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细胞毒性药物对单核细胞增生李斯特菌初次免疫反应的影响。

The effect of cytotoxic agents on the primary immune response to Listeria monocytogenes.

作者信息

Tripathy S P, Mackaness G B

出版信息

J Exp Med. 1969 Jul 1;130(1):1-16. doi: 10.1084/jem.130.1.1.

Abstract

Four drugs, representing four different categories of cytotoxic agents, were studied for their effect on the immune response to Listeria infection in mice. The development of the host's immune response is revealed by a progressive change in the slope of the bacterial growth curve in spleen and liver. It has its onset at 24 hr in untreated mice, but in the presence of effective immunosuppression the organism multiples uninterruptedly until the animal dies from overwhelming infection. When administered as single injections at the time of infection, cyclophosphamide, vinblastine, and azathioprine all produced an effective immunosuppression, characterized by continuous bacterial multiplication. Methotrexate was also immunosuppressive, but unlike the others its effects were reversible. They could be sustained, however, by further treatment. Studies of the time-response relationship indicated that cyclophosphamide was highly active over a broad time-span ranging from 2 days before infection to 4 days after infection. Vinblastine on the other hand was maximally active when given on the day of infection, while methotrexate had its greatest effect when given 48 hr after infection. These differences indicate that these three drugs act on different cell populations involved in the host's immune response. The effects observed have been discussed in relation to what is known of the modes of action of the drugs tested. An observation of interest was the phenomenon of enhanced immunity in animals treated with cyclophosphamide or vinblastine 7-11 days before, and with methotrexate 4 days before infection; reactive hyperplasia of lymphoid tissue following withdrawal of drug was again advanced as an explanation for the occurrence of this paradoxical effect. The experimental model employed is simple, requiring only routine bacteriological facilities and minimal equipment. It seems to offer a useful means of assessing the immunosuppressive activity of drugs and of determining the time-course of their action; it could also be of value in the screening of anticancer agents.

摘要

研究了代表四种不同细胞毒性药物类别的四种药物对小鼠李斯特菌感染免疫反应的影响。宿主免疫反应的发展通过脾脏和肝脏中细菌生长曲线斜率的逐渐变化来揭示。在未治疗的小鼠中,这种变化在24小时开始,但在有效的免疫抑制存在下,病原体持续繁殖,直到动物死于严重感染。当在感染时单次注射给药时,环磷酰胺、长春碱和硫唑嘌呤均产生有效的免疫抑制作用,其特征为细菌持续繁殖。甲氨蝶呤也具有免疫抑制作用,但与其他药物不同的是,其作用是可逆的。然而,通过进一步治疗可以维持其效果。时间-反应关系研究表明,环磷酰胺在感染前2天至感染后4天的广泛时间段内具有高活性。另一方面,长春碱在感染当天给药时活性最大,而甲氨蝶呤在感染后48小时给药时效果最佳。这些差异表明这三种药物作用于宿主免疫反应中不同的细胞群体。已根据所测试药物的已知作用模式对观察到的效果进行了讨论。一个有趣的观察结果是,在感染前7-11天用环磷酰胺或长春碱以及在感染前4天用甲氨蝶呤治疗的动物中出现了免疫增强现象;停药后淋巴组织的反应性增生再次被提出作为这种矛盾效应发生的解释。所采用的实验模型很简单,只需要常规的细菌学设施和最少的设备。它似乎提供了一种评估药物免疫抑制活性和确定其作用时间进程的有用方法;它在抗癌药物筛选中也可能有价值。

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