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通过缺失核糖核苷酸还原酶大亚基生成减毒天坛痘苗病毒。

Generation of an attenuated Tiantan vaccinia virus by deletion of the ribonucleotide reductase large subunit.

机构信息

Institute of Military Veterinary Medicine, Academy of Military Medical Sciences of PLA, Jilin, People's Republic of China,

出版信息

Arch Virol. 2014 Sep;159(9):2223-31. doi: 10.1007/s00705-014-2057-8. Epub 2014 Mar 28.

Abstract

Attenuation of the virulence of vaccinia Tiantan virus (VTT) underlies the strategy adopted for mass vaccination campaigns. This strategy provides advantages of safety and efficacy over traditional vaccines and is aimed at minimization of adverse health effects. In this study, a mutant form of the virus, MVTT was derived from VTT by deletion of the ribonucleotide reductase large subunit (R1) (TI4L). Compared to wild-type parental (VTT) and revertant (VTT-rev) viruses, virulence of the mutant MVTT was reduced by 100-fold based on body weight reduction and by 3,200-fold based on determination of the intracranial 50% lethal infectious dose. However, the immunogenicity of MVTT was equivalent to that of the parental VTT. We also demonstrated that the TI4L gene is not required for efficient replication. These data support the conclusion that MVTT can be used as a replicating virus vector or as a platform for the development of vaccines against infectious diseases and for cancer therapy.

摘要

天坛株牛痘病毒(VTT)毒力的衰减是大规模疫苗接种策略的基础。该策略在安全性和有效性方面优于传统疫苗,旨在最大限度地减少对健康的不良影响。在这项研究中,通过缺失核糖核苷酸还原酶大亚基(R1)(TI4L),从 VTT 中衍生出一种病毒突变株 MVTT。与野生型亲本(VTT)和回复突变体(VTT-rev)病毒相比,突变体 MVTT 的毒力在体重减轻方面降低了 100 倍,在确定颅内 50%致死感染剂量方面降低了 3200 倍。然而,MVTT 的免疫原性与亲本 VTT 相当。我们还证明 TI4L 基因不是有效复制所必需的。这些数据支持以下结论:MVTT 可用作复制病毒载体,或作为开发针对传染病和癌症治疗疫苗的平台。

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