Preventing adverse events during paediatric cancer treatment: protocol for a multi-site hybrid randomised controlled trial of catheter lock solutions (the CLOCK trial)
Paul Monagle,
Andrew Wood,
Robert Ware,
Adam Irwin,
Joshua Byrnes,
Natalie Bradford,
Susan Moloney,
Michelle Martin,
Tricia Kleidon,
Andrew Moore,
Roni Cole,
Fiona Newall,
Victoria Gibson,
Samantha Keogh,
David Eisenstat,
Amanda Ullman,
Mari Takashima,
Elouise Comber,
Eloise Borello,
Nicole Henson,
Philippa Howard,
Karen McCleary,
Jordana McLean,
Michelle Noyes,
Gemma Rowan,
Amanda St John,
Joshua Wolf
Affiliations
Paul Monagle
16 Paediatrics, University of Melbourne, Parkville, Victoria, Australia
Andrew Wood
18 Starship Children`s Health, Auckland, Auckland, New Zealand
Robert Ware
20 Menzies Health Institute Queensland, Griffith University, Nathan, Queensland, Australia
Adam Irwin
7 University Of Queensland Centre for Clinical Research, Herston, Queensland, Australia
Joshua Byrnes
5 Centre for Applied Health Economics, Griffith University, Brisbane, Queensland, Australia
Natalie Bradford
4 Cancer and Palliative Care Outcomes Centre, Queensland University of Technology, South Brisbane, Queensland, Australia
Susan Moloney
15 Gold Coast University Hospital, Southport, Queensland, Australia
Michelle Martin
13 Monash Children`s Hospital, Clayton, New South Wales, Australia
Tricia Kleidon
11 Queensland Children`s Hospital, Queensland Health, South Brisbane, Queensland, Australia
Andrew Moore
2 Children`s Health Queensland Hospital and Health Service, South Brisbane, Queensland, Australia
Roni Cole
6 Sunshine Coast University Hospital, Sunshine Coast, Queensland, Australia
Fiona Newall
3 The Royal Children`s Hospital Melbourne, Melbourne, Victoria, Australia
Victoria Gibson
1 The University of Queensland, Brisbane, Queensland, Australia
Samantha Keogh
9 School of Nursing, Queensland University of Technology, Brisbane, Queensland, Australia
David Eisenstat
3 The Royal Children`s Hospital Melbourne, Melbourne, Victoria, Australia
Amanda Ullman
1 The University of Queensland, Brisbane, Queensland, Australia
Mari Takashima
1 The University of Queensland, Brisbane, Queensland, Australia
Elouise Comber
1 The University of Queensland, Brisbane, Queensland, Australia
Eloise Borello
3 The Royal Children`s Hospital Melbourne, Melbourne, Victoria, Australia
Nicole Henson
6 Sunshine Coast University Hospital, Sunshine Coast, Queensland, Australia
Philippa Howard
1 The University of Queensland, Brisbane, Queensland, Australia
Karen McCleary
14 Sydney Children`s Hospital Randwick, Randwick, New South Wales, Australia
Jordana McLean
6 Sunshine Coast University Hospital, Sunshine Coast, Queensland, Australia
Michelle Noyes
17 Gold Coast Hospital and Health Service, Southport, Queensland, Australia
Gemma Rowan
3 The Royal Children`s Hospital Melbourne, Melbourne, Victoria, Australia
Amanda St John
13 Monash Children`s Hospital, Clayton, New South Wales, Australia
Joshua Wolf
19 St Jude Children`s Research Hospital, Memphis, Tennessee, USA
Introduction Central venous access devices (CVADs) are commonly used for the treatment of paediatric cancer patients. Catheter locking is a routine intervention that prevents CVAD-associated adverse events, such as infection, occlusion and thrombosis. While laboratory and clinical data are promising, tetra-EDTA (T-EDTA) has yet to be rigorously evaluated or introduced in cancer care as a catheter lock.Methods and analysis This is a protocol for a two-arm, superiority type 1 hybrid effectiveness-implementation randomised controlled trial conducted at seven hospitals across Australia and New Zealand. Randomisation will be in a 3:2 ratio between the saline (heparinised saline and normal saline) and T-EDTA groups, with randomly varied blocks of size 10 or 20 and stratification by (1) healthcare facility; (2) CVAD type and (3) duration of dwell since insertion. Within the saline group, there will be a random allocation between normal and heparin saline. Participants can be re-recruited and randomised on insertion of a new CVAD. Primary outcome for effectiveness will be a composite of CVAD-associated bloodstream infections (CABSI), CVAD-associated thrombosis or CVAD occlusion during CVAD dwell or at removal. Secondary outcomes will include CABSI, CVAD-associated-thrombosis, CVAD failure, incidental asymptomatic CVAD-associated-thrombosis, other adverse events, health-related quality of life, healthcare costs and mortality. To achieve 90% power (alpha=0.05) for the primary outcome, data from 720 recruitments are required. A mixed-methods approach will be employed to explore implementation contexts from the perspective of clinicians and healthcare purchasers.Ethics and dissemination Ethics approval has been provided by Children’s Health Queensland Hospital and Health Service Human Research Ethics Committee (HREC) (HREC/22/QCHQ/81744) and the University of Queensland HREC (2022/HE000196) with subsequent governance approval at all sites. Informed consent is required from the substitute decision-maker or legal guardian prior to participation. In addition, consent may also be obtained from mature minors, depending on the legislative requirements of the study site. The primary trial and substudies will be written by the investigators and published in peer-reviewed journals. The findings will also be disseminated through local health and clinical trial networks by investigators and presented at conferences.Trial registration number ACTRN12622000499785.
