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小鼠体内活化的单核吞噬细胞与对衣原体的保护性免疫

In vivo-activated mononuclear phagocytes and protective immunity to chlamydiae in mice.

作者信息

Huebner R E, Byrne G I

机构信息

Department of Medical Microbiology, University of Wisconsin Medical School, Madison 53706.

出版信息

Infect Immun. 1988 Jun;56(6):1492-9. doi: 10.1128/iai.56.6.1492-1499.1988.

Abstract

Peritoneal macrophages (M phi s) collected from Chlamydia psittaci 6BC-immune mice after intraperitoneal challenge with 10(6) 6BC (immune-boosted [IB] M phi s) were compared by various functional criteria with other in vivo- and in vitro-activated M phi populations. While casein-, protease peptone-, and thioglycolate (Thio)-elicited M phi s were equally susceptible to in vitro infection with 6BC, IB M phi s did not support chlamydial growth and M phi s from Mycobacterium tuberculosis BCG- or Listeria monocytogenes-sensitized mice exhibited intermediate susceptibility to infection. The resistance of IB M phi s was not due to the ingestion of fewer 6BC organisms, nor were these cells persistently infected, since chlamydiae could not be recovered from infected IB M phi s after in vitro infection, even after extended incubation times. In contrast, Thio M phi s stimulated in vitro with gamma interferon (IFN-gamma), with or without lipopolysaccharide, resulted in cells that exhibited chlamydiastatic activity which was lost shortly after IFN-gamma was removed from the culture medium. Conversely, the antichlamydial activity of IB M phi s was stable over time but not through the production of autostimulatory cytokines, as evidenced by the lack of stimulation of Thio M phi s to restrict 6BC replication in coculture experiments. IB M phi s exhibited enhanced oxidative activity, but anti-IFN-gamma antibody did not abrogate this response. IB M phi s were recovered only from immunized mice that survived an otherwise lethal 6BC intraperitoneal challenge. These cells appear to be important for development of protective immunity to chlamydiae, and evidence suggests that stimulation by cytokines other than IFN-gamma (with or without lipopolysaccharide) is required for the observed heightened in vivo activation.

摘要

用10(6)个鹦鹉热衣原体6BC株腹腔攻击感染后,从免疫的小鼠中收集腹腔巨噬细胞(Mφs)(免疫增强[IB]Mφs),并根据各种功能标准,将其与其他体内和体外激活的Mφ群体进行比较。虽然酪蛋白、蛋白酶胨和巯基乙酸盐(硫代乙醇酸盐,Thio)诱导的Mφs对6BC株的体外感染同样敏感,但IB Mφs不支持衣原体生长,而来自结核分枝杆菌卡介苗或单核细胞增生李斯特菌致敏小鼠的Mφs对感染表现出中等敏感性。IB Mφs的抗性并非由于吞噬的6BC生物体数量较少,这些细胞也未被持续感染,因为即使在延长培养时间后,体外感染的IB Mφs中也无法回收衣原体。相反,用γ干扰素(IFN-γ)体外刺激硫代乙醇酸盐诱导的Mφs,无论有无脂多糖,都会产生衣原体生长抑制活性,当从培养基中去除IFN-γ后,这种活性很快就会丧失。相反,IB Mφs的抗衣原体活性随时间稳定,但并非通过自身刺激细胞因子的产生,共培养实验中硫代乙醇酸盐诱导的Mφs无法限制6BC复制,证明了这一点。IB Mφs表现出增强的氧化活性,但抗IFN-γ抗体并未消除这种反应。仅从在原本致命的6BC腹腔攻击中存活下来的免疫小鼠中回收了IB Mφs。这些细胞似乎对衣原体保护性免疫的发展很重要,有证据表明,观察到的体内高度激活需要IFN-γ以外的细胞因子(有或无脂多糖)的刺激。

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