Characterization and evolution of the novel gene family FAM90A in primates originated by multiple duplication and rearrangement events

doi:10.1093/hmg/ddm209

Human Molecular Genetics Advance Access originally published online on August 7, 2007
Human Molecular Genetics 2007 16(21):2572-2582; doi:10.1093/hmg/ddm209

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Characterization and evolution of the novel gene family FAM90A in primates originated by multiple duplication and rearrangement events

Nina Bosch¹, Mario Cáceres¹, Maria Francesca Cardone², Anna Carreras¹, Ester Ballana¹, Mariano Rocchi², Lluís Armengol¹ and Xavier Estivill¹^,3^,*

¹ Genes and Disease Program, Center for Genomic Regulation (CRG-UPF) and CIBERESP, Barcelona, Catalonia, Spain, ² Department of Genetics and Microbiology, University of Bari, Bari, Italy and ³ Experimental and Health Sciences Department, Pompeu Fabra University, Barcelona, Cataloniasss, Spain

^* To whom correspondence should be addressed at: Genes and Disease Program, Center for Genomic Regulation (CRG-UPF), and CIBERESP, Plaça Charles Darwin s/n (Carrer Dr Aiguader, 88), PRBB Building, Room 521, 08003 Barcelona, Catalonia, Spain. Tel: +34-933160159; Fax: +34-933160099; Email: xavier.estivill{at}crg.es

Received April 17, 2007; Accepted July 25, 2007

Genomic plasticity of human chromosome 8p23.1 region is highlyinfluenced by two groups of complex segmental duplications (SDs),termed REPD and REPP, that mediate different kinds of rearrangements.Part of the difficulty to explain the wide range of phenotypesassociated with 8p23.1 rearrangements is that REPP and REPDare not yet well characterized, probably due to their polymorphicstatus. Here, we describe a novel primate-specific gene family,named FAM90A (family with sequence similarity 90), found withinthese SDs. According to the current human reference sequenceassembly, the FAM90A family includes 24 members along 8p23.1region plus a single member on chromosome 12p13.31, showingcopy number variation (CNV) between individuals. These genescan be classified into subfamilies I and II, which differ intheir upstream and 5'-untranslated region sequences, but bothshare the same open reading frame and are ubiquitously expressed.Sequence analysis and comparative fluorescence in situ hybridizationstudies showed that FAM90A subfamily II suffered a big expansionin the hominoid lineage, whereas subfamily I members were likelygenerated sometime around the divergence of orangutan and Africangreat apes by a fusion process. In addition, the analysis ofthe Ka/Ks ratios provides evidence of functional constraintof some FAM90A genes in all species. The characterization ofthe FAM90A gene family contributes to a better understandingof the structural polymorphism of the human 8p23.1 region andconstitutes a good example of how SDs, CNVs and rearrangementswithin themselves can promote the formation of new gene sequenceswith potential functional consequences.

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