鼠疫的潜在人类免疫疗法。

IF 4.1 Q2 IMMUNOLOGY
Immunotherapy advances Pub Date : 2021-10-05 eCollection Date: 2021-01-01 DOI:10.1093/immadv/ltab020
Voahangy Andrianaivoarimanana, Lovasoa Nomena Randriantseheno, Kristoffer M Moore, Nicola J Walker, Steven G Lonsdale, Sarah Kempster, Neil A Almond, Minoarisoa Rajerison, E Diane Williamson
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引用次数: 0

摘要

针对鼠疫耶尔森氏菌 V 抗原的两种单克隆抗体在鼠疫模型中的保护效力进行了测试。小鼠感染了来自马达加斯加的当前临床分离株,命名为鼠疫耶尔森菌 10-21/S。Mab7.3 在感染前 24 小时或感染后 24 小时经腹膜腔注射给小鼠,具有完全的保护作用。在-24小时或+24小时腹腔注射马巴29.3,在任一条件下都能保护4/5的小鼠;这首次证明了这种马巴在体内的保护效力。这些结果补充了目前正在进行人源化的 Mab7.3 的累积数据,突出了其作为鼠疫人类免疫疗法的潜力,鼠疫是马达加斯加以及非洲、亚洲和南美洲其他地区的一种持久性地方病。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Potential human immunotherapeutics for plague.

Potential human immunotherapeutics for plague.

Two monoclonal antibodies directed to the V antigen of Yersinia pestis have been tested for protective efficacy in a murine model of bubonic plague. Mice were infected with a current clinical isolate from Madagascar, designated Y. pestis 10-21/S. Mab7.3, delivered to mice intra-periteoneally at either 24 h prior to, or 24 h post-infection, was fully protective, building on many studies which have demonstrated the protective efficacy of this Mab against a number of different clinical isolates of Y. pestis. Mab 29.3, delivered intra-peritoneally at either -24 h or +24 h, protected 4/5 mice in either condition; this has demonstrated the protective efficacy of this Mab in vivo for the first time. These results add to the cumulative data about Mab7.3, which is currently being humanized and highlight its potential as a human immunotherapeutic for plague, which is an enduring endemic disease in Madagascar and other regions of Africa, Asia, and South America.

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