Abnormal social behaviors and altered gene expression rates in a mouse model for Potocki-Lupski Syndrome

doi:10.1093/hmg/ddn148

Human Molecular Genetics Advance Access published online on May 10, 2008
Human Molecular Genetics, doi:10.1093/hmg/ddn148

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Abnormal social behaviors and altered gene expression rates in a mouse model for Potocki-Lupski Syndrome

Jessica Molina¹^,2, Paulina Carmona Mora¹^,2, Jacqueline Chrast³, Paola M. Krall¹^,2, César P. Canales¹^,2, James R. Lupski⁴^,5^,6, Alexandre Reymond³ and Katherina Walz¹^,*

¹ Centro de Estudios Científicos, CECS, Valdivia, Chile, Lausanne, Switzerland ² Universidad Austral de Chile, Valdivia, Chile, Lausanne, Switzerland ³ The Center for Integrative Genomics, University of Lausanne, Lausanne, Switzerland ⁴ Departments of Molecular & Human Genetics and Houston, Texas, USA ⁵ Departments of Pediatrics, Baylor College of Medicine and Houston, Texas, USA ⁶ Texas Children's Hospital, Houston, Texas, USA

^* Corresponding Author: Katherina Walz, Ph.D., Avda. Prat 514, 5110246, Valdivia, Chile. e-mail: kwalz{at}cecs.cl FAX: (56) 63-234517 Phone: (56) 63-234514

Received February 27, 2008; Revised May 7, 2008; Accepted May 7, 2008

The Potocki-Lupski syndrome (PTLS) is associated with a microduplicationof 17p11.2. Clinical features include multiple congenital andneurobehavioral abnormalities and autistic features. We havegenerated a PTLS mouse model, Dp(11)17/+, that recapitulatessome of the physical and neurobehavioral phenotypes presentin patients. Here we investigated the social behavior and geneexpression pattern of this mouse model in a pure genetic background.Dp(11)17/+ male mice displayed normal home cage behavior butincreased anxiety and increased dominant behavior in specifictests. A subtle impairment in the preference for a social targetvs. an inanimate target and abnormal preference for social novelty(the preference to explore an unfamiliar mouse versus a familiarone) was also observed. Our results indicate that these animalscould provide a valuable model to identify the specific gene(s)that confer abnormal social behaviors and that map within thisdelimited genomic deletion interval. In a first attempt to identifycandidate genes and for elucidating the mechanisms of regulationof these important phenotypes we directly assessed the relativetranscription of genes within and around this genomic interval.In this mouse model we found that candidates genes include notonly most of the duplicated genes, but also normal-copy genesthat flank the engineered interval; both categories of genesshowed altered expression levels in the hippocampus of Dp(11)17/+mice.

GEO Series accession number: GSE11013

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