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中性粒细胞Fc受体参与B族链球菌Ⅲ型的吞噬作用。

Neutrophil Fc receptor participation in phagocytosis of type III group B streptococci.

作者信息

Noya F J, Baker C J, Edwards M S

机构信息

Department of Pediatrics, Baylor College of Medicine, Houston, Texas 77030.

出版信息

Infect Immun. 1993 Apr;61(4):1415-20. doi: 10.1128/iai.61.4.1415-1420.1993.

Abstract

Human peripheral blood neutrophils bear receptors for immunoglobulin G, FcRII, and FcRIII that differ structurally and functionally. We investigated the role of FcRII and FcRIII in the phagocytosis of group B streptococci (GBS) by measuring neutrophil uptake of radiolabeled type III GBS. The mean uptake of GBS opsonized with human serum containing complement and specific antibody was 76%, but when this serum was heated, the mean uptake was only 22%. A monoclonal antibody to FcRIII, Leu-11b, inhibited in a dose-dependent manner uptake of GBS opsonized with heated or intact serum to maxima of 40 and 30%, respectively. Conversely, a monoclonal antibody to FcRII, IV.3, inhibited by 77% the uptake of GBS opsonized with heated serum but had no effect when GBS was opsonized with intact serum. Leu-11b and IV.3 had an additive inhibitory effect with heated but not with intact serum. Neither monoclonal antibody inhibited the uptake of GBS opsonized with hypogammaglobulinemic serum. Therefore, FcRII is the primary mediator of the phagocytosis of GBS opsonized by antibody alone, whereas FcRIII plays a lesser role. Surprisingly, FcRII is not necessary for phagocytosis when complement is also present. FcRIII participates, to a limited extent, in phagocytosis of GBS opsonized with antibody whether or not complement is present. These findings suggest that the function of FcRII in triggering phagocytosis may be particularly important in host defense against type III GBS in the setting of complement deficiency of young infants.

摘要

人类外周血中性粒细胞带有免疫球蛋白G、FcRII和FcRIII的受体,这些受体在结构和功能上存在差异。我们通过测量中性粒细胞对放射性标记的III型B族链球菌(GBS)的摄取,研究了FcRII和FcRIII在GBS吞噬作用中的作用。用含有补体和特异性抗体的人血清调理的GBS的平均摄取率为76%,但当该血清加热后,平均摄取率仅为22%。一种针对FcRIII的单克隆抗体Leu-11b以剂量依赖性方式抑制了用加热或完整血清调理的GBS的摄取,分别达到最大值40%和30%。相反,一种针对FcRII的单克隆抗体IV.3抑制了用加热血清调理的GBS摄取的77%,但当GBS用完整血清调理时则没有作用。Leu-11b和IV.3对加热血清有相加抑制作用,但对完整血清没有。两种单克隆抗体均未抑制用低丙种球蛋白血症血清调理的GBS的摄取。因此,FcRII是仅由抗体调理的GBS吞噬作用的主要介质,而FcRIII的作用较小。令人惊讶的是,当也存在补体时,FcRII对于吞噬作用不是必需的。无论是否存在补体,FcRIII在一定程度上参与了用抗体调理的GBS的吞噬作用。这些发现表明,在婴儿补体缺乏的情况下,FcRII在触发吞噬作用中的功能在宿主抵御III型GBS的防御中可能特别重要。

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