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吸入苯对单核细胞增生李斯特菌免疫反应的调节作用。

Modulation of the immune response to Listeria monocytogenes by benzene inhalation.

作者信息

Rosenthal G J, Snyder C A

出版信息

Toxicol Appl Pharmacol. 1985 Sep 30;80(3):502-10. doi: 10.1016/0041-008x(85)90395-3.

Abstract

Benzene is a potent bone marrow toxicant. While all blood cell types are targets for benzene poisoning, lymphocytes are particularly sensitive. The immunotoxic consequences of benzene or its metabolites have been demonstrated in a number of in vitro studies; however, little data exist regarding the effects of benzene on host resistance to infectious agents. This investigation examined the effects of benzene on murine resistance to an infectious agent, Listeria monocytogenes. Four concentrations of benzene were employed, 10, 30, 100, and 300 ppm. To determine recovery from the effects of benzene, two exposure regimens were employed: 5 days prior to infection (preexposure), or 5 days prior to and 7 days during infection (continuous exposure). Appropriate air controls were maintained. Splenic bacterial counts and immune responsive cell populations were determined from mice killed at Days 1, 4, and 7 of infection. Preexposure to benzene produced increased bacterial numbers at Day 4 of the infection only at the highest benzene concentration (300 ppm). In contrast, continuous exposure produced increased bacterial numbers at Day 4 of infection at all but the lowest benzene concentration (10 ppm). Bacteria counts were not increased in any benzene-treated group at Day 1 or Day 7 of infection. The increased bacterial numbers at Day 4 suggest an effect on cell-mediated immune responses. Both T and B lymphocytes were particularly sensitive to benzene exhibiting reductions at all concentrations greater than or equal to 30 ppm for both exposure regimens. Esterase-positive cells, however, were relatively resistant to benzenes effects. The results point to a benzene-induced delay in the immune response to L. monocytogenes.

摘要

苯是一种强效骨髓毒物。虽然所有血细胞类型都是苯中毒的靶标,但淋巴细胞尤其敏感。苯或其代谢产物的免疫毒性后果已在多项体外研究中得到证实;然而,关于苯对宿主抗感染能力影响的数据却很少。本研究考察了苯对小鼠抵抗单核细胞增生李斯特菌这种感染因子能力的影响。使用了四种苯浓度,分别为10、30、100和300 ppm。为了确定从苯的影响中恢复的情况,采用了两种暴露方案:感染前5天(预暴露),或感染前5天及感染期间7天(持续暴露)。维持了适当的空气对照。在感染第1、4和7天处死小鼠,测定脾脏细菌计数和免疫反应性细胞群体。仅在最高苯浓度(300 ppm)下,预暴露于苯会在感染第4天导致细菌数量增加。相比之下,除最低苯浓度(10 ppm)外,持续暴露在感染第4天会使所有组的细菌数量增加。在感染第1天或第7天,任何苯处理组的细菌计数均未增加。第4天细菌数量增加表明对细胞介导的免疫反应有影响。对于两种暴露方案,T淋巴细胞和B淋巴细胞对苯都特别敏感,在所有大于或等于30 ppm的浓度下均表现出减少。然而,酯酶阳性细胞对苯的作用相对具有抗性。结果表明苯会导致对单核细胞增生李斯特菌的免疫反应延迟。

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