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劳氏肉瘤病毒前导RNA中编码的七氨基酸肽的体外合成。

Synthesis in vitro of a seven amino acid peptide encoded in the leader RNA of Rous sarcoma virus.

作者信息

Hackett P B, Petersen R B, Hensel C H, Albericio F, Gunderson S I, Palmenberg A C, Barany G

出版信息

J Mol Biol. 1986 Jul 5;190(1):45-57. doi: 10.1016/0022-2836(86)90074-4.

Abstract

Sequences of avian retroviral RNAs suggest that short open reading frames in the putatively untranslated leader sequences might direct the synthesis of small peptides. Previous analyses indicate that translation of Rous sarcoma virus (RSV) RNA in vitro faithfully reflects translation of the viral RNA in the chick cell. Accordingly, we sought to determine if the heptapeptide LP1, encoded in the open reading frame closest to the 5' end of RSV RNA, could be synthesized in vitro since this would strongly suggest that it might also be synthesized in vivo. Here we confirm that RSV RNA directs the synthesis of LP1 in rabbit reticulocyte lysates. LP1 is rapidly degraded in the lysate by an aminopeptidase activity. On the basis of the following observations, we propose that the open reading frame encoding LP1 plays a role in the life cycle of avian retroviruses. The LP1 open reading frame is ubiquitous with respect to position and length in 12 strains of avian retrovirus. In the amino acid sequences of the 12 strains, only three of the seven residues are invariant. On the basis of the conservation of the -3 and +4 nucleotides flanking the AUG codon, the strengths of initiation for translation of LP1 are approximately the same in the different viruses. The LP1 open reading frame is positioned in front of sites on retrovirus RNA that are required for initiation of cDNA synthesis and for packaging of the RNA into mature virus.

摘要

禽逆转录病毒RNA的序列表明,在假定的非翻译前导序列中的短开放阅读框可能指导小肽的合成。先前的分析表明,劳氏肉瘤病毒(RSV)RNA在体外的翻译忠实地反映了病毒RNA在鸡细胞中的翻译。因此,我们试图确定RSV RNA 5'端最接近的开放阅读框中编码的七肽LP1是否能在体外合成,因为这将有力地表明它也可能在体内合成。在这里,我们证实RSV RNA在兔网织红细胞裂解物中指导LP1的合成。LP1在裂解物中被氨肽酶活性迅速降解。基于以下观察结果,我们提出编码LP1的开放阅读框在禽逆转录病毒的生命周期中起作用。LP1开放阅读框在12种禽逆转录病毒的位置和长度方面普遍存在。在这12种毒株的氨基酸序列中,七个残基中只有三个是不变的。基于AUG密码子侧翼-3和+4核苷酸的保守性,LP1在不同病毒中的翻译起始强度大致相同。LP1开放阅读框位于逆转录病毒RNA上启动cDNA合成和将RNA包装成成熟病毒所需的位点之前。

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