针对丙型肝炎病毒1a、1b、2a、2b、2c和3a基因型的临床相关人单克隆抗体的中和广度及协同作用
Breadth of neutralization and synergy of clinically relevant human monoclonal antibodies against HCV genotypes 1a, 1b, 2a, 2b, 2c, and 3a.
作者信息
Carlsen Thomas H R, Pedersen Jannie, Prentoe Jannick C, Giang Erick, Keck Zhen-Yong, Mikkelsen Lotte S, Law Mansun, Foung Steven K H, Bukh Jens
机构信息
Copenhagen Hepatitis C Program (CO-HEP), Department of Infectious Diseases and Clinical Research Centre, Hvidovre Hospital and Department of International Health, Immunology, and Microbiology, Faculty of Health and Medical Sciences, University of Copenhagen, Denmark.
出版信息
Hepatology. 2014 Nov;60(5):1551-62. doi: 10.1002/hep.27298. Epub 2014 Oct 2.
UNLABELLED
Human monoclonal antibodies (HMAbs) with neutralizing capabilities constitute potential immune-based treatments or prophylaxis against hepatitis C virus (HCV). However, lack of cell culture-derived HCV (HCVcc) harboring authentic envelope proteins (E1/E2) has hindered neutralization investigations across genotypes, subtypes, and isolates. We investigated the breadth of neutralization of 10 HMAbs with therapeutic potential against a panel of 16 JFH1-based HCVcc-expressing patient-derived Core-NS2 from genotypes 1a (strains H77, TN, and DH6), 1b (J4, DH1, and DH5), 2a (J6, JFH1, and T9), 2b (J8, DH8, and DH10), 2c (S83), and 3a (S52, DBN, and DH11). Virus stocks used for in vitro neutralization analysis contained authentic E1/E2, with the exception of full-length JFH1 that acquired the N417S substitution in E2. The 50% inhibition concentration (IC50) for each HMAb against the HCVcc panel was determined by dose-response neutralization assays in Huh7.5 cells with antibody concentrations ranging from 0.0012 to 100 μg/mL. Interestingly, IC50 values against the different HCVcc's exhibited large variations among the HMAbs, and only three HMAbs (HC-1AM, HC84.24, and AR4A) neutralized all 16 HCVcc recombinants. Furthermore, the IC50 values for a given HMAb varied greatly with the HCVcc strain, which supports the use of a diverse virus panel. In cooperation analyses, HMAbs HC84.24, AR3A, and, especially HC84.26, demonstrated synergistic effects towards the majority of the HCVcc's when combined individually with AR4A.
CONCLUSION
Through a neutralization analysis of 10 clinically relevant HMAbs against 16 JFH1-based Core-NS2 recombinants from genotypes 1a, 1b, 2a, 2b, 2c, and 3a, we identified at least three HMAbs with potent and broad neutralization potential. The neutralization synergism obtained when pooling the most potent HMAbs could have significant implications for developing novel strategies to treat and control HCV.
未标记
具有中和能力的人源单克隆抗体(HMAbs)构成了基于免疫的丙型肝炎病毒(HCV)治疗或预防的潜在手段。然而,缺乏携带真实包膜蛋白(E1/E2)的细胞培养衍生的HCV(HCVcc)阻碍了跨基因型、亚型和分离株的中和研究。我们研究了10种具有治疗潜力的HMAbs对一组16种基于JFH1的HCVcc的中和广度,这些HCVcc表达来自1a基因型(菌株H77、TN和DH6)、1b基因型(J4、DH1和DH5)、2a基因型(J6、JFH1和T9)、2b基因型(J8、DH8和DH10)、2c基因型(S83)和3a基因型(S52、DBN和DH11)的患者来源的Core-NS2。用于体外中和分析的病毒株含有真实的E1/E2,但全长JFH1在E2中获得了N417S替换的情况除外。通过在Huh7.5细胞中进行剂量反应中和试验,抗体浓度范围为0.0012至100μg/mL,确定每种HMAb对HCVcc组的50%抑制浓度(IC50)。有趣的是,不同HMAb对不同HCVcc的IC值表现出很大差异,只有三种HMAb(HC-1AM、HC84.24和AR4A)中和了所有16种HCVcc重组体。此外,给定HMAb的IC50值因HCVcc菌株而异,这支持使用多种病毒组。在协同分析中,HMAb HC84.24、AR3A,尤其是HC84.26,在与AR4A单独组合时,对大多数HCVcc表现出协同作用。
结论
通过对10种临床相关HMAb针对来自1a、1b、2a、2b、2c和3a基因型的16种基于JFH1的Core-NS2重组体进行中和分析,我们鉴定出至少三种具有强大且广泛中和潜力的HMAb。将最有效的HMAb组合时获得的中和协同作用可能对开发治疗和控制HCV的新策略具有重要意义。
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