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C57BL/6小鼠和A/J小鼠在抗李斯特菌抗性方面的相对差异不会因主动免疫或转移李斯特菌免疫T细胞而消除。

The relative difference in anti-Listeria resistance of C57BL/6 and A/J mice is not eliminated by active immunization or by transfer of Listeria-immune T cells.

作者信息

Czuprynski C J, Brown J F

出版信息

Immunology. 1986 Jul;58(3):437-43.

Abstract

In this study, we examined the effects of active and adoptive immunization on the anti-Listeria resistance of innately resistant C57BL/6 and innately susceptible A/J mice. Although active immunization with a sublethal dose of viable Listeria monocytogenes markedly enhanced the anti-Listeria resistance of both C57BL/6 and A/J mice, the 100-fold difference between the two strains in innate anti-Listeria resistance was not diminished. Following immunization with an equivalent sublethal dose (0.1 LD50) of L. monocytogenes, both C57BL/6 and A/J mice generated T cells that could transfer significant and comparable protection to syngeneic recipients that were challenged with up to a 10 LD50 dose of L. monocytogenes. When the absolute number of viable Listeria was compared, however, it was clear that T cells from immunized C57BL/6 mice were capable of transferring protection to syngeneic recipients at Listeria challenge doses that were more than 100-fold greater than could T cells from Listeria-immunized A/J mice. Both active immunization and adoptive transfer of syngeneic Listeria-immune T cells enhanced the accumulation of inflammatory neutrophils and macrophages in C57BL/6 and A/J mice. More inflammatory neutrophils were recovered from actively immunized C57BL/6 than from A/J mice, whereas more inflammatory macrophages were obtained from adoptively immunized C57BL/6 than from A/J mice. These results provide further evidence for the beneficial role of inflammation in genetically determined innate resistance and T-cell mediated resistance to listeriosis. These data also suggest that some mechanism in addition to inflammatory responsiveness may be responsible for limiting the expression of acquired anti-Listeria resistance in genetically susceptible A/J mice.

摘要

在本研究中,我们检测了主动免疫和过继免疫对先天具有抗性的C57BL/6小鼠和先天易感的A/J小鼠抗李斯特菌抵抗力的影响。尽管用亚致死剂量的活单核细胞增生李斯特菌进行主动免疫显著增强了C57BL/6和A/J小鼠的抗李斯特菌抵抗力,但这两个品系在先天抗李斯特菌抵抗力方面100倍的差异并未减小。在用等量亚致死剂量(0.1 LD50)的单核细胞增生李斯特菌免疫后,C57BL/6和A/J小鼠均产生了T细胞,这些T细胞能够将显著且相当的保护作用传递给接受高达10 LD50剂量单核细胞增生李斯特菌攻击的同基因受体。然而,当比较存活李斯特菌的绝对数量时,很明显,来自免疫后的C57BL/6小鼠的T细胞能够将保护作用传递给同基因受体,其李斯特菌攻击剂量比来自经李斯特菌免疫的A/J小鼠的T细胞所能承受的剂量高出100倍以上。主动免疫和同基因李斯特菌免疫T细胞的过继转移均增强了C57BL/6和A/J小鼠中炎性中性粒细胞和巨噬细胞的积累。从主动免疫的C57BL/6小鼠中回收的炎性中性粒细胞比A/J小鼠中的多,而从过继免疫的C57BL/6小鼠中获得的炎性巨噬细胞比A/J小鼠中的多。这些结果为炎症在遗传决定的先天抵抗力和T细胞介导的抗李斯特菌病抵抗力中的有益作用提供了进一步证据。这些数据还表明,除了炎症反应性之外,某些机制可能负责限制遗传易感的A/J小鼠中获得性抗李斯特菌抵抗力的表达。

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