The Impact of Rapid Exome Sequencing on Medical Management of Critically Ill Children

Overview

Journal J Pediatr

Specialty Pediatrics

Date 2020 Jun 20

PMID 32553838

Citations 20

Authors

Amanda S Freed

Sarah V Clowes Candadai

Megan C Sikes

Jenny Thies

Heather M Byers

Jennifer N Dines

Mesaki Kenneth Ndugga-Kabuye

Mallory B Smith

Katie Fogus

Heather C Mefford

Christina Lam

Margaret P Adam

Angela Sun

John K McGuire

Robert DiGeronimo

Katrina M Dipple

Gail H Deutsch

Zeenia C Billimoria

James T Bennett

Affiliations

Soon will be listed here.

Abstract

Objectives: To evaluate the clinical usefulness of rapid exome sequencing (rES) in critically ill children with likely genetic disease using a standardized process at a single institution. To provide evidence that rES with should become standard of care for this patient population.

Study Design: We implemented a process to provide clinical-grade rES to eligible children at a single institution. Eligibility included (a) recommendation of rES by a consulting geneticist, (b) monogenic disorder suspected, (c) rapid diagnosis predicted to affect inpatient management, (d) pretest counseling provided by an appropriate provider, and (e) unanimous approval by a committee of 4 geneticists. Trio exome sequencing was sent to a reference laboratory that provided verbal report within 7-10 days. Clinical outcomes related to rES were prospectively collected. Input from geneticists, genetic counselors, pathologists, neonatologists, and critical care pediatricians was collected to identify changes in management related to rES.

Results: There were 54 patients who were eligible for rES over a 34-month study period. Of these patients, 46 underwent rES, 24 of whom (52%) had at least 1 change in management related to rES. In 20 patients (43%), a molecular diagnosis was achieved, demonstrating that nondiagnostic exomes could change medical management in some cases. Overall, 84% of patients were under 1 month old at rES request and the mean turnaround time was 9 days.

Conclusions: rES testing has a significant impact on the management of critically ill children with suspected monogenic disease and should be considered standard of care for tertiary institutions who can provide coordinated genetics expertise.

Citing Articles

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3-hour genome sequencing and targeted analysis to rapidly assess genetic risk.

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Nguyen Y, Vu B, Nguyen D, Quach N, Bui L, Hong J Sci Rep. 2024; 14(1):21606.

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Role of next generation sequencing in diagnosis and management of critically ill children with suspected monogenic disorder.

Bhatia S, Pal S, Kulshrestha S, Gupta D, Soni A, Saxena R Eur J Hum Genet. 2024; 32(9):1106-1115.

PMID: 38605122 PMC: 11369102. DOI: 10.1038/s41431-024-01569-z.

Universal Exome Sequencing in Critically Ill Adults: A Diagnostic Yield of 25% and Race-Based Disparities in Access to Genetic Testing.

Gold J, Kripke C, Drivas T medRxiv. 2024; .

PMID: 38559092 PMC: 10980115. DOI: 10.1101/2024.03.11.24304088.

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