A comprehensive evaluation of rodent malaria parasite genomes and gene expression
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Type
ArticleAuthors
Otto, Thomas DBöhme, Ulrike
Jackson, Andrew P
Hunt, Martin
Franke-Fayard, Blandine
Hoeijmakers, Wieteke A M
Religa, Agnieszka A
Robertson, Lauren
Sanders, Mandy
Ogun, Solabomi A
Cunningham, Deirdre
Erhart, Annette
Billker, Oliver
Khan, Shahid M
Stunnenberg, Hendrik G
Langhorne, Jean
Holder, Anthony A.

Waters, Andrew P
Newbold, Chris I
Pain, Arnab

Berriman, Matthew
Janse, Chris J
KAUST Department
Biological and Environmental Sciences and Engineering (BESE) DivisionBioscience Program
Pathogen Genomics Laboratory
Date
2014-10-30Online Publication Date
2014-10-30Print Publication Date
2014-12Permanent link to this record
http://hdl.handle.net/10754/336369
Metadata
Show full item recordAbstract
Background: Rodent malaria parasites (RMP) are used extensively as models of human malaria. Draft RMP genomes have been published for Plasmodium yoelii, P. berghei ANKA (PbA) and P. chabaudi AS (PcAS). Although availability of these genomes made a significant impact on recent malaria research, these genomes were highly fragmented and were annotated with little manual curation. The fragmented nature of the genomes has hampered genome wide analysis of Plasmodium gene regulation and function. Results: We have greatly improved the genome assemblies of PbA and PcAS, newly sequenced the virulent parasite P. yoelii YM genome, sequenced additional RMP isolates/lines and have characterized genotypic diversity within RMP species. We have produced RNA-seq data and utilized it to improve gene-model prediction and to provide quantitative, genome-wide, data on gene expression. Comparison of the RMP genomes with the genome of the human malaria parasite P. falciparum and RNA-seq mapping permitted gene annotation at base-pair resolution. Full-length chromosomal annotation permitted a comprehensive classification of all subtelomeric multigene families including the `Plasmodium interspersed repeat genes' (pir). Phylogenetic classification of the pir family, combined with pir expression patterns, indicates functional diversification within this family. Conclusions: Complete RMP genomes, RNA-seq and genotypic diversity data are excellent and important resources for gene-function and post-genomic analyses and to better interrogate Plasmodium biology. Genotypic diversity between P. chabaudi isolates makes this species an excellent parasite to study genotype-phenotype relationships. The improved classification of multigene families will enhance studies on the role of (variant) exported proteins in virulence and immune evasion/modulation.Citation
A comprehensive evaluation of rodent malaria parasite genomes and gene expression 2014, 12 (1) BMC BiologyPublisher
Springer NatureJournal
BMC BiologyPubMed ID
25359557PubMed Central ID
PMC4242472Additional Links
http://www.biomedcentral.com/1741-7007/12/86ae974a485f413a2113503eed53cd6c53
10.1186/s12915-014-0086-0
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