Literature DB >> 16873248

New antiviral target revealed by the hexameric structure of mouse hepatitis virus nonstructural protein nsp15.

Xiaoling Xu1, Yujia Zhai, Fei Sun, Zhiyong Lou, Dan Su, Yuanyuan Xu, Rongguang Zhang, Andrzej Joachimiak, Xuejun C Zhang, Mark Bartlam, Zihe Rao.   

Abstract

The unique coronavirus transcription/replication machinery comprised of multiple virus-encoded nonstructural proteins (nsp) plays a vital role during initial and intermediate phases of the viral life cycle. The crystal structure of mouse hepatitis virus strain A59 (MHV-A59) nsp15 is reported at 2.15-A resolution. nsp15 is an XendoU endoribonuclease and is the first one from this family to have its structure unveiled. The MHV-A59 nsp15 monomer structure has a novel protein fold. Two nsp15 trimers form a back-to-back hexamer that is believed to be the functional unit. The structure reveals the catalytic site including the highly conserved residues His262, His277, and Lys317, which is supported by mutagenesis analysis. Gel filtration and enzyme activity assays confirmed that the hexamer is the active form for nsp15 and demonstrate the specificity of nsp15 for uridylate. The high sequence conservation of nsp15 in coronaviruses, including that of severe acute respiratory syndrome, suggests that this protein may provide a new target for the design of antiviral therapeutics.

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Year:  2006        PMID: 16873248      PMCID: PMC1563835          DOI: 10.1128/JVI.00525-06

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  32 in total

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Journal:  J Mol Biol       Date:  2005-10-03       Impact factor: 5.469

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  51 in total

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7.  Recognition of the murine coronavirus genomic RNA packaging signal depends on the second RNA-binding domain of the nucleocapsid protein.

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