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人类Fcγ受体I在介导疟疾保护中的重要性。

The importance of human FcgammaRI in mediating protection to malaria.

作者信息

McIntosh Richard S, Shi Jianguo, Jennings Richard M, Chappel Jonathan C, de Koning-Ward Tania F, Smith Tim, Green Judith, van Egmond Marjolein, Leusen Jeanette H W, Lazarou Maria, van de Winkel Jan, Jones Tarran S, Crabb Brendan S, Holder Anthony A, Pleass Richard J

机构信息

Institute of Genetics, Queen's Medical Centre, University of Nottingham, United Kingdom.

出版信息

PLoS Pathog. 2007 May 18;3(5):e72. doi: 10.1371/journal.ppat.0030072.

Abstract

The success of passive immunization suggests that antibody-based therapies will be effective at controlling malaria. We describe the development of fully human antibodies specific for Plasmodium falciparum by antibody repertoire cloning from phage display libraries generated from immune Gambian adults. Although these novel reagents bind with strong affinity to malaria parasites, it remains unclear if in vitro assays are predictive of functional immunity in humans, due to the lack of suitable animal models permissive for P. falciparum. A potentially useful solution described herein allows the antimalarial efficacy of human antibodies to be determined using rodent malaria parasites transgenic for P. falciparum antigens in mice also transgenic for human Fc-receptors. These human IgG1s cured animals of an otherwise lethal malaria infection, and protection was crucially dependent on human FcgammaRI. This important finding documents the capacity of FcgammaRI to mediate potent antimalaria immunity and supports the development of FcgammaRI-directed therapy for human malaria.

摘要

被动免疫的成功表明基于抗体的疗法在控制疟疾方面将是有效的。我们描述了通过从免疫的冈比亚成年人产生的噬菌体展示文库中克隆抗体库来开发针对恶性疟原虫的完全人源抗体。尽管这些新型试剂与疟原虫具有很强的亲和力,但由于缺乏允许恶性疟原虫生长的合适动物模型,体外试验是否能预测人类的功能性免疫仍不清楚。本文所述的一种潜在有用的解决方案是,使用在表达人Fc受体的转基因小鼠中感染表达恶性疟原虫抗原的转基因啮齿类疟原虫,来确定人源抗体的抗疟效果。这些人IgG1治愈了原本致命的疟疾感染,并且保护作用关键依赖于人FcγRI。这一重要发现证明了FcγRI介导强效抗疟疾免疫的能力,并支持开发针对人类疟疾的FcγRI导向疗法。

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