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Analysis of Plasmodium falciparum var genes expressed in children from Papua New Guinea
JournalArticle (Originalarbeit in einer wissenschaftlichen Zeitschrift)
 
ID 533209
Author(s) Falk, Nicole; Kaestli, Mirjam; Qi, Weihong; Ott, Michael; Baea, Kay; Cortés, Alfred; Beck, Hans-Peter
Author(s) at UniBasel Beck, Hans-Peter
Year 2009
Title Analysis of Plasmodium falciparum var genes expressed in children from Papua New Guinea
Journal Journal of infectious diseases
Volume 200
Number 3
Pages / Article-Number 347-56
Abstract BACKGROUND: The variable antigen P. falciparum erythrocyte membrane protein-1 (PfEMP1) is a major virulence factor in malaria. A large number of var genes encode PfEMP1, and we hypothesized that a restricted PfEMP1 repertoire determines clinical disease presentation. We conducted a case-control study in Papua New Guinea and analyzed transcribed var genes in naturally infected children. METHODS: var messenger RNA was isolated from 78 children with asymptomatic, mild, or severe malaria. We prepared complementary DNA from the upstream region into the DBL1alpha domain and picked, on average, 20 clones for sequencing. RESULTS: Twenty-five percent of centrally located var genes were shared between children, whereas only 5% of subtelomeric genes were shared, indicating lower diversity in the former group. Linkage between group B or C var upstream sequences and DBL1alpha groups was not observed, which impeded prediction by DBL1alpha analysis. A higher proportion of var group A sequences was detected in symptomatic malaria, and a subgroup of frequently encountered var genes with complex head structure seems to be associated with severe malaria. A subset of var group C genes was frequently expressed in older children with asymptomatic high levels of parasitemia. CONCLUSION: Despite this vast diversity, restricted disease-associated var genes were identified and might be used for innovative interventions based on PfEMP1
Publisher Oxford University Press
ISSN/ISBN 0022-1899
edoc-URL http://edoc.unibas.ch/dok/A5843137
Full Text on edoc No
Digital Object Identifier DOI 10.1086/600071
PubMed ID http://www.ncbi.nlm.nih.gov/pubmed/19552523
ISI-Number WOS:000267604000005
Document type (ISI) Journal Article
 
   

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