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补体C3作为调理素在感染早期阶段的作用。

The role of C3 as an opsonin in the early stages of infection.

作者信息

Winkelstein J A, Smith M R, Shin H S

出版信息

Proc Soc Exp Biol Med. 1975 Jun;149(2):397-401. doi: 10.3181/00379727-149-38815.

Abstract

In order to investigate the role of C3 in host defense in vivo, normal AKR/J mice, genetically deficient in C5, were depleted of serum C3 by the injection of purified cobra venom factor (CoVF). Concurrent with their C3 depletion, their serum opsonizing activity decreased to a level less than 20% of normal. When these mice were challenged with an intraperitoneal injection of pneumococci 2 hr after the CoVF treatment, the LD50 was from 30 to 80 times lower than the LD50 in saline-treated control animals. When the CoVF was given only 6 hr after the pneumococcal challenge, the LD50 was the same as in the control mice. If the pneumococci were first preopsonized in vitro and then injected into CoVF-treated animals, the LD50 was the same as that in control animals. These experiments demonstrate that C3 plays a significant role in vivo in the host's defense against infection and that a major part of that role is through its action as an opsonin. Furthermore, these experiments demonstrate that the role of C3 is most significant during the early stages of bacterial invasion.

摘要

为了研究补体3(C3)在体内宿主防御中的作用,将基因缺陷型C5的正常AKR/J小鼠通过注射纯化的眼镜蛇毒因子(CoVF)来消耗血清C3。在其C3被消耗的同时,它们的血清调理活性降至正常水平的20%以下。当这些小鼠在CoVF处理后2小时腹腔注射肺炎球菌进行攻击时,其半数致死量(LD50)比生理盐水处理的对照动物低30至80倍。当在肺炎球菌攻击后仅6小时给予CoVF时,LD50与对照小鼠相同。如果肺炎球菌首先在体外进行预调理,然后注射到CoVF处理的动物体内,LD50与对照动物相同。这些实验表明,C3在体内宿主抗感染防御中起重要作用,且该作用的主要部分是通过其作为调理素的作用。此外,这些实验表明,C3的作用在细菌入侵的早期阶段最为显著。

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