0 citations0 references

The Genome of the Kinetoplastid Parasite, Leishmania major

Science2005Vol. 309(5733), pp. 436–442

Citations Over TimeTop 1% of 2005 papers

Alasdair Ivens, Christopher S. Peacock, Elizabeth A. Worthey, Lee Murphy, Gautam Aggarwal, Matthew Berriman, Ellen Sisk, Marie‐Adèle Rajandream, Ellen Adlem, Rita Aert, Atashi Anupama, Zina Apostolou, Philip Attipoe, Nathalie Bason, Christopher Bauser, Alfred Beck, Stephen M. Beverley, Gabriella Bianchettin, Katja Borzym, Gordana Bothe, Carlo V. Bruschi, Matt Collins, Eithon Cadag, Laura Ciarloni, Christine Clayton, Richard Coulson, Ann Cronin, Ângela K. Cruz, Robert M. Davies, Javier De Gaudenzi, Deborah E. Dobson, Andreas Duesterhoeft, Gholam Fazelina, Nigel Fosker, Alberto C.C. Frasch, Audrey Fraser, Monika Fuchs, Claudia Gabel, Arlette Goble, AndreÌ Goffeau, David Harris, Christiane Hertz‐Fowler, H. Hilbert, David Horn, Yiting Huang, Sven Klages, Andrew Knights, Michael Kube, Natasha Larke, Lyudmila Litvin, Angela Lord, Tin Louie, Marco A. Marra, David Masuy, Keith R. Matthews, Shulamit Michaeli, Jeremy C. Mottram, Silke MuÌller-Auer, Heather Munden, Siri Nelson, Halina Norbertczak, Karen Oliver, Susan O’Neil, Martin Pentony, Thomas Pohl, Claire Price, BeÌneÌdicte Purnelle, Michael A. Quail, Ester Rabbinowitsch, Richard Reinhardt, Michael A. Rieger, Joel Rinta, Johan Robben, Laura Robertson, Jerônimo C. Ruiz, Simon Rutter, David Saunders, Melanie SchaÌfer, Jacquie Schein, David C. Schwartz, Kathy Seeger, Amber Seyler, Sarah Sharp, Heesun Shin, Dhileep Sivam, Rob Squares, Steve Squares, Valentina Tosato, Christy Vogt, Guido Volckaert, R. Wambutt, Tim Warren, Holger Wedler, John R. Woodward, Shiguo Zhou, Wolfgang Zimmermann, Deborah F. Smith, Jenefer M. Blackwell, Kenneth Stuart, Bart Barrell, Peter J. Myler

Abstract

Leishmania species cause a spectrum of human diseases in tropical and subtropical regions of the world. We have sequenced the 36 chromosomes of the 32.8-megabase haploid genome of Leishmania major (Friedlin strain) and predict 911 RNA genes, 39 pseudogenes, and 8272 protein-coding genes, of which 36% can be ascribed a putative function. These include genes involved in host-pathogen interactions, such as proteolytic enzymes, and extensive machinery for synthesis of complex surface glycoconjugates. The organization of protein-coding genes into long, strand-specific, polycistronic clusters and lack of general transcription factors in the L. major, Trypanosoma brucei, and Trypanosoma cruzi (Tritryp) genomes suggest that the mechanisms regulating RNA polymerase II-directed transcription are distinct from those operating in other eukaryotes, although the trypanosomatids appear capable of chromatin remodeling. Abundant RNA-binding proteins are encoded in the Tritryp genomes, consistent with active posttranscriptional regulation of gene expression.

Related Papers

→ The ambiguous boundary between genes and pseudogenes: the dead rise up, or do they?(2007)113 cited
→ Identification and characterization of over 100 mitochondrial ribosomal protein pseudogenes in the human genome☆(2003)31 cited
→ Network analysis of pseudogene-gene relationships: from pseudogene evolution to their functional potentials(2017)9 cited
Advances in Research on Pseudogenes(2010)
Network analysis of pseudogene-gene relationships: from pseudogene evolution to their functional potentials(2018)