| Literature DB >> 28617419 |
Ashleigh R Pavey1,2,3, Dale L Bodian3, Thierry Vilboux3, Alina Khromykh3, Natalie S Hauser3,4, Kathi Huddleston3, Elisabeth Klein3, Aaron Black3, Megan S Kane3, Ramaswamy K Iyer3, John E Niederhuber3,5, Benjamin D Solomon3,4,6.
Abstract
PurposeImmunodeficiency screening has been added to many state-directed newborn screening programs. The current methodology is limited to screening for severe T-cell lymphopenia disorders. We evaluated the potential of genomic sequencing to augment current newborn screening for immunodeficiency, including identification of non-T cell disorders.MethodsWe analyzed whole-genome sequencing (WGS) and clinical data from a cohort of 1,349 newborn-parent trios by genotype-first and phenotype-first approaches. For the genotype-first approach, we analyzed predicted protein-impacting variants in 329 immunodeficiency-related genes in the WGS data. As a phenotype-first approach, electronic health records were used to identify children with clinical features suggestive of immunodeficiency. Genomes of these children and their parents were analyzed using a separate pipeline for identification of candidate pathogenic variants for rare Mendelian disorders.ResultsWGS provides adequate coverage for most known immunodeficiency-related genes. 13,476 distinct variants and 8,502 distinct predicted protein-impacting variants were identified in this cohort; five individuals carried potentially pathogenic variants requiring expert clinical correlation. One clinically asymptomatic individual was found genomically to have complement component 9 deficiency. Of the symptomatic children, one was molecularly identified as having an immunodeficiency condition and two were found to have other molecular diagnoses.ConclusionNeonatal genomic sequencing can potentially augment newborn screening for immunodeficiency.Entities:
Mesh:
Year: 2017 PMID: 28617419 DOI: 10.1038/gim.2017.57
Source DB: PubMed Journal: Genet Med ISSN: 1098-3600 Impact factor: 8.822