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      The Importance of Human FcγRI in Mediating Protection to Malaria

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          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 FcγRI. This important finding documents the capacity of FcγRI to mediate potent antimalaria immunity and supports the development of FcγRI-directed therapy for human malaria.

          Author Summary

          Malaria rivals HIV and tuberculosis as the world's most deadly infection killing a child every 30 seconds. Antibodies and their receptors (Fc-receptors) have been shown to be vital for the development of protective immunity, and as such they act as correlates of protection in studies aimed at defining the best antigens to incorporate into current vaccines. Understanding antibody types and Fc-receptors that optimally induce immunity is therefore vital to developing the best vaccines. Surrogate markers of antibody efficacy currently rely on in vitro assays that are laborious and difficult to reproduce. It remains unclear if such in vitro assays are predictive of functional immunity in humans due to the lack of suitable animal models permissive for Plasmodium falciparum. Here, we create a transgenic in vivo mouse model that has significant advantage over the use of new world primates, the only other model for human malaria. We demonstrate that this model defines an Fc-dependent mechanism of parasite destruction that cannot be assessed in current in vitro assays. The model provides both a test for therapeutic antibody efficacy prior to clinical trials in humans and an important tool in malaria vaccine development.

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          The global distribution of clinical episodes of Plasmodium falciparum malaria.

          Robert W. Snow, Carlos Guerra, Abdisalan Noor (2005)
          Interest in mapping the global distribution of malaria is motivated by a need to define populations at risk for appropriate resource allocation and to provide a robust framework for evaluating its global economic impact. Comparison of older and more recent malaria maps shows how the disease has been geographically restricted, but it remains entrenched in poor areas of the world with climates suitable for transmission. Here we provide an empirical approach to estimating the number of clinical events caused by Plasmodium falciparum worldwide, by using a combination of epidemiological, geographical and demographic data. We estimate that there were 515 (range 300-660) million episodes of clinical P. falciparum malaria in 2002. These global estimates are up to 50% higher than those reported by the World Health Organization (WHO) and 200% higher for areas outside Africa, reflecting the WHO's reliance upon passive national reporting for these countries. Without an informed understanding of the cartography of malaria risk, the global extent of clinical disease caused by P. falciparum will continue to be underestimated.
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            Gamma-globulin and acquired immunity to human malaria.

            S. Cohen, I A McGregor, S Carrington (1961)
            Article 1 comments Cited 387 times – based on 0 reviews     Review now
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              A proteomic view of the Plasmodium falciparum life cycle.

              Laurence Florens, Michael Washburn, J. Raine (2002)
              The completion of the Plasmodium falciparum clone 3D7 genome provides a basis on which to conduct comparative proteomics studies of this human pathogen. Here, we applied a high-throughput proteomics approach to identify new potential drug and vaccine targets and to better understand the biology of this complex protozoan parasite. We characterized four stages of the parasite life cycle (sporozoites, merozoites, trophozoites and gametocytes) by multidimensional protein identification technology. Functional profiling of over 2,400 proteins agreed with the physiology of each stage. Unexpectedly, the antigenically variant proteins of var and rif genes, defined as molecules on the surface of infected erythrocytes, were also largely expressed in sporozoites. The detection of chromosomal clusters encoding co-expressed proteins suggested a potential mechanism for controlling gene expression.
              Article 0 comments Cited 316 times – based on 0 reviews     Review now
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                Author and article information

                Contributors
                : Role: Editor
                Journal
                Journal ID (nlm-ta): PLoS Pathog
                Journal ID (publisher-id): ppat
                Title: PLoS Pathogens
                Publisher: Public Library of Science (San Francisco, USA )
                ISSN (Print): 1553-7366
                ISSN (Electronic): 1553-7374
                Publication date (Print): May 2007
                Publication date (Electronic): 18 May 2007
                Volume: 3
                Issue: 5
                Electronic Location Identifier: e72
                Affiliations
                [1 ] Institute of Genetics, Queen's Medical Centre, University of Nottingham, United Kingdom
                [2 ] Division of Parasitology, National Institute for Medical Research, Medical Research Council, London, United Kingdom
                [3 ] Medical Research Council Technology, London, United Kingdom
                [4 ] Walter and Eliza Hall Institute of Medical Research, Parkville, Victoria, Australia
                [5 ] Department of Molecular Cell Biology and Immunology, VU Medical Centre, Amsterdam, Netherlands
                [6 ] Immunotherapy Laboratory, Department of Immunology, University Medical Centre Utrecht, Utrecht, Netherlands
                [7 ] Genmab, Utrecht, Netherlands
                Center for Global Health and Diseases, United States of America
                Author notes
                * To whom correspondence should be addressed. E-mail: aholder@ 123456nimr.mrc.ac.uk (AAH); richard.pleass@ 123456nottingham.ac.uk (RJP)
                Article
                Publisher ID: 07-PLPA-RA-0042R2 Serial Item and Contribution ID: plpa-03-05-08
                DOI: 10.1371/journal.ppat.0030072
                PMC ID: 1868954
                PubMed ID: 17511516
                SO-VID: 177f3ea4-70fb-434a-8451-68298c5d5119
                Copyright © Copyright: © 2007 McIntosh et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
                History
                Date received : 23 January 2007
                Date accepted : 4 April 2007
                Page count
                Pages: 12
                Categories
                Subject: Research Article
                Subject: Immunology
                Subject: Infectious Diseases
                Subject: Infectious Diseases
                Subject: Microbiology
                Subject: Plasmodium
                Custom metadata
                citation McIntosh RS, Shi J, Jennings RM, Chappel JC, de Koning-Ward TF, et al. (2007) The importance of human FcγRI in mediating protection to malaria. PLoS Pathog 3(5): e72. doi: 10.1371/journal.ppat.0030072

                ScienceOpen disciplines: Infectious disease & Microbiology
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                ScienceOpen disciplines: Infectious disease & Microbiology

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