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The genome of the African trypanosome Trypanosoma brucei
Authors:Berriman Matthew  Ghedin Elodie  Hertz-Fowler Christiane  Blandin Gaëlle  Renauld Hubert  Bartholomeu Daniella C  Lennard Nicola J  Caler Elisabet  Hamlin Nancy E  Haas Brian  Böhme Ulrike  Hannick Linda  Aslett Martin A  Shallom Joshua  Marcello Lucio  Hou Lihua  Wickstead Bill  Alsmark U Cecilia M  Arrowsmith Claire  Atkin Rebecca J  Barron Andrew J  Bringaud Frederic  Brooks Karen  Carrington Mark  Cherevach Inna  Chillingworth Tracey-Jane  Churcher Carol  Clark Louise N  Corton Craig H  Cronin Ann  Davies Rob M  Doggett Jonathon  Djikeng Appolinaire  Feldblyum Tamara  Field Mark C  Fraser Audrey  Goodhead Ian  Hance Zahra
Affiliation:Wellcome Trust Sanger Institute, Wellcome Trust Genome Campus, Hinxton CB10 1SA, UK. mb4@sanger.ac.uk
Abstract:African trypanosomes cause human sleeping sickness and livestock trypanosomiasis in sub-Saharan Africa. We present the sequence and analysis of the 11 megabase-sized chromosomes of Trypanosoma brucei. The 26-megabase genome contains 9068 predicted genes, including approximately 900 pseudogenes and approximately 1700 T. brucei-specific genes. Large subtelomeric arrays contain an archive of 806 variant surface glycoprotein (VSG) genes used by the parasite to evade the mammalian immune system. Most VSG genes are pseudogenes, which may be used to generate expressed mosaic genes by ectopic recombination. Comparisons of the cytoskeleton and endocytic trafficking systems with those of humans and other eukaryotic organisms reveal major differences. A comparison of metabolic pathways encoded by the genomes of T. brucei, T. cruzi, and Leishmania major reveals the least overall metabolic capability in T. brucei and the greatest in L. major. Horizontal transfer of genes of bacterial origin has contributed to some of the metabolic differences in these parasites, and a number of novel potential drug targets have been identified.
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