Feasibility of Ultra-Rapid Exome Sequencing in Critically Ill Infants and Children With Suspected Monogenic Conditions in the Australian Public Health Care System

Australian Genomics Health Alliance Acute Care Flagship; Sebastian Lunke; Stefanie Eggers; Meredith Wilson; Chirag Patel; Christopher Barnett; Jason Pinner; Sarah A. Sandaradura; Michael F. Buckley; Emma Krzesinski; M. De Silva; Gemma R. Brett; Kirsten Boggs; David Mowat; Edwin P. Kirk; Lesley C. Adès; Lauren Akesson; David J. Amor; Samantha Ayres; Anne Baxendale; Sarah C. Borrie; Alessandra Bray; Natasha J. Brown; Cheng Yee Chan; Belinda Chong; Corrina Cliffe; Martin B. Delatycki; Matthew Edwards; George Elakis; Michael Fahey; Andrew Fennell; Lindsay Fowles; Lyndon Gallacher; Megan Higgins; Katherine B. Howell; L. Hunt; Matthew F. Hunter; Kristi Jones; Sarah King; Smitha Kumble; Sarah Lang; Maelle Le Moing; Alan Ma; Dean Phelan; Michael C. Quinn; A. Mark Richards; Christopher M. Richmond; Jessica R. Riseley; Jonathan Rodgers; Rani Sachdev; Simon Sadedin; Luregn J. Schlapbach; Janine Smith; Amanda Springer; Natalie B. Tan; Tiong Yang Tan; Suzanna L. Temple; Christiane Theda; Anand Vasudevan; Susan M. White; Alison Yeung; Ying Zhu; Melissa Martyn; Stephanie Best; Tony Roscioli; John Christodoulou; Zornitza Stark

doi:10.1001/jama.2020.7671

Feasibility of Ultra-Rapid Exome Sequencing in Critically Ill Infants and Children With Suspected Monogenic Conditions in the Australian Public Health Care System

Australian Genomics Health Alliance Acute Care Flagship(The University of Melbourne), Sebastian Lunke(The University of Melbourne), Stefanie Eggers(The University of Sydney), Meredith Wilson(The University of Sydney), Chirag Patel(Royal Brisbane and Women's Hospital), Christopher Barnett(Women's and Children's Hospital), Jason Pinner(The University of Sydney), Sarah A. Sandaradura(The University of Sydney), Michael F. Buckley(New South Wales Department of Health), Emma Krzesinski(The University of Melbourne), M. De Silva(The University of Melbourne), Gemma R. Brett(The University of Melbourne), Kirsten Boggs(UNSW Sydney), David Mowat(New South Wales Department of Health), Edwin P. Kirk(The University of Sydney), Lesley C. Adès(The University of Sydney), Lauren Akesson(Royal Children's Hospital), David J. Amor(Royal Children's Hospital), Samantha Ayres(Women's and Children's Hospital), Anne Baxendale(Women's and Children's Hospital), Sarah C. Borrie(Women's and Children's Hospital), Alessandra Bray(The University of Melbourne), Natasha J. Brown(New South Wales Department of Health), Cheng Yee Chan(New South Wales Department of Health), Belinda Chong(New South Wales Department of Health), Corrina Cliffe(New South Wales Department of Health), Martin B. Delatycki(The University of Melbourne), Matthew Edwards(New South Wales Department of Health), George Elakis(New South Wales Department of Health), Michael Fahey(Monash Health), Andrew Fennell(Royal Brisbane and Women's Hospital), Lindsay Fowles(The University of Melbourne), Lyndon Gallacher(The University of Queensland), Megan Higgins(Royal Children's Hospital), Katherine B. Howell(Royal Children's Hospital), L. Hunt(The University of Queensland), Matthew F. Hunter(The University of Sydney), Kristi Jones(South Australia Pathology), Sarah King(South Australia Pathology), Smitha Kumble(New South Wales Department of Health), Sarah Lang(New South Wales Department of Health), Maelle Le Moing(The University of Sydney), Alan Ma(The University of Sydney), Dean Phelan(Royal Brisbane and Women's Hospital), Michael C. Quinn(New South Wales Department of Health), A. Mark Richards(New South Wales Department of Health), Christopher M. Richmond(Victorian Clinical Genetics Services), Jessica R. Riseley(Royal Brisbane and Women's Hospital), Jonathan Rodgers(Royal Brisbane and Women's Hospital), Rani Sachdev(Victorian Clinical Genetics Services), Simon Sadedin(The University of Queensland), Luregn J. Schlapbach(The University of Sydney), Janine Smith(The University of Sydney), Amanda Springer(Victorian Clinical Genetics Services), Natalie B. Tan(The University of Melbourne), Tiong Yang Tan(New South Wales Department of Health), Suzanna L. Temple(New South Wales Department of Health), Christiane Theda(Royal Women's Hospital), Anand Vasudevan(Royal Women's Hospital), Susan M. White(The University of Melbourne), Alison Yeung(New South Wales Department of Health), Ying Zhu(New South Wales Department of Health), Melissa Martyn(Murdoch Children's Research Institute), Stephanie Best(New South Wales Department of Health), Tony Roscioli(The University of Sydney), John Christodoulou(The University of Sydney), Zornitza Stark(The University of Melbourne)

JAMA

June 23, 2020

10.1001/jama.2020.7671

Cited by 234Open Access

Full Text

Abstract

Importance: Widespread adoption of rapid genomic testing in pediatric critical care requires robust clinical and laboratory pathways that provide equitable and consistent service across health care systems. Objective: To prospectively evaluate the performance of a multicenter network for ultra-rapid genomic diagnosis in a public health care system. Design, Setting, and Participants: Descriptive feasibility study of critically ill pediatric patients with suspected monogenic conditions treated at 12 Australian hospitals between March 2018 and February 2019, with data collected to May 2019. A formal implementation strategy emphasizing communication and feedback, standardized processes, coordination, distributed leadership, and collective learning was used to facilitate adoption. Exposures: Ultra-rapid exome sequencing. Main Outcomes and Measures: The primary outcome was time from sample receipt to ultra-rapid exome sequencing report. The secondary outcomes were the molecular diagnostic yield, the change in clinical management after the ultra-rapid exome sequencing report, the time from hospital admission to the laboratory report, and the proportion of laboratory reports returned prior to death or hospital discharge. Results: The study population included 108 patients with a median age of 28 days (range, 0 days to 17 years); 34% were female; and 57% were from neonatal intensive care units, 33% were from pediatric intensive care units, and 9% were from other hospital wards. The mean time from sample receipt to ultra-rapid exome sequencing report was 3.3 days (95% CI, 3.2-3.5 days) and the median time was 3 days (range, 2-7 days). The mean time from hospital admission to ultra-rapid exome sequencing report was 17.5 days (95% CI, 14.6-21.1 days) and 93 reports (86%) were issued prior to death or hospital discharge. A molecular diagnosis was established in 55 patients (51%). Eleven diagnoses (20%) resulted from using the following approaches to augment standard exome sequencing analysis: mitochondrial genome sequencing analysis, exome sequencing-based copy number analysis, use of international databases to identify novel gene-disease associations, and additional phenotyping and RNA analysis. In 42 of 55 patients (76%) with a molecular diagnosis and 6 of 53 patients (11%) without a molecular diagnosis, the ultra-rapid exome sequencing result was considered as having influenced clinical management. Targeted treatments were initiated in 12 patients (11%), treatment was redirected toward palliative care in 14 patients (13%), and surveillance for specific complications was initiated in 19 patients (18%). Conclusions and Relevance: This study suggests feasibility of ultra-rapid genomic testing in critically ill pediatric patients with suspected monogenic conditions in the Australian public health care system. However, further research is needed to understand the clinical value of such testing, and the generalizability of the findings to other health care settings.

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