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分离鉴定具有抗狂犬病毒中和活性的人源单克隆抗体。

Isolation and characterization of novel human monoclonal antibodies possessing neutralizing ability against rabies virus.

机构信息

Department of Microbiology, Faculty of Medicine, Oita University, Yufu-City, Japan.

出版信息

Microbiol Immunol. 2010 Nov;54(11):673-83. doi: 10.1111/j.1348-0421.2010.00262.x.

Abstract

Rabies is a fatal viral encephalitis which is transmitted by exposure to the bite of rabid animals. Human and equine rabies immunoglobulins are indispensable pharmacological agents for severe bite exposure, as is vaccine. However, several disadvantages, including limited supply, adverse reactions, and high cost, hamper their wide application in developing countries. In the present study, two novel huMabs which neutralize rabies virus were established from vaccinated hyperimmune volunteers using the Epstein-Barr virus transformation method. One MAb (No. 254), which was subclass IgG3, effectively neutralized fixed rabies viruses of CVS, ERA, HEP-Flury, and Nishigahara strains and recognized a well-conserved epitope located in antigenic site II of the rabies virus glycoprotein. No. 254 possessed 68 ng/ml of FRNT₅₀ activity against CVS, 3.7 × 10⁻⁷ M of the Kd value, and the enhancing effect of complement-dependent virolysis. In addition, No. 254 showed effective neutralization potency in vivo in the mouse challenge test. The other MAb, 4D4, was subclass IgM and showed neutralizing activity against CVS and Nishigahara strains. 4D4 recognized a novel antigenic site which is associated with the neurovirulence of rabies, a glycoprotein located between antigenic site I and VI. Both human MAbs against rabies are expected to be utilized as a tool for future post-exposure prophylaxis.

摘要

狂犬病是一种致命的病毒性脑炎,通过接触患有狂犬病的动物的咬伤传播。人用和马用狂犬病免疫球蛋白是严重咬伤暴露时不可或缺的药理学制剂,疫苗也是如此。然而,由于供应有限、不良反应和高成本等几个缺点,它们在发展中国家的广泛应用受到了阻碍。在本研究中,使用 Epstein-Barr 病毒转化法从接种过疫苗的超免疫志愿者中建立了两种能够中和狂犬病病毒的新型 huMabs。一种 MAb(编号 254),属于 IgG3 亚类,能有效中和 CVS、ERA、HEP-Flury 和 Nishigahara 株的固定狂犬病病毒,并识别位于狂犬病病毒糖蛋白抗原位点 II 中的一个保守表位。254 号对 CVS 的 FRNT₅₀ 活性为 68ng/ml,Kd 值为 3.7×10⁻⁷ M,具有补体依赖性溶细胞作用的增强效应。此外,254 号在小鼠攻毒试验中表现出有效的体内中和效力。另一种 MAb,4D4,属于 IgM 亚类,对 CVS 和 Nishigahara 株具有中和活性。4D4 识别一个新的抗原表位,与狂犬病的神经毒力有关,位于抗原位点 I 和 VI 之间的糖蛋白上。这两种针对狂犬病的人源单抗有望被用作未来接触后预防的工具。

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