TY - JOUR
T1 - A Quality Improvement Intervention to Enhance Access to Kidney Transplantation and Living Kidney Donation (EnAKT LKD) in Patients With Chronic Kidney Disease
T2 - Clinical Research Protocol of a Cluster-Randomized Clinical Trial
AU - Yohanna, Seychelle
AU - Naylor, Kyla L.
AU - Mucsi, Istvan
AU - McKenzie, Susan
AU - Belenko, Dmitri
AU - Blake, Peter G.
AU - Coghlan, Candice
AU - Dixon, Stephanie N.
AU - Elliott, Lori
AU - Getchell, Leah
AU - Ki, Vincent
AU - Nesrallah, Gihad
AU - Patzer, Rachel E.
AU - Presseau, Justin
AU - Reich, Marian
AU - Sontrop, Jessica M.
AU - Treleaven, Darin
AU - Waterman, Amy D.
AU - Zaltzman, Jeffrey
AU - Garg, Amit X.
N1 - Funding Information:
The author(s) disclosed receipt of the following financial support for the research, authorship, and/or publication of this article: This trial is funded/sponsored by the ORN (part of Ontario Health) and the Canadian Institutes of Health Research (CIHR) SPOR Networks in Chronic Disease (Canadians Seeking Solutions and Innovations to Overcome Chronic Kidney Disease [Can-SOLVE CKD]). The Lawson Health Research Institute was a sponsor for this work. Partial funding to deliver the Explore Transplant Ontario educational program was provided by Astellas Pharma Canada Inc. A.X.G. is supported by the Dr. Adam Linton Chair in Kidney Health Analytics and is the joint ORN-TGLN Provincial Medical Lead for Access to Kidney Transplantation. He is also supported by a Clinician Investigator Award from the Canadian Institutes of Health Research.
Funding Information:
The authors thank Drs. Adeera Levin and Braden Manns for leading Canadians Seeking Solutions and Innovations to Overcome Chronic Kidney Disease (Can-SOLVE CKD), a patient-orientated research network to transform the care of people affected by kidney disease. They thank the Access to Kidney Transplantation and Living Donation Priority Panel and the ORN-TGLN Partnership Core Project Team. They thank the following individuals for their assistance with the development of the trial protocol and/or their support for this activity: Ahmed Al-Jaishi, Jeanette Chua, Rebecca Cooper, Sonia Eusebio, Charlotte Grieve, Jeremy Grimshaw, Andrew Hinson, Karen Hornby, Andrew House, Noah Ivers, Lisa Joya, Joseph Kim, Iris Lui, Eric McArthur, Megan McCallum, Beth Montesi, Jocelyn Pang, James Rodrigue, Dior Sarr, Colleen Shelton, Kaveh Shojania, Vanessa Simoes, Amanda Stypulkowski, and Irina Voronin. This study was supported by ICES, which is funded by an annual grant from the Ontario Ministry of Health and Long-Term Care (MOHLTC). The study was completed at the ICES Western site, where core funding is provided by the Academic Medical Organization of Southwestern Ontario, the Schulich School of Medicine and Dentistry, Western University, and the Lawson Health Research Institute. Parts of this material are based on data and/or information compiled and provided by Canadian Institute for Health Information (CIHI) and MOHLTC. The analyses, conclusions, opinions, and statements expressed herein are solely those of the authors and do not reflect those of the funding or data sources; no endorsement is intended or should be inferred. Parts of this material are based on data and information provided by Ontario Health (OH). The opinions, results, view, and conclusions reported in this paper are those of the authors and do not necessarily reflect those of OH. No endorsement by OH is intended or should be inferred. The author(s) acknowledge that the data used in this study were provided by the Trillium Gift of Life Network (Toronto, Ontario), which is funded by the Government of Ontario. The opinions, results, view, and conclusions reported in this paper are those of the authors and do not necessarily reflect those of TGLN. The authors thank IMS Brogan Inc. for use of their Drug Information Database. The research was conducted by members of the ICES Kidney, Dialysis and Transplantation team, at the ICES Western facility.
Publisher Copyright:
© The Author(s) 2021.
Copyright:
Copyright 2021 Elsevier B.V., All rights reserved.
© The Author(s) 2021.
PY - 2021
Y1 - 2021
N2 - Background: Many patients with kidney failure will live longer and healthier lives if they receive a kidney transplant rather than dialysis. However, multiple barriers prevent patients from accessing this treatment option. Objective: To determine if a quality improvement intervention provided in chronic kidney disease (CKD) programs (vs. usual care) enables more patients with no recorded contraindications to kidney transplant to complete more steps toward receiving a kidney transplant. Design: This protocol describes a pragmatic 2-arm, parallel-group, open-label, registry-based, cluster-randomized clinical trial—the Enhance Access to Kidney Transplantation and Living Kidney Donation (EnAKT LKD) trial. Setting: All 26 CKD programs in Ontario, Canada, with a trial start date of November 1, 2017. The original end date of March 31, 2021 (3.4 years) has been extended to December 31, 2021 (4.1 years) due to the COVID-19 pandemic. Participants: During the trial, the 26 CKD programs are expected to care for more than 10 000 adult patients with CKD (including patients approaching the need for dialysis and patients receiving dialysis) with no recorded contraindications to a kidney transplant. Intervention: Programs were randomly allocated to provide a quality improvement intervention or usual care. The intervention has 4 main components: (1) local quality improvement teams and administrative support; (2) tailored education and resources for staff, patients, and living kidney donor candidates; (3) support from kidney transplant recipients and living kidney donors; and (4) program-level performance reports and oversight by program leaders. Primary Outcome: The primary outcome is the number of key steps completed toward receiving a kidney transplant analyzed at the cluster level (CKD program). The following 4 unique steps per patient will be counted: (1) patient referred to a transplant center for evaluation, (2) at least one living kidney donor candidate contacts a transplant center for an intended recipient and completes a health history questionnaire to begin their evaluation, (3) patient added to the deceased donor transplant wait list, and (4) patient receives a kidney transplant from a living or deceased donor. Planned Primary Analysis: Study data will be obtained from Ontario’s linked administrative healthcare databases. An intent-to-treat analysis will be conducted comparing the primary outcome between randomized groups using a 2-stage approach. First stage: residuals are obtained from fitting a regression model to individual-level variables ignoring intervention and clustering effects. Second stage: residuals from the first stage are aggregated at the cluster level as the outcome. Limitations: It may not be possible to isolate independent effects of each intervention component, the usual care group could adopt intervention components leading to contamination bias, and the relatively small number of clusters could mean the 2 arms are not balanced on all baseline prognostic factors. Conclusions: The EnAKT LKD trial will provide high-quality evidence on whether a multi-component quality improvement intervention helps patients complete more steps toward receiving a kidney transplant. Trial registration: Clinicaltrials.gov; identifier: NCT03329521.
AB - Background: Many patients with kidney failure will live longer and healthier lives if they receive a kidney transplant rather than dialysis. However, multiple barriers prevent patients from accessing this treatment option. Objective: To determine if a quality improvement intervention provided in chronic kidney disease (CKD) programs (vs. usual care) enables more patients with no recorded contraindications to kidney transplant to complete more steps toward receiving a kidney transplant. Design: This protocol describes a pragmatic 2-arm, parallel-group, open-label, registry-based, cluster-randomized clinical trial—the Enhance Access to Kidney Transplantation and Living Kidney Donation (EnAKT LKD) trial. Setting: All 26 CKD programs in Ontario, Canada, with a trial start date of November 1, 2017. The original end date of March 31, 2021 (3.4 years) has been extended to December 31, 2021 (4.1 years) due to the COVID-19 pandemic. Participants: During the trial, the 26 CKD programs are expected to care for more than 10 000 adult patients with CKD (including patients approaching the need for dialysis and patients receiving dialysis) with no recorded contraindications to a kidney transplant. Intervention: Programs were randomly allocated to provide a quality improvement intervention or usual care. The intervention has 4 main components: (1) local quality improvement teams and administrative support; (2) tailored education and resources for staff, patients, and living kidney donor candidates; (3) support from kidney transplant recipients and living kidney donors; and (4) program-level performance reports and oversight by program leaders. Primary Outcome: The primary outcome is the number of key steps completed toward receiving a kidney transplant analyzed at the cluster level (CKD program). The following 4 unique steps per patient will be counted: (1) patient referred to a transplant center for evaluation, (2) at least one living kidney donor candidate contacts a transplant center for an intended recipient and completes a health history questionnaire to begin their evaluation, (3) patient added to the deceased donor transplant wait list, and (4) patient receives a kidney transplant from a living or deceased donor. Planned Primary Analysis: Study data will be obtained from Ontario’s linked administrative healthcare databases. An intent-to-treat analysis will be conducted comparing the primary outcome between randomized groups using a 2-stage approach. First stage: residuals are obtained from fitting a regression model to individual-level variables ignoring intervention and clustering effects. Second stage: residuals from the first stage are aggregated at the cluster level as the outcome. Limitations: It may not be possible to isolate independent effects of each intervention component, the usual care group could adopt intervention components leading to contamination bias, and the relatively small number of clusters could mean the 2 arms are not balanced on all baseline prognostic factors. Conclusions: The EnAKT LKD trial will provide high-quality evidence on whether a multi-component quality improvement intervention helps patients complete more steps toward receiving a kidney transplant. Trial registration: Clinicaltrials.gov; identifier: NCT03329521.
KW - cluster-randomized clinical trial
KW - kidney transplant
KW - living kidney donation
KW - protocol
KW - quality improvement intervention
UR - http://www.scopus.com/inward/record.url?scp=85104543675&partnerID=8YFLogxK
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U2 - 10.1177/2054358121997266
DO - 10.1177/2054358121997266
M3 - Article
C2 - 33948191
AN - SCOPUS:85104543675
SN - 2054-3581
VL - 8
SP - 2054358121997266
JO - Canadian Journal of Kidney Health and Disease
JF - Canadian Journal of Kidney Health and Disease
ER -