| Literature DB >> 27194972 |
Ashleigh R Pavey1, Thierry Vilboux2, Holly E Babcock3, Margot Ahronovich4, Benjamin D Solomon5.
Abstract
The ability to interrogate the genome via chromosomal microarray and sequencing-based technologies has accelerated the ability to rapidly and accurately define etiologies as well as new candidate genes related to genetic conditions. We describe a male patient with a lethal presentation of a multiple congenital anomaly syndrome that appeared consistent with a ciliopathy phenotype. The patient was found to have a novel maternally inherited 1.9-Mb X chromosome deletion including 4 known genes. Presently, the biological functions of these genes are not well delineated. However, at least one of these genes may be a promising candidate gene for this pattern of anomalies based on the function of related genes and information from publicly available copy number variant databases of control and affected individuals. These genes would bear further scrutiny in larger cohorts of patients with similar phenotypes.Entities:
Keywords: Chromosomal microarray; Ciliopathy; Deletion; Multiple congenital anomalies; X-linked inheritance
Year: 2016 PMID: 27194972 PMCID: PMC4862391 DOI: 10.1159/000444666
Source DB: PubMed Journal: Mol Syndromol ISSN: 1661-8769