New Genes Originated via Multiple Recombinational Pathways in the {beta}-Globin Gene Family of Rodents

doi:10.1093/molbev/msn200

MBE Advance Access originally published online on September 9, 2008
Molecular Biology and Evolution 2008 25(12):2589-2600; doi:10.1093/molbev/msn200

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© The Author 2008. Published by Oxford University Press on behalf of the Society for Molecular Biology and Evolution. All rights reserved. For permissions, please e-mail: journals.permissions@oxfordjournals.org

Research Articles

New Genes Originated via Multiple Recombinational Pathways in the β-Globin Gene Family of Rodents

Federico G. Hoffmann¹, Juan C. Opazo² and Jay F. Storz

School of Biological Sciences, University of Nebraska

E-mail: jstorz2{at}unl.edu.

Accepted for publication September 4, 2008.

Species differences in the size or membership composition ofmultigene families can be attributed to lineage-specific additionsof new genes via duplication, losses of genes via deletion orinactivation, and the creation of chimeric genes via domainshuffling or gene fusion. In principle, it should be possibleto infer the recombinational pathways responsible for each ofthese different types of genomic change by conducting detailedcomparative analyses of genomic sequence data. Here, we reportan attempt to unravel the complex evolutionary history of theβ-globin gene family in a taxonomically diverse set ofrodent species. The main objectives were: 1) to characterizethe genomic structure of the β-globin gene cluster of rodents;2) to assign orthologous and paralogous relationships amongduplicate copies of β-like globin genes; and 3) to inferthe specific recombinational pathways responsible for gene duplications,gene deletions, and the creation of chimeric fusion genes. Resultsof our comparative genomic analyses revealed that variationin gene family size among rodent species is mainly attributableto the differential gain and loss of later expressed β-globingenes via unequal crossing-over. However, two distinct recombinationalmechanisms were implicated in the creation of chimeric fusiongenes. In muroid rodents, a chimeric ${gamma}$ / ${varepsilon}$ fusion gene was createdby unequal crossing-over between the embryonic ${varepsilon}$ - and ${gamma}$ -globingenes. Interestingly, this ${gamma}$ / ${varepsilon}$ fusion gene was generated in thesame fashion as the "anti-Lepore" 5'- ${delta}$ -(β/ ${delta}$ )-β-3' duplicationmutant in humans (the reciprocal exchange product of the pathologicalhemoglobin Lepore deletion mutant). By contrast, in the housemouse, Mus musculus, a chimeric β/ ${delta}$ fusion pseudogene wascreated by a β-globin $->$ ${delta}$ -globin gene conversion event. Althoughthe ${gamma}$ / ${varepsilon}$ and β/ ${delta}$ fusion genes share a similar chimeric genestructure, they originated via completely different recombinationalpathways.

Key Words: chimeric fusion genes • gene conversion • gene duplication • gene family evolution • globin genes • hemoglobin

¹ Present address: Instituto Carlos Chagas—ICC—Fiocruz,Curitiba, Brazil.

² Present address: Instituto de Ecologia y Evolucion, Facultadde Ciencias, Universidad Austral de Chile, Valdivia, Chile.

Adriana Briscoe, Associate Editor

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