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Progress toward the development of a genetically engineered attenuated hepatitis A virus vaccine.

机译:转基因减毒甲型肝炎病毒疫苗的开发进展。

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摘要

Mutations which positively affect growth of hepatitis A virus in cell culture may negatively affect growth in vivo. Therefore, development of an attenuated vaccine for hepatitis A may require a careful balancing of mutations to produce a virus that will grow efficiently in cells suitable for vaccine production and still maintain a satisfactory level of attenuation in vivo. Since such a balance could be achieved most directly by genetic engineering, we are analyzing mutations that accumulated during serial passage of the HM-175 strain of hepatitis A virus in MRC-5 cell cultures in order to determine the relative importance of the mutations for growth in MRC-5 cells and for attenuation in susceptible primates. Chimeric viral genomes of the HM-175 strain were constructed from cDNA clones derived from a virulent virus and from two attenuated viruses adapted to growth in African green monkey kidney (AGMK) and MRC-5 cells, respectively. Viruses encoded by these chimeric genomes were recovered by in vitro or in vivo transfection and assessed for their ability to grow in cultured MRC-5 cells or to cause hepatitis in primates (tamarins). The only MRC-5-specific mutations that substantially increased the efficiency of growth in MRC-5 cells were a group of four mutations in the 5' noncoding (NC) region. These 5' NC mutations and a separate group of 5' NC mutations that accumulated during earlier passages of the HM-175 virus in primary AGMK cells appeared, independently and additively, to result in decreased biochemical evidence of hepatitis in tamarins. However, neither group of 5' NC mutations had a demonstrable effect on the extent of virus excretion or liver pathology in these animals.
机译:对细胞培养物中的甲型肝炎病毒的生长产生积极影响的突变可能对体内的生长产生负面影响。因此,开发用于甲型肝炎的减毒疫苗可能需要仔细平衡突变,以产生病毒,该病毒将在适合疫苗生产的细胞中有效生长,并且仍保持令人满意的体内减毒水平。由于这种平衡可以通过基因工程最直接地实现,因此我们正在分析在MRC-5细胞培养物中甲型肝炎病毒HM-175菌株的连续传代过程中积累的突变,以确定该突变对于生长的相对重要性在MRC-5细胞中的表达以及对敏感灵长类动物的减毒作用。 HM-175菌株的嵌合病毒基因组是由分别来自强毒病毒和两种减毒病毒的cDNA克隆构建的,分别适应于非洲绿猴肾(AGMK)和MRC-5细胞的生长。通过体外或体内转染回收由这些嵌合基因组编码的病毒,并评估它们在培养的MRC-5细胞中生长或在灵长类动物中引起肝炎的能力(ability猴)。实质上增加MRC-5细胞生长效率的唯一MRC-5特异性突变是5'非编码(NC)区域中的一组四个突变。在原代AGMK细胞中HM-175病毒较早传代期间积累的这些5'NC突变和一组单独的5'NC突变单独或累加地出现,从而导致绢毛猴肝炎的生化证据降低。但是,这组5'NC突变均未对这些动物的病毒排泄或肝脏病理状况产生明显影响。

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