Positioning whole exome sequencing in the diagnostic pathway for rare disease to optimise utility: a protocol for an observational cohort study and an economic evaluation

Robin Z Hayeems; Francois Bernier; Kym M Boycott; Taila Hartley; Christine Michaels-Igbokwe; Deborah A Marshall

doi:10.1136/bmjopen-2022-061468

Positioning whole exome sequencing in the diagnostic pathway for rare disease to optimise utility: a protocol for an observational cohort study and an economic evaluation

BMJ Open. 2022 Oct 10;12(10):e061468. doi: 10.1136/bmjopen-2022-061468.

Authors

Robin Z Hayeems^{1

2}, Francois Bernier^{3

4}, Kym M Boycott^{5

6}, Taila Hartley⁵, Christine Michaels-Igbokwe^{4

7}, Deborah A Marshall^{4

7}

Affiliations

¹ Child Health Evaluative Sciences, Hospital for Sick Children Research Institute, Toronto, Ontario, Canada robin.hayeems@sickkids.ca.
² Institute of Health Policy Management and Evaluation, University of Toronto, Toronto, Ontario, Canada.
³ Department of Medical Genetics, Alberta Children's Hospital, Calgary, Alberta, Canada.
⁴ Cummings School of Medicine, University of Calgary, Calgary, Alberta, Canada.
⁵ Department of Genetics, Children's Hospital of Eastern Ontario Research Institute, Ottawa, Ontario, Canada.
⁶ Department of Paediatrics, Facuty of Medicine, University of Ottawa, Ottawa, Ontario, Canada.
⁷ O'Brien Institute for Public Health, University of Calgary, Calgary, Alberta, Canada.

Abstract

Introduction: Despite the superior diagnostic performance of exome and genome sequencing compared with conventional genetic tests, evidence gaps related to clinical utility and cost effectiveness have limited their availability in routine clinical practice in many jurisdictions. To inform adoption and reimbursement policy, this protocol provides a chain of evidence approach to determining the diagnostic utility, clinical utility and cost-effectiveness of whole exome sequencing (WES) from seven medical genetic centres in two Canadian provinces.

Methods and analysis: Using a multicentre observational cohort design, we will extract data specific to the pre-WES diagnostic pathway and 1-year post-WES medical management from electronic medical records for 650 patients with rare disease of suspected genetic aetiology who receive WES. The date from the clinical record will be linked to provincial administrative health database to capture healthcare resource use and estimate costs. Our analysis will: (1) define and describe diagnostic testing pathways that occur prior to WES among patients with rare disease, (2) determine the diagnostic utility of WES, characterised as the proportion of patients for whom causative DNA variants are identified, (3) determine the clinical utility of WES, characterised as a change in medical management triggered by WES results, (4) determine the pattern and cost of health service utilisation prior and 1 year following WES among patients who receive a diagnosis, do not receive a diagnosis, or receive an uncertain diagnosis and (5) estimate the cost-effectiveness of WES compared with conventional diagnostic testing pathways, measured by the incremental cost per additional patient diagnosed by WES using simulation modelling.

Ethics and dissemination: This protocol was approved by Clinical Trials Ontario (CTO-1577) and research ethics boards at the University of Calgary (REB18-0744 and REB20-1449) and University of Alberta (Pro0009156). Findings will be disseminated through academic publications and policy reports.

Keywords: GENETICS; HEALTH ECONOMICS; Health policy.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Cohort Studies
Cost-Benefit Analysis
Exome Sequencing / methods
Genetic Testing* / methods
Humans
Observational Studies as Topic
Ontario
Rare Diseases* / diagnosis
Rare Diseases* / genetics