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C3在调节兔脾脏抗体形成细胞反应中的作用。

Role of C3 in the regulation of a splenic PFC response in rabbits.

作者信息

Romball C G, Ulevitch R J, Weigle W O

出版信息

J Immunol. 1980 Jan;124(1):151-5.

PMID:6153091
Abstract

The effects of in vivo C3 depletion on the immune response were examined in rabbits by assaying for splenic PFC after immunizing normal or cobra venom factor-treated animals with aggregated human gamma-globulin. The response to this T-dependent antigen has previously been shown to be regulated such that several cycles of PFC appear following a single intravenous injection of antigen. C3 depletion had no effect on the first peak of PFC (appearing 5 days after injection), but resulted in depression of the second peak of PFC (day 13). In rabbits depleted of C3, antigen localization in splenic germinal centers was markedly decreased. Delaying C3 depletion until after antigen localization had occurred resulted in no depression of the second peak of PFC. These results suggest that one mechanism by which C3 affects immune responses in vivo is via its role in influencing the persistence of antigen. In the absence of C3, no significant localization of antigen occurs, resulting in interference with the cyclical production of antibody.

摘要

通过在用聚合人γ-球蛋白免疫正常或眼镜蛇毒因子处理的动物后检测脾脏PFC,研究了体内C3耗竭对兔免疫反应的影响。先前已证明对这种T细胞依赖性抗原的反应受到调节,以至于在单次静脉注射抗原后会出现几个PFC周期。C3耗竭对PFC的第一个峰值(注射后5天出现)没有影响,但导致PFC的第二个峰值(第13天)降低。在C3耗竭的兔中,脾脏生发中心的抗原定位明显减少。将C3耗竭延迟到抗原定位发生之后,PFC的第二个峰值没有降低。这些结果表明,C3在体内影响免疫反应的一种机制是通过其在影响抗原持久性方面的作用。在没有C3的情况下,抗原没有明显的定位,导致抗体的周期性产生受到干扰。

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