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C1q增强人单核细胞对新型隐球菌芽生孢子的吞噬作用。

C1q enhances the phagocytosis of Cryptococcus neoformans blastospores by human monocytes.

作者信息

Bobak D A, Washburn R G, Frank M M

机构信息

Laboratory of Clinical Investigation, National Institute of Allergy and Infectious Diseases, Bethesda, MD 20892.

出版信息

J Immunol. 1988 Jul 15;141(2):592-7.

PMID:3290342
Abstract

We investigated whether C1q, a subunit of the first component of C, could modulate human peripheral blood monocyte-mediated phagocytosis of Cryptococcus neoformans (CN). Adherence of monocytes to C1q-coated surfaces induced a significant enhancement of ingestion of CN blastospores that had been opsonized with specific anticapsular IgG (IgG-CN). Additionally, C1q enhanced the monocyte-mediated phagocytosis of CN opsonized with C (CN-absorbed, nonimmune, normal human serum; C-CN). Ingestion of IgG- and C-CN by control and C1q-stimulated monocytes was maximal by 1 h of incubation. The monocyte-mediated enhancement of phagocytosis caused by C1q was paralleled by a proportionate increase in fungicidal activity, an effect which was maximal by 3 h of incubation. Human serum albumin-adherent, control monocytes exhibited only a low level of killing after 3 h of incubation. C1q enhancement was blocked by preincubation of the surfaces with a goat, polyclonal F(ab')2 anti-C1q. This study describes a new cellular function for the cell surface C1q receptor: the enhancement of phagocytosis of a pathogenic organism by monocytes.

摘要

我们研究了补体第一成分的一个亚基C1q是否能够调节人外周血单核细胞介导的新型隐球菌(CN)吞噬作用。单核细胞与包被C1q的表面黏附,可显著增强对已用特异性抗荚膜IgG(IgG-CN)调理过的CN芽生孢子的摄取。此外,C1q增强了单核细胞介导的对用补体调理过的CN(CN-吸收的、非免疫的正常人血清;C-CN)的吞噬作用。对照单核细胞和C1q刺激的单核细胞对IgG-CN和C-CN的摄取在孵育1小时后达到最大值。C1q引起的单核细胞介导的吞噬作用增强与杀菌活性的相应增加平行,这种效应在孵育3小时后达到最大值。人血清白蛋白黏附的对照单核细胞在孵育3小时后仅表现出低水平的杀伤作用。用山羊多克隆F(ab')2抗C1q预孵育表面可阻断C1q的增强作用。本研究描述了细胞表面C1q受体的一种新的细胞功能:增强单核细胞对致病生物体的吞噬作用。

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