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A G-quadruplex-binding macrodomain within the 'SARS-unique domain' is essential for the activity of the SARS-coronavirus replication-transcription complex

机译:“ SARS唯一域”中的G四联体结合宏域对于SARS冠状病毒复制转录复合体的活性至关重要

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摘要

The multi-domain non-structural protein 3 of SARS-coronavirus is a component of the viral replication/transcription complex (RTC). Among other domains, it contains three sequentially arranged macrodomains: the X domain and subdomains SUD-N as well as SUD-M within the "SARS-unique domain". The X domain was proposed to be an ADP-ribose-1"-phosphatase or a poly(ADP-ribose)-binding protein, whereas SUD-NM binds oligo(G)-nucleotides capable of forming G-quadruplexes. Here, we describe the application of a reverse genetic approach to assess the importance of these macrodomains for the activity of the SARS-CoV RTC. To this end, Renilla luciferase-encoding SARS-CoV replicons with selectively deleted macrodomains were constructed and their ability to modulate the RTC activity was examined. While the SUD-N and the X domains were found to be dispensable, the SUD-M domain was crucial for viral genome replication/transcription. Moreover, alanine replacement of charged amino-acid residues of the SUD-M domain, which are likely involved in G-quadruplex-binding, caused abrogation of RTC activity. (C) 2015 Elsevier Inc. All rights reserved.
机译:SARS冠状病毒的多结构域非结构蛋白3是病毒复制/转录复合物(RTC)的组成部分。在其他域中,它包含三个顺序排列的宏域:X域和子域SUD-N以及“ SARS唯一域”内的SUD-M。 X结构域被提议为ADP-核糖-1”-磷酸酶或聚(ADP-核糖)结合蛋白,而SUD-NM结合能够形成G-四链体的寡核苷酸(G)。为了评估这些大域对SARS-CoV RTC活性的重要性,运用反向遗传学方法构建了编码有选择性缺失大域的海肾荧光素酶编码SARS-CoV复制子,并调节了RTC活性。虽然发现SUD-N和X结构域是可有可无的,但SUD-M结构域对于病毒基因组的复制/转录至关重要,而且,丙氨酸取代了SUD-M结构域的带电氨基酸残基,可能参与了G-四链体结合,导致RTC活性被废除(C)2015 Elsevier Inc.保留所有权利。

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