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用于兔热病免疫治疗的杂交瘤抗体的产生与特性分析

Generation and characterization of hybridoma antibodies for immunotherapy of tularemia.

作者信息

Lu Zhaohua, Roche Marly I, Hui Julia H, Unal Berkay, Felgner Philip L, Gulati Sunita, Madico Guillermo, Sharon Jacqueline

机构信息

Department of Pathology and Laboratory Medicine, Boston University School of Medicine, Boston, MA 02118, USA.

出版信息

Immunol Lett. 2007 Oct 15;112(2):92-103. doi: 10.1016/j.imlet.2007.07.006. Epub 2007 Aug 8.

Abstract

Tularemia is caused by the Gram-negative facultative intracellular bacterium Francisella tularensis, which has been classified as a category A select agent-a likely bioweapon. The high virulence of F. tularensis and the threat of engineered antibiotic resistant variants warrant the development of new therapies to combat this disease. We have characterized 14 anti-Francisella hybridoma antibodies derived from mice infected with F. tularensis live vaccine strain (LVS) for potential use as immunotherapy of tularemia. All 14 antibodies cross-reacted with virulent F. tularensis type A clinical isolates, 8 bound to a purified preparation of LVS LPS, and 6 bound to five protein antigens, identified by proteome microarray analysis. An IgG2a antibody, reactive with the LPS preparation, conferred full protection when administered either systemically or intranasally to BALB/c mice post challenge with a lethal dose of intranasal LVS; three other antibodies prolonged survival. These anti-Francisella hybridoma antibodies could be converted to chimeric versions with mouse V regions and human C regions to serve as components of a recombinant polyclonal antibody for clinical testing as immunotherapy of tularemia. The current study is the first to employ proteome microarrays to identify the target antigens of anti-Francisella monoclonal antibodies and the first to demonstrate the systemic and intranasal efficacy of monoclonal antibodies for post-exposure treatment of respiratory tularemia.

摘要

兔热病由革兰氏阴性兼性细胞内细菌土拉弗朗西斯菌引起,该菌已被列为A类选择生物制剂——一种可能的生物武器。土拉弗朗西斯菌的高毒力以及工程化抗生素抗性变体的威胁促使人们开发新的疗法来对抗这种疾病。我们对14种源自感染土拉弗朗西斯菌活疫苗株(LVS)的小鼠的抗土拉弗朗西斯菌杂交瘤抗体进行了表征,以作为兔热病免疫疗法的潜在用途。所有14种抗体均与强毒A型土拉弗朗西斯菌临床分离株发生交叉反应,8种与LVS脂多糖的纯化制剂结合,6种与通过蛋白质组微阵列分析鉴定的5种蛋白质抗原结合。一种与脂多糖制剂反应的IgG2a抗体,在给BALB/c小鼠经鼻内给予致死剂量的LVS攻击后,通过全身或鼻内给药可提供完全保护;其他三种抗体可延长生存期。这些抗土拉弗朗西斯菌杂交瘤抗体可以转化为具有小鼠V区和人C区的嵌合形式,作为重组多克隆抗体的组成部分用于临床测试,作为兔热病的免疫疗法。本研究首次采用蛋白质组微阵列来鉴定抗土拉弗朗西斯菌单克隆抗体的靶抗原,也是首次证明单克隆抗体对呼吸道兔热病暴露后治疗的全身和鼻内疗效。

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