一种双位内体使 Vero 细胞不受蓖麻毒素侵袭

Timothy F. Czajka, David J. Vance, Renji Song, Nicholas J. Mantis
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引用次数: 0

摘要

在哺乳动物细胞的细胞质中以 "体内抗体 "的形式表达源自驼科动物的单域抗体(VHHs),为针对速效生物威胁制剂的医疗对策开辟了一条新途径。在本报告中,我们描述了一种异源二聚体内体,它能使 Vero 细胞几乎不受蓖麻毒素(RT)的影响,RT 是一种强效的 B 类核糖体失活蛋白。这种体内抗体由两个结构明确的 VHH 组成,它们针对 RT 的酶亚基(RTA)上的不同表位:V9E1 以 RTA 的 P-stalk 招募位点为靶点,V2A11 以 RTA 的活性位点为靶点。双位点 VHH 构建物对 RT 的抗性远远超过了单独的任何一种 VHH,并有效抑制了体外所有可测量的 RT 诱导的细胞毒性。我们认为,将双特异性内抗体定向递送到肺组织可能是保护呼吸道免受吸入性 RT 暴露影响的一种新方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

A Biparatopic Intrabody Renders Vero Cells Impervious to Ricin Intoxication

A Biparatopic Intrabody Renders Vero Cells Impervious to Ricin Intoxication
Expression of camelid-derived, single-domain antibodies (VHHs) within the cytoplasm of mammalian cells as “intrabodies” has opened up novel avenues for medical countermeasures against fast-acting biothreat agents. In this report, we describe a heterodimeric intrabody that renders Vero cells virtually impervious to ricin toxin (RT), a potent Category B ribosome-inactivating protein. The intrabody consists of two structurally defined VHHs that target distinct epitopes on RT’s enzymatic subunit (RTA): V9E1 targets RTA’s P-stalk recruitment site, and V2A11 targets RTA’s active site. Resistance to RT conferred by the biparatopic VHH construct far exceeded that of either of the VHHs alone and effectively inhibited all measurable RT-induced cytotoxicity in vitro. We propose that the targeted delivery of bispecific intrabodies to lung tissues may represent a novel means to shield the airways from the effects of inhalational RT exposure.
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