BMJ Open (Jul 2024)

Same-visit hepatitis C testing and treatment to accelerate cure among people who inject drugs (the QuickStart Study): a cluster randomised cross-over trial protocol

  • Andrew B Forbes,
  • Jessica Kasza,
  • Thomas L Snelling,
  • David Anderson,
  • Joseph S Doyle,
  • Peter Higgs,
  • Margaret E Hellard,
  • Nick Scott,
  • Alisa E Pedrana,
  • Alexander J Thompson,
  • Jessica Howell,
  • Timothy Spelman,
  • Beatriz Camesella,
  • Imogen Elsum,
  • Kico Chan,
  • Mark A Stoové,
  • Paul M Dietze,
  • Mellissa Bryant,
  • Katherine Heath,
  • Rodney Guzman,
  • Caitlin Douglass,
  • Amanda Wade,
  • Kate Allardice,
  • Sally Von Bibra,
  • Jacqui Richmond,
  • Nada Andric,
  • Rachel Sacks‐Davis

DOI
https://doi.org/10.1136/bmjopen-2023-083502
Journal volume & issue
Vol. 14, no. 7

Abstract

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Introduction Despite universal access to government-funded direct-acting antivirals (DAAs) in 2016, the rate of hepatitis C treatment uptake in Australia has declined substantially. Most hepatitis C is related to injecting drug use; reducing the hepatitis C burden among people who inject drugs (PWID) is, therefore, paramount to reach hepatitis C elimination targets. Increasing DAA uptake by PWID is important for interrupting transmission and reducing incidence, as well as reducing morbidity and mortality and improving quality of life of PWID and meeting Australia’s hepatitis C elimination targets.Methods and analysis A cluster randomised cross-over trial will be conducted with three intervention arms and a control arm. Arm A will receive rapid hepatitis C virus (HCV) antibody testing; arm B will receive rapid HCV antibody and rapid RNA testing; arm C will receive rapid HCV antibody testing and same-day treatment initiation for HCV antibody-positive participants; the control arm will receive standard of care. The primary outcomes will be (a) the proportion of participants with HCV commencing treatment and (b) the proportion of participants with HCV achieving cure. Analyses will be conducted on an intention-to-treat basis with mixed-effects logistic regression models.Ethics and dissemination The study has been approved by the Alfred Ethics Committee (number HREC/64731/Alfred-2020-217547). Each participant will provide written informed consent. Reportable adverse events will be reported to the reviewing ethics committee. The findings will be presented at scientific conferences and published in peer-reviewed journals.Trial registration number NCT05016609.Trial progression The study commenced recruitment on 9 March 2022 and is expected to complete recruitment in December 2024.