The CDY-related gene family: coordinated evolution in copy number, expression profile and protein sequence

doi:10.1093/hmg/ddg185

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Human Molecular Genetics, 2003, Vol. 12, No. 14 1643-1650
DOI: 10.1093/hmg/ddg185
© 2003 Oxford University Press

The CDY-related gene family: coordinated evolution in copy number, expression profile and protein sequence

Steve Dorus¹^,2, Sandra L. Gilbert¹, Michele L. Forster¹, Robert J. Barndt¹ and Bruce T. Lahn¹^,*

¹Howard Hughes Medical Institute, Department of Human Genetics and ²Committee on Genetics, University of Chicago, Chicago, IL 60637, USA

Received April 8, 2003; Accepted May 10, 2003

Theories predict that the long-term survival of duplicated genesrequires their functional diversification, which can be accomplishedby either subfunctionalization (the partitioning of ancestralfunctions among duplicates) or neofunctionalization (the acquisitionof novel function). Here, we characterize the CDY-related mammaliangene family, focusing on three aspects of its evolution: genecopy number, tissue expression profile and amino acid sequence.We show that the progenitor of this gene family arose de novoin the mammalian ancestor via domain accretion. This progenitorlater duplicated to generate CDYL and CDYL2, two autosomal genesfound in all extant mammals. Prior to human–mouse divergence(and perhaps preceding the eutherian radiation), a processedCDYL transcript retroposed onto the Y chromosome to create CDY,the Y-linked member of the family. In the simian lineage, CDYwas retained and subsequently amplified on the Y. In non-simianmammals, however, CDY appears to have been lost. The retentionof the Y-linked CDY genes in simians spurred the process ofsubfunctionalization and possibly neofunctionalization. Subfunctionalizationis evidenced by the observation that simian CDYL and CDYL2 retainedtheir somatic housekeeping transcripts but lost the spermatogenictranscripts to the newly arisen CDY. Neo-functionalization issuggested by the rapid evolution of the CDY protein sequence.Thus, the CDY-related family offers an instructive example ofhow duplicated genes undergo functional diversification in bothexpression profile and protein sequence. It also supports thepreviously postulated notion that there is a tendency for spermatogenicfunctions to transfer from autosomes to the Y chromosome.

^* To whom correspondence should be addressed. Tel: +1 7738344393;Fax: +1 7738348470; Email: blahn{at}genetics.uchicago.edu

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