| Literature DB >> 25439725 |
Claudia M B Carvalho1, Shivakumar Vasanth2, Marwan Shinawi3, Chad Russell2, Melissa B Ramocki4, Chester W Brown5, Jesper Graakjaer6, Anne-Bine Skytte6, Angela M Vianna-Morgante7, Ana C V Krepischi7, Gayle S Patel8, LaDonna Immken9, Kyrieckos Aleck10, Cynthia Lim10, Sau Wai Cheung11, Carla Rosenberg7, Nicholas Katsanis12, James R Lupski13.
Abstract
The 17p13.1 microdeletion syndrome is a recently described genomic disorder with a core clinical phenotype of intellectual disability, poor to absent speech, dysmorphic features, and a constellation of more variable clinical features, most prominently microcephaly. We identified five subjects with copy-number variants (CNVs) on 17p13.1 for whom we performed detailed clinical and molecular studies. Breakpoint mapping and retrospective analysis of published cases refined the smallest region of overlap (SRO) for microcephaly to a genomic interval containing nine genes. Dissection of this phenotype in zebrafish embryos revealed a complex genetic architecture: dosage perturbation of four genes (ASGR1, ACADVL, DVL2, and GABARAP) impeded neurodevelopment and decreased dosage of the same loci caused a reduced mitotic index in vitro. Moreover, epistatic analyses in vivo showed that dosage perturbations of discrete gene pairings induce microcephaly. Taken together, these studies support a model in which concomitant dosage perturbation of multiple genes within the CNV drive the microcephaly and possibly other neurodevelopmental phenotypes associated with rearrangements in the 17p13.1 SRO.Entities:
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Year: 2014 PMID: 25439725 PMCID: PMC4225592 DOI: 10.1016/j.ajhg.2014.10.006
Source DB: PubMed Journal: Am J Hum Genet ISSN: 0002-9297 Impact factor: 11.025