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Comparative genomics of the neglected human malaria parasite Plasmodium vivax
Authors:Carlton Jane M  Adams John H  Silva Joana C  Bidwell Shelby L  Lorenzi Hernan  Caler Elisabet  Crabtree Jonathan  Angiuoli Samuel V  Merino Emilio F  Amedeo Paolo  Cheng Qin  Coulson Richard M R  Crabb Brendan S  Del Portillo Hernando A  Essien Kobby  Feldblyum Tamara V  Fernandez-Becerra Carmen  Gilson Paul R  Gueye Amy H  Guo Xiang  Kang'a Simon  Kooij Taco W A  Korsinczky Michael  Meyer Esmeralda V-S  Nene Vish  Paulsen Ian  White Owen  Ralph Stuart A  Ren Qinghu  Sargeant Tobias J  Salzberg Steven L  Stoeckert Christian J  Sullivan Steven A  Yamamoto Marcio M  Hoffman Stephen L  Wortman Jennifer R  Gardner Malcolm J
Affiliation:The Institute for Genomic Research/J. Craig Venter Institute, 9704 Medical Research Drive, Rockville, Maryland 20850, USA. jane.carlton@nyumc.org
Abstract:The human malaria parasite Plasmodium vivax is responsible for 25-40% of the approximately 515 million annual cases of malaria worldwide. Although seldom fatal, the parasite elicits severe and incapacitating clinical symptoms and often causes relapses months after a primary infection has cleared. Despite its importance as a major human pathogen, P. vivax is little studied because it cannot be propagated continuously in the laboratory except in non-human primates. We sequenced the genome of P. vivax to shed light on its distinctive biological features, and as a means to drive development of new drugs and vaccines. Here we describe the synteny and isochore structure of P. vivax chromosomes, and show that the parasite resembles other malaria parasites in gene content and metabolic potential, but possesses novel gene families and potential alternative invasion pathways not recognized previously. Completion of the P. vivax genome provides the scientific community with a valuable resource that can be used to advance investigation into this neglected species.
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