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对恙虫病立克次氏体免疫的小鼠中γ干扰素的产生。

Production of gamma interferon in mice immune to Rickettsia tsutsugamushi.

作者信息

Palmer B A, Hetrick F M, Jerrells T J

出版信息

Infect Immun. 1984 Jan;43(1):59-65. doi: 10.1128/iai.43.1.59-65.1984.

Abstract

C3H/He mice immunized by subcutaneous infection with Rickettsia tsutsugamushi Gilliam were examined for the production of immune interferon after intravenous administration of irradiated strain Gilliam antigen, in supernatants of immune lymphocytes stimulated with specific antigen, and after a secondary challenge with viable rickettsiae. Mice administered various doses of irradiated whole-organism antigen 28 days after immunization showed circulating levels of interferon which peaked 4 h after inoculation and were antigen dose dependent. The interferon produced was pH 2 sensitive and stable at 56 degrees C for 1 h and was neutralized by antiserum directed against immune, but not against alpha/beta, interferon. The production of another lymphokine, macrophage migration inhibition factor, paralleled that of interferon. The interferon produced by cultures of spleen cells obtained from immune animals was antigen specific and dose dependent. Peak levels were obtained 48 to 72 h after the addition of antigen. The interferon produced by spleen cell cultures after stimulation with Gilliam antigen was characterized as immune interferon by the same physical and antigenic criteria used for serum interferon. Interferon was produced in vitro by the Thy-1.2+ lymphocyte and required the presence of a spleen-adherent cell population. Immune mice produced high circulating levels of immune interferon after intraperitoneal challenge with viable rickettsiae, which suggested a possible role for interferon in the resistance of immune mice to rechallenge with R. tsutsugamushi.

摘要

用恙虫病东方体吉氏株皮下感染免疫的C3H/He小鼠,在静脉注射经辐照的吉氏株抗原后、在特异性抗原刺激的免疫淋巴细胞上清液中以及在再次用活立克次体攻击后,检测其免疫干扰素的产生情况。免疫28天后给予不同剂量经辐照的全菌体抗原的小鼠,其循环中的干扰素水平在接种后4小时达到峰值,且与抗原剂量有关。所产生的干扰素对pH 2敏感,在56℃下1小时稳定,并且被针对免疫干扰素而非α/β干扰素的抗血清中和。另一种淋巴因子巨噬细胞移动抑制因子的产生与干扰素平行。从免疫动物获得的脾细胞培养物产生的干扰素具有抗原特异性且与剂量有关。添加抗原后48至72小时达到峰值水平。用与血清干扰素相同的物理和抗原标准,将吉氏株抗原刺激后脾细胞培养物产生的干扰素鉴定为免疫干扰素。干扰素由Thy-1.2+淋巴细胞在体外产生,并且需要存在脾黏附细胞群体。免疫小鼠在用活立克次体腹腔攻击后产生高循环水平的免疫干扰素,这表明干扰素在免疫小鼠抵抗再次感染恙虫病东方体中可能起作用。

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