The role of exome sequencing in childhood interstitial or diffuse lung disease

Author:

Temple Suzanna E. L.ORCID,Ho Gladys,Bennetts Bruce,Boggs Kirsten,Vidic Nada,Mowat David,Christodoulou John,Schultz André,Gayagay Thet,Roscioli Tony,Zhu Ying,Lunke Sebastian,Armstrong David,Harrison Joanne,Kapur Nitin,McDonald Tim,Selvadurai Hiran,Tai Andrew,Stark Zornitza,Jaffe Adam

Abstract

Abstract Background Children’s interstitial and diffuse lung disease (chILD) is a complex heterogeneous group of lung disorders. Gene panel approaches have a reported diagnostic yield of ~ 12%. No data currently exist using trio exome sequencing as the standard diagnostic modality. We assessed the diagnostic utility of using trio exome sequencing in chILD. We prospectively enrolled children meeting specified clinical criteria between 2016 and 2020 from 16 Australian hospitals. Exome sequencing was performed with analysis of an initial gene panel followed by trio exome analysis. A subset of critically ill infants underwent ultra-rapid trio exome sequencing as first-line test. Results 36 patients [median (range) age 0.34 years (0.02–11.46); 11F] were recruited from multiple States and Territories. Five patients had clinically significant likely pathogenic/pathogenic variants (RARB, RPL15, CTCF, RFXANK, TBX4) and one patient had a variant of uncertain significance (VIP) suspected to contribute to their clinical phenotype, with VIP being a novel gene candidate. Conclusions Trio exomes (6/36; 16.7%) had a better diagnostic rate than gene panel (1/36; 2.8%), due to the ability to consider a broader range of underlying conditions. However, the aetiology of chILD in most cases remained undetermined, likely reflecting the interplay between low penetrant genetic and environmental factors.

Funder

Australian Genomics Health Alliance

Royal Children's Hospital Foundation

Publisher

Springer Science and Business Media LLC

Subject

Pharmacology (medical),Genetics (clinical),General Medicine

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