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鼠实验模型中马红球菌感染期间的T细胞应答

T-cell response during Rhodococcus equi infection in a murine experimental model.

作者信息

Matsiota-Bernard P, Lair I, Vogiatzakis E, Bernemann A

机构信息

Laboratoire de Microbiologie, Hôpital Raymond Poincaré, Garches, France.

出版信息

Res Immunol. 1997 Jul-Aug;148(6):387-97. doi: 10.1016/s0923-2494(97)82872-6.

Abstract

Rhodococcus equi is a facultative intracellular bacterium that can cause pneumonia in both young horses and immunocompromised humans. In this study, we have tried to determine the T-cell populations that recognize this pathogen during murine infection, as well as the bacterial antigens recognized by these cells. When BALB/c mice were hyperimmunized with a virulent R. equi strain, we did not observe preferential expansion of a particular T-cell subset in their spleens. However, when the splenic T lymphocytes of the hyperimmunized BALB/c mice were cultured in the presence of killed bacteria, we found that alpha/beta CD4+ T cells proliferated and exhibited increased levels of the interleukin-2 receptor (IL2R). In order to ensure antigen specificity, two different controls were included in these experiments: (i) T-cell proliferation and expression of the IL2R in the presence of the major membrane constituent of Bacillus megaterium were studied comparatively with the presence of the R. equi bacterial antigen, and (ii) T-cell proliferation and expression of the IL2R from naive, non-infected mice in the presence of bacterial antigens were compared to those observed in hyperimmunized mice. In our study, the T cells from hyperimmunized mice did not significantly proliferate nor were they activated in the presence of non-related bacterial antigens, and T cells from naive mice were not found to significantly recognize R. equi antigens. When we studied the localization of R. equi antigens that could stimulate the in vitro proliferation and activation of T cells, we found that they were constituents of the bacterial cell wall and the cytoplasm, but they were not excreted in the culture medium. For these experiments, T-cell recognition of the bacterial antigens in hyperimmunized mice was compared to that of naive mice. With T-cell immunoblotting, we found that T-cell proliferation and activation were obtained with proteins having molecular masses of approximately 65, 43, 30, 22-27 and 15-17 kDa. It is noteworthy that among the recognized bacterial antigens, some have been described as being associated with virulence.

摘要

马红球菌是一种兼性胞内细菌,可导致幼马和免疫功能低下的人类患肺炎。在本研究中,我们试图确定在小鼠感染期间识别该病原体的T细胞群体,以及这些细胞识别的细菌抗原。当用强毒马红球菌菌株对BALB/c小鼠进行超免疫时,我们未观察到其脾脏中特定T细胞亚群的优先扩增。然而,当在存在热灭活细菌的情况下培养超免疫BALB/c小鼠的脾脏T淋巴细胞时,我们发现α/β CD4+ T细胞增殖并表现出白细胞介素-2受体(IL2R)水平升高。为确保抗原特异性,这些实验纳入了两个不同的对照:(i)比较在巨大芽孢杆菌主要膜成分存在下与马红球菌细菌抗原存在下T细胞的增殖及IL2R的表达;(ii)将未感染的 naive 小鼠在细菌抗原存在下T细胞的增殖及IL2R的表达与超免疫小鼠中观察到的情况进行比较。在我们的研究中,超免疫小鼠的T细胞在存在非相关细菌抗原时未显著增殖,也未被激活,且未发现来自 naive 小鼠的T细胞能显著识别马红球菌抗原。当我们研究可刺激T细胞体外增殖和激活的马红球菌抗原的定位时,我们发现它们是细菌细胞壁和细胞质的成分,但它们不会分泌到培养基中。对于这些实验,将超免疫小鼠中T细胞对细菌抗原的识别与 naive 小鼠的进行了比较。通过T细胞免疫印迹法,我们发现分子量约为65、43、30、22 - 27和15 - 17 kDa的蛋白质可导致T细胞增殖和激活。值得注意的是,在识别出的细菌抗原中,有些已被描述与毒力相关。

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