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Автор Kyes, Sue
Автор Horrocks, Paul
Автор Newbold, Chris
Дата выпуска 2001
dc.description ▪ Abstract  Many pathogens that either rely on an insect vector to complete their life cycle (e.g., Trypanosoma spp. and Borrelia spp.) or exist in a unique ecological niche where transmission from host to host is sporadic (e.g., Neisseria spp.) have evolved strategies to maintain infection of their mammalian hosts for long periods of time in order to ensure their survival. Because they have to survive in the face of a fully functional immune system, a common feature of many of these organisms is their development of sophisticated strategies for immune evasion. For the above organisms and for malaria parasites of the genus Plasmodium, a common theme is the ability to undergo clonal antigenic variation. In all cases, surface molecules that are important targets of the humoral immune response are encoded in the genome as multicopy, nonallelic gene families. Antigenic variation is accomplished by the successive expression of members of these gene families that show little or no immunological cross-reactivity. In the case of malaria parasites, however, some of the molecules that undergo antigenic variation are also major virulence factors, adding an additional level of complication to the host-parasite interaction. In this review, we cover the history of antigenic variation in malaria and then summarize the more recent data with particular emphasis on Plasmodium falciparum, the etiological agent of the most severe form of human malaria.
Формат application.pdf
Издатель Annual Reviews
Копирайт Annual Reviews
Название ANTIGENIC VARIATION AT THE INFECTED RED CELL SURFACE IN MALARIA
DOI 10.1146/annurev.micro.55.1.673
Print ISSN 0066-4227
Журнал Annual Review of Microbiology
Том 55
Первая страница 673
Последняя страница 707
Аффилиация Kyes, Sue; Molecular Parasitology Group, Weatherall Institute of Molecular Medicine, Headington, Oxford OX3 9DS United Kingdom; e-mail: skyes@molbiol.ox.ac.uk horrocks@hammer.imm.ox.ac.uk cnewbold@hammer.imm.ox.ac.uk

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