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逆转录病毒移码位点下游的RNA假结

RNA pseudoknots downstream of the frameshift sites of retroviruses.

作者信息

Le S Y, Shapiro B A, Chen J H, Nussinov R, Maizel J V

机构信息

Institute of Biological Sciences, National Research Council of Canada, Ottawa.

出版信息

Genet Anal Tech Appl. 1991 Nov;8(7):191-205. doi: 10.1016/1050-3862(91)90013-h.

DOI:10.1016/1050-3862(91)90013-h
PMID:1663382
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7128882/
Abstract

RNA pseudoknot structural motifs could have implications for a wide range of biological processes of RNAs. In this study, the potential RNA pseudoknots just downstream from the known and suspected retroviral frame-shift sites were predicted in the Rous sarcoma virus, primate immunodeficiency viruses (HIV-1, HIV-2, and SIV), equine infectious anemia virus, visna virus, bovine leukemia virus, human T-cell leukemia virus (types I and II), mouse mammary tumor virus, Mason-Pfizer monkey virus, and simian SRV-1 type-D retrovirus. Also, the putative RNA pseudoknots were detected in the gag-pol overlaps of two retrotransposons of Drosophila, 17.6 and gypsy, and the mouse intracisternal A particle. For each sequence, the thermodynamic stability and statistical significance of the secondary structure involved in the predicted tertiary structure were assessed and compared. Our results show that the stem-loop structures in the pseudoknots are both thermodynamically highly stable and statistically significant relative to other such configurations that potentially occur in the gag-pol or gag-pro and pro-pol junction domains of these viruses (300 nucleotides upstream and downstream from the possible frameshift sites are included). Moreover, the structural features of the predicted pseudoknots following the frameshift site of pro-pol overlaps of the HTLV-1 and HTLV-2 retroviruses are structurally well conserved. The occurrence of eight compensatory base changes in the tertiary interaction of the two related sequences allow the conservation of their tertiary structures in spite of the sequence divergence. The results support the possible control mechanism for frameshifting proposed by Brierley et al. and Jacks et al.

摘要

RNA假结结构基序可能对RNA的广泛生物学过程产生影响。在本研究中,我们对劳氏肉瘤病毒、灵长类免疫缺陷病毒(HIV-1、HIV-2和SIV)、马传染性贫血病毒、维斯纳病毒、牛白血病病毒、人类T细胞白血病病毒(I型和II型)、小鼠乳腺肿瘤病毒、梅森- Pfizer猴病毒和猿猴SRV-1 D型逆转录病毒中已知和疑似逆转录病毒移码位点下游的潜在RNA假结进行了预测。此外,在果蝇的两个逆转座子17.6和gypsy以及小鼠脑内A颗粒的gag-pol重叠区域中检测到了推定的RNA假结。对于每个序列,评估并比较了预测三级结构中涉及的二级结构的热力学稳定性和统计学意义。我们的结果表明,相对于这些病毒的gag-pol或gag-pro和pro-pol连接域中可能出现的其他此类构型(包括可能的移码位点上游和下游300个核苷酸),假结中的茎环结构在热力学上高度稳定且具有统计学意义。此外,HTLV-1和HTLV-2逆转录病毒的pro-pol重叠移码位点之后预测的假结的结构特征在结构上高度保守。尽管序列存在差异,但两个相关序列的三级相互作用中出现的八个补偿性碱基变化使它们的三级结构得以保留。这些结果支持了Brierley等人和Jacks等人提出的移码可能的控制机制。

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