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呼吸道合胞病毒RNA类似物进行的RNA复制不遵循六规则,并且在前导端保留了一个非病毒的三核苷酸延伸。

RNA replication by a respiratory syncytial virus RNA analog does not obey the rule of six and retains a nonviral trinucleotide extension at the leader end.

作者信息

Samal S K, Collins P L

机构信息

Regional College of Veterinary Medicine, University of Maryland, College Park 20742, USA.

出版信息

J Virol. 1996 Aug;70(8):5075-82. doi: 10.1128/JVI.70.8.5075-5082.1996.

Abstract

Genome analogs ("minigenomes") of Sendai and measles viruses replicate efficiently only if their nucleotide length is an even multiple of six, a requirement called the rule of six (P. Calain and L. Roux, J. Virol. 67:4822-4830, 1993; M. S. Sidhu, J. Chan, K. Kaelin, P. Spielhofer, F. Radecke, H. Schneider, M. Masurekar, P. C. Dowling, M. A. Billeter, and S. A. Udem, Virology 208:800-807, 1995). The existence of a comparable requirement was tested for respiratory syncytial virus (RSV), which also is a member of family Paramyxoviridae and whose natural genome length also is a multiple of six. An internally truncated analog of RSV positive-sense replicative intermediate RNA (antigenome) bearing the chloramphenicol acetyltransferase gene as a reporter was synthesized from cDNA in vitro. This RNA was transfected into cells which were infected with RSV as a helper. Miniantigenomic RNA was indistinguishable from previously studied negative-sense minigenome RNA in its ability to participate in transcription, RNA replication, and incorporation into transmissible particles. Sixteen miniantigenomes which were of slightly different lengths and which in aggregate represented multiples of a wide range of integers including 1 to 15 were constructed. During transfection and two serial passages, the various miniantigenomes were essentially indistinguishable with regard to the efficiency of transcription, RNA replication, and packaging into transmissible particles. Progeny minigenomes of six different mutants were recovered postpassage, copied into cDNA, cloned, and sequenced completely. The length of each of these RNAs was found to have remained unchanged during replication and passage. Thus, RSV transcription and replication appear to lack the requirement that the template length be an even multiple of an integer such as six, which for Sendai and measles viruses is obligatory for nucleocapsid function. Each of the in vitro-synthesized miniantigenomes used in transfection contained a nonviral extension of three nucleotides, GGG, on the 5' (leader) end contributed by the T7 promoter. The termini of the recovered minigenomes were examined for five mutants by RNA circularization followed by cDNA synthesis, amplification, cloning, and sequencing. Unexpectedly, each recovered minigenome contained the complement of this nonviral extension on the 3' (leader) end, showing that it had been faithfully copied and maintained during RNA replication and passage. The nonviral trinucleotide did not appear to affect the activity of the template.

摘要

仙台病毒和麻疹病毒的基因组类似物(“微型基因组”)只有在其核苷酸长度是6的偶数倍时才能高效复制,这一要求被称为六规则(P. 卡拉安和L. 鲁克斯,《病毒学杂志》67:4822 - 4830, 1993;M. S. 西杜、J. 陈、K. 凯林、P. 施皮尔霍费尔、F. 拉德克、H. 施奈德、M. 马苏雷卡尔、P. C. 道林、M. A. 比勒特和S. A. 乌德姆,《病毒学》208:800 - 807, 1995)。呼吸道合胞病毒(RSV)也属于副粘病毒科,其天然基因组长度也是6的倍数,因此对其是否存在类似要求进行了测试。从cDNA体外合成了一种内部截短的RSV正链复制中间RNA(反基因组)类似物,该类似物带有氯霉素乙酰转移酶基因作为报告基因。将这种RNA转染到感染了RSV作为辅助病毒的细胞中。微型反基因组RNA在参与转录、RNA复制以及整合到可传播颗粒中的能力方面,与先前研究的负链微型基因组RNA没有区别。构建了16个长度略有不同的微型反基因组,它们总共代表了包括1到15在内的广泛整数的倍数。在转染和两次连续传代过程中,各种微型反基因组在转录效率、RNA复制以及包装到可传播颗粒方面基本没有区别。传代后回收了六个不同突变体的子代微型基因组,将其复制成cDNA,进行克隆并完全测序。发现这些RNA中的每一个在复制和传代过程中长度都保持不变。因此,RSV的转录和复制似乎并不要求模板长度是诸如6这样的整数的偶数倍,而对于仙台病毒和麻疹病毒来说,这是核衣壳功能所必需的。转染中使用的每个体外合成的微型反基因组在其5'(前导)端都包含由T7启动子贡献的三个核苷酸GGG的非病毒延伸。通过RNA环化,然后进行cDNA合成、扩增、克隆和测序,对五个突变体回收的微型基因组的末端进行了检查。出乎意料的是,每个回收的微型基因组在其3'(前导)端都包含这个非病毒延伸的互补序列,这表明它在RNA复制和传代过程中被忠实地复制和保留。这个非病毒三核苷酸似乎不影响模板的活性。

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本文引用的文献

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Rescue of measles viruses from cloned DNA.从克隆DNA中拯救麻疹病毒。
EMBO J. 1995 Dec 1;14(23):5773-84. doi: 10.1002/j.1460-2075.1995.tb00266.x.

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