GRID – Genomics of Rare Immune Disorders: a highly sensitive and specific diagnostic gene panel for patients with primary immunodeficiencies

Author:

Simeoni Ilenia,Shamardina Olga,Deevi Sri VV,Thomas Moira,Megy Karyn,Staples Emily,Whitehorn Deborah,Duarte Daniel,Mapeta Rutendo,Ouwehand Willem H,Penkett Christopher J,Rayner-Matthews Paula,Stark Hannah,Stephens Jonathan C,Stirrups Kathleen E,Turro Ernest,Thrasher Adrian,Kuijpers Taco W,Smith Kenneth GC,Savic Sinisa,Burns Siobhan O,Thaventhiran James E,Allen Hana LangoORCID,

Abstract

AbstractPrimary Immune disorders affect 15,000 new patients every year in Europe. Genetic tests are usually performed on a single or very limited number of genes leaving the majority of patients without a genetic diagnosis. We designed, optimised and validated a new clinical diagnostic platform called GRID, Genomics of Rare Immune Disorders, to screen in parallel 279 genes, including 2015 IUIS genes, known to be causative of Primary Immune disorders (PID). Validation to clinical standard using more than 58,000 variants in 176 PID patients shows an excellent sensitivity, specificity. The customised and automated bioinformatics pipeline prioritises and reports pertinent Single Nucleotide Variants (SNVs), INsertions and DELetions (INDELs) as well as Copy Number Variants (CNVs). An example of the clinical utility of the GRID panel, is represented by a patient initially diagnosed with X-linked agammaglobulinemia due to a missense variant in the BTK gene with severe inflammatory bowel disease. GRID results identified two additional compound heterozygous variants in IL17RC, potentially driving the altered phenotype.

Publisher

Cold Spring Harbor Laboratory

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