Diagnostic yield of rare skeletal dysplasia conditions in the radiogenomics era.
Ataf Hussain SabirElizabeth MorleyJameela SheikhAlistair D CalderAna Beleza-MeirelesMoira S CheungAlessandra CoccaMattias JanssonSuzanne LillisYogen PatelShu YauChristine M HallAmaka C OffiahMelita IrvingPublished in: BMC medical genomics (2021)
Our results highlight the cost-effective use of WES-targeted bioinformatic analysis as a diagnostic tool for SD, particularly patients with presumed SD, where detailed phenotyping is essential. Thorough co-ordinated clinical evaluation between clinical, radiological, and molecular teams is essential for improved yield and clinical care. WES (and WGS) yields will increase with time, allowing faster diagnoses, avoiding needless investigations, ensuring individualised patient care and patient reassurance. Further diagnoses will lead to increased information on natural history/mechanistic details, and likely increased therapies and clinical trials.