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劳氏肉瘤病毒RNA无细胞翻译为高分子量多肽。

The cell-free translation of Rauscher leukemia virus RNA into high molecular weight polypeptides.

作者信息

Naso R B, Arcement L J, Wood G, Saunders T E, Arlinghaus R B

出版信息

Biochim Biophys Acta. 1975 Mar 10;383(2):195-206. doi: 10.1016/0005-2787(75)90261-0.

Abstract

Rauscher leukemia virus (RLV) 65-S RNA, 35-S mengovirus RNA and reticulocyte A-rich RNA each stimulated cell-free protein synthesis in a JLS-V5 cell derived S-30 system. rRNA, however, was not stimulatory in this system. Of the stimulated protein products only those synthesized in response to added RLV RNA were immune-precipitable with anti-RLV rabbit serum. Furthermore, cell-free incubations with pactamycin at a concentration which specifically inhibits initiation and not elongation prevented the stimulation of amino acid incorporation in response to added RLV RNA. Analysis of the polypeptides synthesized by the cell-free system in response to reticulocyte A-rich RNA, showed them to be globin-like and, therefore, also mRNA specific. The RLV RNA-directed product included at least two classes of polypeptides (mol. wts of 140 000-185 000 and 50 000-75 000) both of which were larger than the group specific polypeptides of mature virions. None of the internal structural polypeptides of mature virions were synthesized in response to RLV RNA. The large molecular weight, viral-specific polypeptides are candidate precursor polyproteins which may represent the translational products of a polycistronic mRNA with a single initiation site.

摘要

劳舍尔白血病病毒(RLV)65-S RNA、35-S脑心肌炎病毒RNA和网织红细胞富含A的RNA,均可在JLS-V5细胞来源的S-30系统中刺激无细胞蛋白质合成。然而,rRNA在该系统中并无刺激作用。在受刺激产生的蛋白质产物中,只有那些因添加RLV RNA而合成的产物,才能被抗RLV兔血清免疫沉淀。此外,在无细胞孵育体系中加入能特异性抑制起始而不抑制延伸的放线菌酮,可阻止因添加RLV RNA而引起的氨基酸掺入刺激。对无细胞系统在富含网织红细胞A的RNA刺激下合成的多肽进行分析,结果表明它们类似珠蛋白,因此也是mRNA特异性的。RLV RNA指导合成的产物至少包括两类多肽(分子量分别为140 000 - 185 000和50 000 - 75 000),这两类多肽都比成熟病毒粒子的群特异性多肽大。成熟病毒粒子的内部结构多肽均未因RLV RNA而合成。这些大分子病毒特异性多肽是候选前体多蛋白,可能代表具有单个起始位点的多顺反子mRNA的翻译产物。

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