Mechanism of genetic exchange in American trypanosomes

Gaunt, Michael W.; Yeo, Matthew; Frame, Iain A.; Stothard, J. Russell; Carrasco, Hernan J.; Taylor, Martin C.; Mena, Susana Solis; Veazey, Paul; Miles, Graham A. J.; Acosta, Nidia; de Arias, Antonieta Rojas; Miles, Michael A.

Mechanism of genetic exchange in American trypanosomes

Michael W. Gaunt, Matthew Yeo, Iain A. Frame, J. Russell Stothard, Hernan J. Carrasco, Martin C. Taylor, Susana Solis Mena, Paul Veazey, Graham A. J. Miles, Nidia Acosta, Antonieta Rojas de Arias and Michael A. Miles ()
Additional contact information
Michael W. Gaunt: London School of Hygiene and Tropical Medicine
Matthew Yeo: London School of Hygiene and Tropical Medicine
Iain A. Frame: London School of Hygiene and Tropical Medicine
J. Russell Stothard: The Natural History Museum
Hernan J. Carrasco: Universidad Central de Venezuela
Martin C. Taylor: London School of Hygiene and Tropical Medicine
Susana Solis Mena: London School of Hygiene and Tropical Medicine
Paul Veazey: London School of Hygiene and Tropical Medicine
Graham A. J. Miles: London School of Hygiene and Tropical Medicine
Nidia Acosta: Universidad Nacional de Asuncion
Antonieta Rojas de Arias: Universidad Nacional de Asuncion
Michael A. Miles: London School of Hygiene and Tropical Medicine

Nature, 2003, vol. 421, issue 6926, 936-939

Abstract: Abstract The kinetoplastid Protozoa are responsible for devastating diseases1. In the Americas, Trypanosoma cruzi is the agent of Chagas' disease—a widespread disease transmissible from animals to humans (zoonosis)—which is transmitted by exposure to infected faeces of blood-sucking triatomine bugs2. The presence of genetic exchange in T. cruzi and in Leishmania is much debated3,4. Here, by producing hybrid clones, we show that T. cruzi has an extant capacity for genetic exchange. The mechanism is unusual and distinct from that proposed for the African trypanosome, Trypanosoma brucei5. Two biological clones6 of T. cruzi were transfected to carry different drug-resistance markers7,8, and were passaged together through the entire life cycle. Six double-drug-resistant progeny clones, recovered from the mammalian stage of the life cycle, show fusion of parental genotypes, loss of alleles, homologous recombination, and uniparental inheritance of kinetoplast maxicircle DNA. There are strong genetic parallels between these experimental hybrids and the genotypes among natural isolates of T. cruzi. In this instance, aneuploidy through nuclear hybridization results in recombination across far greater genetic distances than mendelian genetic exchange. This mechanism also parallels genome duplication9,10.

Date: 2003
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DOI: 10.1038/nature01438

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