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Acquisition of a Polybasic Hemagglutinin Cleavage Site by a Low-Pathogenic Avian Influenza Virus Is Not Sufficient for Immediate Transformation into a Highly Pathogenic Strain▿

机译:低致病性禽流感病毒获得的多元血凝素切割位点不足以立即转化为高致病性菌株S

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摘要

Highly pathogenic avian influenza viruses (HPAIV) differ from all other strains by a polybasic cleavage site in their hemagglutinin. All these HPAIV share the H5 or H7 subtype. In order to investigate whether the acquisition of a polybasic cleavage site by an avirulent avian influenza virus strain with a hemagglutinin other than H5 or H7 is sufficient for immediate transformation into an HPAIV, we adapted the hemagglutinin cleavage site of A/Duck/Ukraine/1/1963 (H3N8) to that of the HPAIV A/Chicken/Italy/8/98 (H5N2), A/Chicken/HongKong/220/97 (H5N1), or A/Chicken/Germany/R28/03 (H7N7) and generated the recombinant wild-type and cleavage site mutants. In contrast to the wild type, multicycle replication of these mutants in tissue culture was demonstrated by positive plaque assays and viral multiplication in the absence of exogenous trypsin. Therefore, in vitro all cleavage site mutants resemble an HPAIV. However, in chicken they did not exhibit high pathogenicity, although they could be reisolated from cloacal swabs to some extent, indicating enhanced replication in vivo. These results demonstrate that beyond the polybasic hemagglutinin cleavage site, the virulence of HPAIV in chicken is based on additional pathogenicity determinants within the hemagglutinin itself or in the other viral proteins. Taken together, these observations support the notion that acquisition of a polybasic hemagglutinin cleavage site by an avirulent strain with a non-H5/H7 subtype is only one among several alterations necessary for evolution into an HPAIV.
机译:高致病性禽流感病毒(HPAIV)与所有其他菌株的不同之处在于其血凝素中有一个多碱基切割位点。所有这些HPAIV都具有H5或H7亚型。为了研究用除H5或H7以外的血凝素的无毒禽流感病毒株获得的多价裂解位点是否足以立即转化为HPAIV,我们采用了A / Duck / Ukraine / 1的血凝素裂解位点/ 1963(H3N8)至HPAIV A /鸡肉/意大利/ 8/98(H5N2),A /鸡肉/香港/ 220/97(H5N1)或A /鸡肉/德国/ R28 / 03(H7N7)的产生了重组的野生型和切割位点突变体。与野生型相反,这些突变体在组织培养中的多周期复制通过阳性噬斑测定和在没有外源胰蛋白酶的情况下的病毒繁殖而得以证实。因此,在体外,所有切割位点突变体均类似于HPAIV。但是,在鸡中它们没有表现出高致病性,尽管它们可以从泄殖腔拭子中重新分离到一定程度,表明它们在体内的复制增强了。这些结果表明,在多元血凝素裂解位点之外,鸡中HPAIV的毒性是基于血凝素本身或其他病毒蛋白中的其他致病性决定因素。综上所述,这些观察结果支持这样的观点,即具有非H5 / H7亚型的无毒力菌株获得多聚血球凝集素裂解位点只是进化为HPAIV所必需的几种改变之一。

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