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正常小鼠和免疫小鼠感染莫氏立克次体的特征

Characteristics of Rickettsia mooseri infection of normal and immune mice.

作者信息

Crist A E, Wisseman C L, Murphy J R

出版信息

Infect Immun. 1984 Jan;43(1):38-42. doi: 10.1128/iai.43.1.38-42.1984.

Abstract

Rickettsia mooseri infection initiated by subcutaneous injection has been studied in BALB/c mice with the objective of developing a model for the study of immune mechanisms. Characterization of infection included the following: measurement of the replication, dissemination, and clearance of rickettsiae; measurement of correlates of the immune response, including humoral antibody, hypersensitivity to subcutaneously inoculated rickettsial antigen, and activation of nonspecific macrophage microbicidal capacity; and measurement of resistance to a second homologous challenge. Local infection at the site of subcutaneous injection progressed through day 5 and was controlled by day 7. Systemic infection as determined by the presence of rickettsiae in spleen was first detected on day 7 and progressed through day 14; however, rickettsiae persisted in this organ at reduced numbers through at least day 28. Control of the local infection at the site of subcutaneous injection occurred at about the time humoral antibodies and hypersensitivity reactions to subcutaneously injected rickettsial antigens became demonstrable and was paralleled by a capacity to resist homologous subcutaneous challenge at a site distant from that of the primary infection. Systemic infection progressed in spite of this acquired immune capacity and was controlled in the spleen in parallel with the development of enhanced macrophage microbicidal capacity in the liver. The results show that an acquired immunity is capable of restricting rickettsial growth at subcutaneous sites at a time when rickettsiae are increasing in titer in deep organs.

摘要

为了建立一个研究免疫机制的模型,对通过皮下注射引发的穆氏立克次体感染在BALB/c小鼠中进行了研究。感染的特征包括以下方面:测量立克次体的复制、扩散和清除;测量免疫反应的相关指标,包括体液抗体、对皮下接种立克次体抗原的超敏反应以及非特异性巨噬细胞杀菌能力的激活;以及测量对第二次同源攻击的抵抗力。皮下注射部位的局部感染在第5天进展,并在第7天得到控制。通过脾脏中存在立克次体确定的全身感染在第7天首次检测到,并在第14天进展;然而,立克次体在该器官中至少持续到第28天,数量减少。皮下注射部位的局部感染在体液抗体和对皮下注射立克次体抗原的超敏反应变得明显时得到控制,并且与在远离原发感染部位抵抗同源皮下攻击的能力同时出现。尽管有这种获得性免疫能力,全身感染仍在进展,并在脾脏中得到控制,同时肝脏中巨噬细胞杀菌能力增强。结果表明,在深部器官中立克次体滴度增加时,获得性免疫能够限制皮下部位的立克次体生长。

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