Case of 7p22.1 Microduplication Detected by Whole Genome Microarray (REVEAL) in Workup of Child Diagnosed with Autism

Author:

Goitia Veronica1,Oquendo Marcial1,Stratton Robert2

Affiliation:

1. Department of Pediatrics, Driscoll Children’s Hospital, Corpus Christi, TX 78411, USA

2. Department of Medical Genetics, Driscoll Children’s Hospital, Corpus Christi, TX 78411, USA

Abstract

Introduction. More than 60 cases of 7p22 duplications and deletions have been reported with over 16 of them occurring without concomitant chromosomal abnormalities.Patient and Methods. We report a 29-month-old male diagnosed with autism. Whole genome chromosome SNP microarray (REVEAL) demonstrated a 1.3 Mb interstitial duplication of 7p22.1 ->p22.1 arr 7p22.1 (5,436,367–6,762,394), the second smallest interstitial 7p duplication reported to date. This interval included 14 OMIM annotated genes (FBXL18, ACTB, FSCN1, RNF216, OCM, EIF2AK1, AIMP2, PMS2, CYTH3, RAC1, DAGLB, KDELR2, GRID2IP,and ZNF12).Results. Our patient presented features similar to previously reported cases with 7p22 duplication, including brachycephaly, prominent ears, cryptorchidism, speech delay, poor eye contact, and outburst of aggressive behavior with autism-like features. Among the genes located in the duplicated segment,ACTBgene has been proposed as a candidate gene for the alteration of craniofacial development. Overexpression ofRNF216Lhas been linked to autism. FSCN1 may play a role in neurodevelopmental disease.Conclusion. Characterization of a possible 7p22.1 Duplication Syndrome has yet to be made. Recognition of the clinical spectrum in patients with a smaller duplication of 7p should prove valuable for determining the minimal critical region, helping delineate a better prediction of outcome and genetic counseling

Publisher

Hindawi Limited

Subject

General Medicine

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