AI Article Synopsis

  • Whole-exome sequencing (WES) has significantly improved the diagnosis of Mendelian disorders, but there's uncertainty about when to review the data for undiagnosed patients and limited information on its cost-effectiveness.
  • A study of 54 patients showed that reanalyzing WES data after 12 months led to an increase in diagnostic success from 30% to 41%, thanks to new disease gene publications and improved analysis methods.
  • The cost analysis indicated that using WES can save an average of $586 per additional diagnosis in patients with intellectual disabilities, making early WES application both effective and financially advantageous.

Article Abstract

Purpose: Whole-exome sequencing (WES) has revolutionized Mendelian diagnostics, however, there is no consensus on the timing of data review in undiagnosed individuals and only preliminary data on the cost-effectiveness of this technology. We aimed to assess the utility of WES data reanalysis for diagnosis in Mendelian disorders and to analyze the cost-effectiveness of this technology compared with a traditional diagnostic pathway.

Methods: WES was applied to a cohort of 54 patients from 37 families with a variety of Mendelian disorders to identify the genetic etiology. Reanalysis was performed after 12 months with an improved WES diagnostic pipeline. A comparison was made between costs of a modeled WES pathway and a traditional diagnostic pathway in a cohort with intellectual disability (ID).

Results: Reanalysis of WES data at 12 months improved diagnostic success from 30 to 41% due to interim publication of disease genes, expanded phenotype data from referrer, and an improved bioinformatics pipeline. Cost analysis on the ID cohort showed average cost savings of US$586 (AU$782) for each additional diagnosis.

Conclusion: Early application of WES in Mendelian disorders is cost-effective and reanalysis of an undiagnosed individual at a 12-month time point increases total diagnoses by 11%.

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Source
http://dx.doi.org/10.1038/gim.2018.39DOI Listing

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