Protective Antigens of Bloodstage Plasmodium knowlesi Parasites [and Discussion]

Protective Antigens of Bloodstage Plasmodium knowlesi Parasites [and Discussion]

The simian malaria Plasmodium knowlesi provides many favourable features as an experimental model; it can be grown in vivo or in vitro. Parasites of defined variant specificity and stage of development are readily obtained and both the natural host and a highly susceptible host are available for exp...

Full description

Saved in:
Bibliographic Details
Published in:Philosophical transactions of the Royal Society of London. Series B, Biological sciences Vol. 307; no. 1131; pp. 159 - 169
Main Authors: Dean, Judith A., Mach, B.
Format: Journal Article
Language:English
Published: London The Royal Society 13-11-1984
Subjects:
Animals
Antibodies
Antibodies - immunology
Antibodies, Monoclonal
Antigens
Antigens, Protozoan - immunology
Erythrocyte invasion
Erythrocytes
Erythrocytes - parasitology
Humans
Immunization
Infections
Macaca mulatta
Malaria
Malaria - blood
Malaria - immunology
Malaria - prevention & control
Merozoites
Monoclonal antibodies
Parasites
Peptides - immunology
Plasmodium - growth & development
Plasmodium - immunology
Schizonts
Online Access:Get full text
Tags: Add Tag
No Tags, Be the first to tag this record!
Description
Summary:The simian malaria Plasmodium knowlesi provides many favourable features as an experimental model; it can be grown in vivo or in vitro. Parasites of defined variant specificity and stage of development are readily obtained and both the natural host and a highly susceptible host are available for experimental infection and vaccination trials. Proteins synthesized by erythrocytic P. knowlesi parasites are characteristic of the developmental stage, as are the alterations that the parasite induces in the red cell surface. Erythrocytic merozoites are anatomically and biochemically complex, their surface alone is covered by at least eight distinct polypeptides. Immune serum from merozoite-immunized rhesus recognizes many parasite components, especially those synthesized by schizonts. All of the merozoite surface components and some of the schizont-infected red cell surface antigens are recognized by such immune sera. Rhesus monkeys rendered immune by repeated infection may by contrast recognize comparatively few antigens; a positive correlation was established for these `naturally' immunized monkeys between protection and antibody directed against a 74000 molecular mass antigen. Immunization with this purified antigen confers partial protection. Other putative protective antigens have been identified by monoclonal antibodies that inhibit merozoite invasion of red cells in vitro. The antigens recognized by inhibitory monoclonal antibodies are synthesized exclusively by schizonts and are processed, at the time of schizont rupture and merozoite release, to smaller molecules that are present on the merozoite surface. The multiplicity of protective antigens is clearly demonstrated by the fact that seven distinct merozoite surface antigens are recognized by three different inhibitory monoclonals. None of the protective antigens identified are variant or strain specific.
ISSN:0080-4622
0962-8436
2054-0280
DOI:10.1098/rstb.1984.0116