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人类单核细胞CD36和CD16是信号分子。使用抗体诱导化学发光作为探测信号转导工具的研究证据。

Human monocytes CD36 and CD16 are signaling molecules. Evidence from studies using antibody-induced chemiluminescence as a tool to probe signal transduction.

作者信息

Trezzini C, Jungi T W, Spycher M O, Maly F E, Rao P

机构信息

Institute of Veterinary Virology, University of Berne, Switzerland.

出版信息

Immunology. 1990 Sep;71(1):29-37.

Abstract

A panel of monoclonal antibodies (mAb) directed against human monocyte surface antigens was tested for their capacity to mediate signal transduction by measuring luminol-enhanced chemiluminescence (CL). The response patterns fell into three categories. The mAb Mo4, OKM3, OKM6 and antibodies specific for Fc receptor (FcR) type I and II did not mediate signal transduction directly or were weak triggers, but upon second-order cross-linking by goat anti-mouse immunoglobulin (Ig) F(ab')2 or rabbit anti-mouse Ig, a strong CL response was induced. The mAb recognizing different epitopes on CD11b (complement receptor type III alpha chain) were unique in their ability to induce a CL response either by direct stimulation or by second-order cross-linking. The mAb 3G8 recognizing FcR type III (FcRIII; CD16) on a monocyte subpopulation and CD36-specific monoclonals directly elicited a CL response. A response of similar magnitude was obtained with 3G8 F(ab')2 or with intact 3G8. Furthermore, elutriation-centrifugation-purified monocytes were stimulated by 3G8 to a similar extent as unseparated mononuclear cells, whereas lymphocytes did not respond. This suggests that a FcRIII-expressing monocyte subpopulation may mediate effector functions, including the generation of reactive oxygen species, via FcRIII triggering. Our finding that anti-CD36 F(ab')2 directly induces an oxidative burst is the first evidence that CD36 itself is a trigger molecule. CD36, which is thought to interact with erythrocytes infected with Plasmodium falciparum and with thrombospondin, may constitute a signal-transducing element and thus may have functions extending beyond mediation of adherence. The present CL system constitutes a simple assay for detecting mAb directed against monocyte surface signalling elements. Probing mAb for signal transduction requires suspended cells and antibodies in the fluid phase in order to avoid inadvertent FcR triggering, which may occur when cells are stimulated by surface-adherent whole antibodies.

摘要

通过测量鲁米诺增强的化学发光(CL),检测了一组针对人单核细胞表面抗原的单克隆抗体(mAb)介导信号转导的能力。反应模式分为三类。单克隆抗体Mo4、OKM3、OKM6以及I型和II型Fc受体(FcR)特异性抗体不能直接介导信号转导或只是弱触发剂,但在用山羊抗小鼠免疫球蛋白(Ig)F(ab')2或兔抗小鼠Ig进行二级交联后,会诱导强烈的CL反应。识别CD11b(III型补体受体α链)上不同表位的单克隆抗体在通过直接刺激或二级交联诱导CL反应的能力方面具有独特性。识别单核细胞亚群上III型Fc受体(FcRIII;CD16)的单克隆抗体3G8和CD36特异性单克隆抗体可直接引发CL反应。用3G8 F(ab')2或完整的3G8可获得相似强度的反应。此外,淘洗-离心纯化的单核细胞受3G8刺激的程度与未分离的单核细胞相似,而淋巴细胞无反应。这表明表达FcRIII的单核细胞亚群可能通过FcRIII触发介导效应功能,包括活性氧的产生。我们发现抗CD36 F(ab')2直接诱导氧化爆发,这是CD36本身是触发分子的首个证据。CD36被认为与感染恶性疟原虫的红细胞以及血小板反应蛋白相互作用,可能构成信号转导元件,因此其功能可能超出介导黏附作用。目前的CL系统构成了一种检测针对单核细胞表面信号元件的单克隆抗体的简单测定法。检测信号转导的单克隆抗体需要悬浮细胞和液相中的抗体,以避免意外触发FcR,当细胞受到表面黏附的完整抗体刺激时可能会发生这种情况。

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