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莫洛尼鼠白血病病毒gag-pol连接区UAA和UGA终止密码子抑制过程中插入氨基酸的鉴定。

Identification of amino acids inserted during suppression of UAA and UGA termination codons at the gag-pol junction of Moloney murine leukemia virus.

作者信息

Feng Y X, Copeland T D, Oroszlan S, Rein A, Levin J G

机构信息

Laboratory of Molecular Genetics, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, MD 20892.

出版信息

Proc Natl Acad Sci U S A. 1990 Nov;87(22):8860-3. doi: 10.1073/pnas.87.22.8860.

Abstract

Expression of the murine leukemia virus pol gene occurs by translational readthrough of an in-frame UAG codon between the gag and pol coding regions. In a previous study, we mutated the UAG codon to UAA or UGA and demonstrated that both of these termination codons could be suppressed in reticulocyte lysates and in infected cells with the same efficiency as UAG. We now report the identity of the amino acids inserted in vitro in response to UAA and UGA in fusion products containing the gag-pol junction region. The results show that UAA, like UAG, directs the incorporation of glutamine, whereas UGA directs the incorporation of three amino acids, arginine, cysteine, and tryptophan. To our knowledge, this is the first report indicating misreading of UAA as glutamine and UGA as arginine and cysteine in higher eukaryotes. Interestingly, although our protein synthesis system presumably contains other known UAG and UGA suppressors, these tRNAs did not suppress the termination codons in our experiments. Thus, it seems possible that the sequence surrounding the gag-pol junction not only promotes suppression but also helps determine which tRNAs function in suppression.

摘要

鼠白血病病毒pol基因的表达是通过对gag和pol编码区之间一个符合读码框的UAG密码子进行翻译通读实现的。在先前的一项研究中,我们将UAG密码子突变为UAA或UGA,并证明这两个终止密码子在网织红细胞裂解物和感染细胞中都能被抑制,其效率与UAG相同。我们现在报告在含有gag-pol连接区的融合产物中,体外响应UAA和UGA插入的氨基酸的身份。结果表明,UAA与UAG一样,指导谷氨酰胺的掺入,而UGA指导三种氨基酸的掺入,即精氨酸、半胱氨酸和色氨酸。据我们所知,这是第一份表明在高等真核生物中UAA被误读为谷氨酰胺以及UGA被误读为精氨酸和半胱氨酸的报告。有趣的是,尽管我们的蛋白质合成系统可能含有其他已知的UAG和UGA抑制因子,但在我们的实验中这些tRNA并没有抑制终止密码子。因此,gag-pol连接区周围的序列似乎不仅促进抑制作用,还有助于确定哪些tRNA在抑制过程中发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c1b6/55059/d796bf539295/pnas01047-0184-a.jpg

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