Design and Rationale of HiLo: A Pragmatic, Randomized Trial of Phosphate Management for Patients Receiving Maintenance Hemodialysis

Daniel L. Edmonston; Tamara Isakova; Laura M. Dember; Steven Brunelli; Amy Young; Rebecca Brosch; Srinivasan Beddhu; Hrishikesh Chakraborty; Myles Wolf

doi:10.1053/j.ajkd.2020.10.008

Design and Rationale of HiLo: A Pragmatic, Randomized Trial of Phosphate Management for Patients Receiving Maintenance Hemodialysis

Daniel L. Edmonston, Tamara Isakova, Laura M. Dember, Steven Brunelli, Amy Young, Rebecca Brosch, Srinivasan Beddhu, Hrishikesh Chakraborty, Myles Wolf^*

^*Corresponding author for this work

Medicine, Nephrology Division

Research output: Contribution to journal › Article › peer-review

14 Scopus citations

Abstract

Rationale & Objective: Hyperphosphatemia is a risk factor for poor clinical outcomes in patients with kidney failure receiving maintenance dialysis. Opinion-based clinical practice guidelines recommend the use of phosphate binders and dietary phosphate restriction to lower serum phosphate levels toward the normal range in patients receiving maintenance dialysis, but the benefits of these approaches and the optimal serum phosphate target have not been tested in randomized trials. It is also unknown if aggressive treatment that achieves unnecessarily low serum phosphate levels worsens outcomes. Study Design: Multicenter, pragmatic, cluster-randomized clinical trial. Setting & Participants: HiLo will randomize 80-120 dialysis facilities operated by DaVita Inc and the University of Utah to enroll 4,400 patients undergoing 3-times-weekly, in-center hemodialysis. Intervention: Phosphate binder prescriptions and dietary recommendations to achieve the “Hi” serum phosphate target (≥6.5 mg/dL) or the “Lo” serum phosphate target (<5.5 mg/dL). Outcomes: Primary outcome: Hierarchical composite outcome of all-cause mortality and all-cause hospitalization. Main secondary outcomes: Individual components of the primary outcome. Results: The trial is currently enrolling. Limitations: HiLo will not adjudicate causes of hospitalizations or mortality and does not protocolize use of specific phosphate binder classes. Conclusions: HiLo aims to address an important clinical question while more generally advancing methods for pragmatic clinical trials in nephrology by introducing multiple innovative features including stakeholder engagement in the study design, liberal eligibility criteria, use of electronic informed consent, engagement of dietitians to implement the interventions in real-world practice, leveraging electronic health records to eliminate dedicated study visits, remote monitoring of serum phosphate separation between trial arms, and use of a novel hierarchical composite outcome. Trial Registration: Registered at ClinicalTrials.gov with study number NCT04095039.

Original language	English (US)
Pages (from-to)	920-930.e1
Journal	American Journal of Kidney Diseases
Volume	77
Issue number	6
DOIs	https://doi.org/10.1053/j.ajkd.2020.10.008
State	Published - Jun 2021

Keywords

End-stage kidney disease (ESKD)
cluster-randomized trial
dialysis clinics
hemodialysis
hierarchical composite outcome
hospitalization
hyperphosphatemia
mortality
pragmatic clinical trial
serum phosphate
study design

ASJC Scopus subject areas

Nephrology

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10.1053/j.ajkd.2020.10.008

Cite this

@article{7b4c30c16de24f74a3ae70376ac08b65,

title = "Design and Rationale of HiLo: A Pragmatic, Randomized Trial of Phosphate Management for Patients Receiving Maintenance Hemodialysis",

abstract = "Rationale & Objective: Hyperphosphatemia is a risk factor for poor clinical outcomes in patients with kidney failure receiving maintenance dialysis. Opinion-based clinical practice guidelines recommend the use of phosphate binders and dietary phosphate restriction to lower serum phosphate levels toward the normal range in patients receiving maintenance dialysis, but the benefits of these approaches and the optimal serum phosphate target have not been tested in randomized trials. It is also unknown if aggressive treatment that achieves unnecessarily low serum phosphate levels worsens outcomes. Study Design: Multicenter, pragmatic, cluster-randomized clinical trial. Setting & Participants: HiLo will randomize 80-120 dialysis facilities operated by DaVita Inc and the University of Utah to enroll 4,400 patients undergoing 3-times-weekly, in-center hemodialysis. Intervention: Phosphate binder prescriptions and dietary recommendations to achieve the “Hi” serum phosphate target (≥6.5 mg/dL) or the “Lo” serum phosphate target (<5.5 mg/dL). Outcomes: Primary outcome: Hierarchical composite outcome of all-cause mortality and all-cause hospitalization. Main secondary outcomes: Individual components of the primary outcome. Results: The trial is currently enrolling. Limitations: HiLo will not adjudicate causes of hospitalizations or mortality and does not protocolize use of specific phosphate binder classes. Conclusions: HiLo aims to address an important clinical question while more generally advancing methods for pragmatic clinical trials in nephrology by introducing multiple innovative features including stakeholder engagement in the study design, liberal eligibility criteria, use of electronic informed consent, engagement of dietitians to implement the interventions in real-world practice, leveraging electronic health records to eliminate dedicated study visits, remote monitoring of serum phosphate separation between trial arms, and use of a novel hierarchical composite outcome. Trial Registration: Registered at ClinicalTrials.gov with study number NCT04095039.",

keywords = "End-stage kidney disease (ESKD), cluster-randomized trial, dialysis clinics, hemodialysis, hierarchical composite outcome, hospitalization, hyperphosphatemia, mortality, pragmatic clinical trial, serum phosphate, study design",

author = "Edmonston, {Daniel L.} and Tamara Isakova and Dember, {Laura M.} and Steven Brunelli and Amy Young and Rebecca Brosch and Srinivasan Beddhu and Hrishikesh Chakraborty and Myles Wolf",

note = "Funding Information: Research reported in this publication was supported by cooperative agreement UG3/UH3DK118748 from the National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK). This work also received logistical and technical support from the National Institute of Health (NIH) Collaboratory Coordinating Center through cooperative agreement U24AT009676 with cofunding by NIDDK. Representatives from the funding agency contributed to the design of this study. Funding Information: Daniel L. Edmonston, MD, Tamara Isakova, MD, MMSc, Laura M. Dember, MD, Steven Brunelli, MD, Amy Young, PhD, Rebecca Brosch, RD, Srinivasan Beddhu, MD, Hrishikesh Chakraborty, DrPH, and Myles Wolf, MD, MMSc. Research idea and study design: MW, TI, DLE, LMD, SBrunelli, AY, RB, SBeddhu, HC, DLE; statistical analysis: HC; supervision or mentorship: TI, MW. Each author contributed important intellectual content during manuscript drafting or revision and agrees to be personally accountable for the individual's own contributions and to ensure that questions pertaining to the accuracy or integrity of any portion of the work, even one in which the author was not directly involved, are appropriately investigated and resolved, including with documentation in the literature if appropriate. Research reported in this publication was supported by cooperative agreement UG3/UH3DK118748 from the National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK). This work also received logistical and technical support from the National Institute of Health (NIH) Collaboratory Coordinating Center through cooperative agreement U24AT009676 with cofunding by NIDDK. Representatives from the funding agency contributed to the design of this study. Dr Wolf reports honoraria from Akebia and Ardelyx. The remaining authors declare that they have no relevant financial interests. The Duke Clinical Research Institute is home to the Data Coordinating Center of HiLo. The HiLo Steering Committee includes all authors of this report. Additional members of the HiLo team at the Duke Clinical Research Institute include Laura Johnson, Davy Andersen, MHA, and Yashika Johnson, MS (Clinical Operations); Andrew MacKelfresh, MBA, and James Topping (Informatics); and Peter Merrill, PhD (Biostatistics). We thank the leadership of the American Association of Kidney Patients, including Richard Knight, MBA, President, and Diana Clynes, Executive Director, for their support for HiLo and for convening the members of the HiLo Patient Advisory Group: Malie Robb (deceased), Scott Burton, and Dale Rogers. The content is solely the responsibility of the authors and does not necessarily represent the official views of the NIH. Received May 12, 2020. Evaluated by 3 external peer reviewers, with editorial input from a Statistics/Methods Editor and an Acting Editor-in-Chief (Editorial Board Member Chirag R. Parikh, MD, PhD). Accepted in revised form October 1, 2020. The involvement of an Acting Editor-in-Chief to handle the peer-review and decision-making processes was to comply with AJKD's procedures for potential conflicts of interest for editors, described in the Information for Authors & Journal Policies. Publisher Copyright: {\textcopyright} 2020 The Authors",

year = "2021",

month = jun,

doi = "10.1053/j.ajkd.2020.10.008",

language = "English (US)",

volume = "77",

pages = "920--930.e1",

journal = "American Journal of Kidney Diseases",

issn = "0272-6386",

publisher = "W.B. Saunders Ltd",

number = "6",

}

TY - JOUR

T1 - Design and Rationale of HiLo

T2 - A Pragmatic, Randomized Trial of Phosphate Management for Patients Receiving Maintenance Hemodialysis

AU - Edmonston, Daniel L.

AU - Isakova, Tamara

AU - Dember, Laura M.

AU - Brunelli, Steven

AU - Young, Amy

AU - Brosch, Rebecca

AU - Beddhu, Srinivasan

AU - Chakraborty, Hrishikesh

AU - Wolf, Myles

N1 - Funding Information: Research reported in this publication was supported by cooperative agreement UG3/UH3DK118748 from the National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK). This work also received logistical and technical support from the National Institute of Health (NIH) Collaboratory Coordinating Center through cooperative agreement U24AT009676 with cofunding by NIDDK. Representatives from the funding agency contributed to the design of this study. Funding Information: Daniel L. Edmonston, MD, Tamara Isakova, MD, MMSc, Laura M. Dember, MD, Steven Brunelli, MD, Amy Young, PhD, Rebecca Brosch, RD, Srinivasan Beddhu, MD, Hrishikesh Chakraborty, DrPH, and Myles Wolf, MD, MMSc. Research idea and study design: MW, TI, DLE, LMD, SBrunelli, AY, RB, SBeddhu, HC, DLE; statistical analysis: HC; supervision or mentorship: TI, MW. Each author contributed important intellectual content during manuscript drafting or revision and agrees to be personally accountable for the individual's own contributions and to ensure that questions pertaining to the accuracy or integrity of any portion of the work, even one in which the author was not directly involved, are appropriately investigated and resolved, including with documentation in the literature if appropriate. Research reported in this publication was supported by cooperative agreement UG3/UH3DK118748 from the National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK). This work also received logistical and technical support from the National Institute of Health (NIH) Collaboratory Coordinating Center through cooperative agreement U24AT009676 with cofunding by NIDDK. Representatives from the funding agency contributed to the design of this study. Dr Wolf reports honoraria from Akebia and Ardelyx. The remaining authors declare that they have no relevant financial interests. The Duke Clinical Research Institute is home to the Data Coordinating Center of HiLo. The HiLo Steering Committee includes all authors of this report. Additional members of the HiLo team at the Duke Clinical Research Institute include Laura Johnson, Davy Andersen, MHA, and Yashika Johnson, MS (Clinical Operations); Andrew MacKelfresh, MBA, and James Topping (Informatics); and Peter Merrill, PhD (Biostatistics). We thank the leadership of the American Association of Kidney Patients, including Richard Knight, MBA, President, and Diana Clynes, Executive Director, for their support for HiLo and for convening the members of the HiLo Patient Advisory Group: Malie Robb (deceased), Scott Burton, and Dale Rogers. The content is solely the responsibility of the authors and does not necessarily represent the official views of the NIH. Received May 12, 2020. Evaluated by 3 external peer reviewers, with editorial input from a Statistics/Methods Editor and an Acting Editor-in-Chief (Editorial Board Member Chirag R. Parikh, MD, PhD). Accepted in revised form October 1, 2020. The involvement of an Acting Editor-in-Chief to handle the peer-review and decision-making processes was to comply with AJKD's procedures for potential conflicts of interest for editors, described in the Information for Authors & Journal Policies. Publisher Copyright: © 2020 The Authors

PY - 2021/6

Y1 - 2021/6

N2 - Rationale & Objective: Hyperphosphatemia is a risk factor for poor clinical outcomes in patients with kidney failure receiving maintenance dialysis. Opinion-based clinical practice guidelines recommend the use of phosphate binders and dietary phosphate restriction to lower serum phosphate levels toward the normal range in patients receiving maintenance dialysis, but the benefits of these approaches and the optimal serum phosphate target have not been tested in randomized trials. It is also unknown if aggressive treatment that achieves unnecessarily low serum phosphate levels worsens outcomes. Study Design: Multicenter, pragmatic, cluster-randomized clinical trial. Setting & Participants: HiLo will randomize 80-120 dialysis facilities operated by DaVita Inc and the University of Utah to enroll 4,400 patients undergoing 3-times-weekly, in-center hemodialysis. Intervention: Phosphate binder prescriptions and dietary recommendations to achieve the “Hi” serum phosphate target (≥6.5 mg/dL) or the “Lo” serum phosphate target (<5.5 mg/dL). Outcomes: Primary outcome: Hierarchical composite outcome of all-cause mortality and all-cause hospitalization. Main secondary outcomes: Individual components of the primary outcome. Results: The trial is currently enrolling. Limitations: HiLo will not adjudicate causes of hospitalizations or mortality and does not protocolize use of specific phosphate binder classes. Conclusions: HiLo aims to address an important clinical question while more generally advancing methods for pragmatic clinical trials in nephrology by introducing multiple innovative features including stakeholder engagement in the study design, liberal eligibility criteria, use of electronic informed consent, engagement of dietitians to implement the interventions in real-world practice, leveraging electronic health records to eliminate dedicated study visits, remote monitoring of serum phosphate separation between trial arms, and use of a novel hierarchical composite outcome. Trial Registration: Registered at ClinicalTrials.gov with study number NCT04095039.

AB - Rationale & Objective: Hyperphosphatemia is a risk factor for poor clinical outcomes in patients with kidney failure receiving maintenance dialysis. Opinion-based clinical practice guidelines recommend the use of phosphate binders and dietary phosphate restriction to lower serum phosphate levels toward the normal range in patients receiving maintenance dialysis, but the benefits of these approaches and the optimal serum phosphate target have not been tested in randomized trials. It is also unknown if aggressive treatment that achieves unnecessarily low serum phosphate levels worsens outcomes. Study Design: Multicenter, pragmatic, cluster-randomized clinical trial. Setting & Participants: HiLo will randomize 80-120 dialysis facilities operated by DaVita Inc and the University of Utah to enroll 4,400 patients undergoing 3-times-weekly, in-center hemodialysis. Intervention: Phosphate binder prescriptions and dietary recommendations to achieve the “Hi” serum phosphate target (≥6.5 mg/dL) or the “Lo” serum phosphate target (<5.5 mg/dL). Outcomes: Primary outcome: Hierarchical composite outcome of all-cause mortality and all-cause hospitalization. Main secondary outcomes: Individual components of the primary outcome. Results: The trial is currently enrolling. Limitations: HiLo will not adjudicate causes of hospitalizations or mortality and does not protocolize use of specific phosphate binder classes. Conclusions: HiLo aims to address an important clinical question while more generally advancing methods for pragmatic clinical trials in nephrology by introducing multiple innovative features including stakeholder engagement in the study design, liberal eligibility criteria, use of electronic informed consent, engagement of dietitians to implement the interventions in real-world practice, leveraging electronic health records to eliminate dedicated study visits, remote monitoring of serum phosphate separation between trial arms, and use of a novel hierarchical composite outcome. Trial Registration: Registered at ClinicalTrials.gov with study number NCT04095039.

KW - End-stage kidney disease (ESKD)

KW - cluster-randomized trial

KW - dialysis clinics

KW - hemodialysis

KW - hierarchical composite outcome

KW - hospitalization

KW - hyperphosphatemia

KW - mortality

KW - pragmatic clinical trial

KW - serum phosphate

KW - study design

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U2 - 10.1053/j.ajkd.2020.10.008

DO - 10.1053/j.ajkd.2020.10.008

M3 - Article

C2 - 33279558

AN - SCOPUS:85099947502

SN - 0272-6386

VL - 77

SP - 920-930.e1

JO - American Journal of Kidney Diseases

JF - American Journal of Kidney Diseases

IS - 6

ER -

Design and Rationale of HiLo: A Pragmatic, Randomized Trial of Phosphate Management for Patients Receiving Maintenance Hemodialysis

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