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“治愈型”和“非治愈型”小鼠在硕大利什曼原虫感染过程中细胞介导免疫的动力学:白细胞介素-2应答及产生的渐进性损伤

Kinetics of cell-mediated immunity developing during the course of Leishmania major infection in 'healer' and 'non-healer' mice: progressive impairment of response to and generation of interleukin-2.

作者信息

Solbach W, Lohoff M, Streck H, Rohwer P, Röllinghoff M

机构信息

Institut für Klinische Mikrobiologie, Universität Erlangen-Nürnberg, Western Germany.

出版信息

Immunology. 1987 Nov;62(3):485-92.

Abstract

Leishmania major (L. major)-infected mice of 'non-healer' (BALB/c) and 'healer' (C57BL/6) mouse-strain origin were studied with regard to the kinetics of cell-mediated immunity developing during the course of the disease. Cells obtained from lymph nodes draining L. major-infected footpads were comparatively analysed for their representation in the respective L3T4+, Lyt-2+ and sIg+ lymphocyte subsets; they were studied for their capacity to release interleukin-2 and to proliferate in response to L. major antigen and concanavalin A, including the determination of the frequencies of T cells proliferating antigen-specifically with or without an exogenous source of IL-2. The data obtained indicate L. major infection-induced long-lasting alterations in the cellular composition of the lymph node in both 'healer' and 'non-healer' mice. Moreover, they suggest that the inability of 'non-healer' mice to recover from L. major infection is associated with a progressive impairment of their lymph node T cells to release interleukin-2 in the culture supernatant and to respond to this lymphokine in vitro.

摘要

对源自“非治愈型”(BALB/c)和“治愈型”(C57BL/6)小鼠品系、感染硕大利什曼原虫(L. major)的小鼠,研究了疾病过程中细胞介导免疫发展的动力学。对从感染L. major的足垫引流淋巴结获得的细胞,比较分析了它们在各自的L3T4 +、Lyt-2 +和sIg +淋巴细胞亚群中的占比;研究了它们释放白细胞介素-2的能力以及对L. major抗原和刀豆球蛋白A的增殖反应,包括测定有无外源性IL-2时特异性增殖抗原的T细胞频率。所获数据表明,L. major感染在“治愈型”和“非治愈型”小鼠的淋巴结细胞组成中均引起了持久变化。此外,这些数据表明,“非治愈型”小鼠无法从L. major感染中恢复,与其淋巴结T细胞在培养上清液中释放白细胞介素-2以及在体外对这种淋巴因子作出反应的能力逐渐受损有关。

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Antibodies to Leishmania tropica promastigotes during infection in mice of various genotypes.
Aust J Exp Biol Med Sci. 1980 Dec;58(6):595-601. doi: 10.1038/icb.1980.61.

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