CD14(高表达)CD16+单核细胞比其他单核细胞亚群更有效地吞噬抗体调理的恶性疟原虫感染的红细胞,并且这样做需要CD16和补体。
CD14(hi)CD16+ monocytes phagocytose antibody-opsonised Plasmodium falciparum infected erythrocytes more efficiently than other monocyte subsets, and require CD16 and complement to do so.
作者信息
Zhou Jingling, Feng Gaoqian, Beeson James, Hogarth P Mark, Rogerson Stephen J, Yan Yan, Jaworowski Anthony
机构信息
Centre for Biomedical Research, Burnet Institute, Melbourne, Victoria, 3004, Australia.
Department of Medicine, University of Melbourne, Melbourne, Victoria, 3050, Australia.
出版信息
BMC Med. 2015 Jul 7;13:154. doi: 10.1186/s12916-015-0391-7.
BACKGROUND
With more than 600,000 deaths from malaria, mainly of children under five years old and caused by infection with Plasmodium falciparum, comes an urgent need for an effective anti-malaria vaccine. Limited details on the mechanisms of protective immunity are a barrier to vaccine development. Antibodies play an important role in immunity to malaria and monocytes are key effectors in antibody-mediated protection by phagocytosing antibody-opsonised infected erythrocytes (IE). Eliciting antibodies that enhance phagocytosis of IE is therefore an important potential component of an effective vaccine, requiring robust assays to determine the ability of elicited antibodies to stimulate this in vivo. The mechanisms by which monocytes ingest IE and the nature of the monocytes which do so are unknown.
METHODS
Purified trophozoite-stage P. falciparum IE were stained with ethidium bromide, opsonised with anti-erythrocyte antibodies and incubated with fresh whole blood. Phagocytosis of IE and TNF production by individual monocyte subsets was measured by flow cytometry. Ingestion of IE was confirmed by imaging flow cytometry.
RESULTS
CD14(hi)CD16+ monocytes phagocytosed antibody-opsonised IE and produced TNF more efficiently than CD14(hi)CD16- and CD14(lo)CD16+ monocytes. Blocking experiments showed that Fcγ receptor IIIa (CD16) but not Fcγ receptor IIa (CD32a) or Fcγ receptor I (CD64) was necessary for phagocytosis. CD14(hi)CD16+ monocytes ingested antibody-opsonised IE when peripheral blood mononuclear cells were reconstituted with autologous serum but not heat-inactivated autologous serum. Antibody-opsonised IE were rapidly opsonised with complement component C3 in serum (t1/2 = 2-3 minutes) and phagocytosis of antibody-opsonised IE was inhibited in a dose-dependent manner by an inhibitor of C3 activation, compstatin. Compared to other monocyte subsets, CD14(hi)CD16+ monocytes expressed the highest levels of complement receptor 4 (CD11c) and activated complement receptor 3 (CD11b) subunits.
CONCLUSIONS
We show a special role for CD14(hi)CD16+ monocytes in phagocytosing opsonised P. falciparum IE and production of TNF. While ingestion was mediated by Fcγ receptor IIIa, this receptor was not sufficient to allow phagocytosis; despite opsonisation with antibody, phagocytosis of IE also required complement opsonisation. Assays which measure the ability of vaccines to elicit a protective antibody response to P. falciparum should consider their ability to promote phagocytosis and fix complement.
背景
疟疾导致超过60万人死亡,主要是五岁以下儿童,由恶性疟原虫感染引起,因此迫切需要一种有效的抗疟疾疫苗。关于保护性免疫机制的细节有限是疫苗开发的一个障碍。抗体在疟疾免疫中起重要作用,单核细胞是抗体介导保护的关键效应细胞,通过吞噬抗体调理的感染红细胞(IE)发挥作用。因此,诱导增强IE吞噬作用的抗体是有效疫苗的一个重要潜在组成部分,这需要可靠的检测方法来确定诱导抗体在体内刺激这种作用的能力。单核细胞摄取IE的机制以及进行摄取的单核细胞的性质尚不清楚。
方法
将纯化的恶性疟原虫滋养体阶段的IE用溴化乙锭染色,用抗红细胞抗体进行调理,然后与新鲜全血孵育。通过流式细胞术测量单个单核细胞亚群对IE的吞噬作用和TNF的产生。通过成像流式细胞术确认IE的摄取。
结果
与CD14(hi)CD16-和CD14(lo)CD16+单核细胞相比,CD14(hi)CD16+单核细胞吞噬抗体调理的IE并产生TNF的效率更高。阻断实验表明,吞噬作用需要Fcγ受体IIIa(CD16),而不是Fcγ受体IIa(CD32a)或Fcγ受体I(CD64)。当用自体血清而不是热灭活的自体血清重建外周血单核细胞时,CD14(hi)CD16+单核细胞摄取抗体调理的IE。抗体调理的IE在血清中迅速被补体成分C3调理(t1/2 = 2 - 3分钟),C3激活抑制剂compstatin以剂量依赖性方式抑制抗体调理的IE的吞噬作用。与其他单核细胞亚群相比,CD14(hi)CD16+单核细胞表达补体受体4(CD11c)和活化补体受体3(CD11b)亚基的水平最高。
结论
我们展示了CD14(hi)CD16+单核细胞在吞噬调理的恶性疟原虫IE和产生TNF方面的特殊作用。虽然摄取是由Fcγ受体IIIa介导的,但该受体不足以允许吞噬作用;尽管用抗体进行了调理,但IE的吞噬作用也需要补体调理。测量疫苗诱导针对恶性疟原虫的保护性抗体反应能力的检测方法应考虑其促进吞噬作用和固定补体的能力。
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