Gene expression in pharyngeal arch 1 during human embryonic development

doi:10.1093/hmg/ddi083

Human Molecular Genetics Advance Access originally published online on February 9, 2005
Human Molecular Genetics 2005 14(7):903-912; doi:10.1093/hmg/ddi083

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Gene expression in pharyngeal arch 1 during human embryonic development

Juanliang Cai¹, David Ash¹, Lori E. Kotch¹, Ethylin Wang Jabs¹^,*, Tania Attie-Bitach², Joelle Auge², Geraldine Mattei², Heather Etchevers², Michel Vekemans², Yulia Korshunova³, Rose Tidwell³, David N. Messina³, Julia B. Winston³ and Michael Lovett³

¹Institute of Genetic Medicine, Johns Hopkins University, Baltimore, MD 21205, USA, ²Department of Genetics and INSERM U-393, Hopital Necker Enfants Malades, 75743 Paris, France and ³Department of Genetics, Washington University School of Medicine, St Louis, MO 63110, USA

^* To whom correspondence should be addressed at: McKusick-Nathans Institute of Genetic Medicine, The Johns Hopkins University, 733 N Broadway, Room 419, Baltimore, MD 21205, USA. Tel: +1 4109554160; Fax: +1 4105025677; Email: ejabs1{at}jhem.jhmi.edu

Received December 3, 2004; Accepted February 1, 2005

Craniofacial abnormalities are one of the most common birthdefects in humans, but little is known about the human genesthat control these important developmental processes. To identifyrelevant genes, we analyzed transcription profiles of humanpharyngeal arch 1 (PA1), a conserved embryonic structure thatdevelops into the palate and jaw. Using microdissected, normalhuman craniofacial structures, we constructed 12 SAGE (serialanalysis of gene expression) libraries and sequenced 606 532tags. We also performed Affymetrix microarray analysis on 25craniofacial targets. Our data revealed not only genes ‘enriched’or differentially expressed in PA1 during fourth and fifth weekof human development, but also 6927 genes newly identified tobe expressed in human PA1. Many of these genes are involvedin biosynthetic processes and have binding function and catalyticactivity. We compared expression profiles of human genes withthose of mouse homologs to look for genes more specific to humancraniofacial development and found 766 genes expressed in humanPA1, but not in mouse PA1. We also identified 1408 genes thatwere expressed in mouse as well as human PA1 and could be usefulin creating mouse models for human conditions. We confirmedconservation of some human PA1 expression patterns in mouseembryonic samples with whole mount in situ hybridization andreal-time RT–PCR. This comprehensive approach to expressionprofiling gives insights into the early development of the craniofacialregion and provides markers for developmental structures andcandidate genes, including SET and CCT3, for diseases such asorofacial clefting and micrognathia.

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