元件(CRE)。为了确定IFN作用的精确序列要求,将ICS和CRE分别置于I类或异源猿猴病毒40启动子的上游,并测试CAT活性。尽管当ICS和CRE组合时观察到更大的反应,但ICS而非CRE在暴露于IFN-α/β时将两个启动子的活性提高了约两倍。这些结果表明,单独的ICS能够响应IFN-α/β处理增强启动子活性,并且CRE发挥协同作用。此外,我们表明ICS作为一种诱导型增强子起作用,因为它在猿猴病毒40启动子中的作用与其方向和距离无关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0849/365402/4f94f8bba012/molcellb00079-0336-a.jpg

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