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Population genomics of the immune evasion (var) genes of Plasmodium falciparum

journal contribution
posted on 2007-03-16, 00:00 authored by Alyssa BarryAlyssa Barry, A Leliwa-Sytek, L Tavul, H Imrie, F Migot-Nabias, S M Brown, G A V McVean, K P Day
Var genes encode the major surface antigen (PfEMP1) of the blood stages of the human malaria parasite Plasmodium falciparum. Differential expression of up to 60 diverse var genes in each parasite genome underlies immune evasion. We compared the diversity of the DBLα domain of var genes sampled from 30 parasite isolates from a malaria endemic area of Papua New Guinea (PNG) and 59 from widespread geographic origins (global). Overall, we obtained over 8,000 quality-controlled DBLα sequences. Within our sampling frame, the global population had a total of 895 distinct DBLα "types" and negligible overlap among repertoires. This indicated that var gene diversity on a global scale is so immense that many genomes would need to be sequenced to capture its true extent. In contrast, we found a much lower diversity in PNG of 185 DBLα types, with an average of approximately 7% overlap among repertoires. While we identify marked geographic structuring, nearly 40% of types identified in PNG were also found in samples from different countries showing a cosmopolitan distribution for much of the diversity. We also present evidence to suggest that recombination plays a key role in maintaining the unprecedented levels of polymorphism found in these immune evasion genes. This population genomic framework provides a cost effective molecular epidemiological tool to rapidly explore the geographic diversity of var genes. © 2007 Barry et al.

History

Journal

PLoS Pathogens

Volume

3

Issue

3

Article number

e34

Pagination

1 - 9

Publisher

Public Library of Science

Location

San Francisco, Calif.

ISSN

1553-7366

eISSN

1553-7374

Language

eng

Publication classification

C1.1 Refereed article in a scholarly journal