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在成年C5缺陷型DBA/2小鼠中诱导对C5的主动免疫低反应性/无反应性。

Induction of active immunological hypo/non-responsiveness to C5 in adult C5-deficient DBA/2 mice.

作者信息

van den Berg C W, Hofhuis F M, Rademaker P M, van Dijk H

机构信息

Department of Experimental Microbiology, University Hospital, Utrecht, The Netherlands.

出版信息

Immunology. 1991 Nov;74(3):380-5.

Abstract

Injection of C5-sufficient BALB/c serum rendered DBA/2 mice (C5-deficient) immunologically hypo- or non-responsive to C5. This was indicated by C5-elimination studies in the C5-deficient mice showing similar half-lives for C5 upon single and repeated BALB/c serum injection. Concrete evidence for C5 non-responsiveness came from experiments showing that C5-injected DBA/2 mice were unable to mount an anti-C5 antibody response after active immunization with C5-sufficient serum in Freund's complete adjuvant. C5 hypo/non-responsiveness could be induced in DBA/2 mice via the intravenous as well as the intraperitoneal route, provided the C5-sufficient serum was administered in the very narrow dose range of 10-100 microliters (approximately 0.3-3 micrograms of C5). Upon i.v. C5 injection, C5 non-responsiveness was nearly complete on Day 4 and lasted about 3 weeks. Hyporesponsiveness was still present 6 weeks after serum injection. C3-/C5-depleting cobra venom factor reversed tolerization for C5, at least when applied within 48 hr after i.v. C5 injection. Similarity between the acquired C5 hypo/non-responsiveness of DBA/2 mice and the established C5 tolerance of BALB/c mice was suggested by adoptive cell transfer experiments: spleen cells from naive DBA/2 mice stimulated B cells of C5-sufficient nude mice to produce C5-neutralizing antibodies. In contrast, splenocytes from C5-tolerized DBA/2 mice, like those of BALB/c mice, did not decrease haemolytic C5 levels in C5-sufficient nude mice.

摘要

注射含有补体C5的BALB/c血清会使DBA/2小鼠(缺乏补体C5)在免疫上对补体C5反应低下或无反应。这在对缺乏补体C5的小鼠进行的补体C5清除研究中得到了证实,该研究表明,单次和重复注射BALB/c血清后,补体C5的半衰期相似。补体C5无反应性的确凿证据来自实验,这些实验表明,用含有补体C5的血清在弗氏完全佐剂中进行主动免疫后,注射了补体C5的DBA/2小鼠无法产生抗补体C5抗体反应。只要以10 - 100微升(约0.3 - 3微克补体C5)的非常窄的剂量范围静脉内或腹腔内给予含有补体C5的血清,就可以在DBA/2小鼠中诱导补体C5反应低下/无反应性。静脉内注射补体C5后,补体C5无反应性在第4天几乎完全出现,并持续约3周。血清注射6周后仍存在反应低下的情况。至少在静脉内注射补体C5后48小时内应用时,消耗补体C3/C5的眼镜蛇毒因子可逆转对补体C5的耐受。过继性细胞转移实验表明,DBA/2小鼠获得性补体C5反应低下/无反应性与已建立的BALB/c小鼠补体C5耐受性之间存在相似性:来自未接触过抗原的DBA/2小鼠的脾细胞刺激了含有补体C5的裸鼠的B细胞产生补体C5中和抗体。相比之下,来自耐受补体C5的DBA/2小鼠的脾细胞,与BALB/c小鼠的脾细胞一样,不会降低含有补体C5的裸鼠中的补体C5溶血水平。

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