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使用嵌合单克隆抗体的联合疗法可保护小鼠免受致命的H5N1感染,并防止逃逸突变体的形成。

Combination therapy using chimeric monoclonal antibodies protects mice from lethal H5N1 infection and prevents formation of escape mutants.

作者信息

Prabakaran Mookkan, Prabhu Nayana, He Fang, Hongliang Qian, Ho Hui-Ting, Qiang Jia, Meng Tao, Goutama Michael, Kwang Jimmy

机构信息

Animal Health Biotechnology, Temasek Life Sciences Laboratory, National University of Singapore, Singapore, Singapore.

出版信息

PLoS One. 2009 May 22;4(5):e5672. doi: 10.1371/journal.pone.0005672.

Abstract

BACKGROUND

Given that there is a possibility of a human H5N1 pandemic and the fact that the recent H5N1 viruses are resistant to the anti-viral drugs, newer strategies for effective therapy are warranted. Previous studies show that single mAbs in immune prophylaxis can be protective against H5N1 infection. But a single mAb may not be effective in neutralization of a broad range of different strains of H5N1 and control of potential neutralization escape mutants.

METHODS/PRINCIPAL FINDINGS: We selected two mAbs which recognized different epitopes on the hemagglutinin molecule. These two mAbs could each neutralize in vitro escape mutants to the other and in combination could effectively neutralize viruses from clades 0, 1, 2.1, 2.2, 2.3, 4, 7 and 8 of influenza A H5N1 viruses. This combination of chimeric mAbs when administered passively, pre or post challenge with 10 MLD50 (50% mouse lethal dose) HPAI H5N1 influenza A viruses could protect 100% of the mice from two different clades of viruses (clades 1 and 2.1). We also tested the efficacy of a single dose of the combination of mAbs versus two doses. Two doses of the combination therapy not only affected early clearance of the virus from the lung but could completely prevent lung pathology of the H5N1 infected mice. No escape variants were detected after therapy.

CONCLUSIONS/SIGNIFICANCE: Our studies provide proof of concept that the synergistic action of two or more mAbs in combination is required for preventing the generation of escape mutants and also to enhance the therapeutic efficacy of passive therapy against H5N1 infection. Combination therapy may allow for a lower dose of antibody to be administered for passive therapy of influenza infection and hence can be made available at reduced economic costs during an outbreak.

摘要

背景

鉴于存在人类H5N1大流行的可能性,且近期的H5N1病毒对抗病毒药物具有抗性,因此需要新的有效治疗策略。先前的研究表明,免疫预防中的单克隆抗体可预防H5N1感染。但单克隆抗体可能无法有效中和多种不同的H5N1毒株,也无法控制潜在的中和逃逸突变体。

方法/主要发现:我们选择了两种识别血凝素分子上不同表位的单克隆抗体。这两种单克隆抗体各自可在体外中和针对另一种抗体的逃逸突变体,联合使用时可有效中和甲型H5N1流感病毒0、1、2.1、2.2、2.3、4、7和8分支的病毒。这种嵌合单克隆抗体组合在以10个半数致死剂量(50%小鼠致死剂量)的高致病性甲型H5N1流感病毒进行攻毒前或攻毒后被动给药时,可保护100%的小鼠免受两种不同分支病毒(1和2.1分支)的感染。我们还测试了单剂量与两剂量单克隆抗体组合的疗效。两剂量的联合疗法不仅影响病毒从肺部的早期清除,还可完全预防H5N1感染小鼠的肺部病变。治疗后未检测到逃逸变体。

结论/意义:我们的研究提供了概念验证,即需要两种或更多单克隆抗体的协同作用来防止逃逸突变体的产生,并提高被动治疗H5N1感染的疗效。联合疗法可降低流感感染被动治疗所需的抗体剂量,因此在疫情爆发期间可降低经济成本。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/853d/2682562/b92a2d101ce3/pone.0005672.g001.jpg

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