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一种新型的针对狂犬病病毒 G 蛋白的二硫键稳定的单链可变抗体片段,具有增强的体内中和效力。

A novel disulfide-stabilized single-chain variable antibody fragment against rabies virus G protein with enhanced in vivo neutralizing potency.

机构信息

National Engineering Laboratory for AIDS Vaccine, College of Life Science, Jilin University, Changchun 130012, China.

出版信息

Mol Immunol. 2012 Jun;51(2):188-96. doi: 10.1016/j.molimm.2012.03.015. Epub 2012 Apr 6.

DOI:10.1016/j.molimm.2012.03.015
PMID:22484084
Abstract

Rabies is a fatal infectious disease requiring efficient protection provided by post-exposure prophylaxis (PEP) with rabies immunoglobulin (RIG). The single-chain Fv fragment (scFv) is a small engineered antigen binding protein derived from antibody variable heavy (V(H)) and light (V(L)) chains. This novel antibody format may potentially replace the current application of RIG to detect and neutralize rabies virus (RV). However, the broad use of scFvs is confined by their generally low stability. In this study, a scFv (FV57) was constructed based on the monoclonal antibody, MAB57, against RV. To enhance its stability and neutralizing potency, a disulfide-stabilized scFv, ds-FV57, was also derived by introduction of cysteines at V(H)44 and V(L)100. Furthermore, the cysteine at V(L)85 of ds-FV57 was mutated to serine to construct ds-FV57(VL85Ser) in order to avoid potential mis-formed disulfide bonds which would alter the affinity of the scFv. The stability and activity of all three proteins expressed in Escherichia coli were evaluated. All of the constructed scFvs could provide efficient protection against RV infection both in vivo and in vitro. However, the stability of ds-FV57(VL85Ser) was notably improved, and its in vitro neutralizing potency against RV infection was enhanced. Our findings from these stabilization modifications support the feasibility of developing scFvs for PEP treatment of rabies.

摘要

狂犬病是一种致命的传染病,需要通过狂犬病免疫球蛋白(RIG)的暴露后预防(PEP)来提供有效的保护。单链 Fv 片段(scFv)是一种源自抗体可变重链(V(H))和轻链(V(L))的小型工程抗原结合蛋白。这种新型抗体形式有可能替代当前 RIG 用于检测和中和狂犬病病毒(RV)的应用。然而,scFv 的广泛应用受到其普遍低稳定性的限制。在这项研究中,构建了一种基于针对 RV 的单克隆抗体 MAB57 的 scFv(FV57)。为了提高其稳定性和中和效力,还通过在 V(H)44 和 V(L)100 处引入半胱氨酸来衍生出二硫键稳定的 scFv,ds-FV57。此外,为了避免可能形成错误的二硫键从而改变 scFv 的亲和力,ds-FV57 的 V(L)85 处的半胱氨酸突变为丝氨酸,构建了 ds-FV57(VL85Ser)。在大肠杆菌中表达的所有三种蛋白质的稳定性和活性都进行了评估。所有构建的 scFv 都能在体内和体外有效地提供针对 RV 感染的保护。然而,ds-FV57(VL85Ser)的稳定性显著提高,其体外中和 RV 感染的效力增强。这些稳定性修饰的研究结果支持了开发 scFv 用于狂犬病 PEP 治疗的可行性。

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