Systemic Lupus Erythematosus Clinical Trial
Official title:
Hydroxychloroquine Exposure in Systemic Lupus Erythematosus (SLE)
A Systemic lupus erythematosus, SLE is disease in which immune system is over-active causing inflammation in joints skin or any organ system. There are many areas where better approaches in SLE could improve outcomes. One example relates to hydroxychloroquine (HCQ) key drug which can reduce risk of serious disease flares. There are increasing concerns about eye damage main side effect with long-term use of HCQ. At present investigators cannot precisely predict which SLE patient is most likely to flare once HCQ is tapered. It is not clear what drives risk of eye damage. Investigators' study will fill these knowledge gaps. Investigators' hypothesis is that baseline demographic and clinical factors are associated with risk of SLE flare after HCQ taper/discontinuation and with risk of retinal toxicity in all HCQ exposed patients. Research will link and analyze data on 3700 SLE patients across Canada.
B OBJECTIVES B1 To evaluate in SLE patients who lower but do not discontinue HCQ factors
associated with flare (significant increase in disease activity, augmentation of therapy or
hospitalization for SLE).
B2 To determine in SLE patients who discontinue HCQ factors associated with flare
(significant increase in disease activity, therapy augmentation or hospitalization for SLE).
B3 To evaluate temporal relationship between HCQ use and retinal toxicity in SLE patients and
how this may be associated with demographic and clinical factors.
B4 To assess SLE patient preferences for HCQ therapy and how preferences are associated with
demographic and clinical factors.
B5 To evaluate temporal relationship between antimalarial use and other forms of toxicity in
SLE patients and how this may be associated with demographic and clinical factors.
Team members have prospectively followed cohorts > 3700 adult SLE patients (90% HCQ exposed)
with collected and harmonized data on demographics and clinical factors. Team members
(Bernatsky Abrahamowicz Fortin Hazlewood) are founding members of CAN-AIM CIHR-funded Drug
Safety and Effectiveness Network team.
Members have history of working with patients as research partners (Bartlett Li Bernatsky
Fortin Hazlewood). Investigators' ties to stakeholders including patient research partners
and Lupus Canada facilitates knowledge translation.
METHODS C1 Cohorts: Investigators will use existing data on adult SLE patients enrolled into
study cohorts in Montreal Quebec Halifax Winnipeg Calgary and Toronto.
Investigators are members of national (Canadian Network for Improved Outcomes in SLE CaNIOS)
and/or international (Systemic Lupus International Collaborating Clinics SLICC) research
networks. CaNIOS and SLICC have worked decades on harmonized approach to
prospectively-collected. Cohorts enroll unselected patients when they present to clinic. At
annual assessments data are collected on drugs disease activity organ damage etc C2.1 Patient
selection for Objective 1: At baseline and follow up visits records are made of patient HCQ
doses. Starting with first visit with HCQ exposure investigators will determine how many
patients are recorded as receiving lower dose or discontinuing HCQ at follow-up visit.
Patients identified as having lowered HCQ dose will form sub-cohort for time-to-event
(survival) analyses. Investigators will evaluate only first-ever lowering of HCQ. Analysis
will evaluate patients from time zero (annual visit at which lower HCQ dose was recorded) to
assess combined outcome of earliest of a) increase in SLEDAI-2K of at least 4 points and/or
b) hospitalization for SLE and/or c) augmented SLE therapy defined as increase in HCQ or new
start or increase in corticosteroids or other immunosuppressant. In addition to accepted
minimal clinically significant SLEDAI-2K change investigators include drug changes and
SLE-related hospitalizations.
Patients studied in Objective 1 will be right censored if HCQ is discontinued completely;
these will enter into analyses for Objective 2. Otherwise patients will be followed until
outcome of interest or end of study.
C2.3 Subject selection for Objective 2 Analyses will be similarly conducted but time zero
will begin when individual discontinues HCQ. Objective 1 and 2 analyses conducted separately;
patients who have HCQ dose lowered but then discontinued will be in analyses for Objective 1
up to point of discontinuation then patients will be right censored for Objective 1. Subjects
are able to contribute data (from the point of HCQ discontinuation) to analyses for Objective
2. Patient can contribute to analyses for one or both objectives and contributing to
Objective 3. If not right-censored patients will be followed until outcome of interest or end
of study.
C2.3 Subject selection for Objective 3 Outcome is retinal toxicity assessed in HCQ-exposed
patients from time of first visit with HCQ exposure up to time of retinal toxicity
documentation or end of study for patients without outcome. Exposure to CQ (relatively
uncommon drug exposure) is also risk factor for retinal toxicity but essentially patients
exposed to CQ will have prior exposure to HCQ.
C3 Demographic and clinical factors C3.1 Variables assessed include sex age at SLE onset and
race/ethnicity. Analyses adjusted for education as education can alter adherence.
C3.2 Clinical factors for multivariable analyses include smoking BMI baseline disease
activity malignancy data and renal damage. Baseline refers to time zero. Renal damage is
captured with SLICC Damage Index measuring accumulated damage. Baseline disease activity
measured by internationally used SLEDAI-2K reliable validated widely used global score
index.Investigators will model time-varying drug exposures with step-up approach initially
with baseline use ie current, recent, ever or total past dose. Investigators use
sophisticated and novel weighted cumulative dose modelling to flexibly represent exposures
accumulated by individual subjects up to given time-point corresponding to each risk set for
time-to-event analyses. In multivariable analyses approach will allow investigators to
explore how risk of retinal toxicity may depend on details of past HCQ exposure including not
only total cumulative dose but temporal pattern of doses at various time in past with
differential weights for early versus later exposures.
C4 Outcome assessment: SLEDAI-2K and drugs are recorded. SLICC Damage Index has item for
retinal damage and updated yearly.
C5 Model development: Investigators will perform multivariable time-to-event analyses in
patients who lower or discontinue HCQ. Data for outcomes are available longitudinally at
annual visit with actual dates only available for addition/increase in corticosteroid or SLE
hospitalization. For other outcomes investigators will deal with interval-censored data
familiar issue in pharmacoepidemiology.
Models include baseline demographics education BMI SLE duration SLEDAI-2K renal damage and
medications. Simplistic survival analyses often assume linear effects of continuous
covariates and impose conventional proportional hazards (PH) assumptions; investigators know
that prognostic factors may have time-dependent and/or nonlinear effects that violate
assumptions. Investigators will account for this. Methods account for possible changes in
hazard ratio over time (violation of the PH) and allow estimation of relative risks (hazard
ratios) and actual probabilities of event of interest occurring.
Similar approach will be used for Objective 3 in time-to-event analyses of retinal toxicity
in patients exposed to HCQ.
Competing risks occur when subjects can experience one or more events that may compete with
outcome of interest and hinder observation of event of interest or modify chances for event
to occur. In sensitivity analyses investigators use competing risks models to simultaneously
estimate associations between HCQ exposures and hazards of competing event.
D POWER/SAMPLE CALCULATIONS D1 Power calculations for multivariate models Combined cohorts
include over 3300 patients have exposed to HCQ. Patients have had lowering of dose 45% or
discontinuation of HCQ during their follow-up. Power calculations are based on available data
suggesting that 45%-60% of SLE patients may flare over ten years of follow-up.
For baseline SLEDAI-2K assuming 35% of patients score less than 3 investigators would have
90% power to detect unadjusted HR of 1.30 and adjusted HR of 1.37 for variable. Assuming 20%
of patients have renal damage investigators will have 90% power to detect an unadjusted HR of
1.37 and an adjusted HR of 1.45 for variable.
E KNOWLEDGE TRANSLATION activities are informed by history of partnerships between
investigators and knowledge-users directed by Dr. Linda Li Canada Research Chair in
Patient-Oriented KT and Director of Knowledge Translation Research Program at UBC's Arthritis
Research Centre of Canada.
E1 Integrated KT Proposal developed in consultation patients from Lupus Canada patients
Canadian Alliance of Patients with Arthritis (CAPA) and Singer Family Fund for Lupus
Research. Wendy Singer (providing expertise health information dissemination and provides
insight of SLE patient who has been affected by HCQ-induced retinal toxicity) will assist
with educational tool developments. Co-PI Dr. Bartlett has over decade of work with patient
partners through OMERACT (Outcome Measures in Rheumatology) and other organizations to help
disseminate findings patient communities.
E2 Dissemination via MyLupusGuide: Data on HCQ from current study will be incorporated into
MyLupusGuide web-based patient-centred health-management tool developed by Dr. Fortin in
partnership with Jack Digital Productions CaNIOS Lupus Canada. Development
validation/dissemination of current version funded by CIHR operating and dissemination
grants.
E3 Clinicians and professional groups: Dr. Bernatsky is member of CRA Therapeutics Committee
which advises CRA on policies related to drug use for rheumatic diseases. Group monitors
information about adverse events related to drugs used in rheumatology including HCQ.
Investigators submit abstracts to scientific meetings (American College of Rheumatology,
European League Against Rheumatism, CRA meeting). Investigators will seek feedback on
feasibility/approaches to integrate MyLupusGuide as gold standard for patient education tool
concerning HCQ.
E4 Informing future guidelines: Team member Dr. S. Keeling has already produced Canadian SLE
care guidelines (funded by the CIHR and endorsed by the CRA and CaNIOS) . In 2019, again
mandated by these groups, Dr. Keeling will spearhead guidelines for SLE therapies.
E5 Health agency stakeholders: Investigators have connections Drug Safety and Effectiveness
Network (DSEN) Health Canada's Marketed Health Product Directorate and Canadian Agency for
Drugs and Technologies in Health (CADTH). Drs. Abrahamowicz and Bernatsky are co-leads
DSEN-funded team.
;
Status | Clinical Trial | Phase | |
---|---|---|---|
Terminated |
NCT03843125 -
A Study of Baricitinib in Participants With Systemic Lupus Erythematosus (SLE)
|
Phase 3 | |
Recruiting |
NCT05698173 -
Systemic Lupus Erythematosus and Accelerated Aging
|
N/A | |
Active, not recruiting |
NCT01649765 -
Pediatric Lupus Trial of Belimumab Plus Background Standard Therapy
|
Phase 2 | |
Recruiting |
NCT05704153 -
Modelling and Control of Non-invasive Vagus Nerve Stimulation for Autoimmune Diseases (1A)
|
N/A | |
Completed |
NCT05048238 -
Evaluation of Tofacitinib in Prevention of Photosensitivity in Lupus
|
Phase 1 | |
Recruiting |
NCT06056778 -
The Prevalence Evaluation of Systemic Lupus Erythematosus in Russian Patients With Reproductive Issues (PRISMA)
|
||
Completed |
NCT04358302 -
Individual Patient Exposure and Response in Pediatric Lupus
|
N/A | |
Completed |
NCT03802578 -
The Impact of Exercise on Hand Function, Daily Activities Performance and Quality of Life of SLE' Patients
|
N/A | |
Completed |
NCT02554019 -
Proof-of-Concept Study With BT063 in Subjects With Systemic Lupus Erythematosus
|
Phase 2 | |
Recruiting |
NCT04835883 -
Exploring the Efficacy and Safety of CS20AT04 (Allogenic Bone Marrow-Derived Stem Cell) in Systemic Lupus Erythematosus Patients
|
Phase 2 | |
Terminated |
NCT02665364 -
Phase IIb Study of IFN-K in Systemic Lupus Erythematosus
|
Phase 2 | |
Completed |
NCT00278538 -
Cyclophosphamide and Rabbit Antithymocyte Globulin (rATG)/Rituximab in Patients With Systemic Lupus Erythematosus
|
Phase 2 | |
Completed |
NCT00069342 -
Health Beliefs and Health Behaviors Among Minorities With Rheumatic Diseases
|
||
Completed |
NCT03252587 -
An Investigational Study to Evaluate BMS-986165 in Participants With Systemic Lupus Erythematosus
|
Phase 2 | |
Terminated |
NCT02066311 -
Nelfinavir in Systemic Lupus Erythematosus
|
Phase 2 | |
Recruiting |
NCT01892748 -
Cholecalciferol Supplementation on Disease Activity, Fatigue and Bone Mass on Juvenile Systemic Lupus Erythematosus.
|
N/A | |
Terminated |
NCT01689025 -
An Investigation of Safety and Tolerability of NNC0114-0006 in Subjects With Systemic Lupus Erythematosus (SLE)
|
Phase 1 | |
Unknown status |
NCT01712529 -
Physical Exercise, Endothelial Function and Progenitor Endothelial Cells in Systemic Lupus Erythematosus Patients
|
N/A | |
Completed |
NCT01475149 -
Effect of HCQ on AnxA5 Resistance Assay in Antiphospholipid (aPL) Positive Patients With and Without Systemic Lupus Erythematosus (SLE)
|
N/A | |
Completed |
NCT00962832 -
A Study to Evaluate the Efficacy and Safety of Rontalizumab in Patients With Moderately to Severely Active Systemic Lupus Erythematosus
|
Phase 2 |