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Expression of the human immunodeficiency virus frameshift signal in a bacterial cell-free system: influence of an interaction between the ribosome and a stem-loop structure downstream from the slippery site.

机译:人类免疫缺陷病毒移码信号在无细菌细胞系统中的表达:核糖体与湿滑部位下游的茎环结构之间相互作用的影响。

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摘要

A-1 frameshift event is required for expression of the pol gene when ribosomes translate the mRNA of human immunodeficiency virus type-1 (HIV-1). In this study, we inserted the frameshift region of HIV-1 (a slippery heptanucleotide motif followed by a stem-loop) in a reporter gene coding for firefly luciferase. The ability of the corresponding mRNA, generated by in vitro transcription, to be translated in an Escherichia coli cell-free extract is the first demonstration that the HIV-1 frameshift can be reproduced in a bacterial cell-free extract, providing a powerful approach for analysis of the frameshift mechanism. The responses of the frameshift signal to chloramphenicol, an inhibitor of peptide bond formation, and spectinomycin, an inhibitor of translocation, suggest that the frameshift complies with the same rules found in eukaryotic translation systems. Furthermore, when translation was performed in the presence of streptomycin and neamine, two error-inducing antibiotics, or with hyperaccurate ribosomes mutated in S12, the frameshift efficiency was increased or decreased, respectively, but only in the presence of the stem-loop, suggesting that the stem-loop can influence the frameshift through a functional interaction with the ribosomes.
机译:当核糖体翻译人类免疫缺陷病毒1型(HIV-1)的mRNA时,pol基因的表达需要A-1移码事件。在这项研究中,我们在编码萤火虫荧光素酶的报告基因中插入了HIV-1的移码区(一个光滑的七核苷酸基序,然后是一个茎环)。通过体外转录产生的相应mRNA在大肠杆菌无细胞提取物中被翻译的能力是第一个证明HIV-1移码可以在细菌无细胞提取物中再现的能力,这提供了一种有力的方法移码机制的分析。移码信号对氯霉素(肽键形成的抑制剂)和壮观霉素(易位抑制剂)的响应表明,移码符合真核翻译系统中发现的相同规则。此外,当在链霉素和神经胺,两种诱导错误的抗生素存在下或在S12中突变的超高精度核糖体存在下进行翻译时,移码效率分别提高或降低,但仅在茎环存在下提示茎环可以通过与核糖体的功能性相互作用影响移码。

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