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在体外激活HIV-1前体mRNA 3'加工需要一个上游元件和TAR。

Activation of HIV-1 pre-mRNA 3' processing in vitro requires both an upstream element and TAR.

作者信息

Gilmartin G M, Fleming E S, Oetjen J

机构信息

Department of Microbiology and Molecular Genetics, University of Vermont, Burlington 05405.

出版信息

EMBO J. 1992 Dec;11(12):4419-28. doi: 10.1002/j.1460-2075.1992.tb05542.x.

Abstract

The architecture of the human immunodeficiency virus type 1 (HIV-1) genome presents an intriguing dilemma for the 3' processing of viral transcripts--to disregard a canonical 'core' poly(A) site processing signal present at the 5' end of the transcript and yet to utilize efficiently an identical signal that resides at the 3' end of the message. The choice of processing sites in HIV-1 appears to be influenced by two factors: (i) proximity to the cap site, and (ii) sequences upstream of the core poly(A) site. We now demonstrate that an in vivo-defined upstream element that resides within the U3 region, 76 nucleotides upstream of the AAUAAA hexamer, acts specifically to enhance 3' processing at the HIV-1 core poly(A) site in vitro. We furthermore show that efficient in vitro 3' processing requires the RNA stem-loop structure of TAR, which serves to juxtapose spatially the upstream element and the core poly(A) site. An analysis of the stability of 3' processing complexes formed at the HIV-1 poly(A) site in vitro suggests that the upstream element may function by increasing processing complex stability at the core poly(A) site.

摘要

人类免疫缺陷病毒1型(HIV-1)基因组的结构在病毒转录本的3'加工方面呈现出一个有趣的难题——忽略转录本5'端存在的典型“核心”聚腺苷酸化位点加工信号,却又能有效利用位于信息3'端的相同信号。HIV-1加工位点的选择似乎受两个因素影响:(i)与帽位点的距离,以及(ii)核心聚腺苷酸化位点上游的序列。我们现在证明,位于U3区域、AAUAAA六聚体上游76个核苷酸处的一个体内定义的上游元件,在体外能特异性增强HIV-1核心聚腺苷酸化位点的3'加工。我们还进一步表明,高效的体外3'加工需要TAR的RNA茎环结构,它在空间上使上游元件和核心聚腺苷酸化位点并列。对体外在HIV-1聚腺苷酸化位点形成的3'加工复合物稳定性的分析表明,上游元件可能通过增加核心聚腺苷酸化位点处加工复合物的稳定性来发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/189e/557016/2b79045c47bf/emboj00097-0179-a.jpg

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