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将一个多碱性切割基序插入低致病性禽流感 H6N1 病毒的血凝素中,可诱导产生高致病性表型。

Insertion of a multibasic cleavage motif into the hemagglutinin of a low-pathogenic avian influenza H6N1 virus induces a highly pathogenic phenotype.

机构信息

Department of Virology, Erasmus Medical Center, PO Box 2040, Rotterdam, Netherlands.

出版信息

J Virol. 2010 Aug;84(16):7953-60. doi: 10.1128/JVI.00449-10. Epub 2010 Jun 2.

Abstract

The highly pathogenic avian influenza (HPAI) virus phenotype is restricted to influenza A viruses of the H5 and H7 hemagglutinin (HA) subtypes. To obtain more information on the apparent subtype-specific nature of the HPAI virus phenotype, a low-pathogenic avian influenza (LPAI) H6N1 virus was generated, containing an HPAI H5 RRRKKR [downward arrow] G multibasic cleavage site (MBCS) motif in HA (the downward arrow indicates the site of cleavage). This insertion converted the LPAI virus phenotype into an HPAI virus phenotype in vitro and in vivo. The H6N1 virus with an MBCS displayed in vitro characteristics similar to those of HPAI H5 viruses, such as cleavage of HA(0) (the HA protein of influenza A virus initially synthesized as a single polypeptide precursor) and virus replication in the absence of exogenous trypsin. Studies of chickens confirmed the HPAI phenotype of the H6N1 virus with an MBCS, with an intravenous pathogenicity index of 1.4 and systemic virus replication upon intranasal inoculation, the hallmarks of HPAI viruses. This study provides evidence that the subtype-specific nature of the emergence of HPAI viruses is not at the molecular, structural, or functional level, since the introduction of an MBCS resulted in a fully functional virus with an HPAI virus genotype and phenotype.

摘要

高致病性禽流感(HPAI)病毒表型仅限于血凝素(HA)亚型为 H5 和 H7 的流感 A 病毒。为了获得更多关于 HPAI 病毒表型明显的亚型特异性的信息,我们生成了一种低致病性禽流感(LPAI)H6N1 病毒,其 HA 中含有一个 HPAI H5 RRRKKR[向下箭头]G 多碱性裂解位点(MBCS)基序(向下箭头表示裂解位点)。该插入使 LPAI 病毒表型在体外和体内转化为 HPAI 病毒表型。具有 MBCS 的 H6N1 病毒在体外表现出与 HPAI H5 病毒相似的特征,例如 HA(0)的裂解(流感 A 病毒最初合成的作为单一多肽前体的 HA 蛋白)和在没有外源性胰酶的情况下病毒复制。对鸡的研究证实了具有 MBCS 的 H6N1 病毒的 HPAI 表型,其静脉致病性指数为 1.4,并且通过鼻腔接种进行全身性病毒复制,这是 HPAI 病毒的标志。本研究提供的证据表明,HPAI 病毒出现的亚型特异性不是在分子、结构或功能水平上,因为引入 MBCS 导致具有 HPAI 病毒基因型和表型的完全功能性病毒。

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