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裂殖子表面蛋白 2 等位基因特异性人抗体对恶性疟原虫的跨株 Fc 依赖性杀伤作用。

Strain-transcending Fc-dependent killing of Plasmodium falciparum by merozoite surface protein 2 allele-specific human antibodies.

机构信息

Institute for Research in Biomedicine, Bellinzona, Switzerland.

出版信息

Infect Immun. 2011 Mar;79(3):1143-52. doi: 10.1128/IAI.01034-10. Epub 2010 Dec 28.

Abstract

It is widely accepted that antibody responses against the human parasitic pathogen Plasmodium falciparum protect the host from the rigors of severe malaria and death. However, there is a continuing need for the development of in vitro correlate assays of immune protection. To this end, the capacity of human monoclonal and polyclonal antibodies in eliciting phagocytosis and parasite growth inhibition via Fcγ receptor-dependent mechanisms was explored. In examining the extent to which sequence diversity in merozoite surface protein 2 (MSP2) results in the evasion of antibody responses, an unexpectedly high level of heterologous function was measured for allele-specific human antibodies. The dependence on Fcγ receptors for opsonic phagocytosis and monocyte-mediated antibody-dependent parasite inhibition was demonstrated by the mutation of the Fc domain of monoclonal antibodies against both MSP2 and a novel vaccine candidate, peptide 27 from the gene PFF0165c. The described flow cytometry-based functional assays are expected to be useful for assessing immunity in naturally infected and vaccinated individuals and for prioritizing among blood-stage antigens for inclusion in blood-stage vaccines.

摘要

人们普遍认为,针对人体寄生虫病原体疟原虫的抗体反应可保护宿主免受严重疟疾和死亡的威胁。然而,人们仍然需要开发体外免疫保护相关性检测方法。为此,人们探索了人类单克隆和多克隆抗体通过 Fcγ 受体依赖性机制引发吞噬作用和寄生虫生长抑制的能力。在研究裂殖子表面蛋白 2(MSP2)的序列多样性在多大程度上导致抗体反应的逃逸时,出人意料地发现,针对特定等位基因的人类抗体具有很高的异源功能。通过对针对 MSP2 和新型疫苗候选物肽 27(来自 PFF0165c 基因)的单克隆抗体的 Fc 结构域进行突变,证明了调理吞噬作用和单核细胞介导的抗体依赖性寄生虫抑制作用依赖于 Fcγ 受体。所描述的基于流式细胞术的功能检测方法有望用于评估自然感染和接种疫苗个体的免疫情况,并优先考虑纳入血期疫苗的血期抗原。

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