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重组白细胞介素-4治疗可增强正常易感小鼠和抗体缺陷易感小鼠对伯氏疏螺旋体感染的抵抗力。

Recombinant IL-4 treatment augments resistance to Borrelia burgdorferi infections in both normal susceptible and antibody-deficient susceptible mice.

作者信息

Keane-Myers A, Maliszewski C R, Finkelman F D, Nickell S P

机构信息

Department of Molecular Microbiology and Immunology, The John Hopkins School of Hygiene and Public Health, Baltimore, MD 21205, USA.

出版信息

J Immunol. 1996 Apr 1;156(7):2488-94.

PMID:8786309
Abstract

Recent evidence suggests that T cells and their associated cytokines critically influence outcome in mice experimentally infected with Borrelia burgdorferi (Bb), the causative agent of human Lyme disease. In vivo T cell subset and cytokine depletion studies suggest that CD4+ T cell-derived IL-4 plays a critical role in control of spirochete growth in vivo, whereas CD8+ T cell-derived IFN-gamma appears to promote disease, particularly in susceptible mouse strains. To further investigate the immunologic basis of protection and the role of IL-4, we have examined the effects of early rIL-4 treatment on outcome in susceptible mice infected with Bb. In this study, we show that administration of rIL-4 to susceptible C3H mice during the first week of infection with Bb leads to early control of their infections, as evidenced by significant reductions in joint swelling at wk 5, 6, and 7 postinfection, and in the numbers of spirochetes recovered from their joints and skin at wk 7 when compared with sham-treated mice. Increased resistance in rIL-4-treated mice was accompanied by significant reductions in their in vitro splenic Bb-specific IFN-gamma responses and in serum levels of specific IgG2a and IgG3 Abs and significant increases in specific IgG1 Abs. We also show that the inherent susceptibility of Ab-deficient, C57BL/6-IgM knockout (B6-MKO) mice to Rh infection is intermediate relative to C57BL/6 severe combined immunodeficient (B6-SCID) mice (susceptible) or normal C57BL/6 mice (resistant), confirming the importance of both Ab-dependent and Ab-independent, T cell-dependent immune mechanisms in control of Bb infections. The additional finding that early treatment with rIL-4 significantly reduced the severity of Bb infections in B6-MKO mice indicates that IL-4 may augment anti-spirochetal immunity via an Ab-independent mechanism.

摘要

近期证据表明,T细胞及其相关细胞因子对感染莱姆病病原体——伯氏疏螺旋体(Bb)的实验小鼠的病情转归具有关键影响。体内T细胞亚群及细胞因子耗竭研究表明,CD4⁺T细胞衍生的IL-4在体内控制螺旋体生长中起关键作用,而CD8⁺T细胞衍生的IFN-γ似乎会促进疾病发展,尤其是在易感小鼠品系中。为进一步研究保护的免疫基础及IL-4的作用,我们检测了早期重组IL-4(rIL-4)治疗对感染Bb的易感小鼠病情转归的影响。在本研究中,我们发现,在感染Bb的第一周给易感C3H小鼠注射rIL-4可使其感染得到早期控制,感染后第5、6和7周关节肿胀明显减轻,且与假处理小鼠相比,感染后第7周从其关节和皮肤中回收的螺旋体数量显著减少,这证明了这一点。rIL-4处理小鼠抵抗力增强的同时,其体外脾脏Bb特异性IFN-γ反应、血清中特异性IgG2a和IgG3抗体水平显著降低,特异性IgG1抗体水平显著升高。我们还发现,抗体缺陷的C57BL/6-IgM基因敲除(B6-MKO)小鼠对Bb感染的固有易感性介于C57BL/6严重联合免疫缺陷(B6-SCID)小鼠(易感)和正常C57BL/6小鼠(有抵抗力)之间,这证实了抗体依赖性和非抗体依赖性、T细胞依赖性免疫机制在控制Bb感染中的重要性。另外一项发现是,早期用rIL-4治疗可显著降低B6-MKO小鼠Bb感染的严重程度,这表明IL-4可能通过非抗体依赖性机制增强抗螺旋体免疫力。

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