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TREAT-MS: Traditional Versus Early Aggressive Therapy for Multiple Sclerosis Trial

Sponsor
Johns Hopkins University (Other)
Overall Status
Recruiting
CT.gov ID
NCT03500328
Collaborator
Patient-Centered Outcomes Research Institute (Other)
900
Enrollment
52
Locations
2
Arms
87
Anticipated Duration (Months)
17.3
Patients Per Site
0.2
Patients Per Site Per Month

Study Details

Study Description

Brief Summary

FDA-approved multiple sclerosis (MS) disease-modifying therapies (DMTs) target the relapsing phase of MS but have minimal impact once the progressive phase has begun. It is unclear if, in the relapsing phase, there is an advantage of early aggressive therapy with respect to preventing long-term disability. The infectious risks and other complications associated with higher-efficacy treatments highlight the need to quantify their effectiveness in preventing disability.

The TRaditional versus Early Aggressive Therapy for MS (TREAT-MS) trial is a pragmatic, randomized controlled trial that has two primary aims: 1) to evaluate, jointly and independently among patients deemed at higher risk vs. lower risk for disability accumulation, whether an "early aggressive" therapy approach, versus starting with a traditional, first-line therapy, influences the intermediate-term risk of disability, and 2) to evaluate if, among patients deemed at lower risk for disability who start on first-line MS therapies but experience breakthrough disease, those who switch to a higher-efficacy versus a new first-line therapy have different intermediate-term risk of disability.

Condition or Disease Intervention/Treatment Phase
  • Other: Early Aggressive Therapy or Traditional Therapy
 N/A

Detailed Description

FDA-approved multiple sclerosis (MS) disease-modifying therapies (DMTs) target the relapsing phase of MS but have minimal impact once the progressive phase has begun. It is unclear if, in the relapsing phase, there is an advantage of early aggressive therapy with respect to preventing long-term disability. The infectious risks and other complications associated with higher-efficacy treatments highlight the need to quantify their effectiveness in preventing disability.

The TRaditional versus Early Aggressive Therapy for MS (TREAT-MS) trial is a pragmatic, randomized controlled trial that has two primary aims: 1) to evaluate, jointly and independently among patients deemed at higher risk vs. lower risk for disability accumulation, whether an "early aggressive" therapy approach, versus starting with a traditional, first-line therapy, influences the intermediate-term risk of disability, and 2) to evaluate if, among patients deemed at lower risk for disability who start on first-line MS therapies but experience breakthrough disease, those who switch to a higher-efficacy versus a new first-line therapy have different intermediate-term risk of disability.

Hypotheses/Objectives: The main hypothesis is that intermediate-term disability will be reduced by earlier use of higher-efficacy medications. Additional objectives include a) evaluating the magnitude of the treatment effect in patients deemed to be at higher risk versus lower risk of longer-term disability (we hypothesize that the effect size will be greater in the former group) and b) evaluating if, among those without indications of a high risk of longer-term disability, breakthrough disease can be successfully managed by switching to a different first-line therapy or if escalation is required at that time (we hypothesize that switching to a higher-efficacy therapy will be more effective in preventing disability in this group).

There is a great unmet need to identify the most appropriate treatment strategy for people with MS, especially early in the disease course when it may be possible to maximize an individual's chance for preventing long-term disability. There is a paucity of evidence-based guidelines to help clinicians, patients, and payers determine which treatment strategy is best for an individual with MS. Making treatment decisions is a daunting task, and the individualized benefit-risk assessment becomes increasingly difficult as new therapies emerge. Without the availability of direct comparative trials, clinicians and patients are forced to scrutinize observational studies that only provide basic insights into what may be the best treatment path moving forward. It is equally challenging to define what constitutes a suboptimal response to a DMT for an individual patient. Clinicians lack guidance on when to switch therapies and whether to consider a different first-line or if clinicians should escalate immediately to higher-efficacy therapies, so further consensus is needed to determine the optimal time to switch therapies and escalate therapy if an individual is on a first-line therapy from the start. The TREAT-MS trial will help inform patients and the broader health care community on whether patients would most benefit from early, possibly more risky aggressive therapy or if starting with a less aggressive (and, often, less risky) therapy, followed by a switch if breakthrough disease occurs, is warranted. In addition, this study may help identify specific patient populations and/or short-term clinical and paraclinical biomarkers that are strongly predictive of long-term disability that can ensue from MS.

Accrual of sustained disability is the most feared complication for people with MS, and the patient's own perception of their well-being or ill-being has a profound impact on their quality of life. The heterogeneity and unpredictability of MS, along with lack of agreed upon treatment guidelines, augments this fear, leading to a significant negative impact on quality of life. Even patients who are deemed to have "mild" MS experience a significant negative impact on their health-related quality of life that is similar in magnitude to what patients with other severe chronic conditions (i.e., congestive heart failure and chronic obstructive pulmonary disease) report. An extremely important goal for any intervention is to help improve or maintain a high quality of life; therefore, in addition to classic clinical endpoints (e.g. slowing disability progression), the TREAT-MS trial will capture several important and meaningful PROs that will shed light on what treatment strategies may be the best from a patient-centered perspective.

COVID-19 Related Substudy:

Since early 2020, the coronavirus disease 2019 (COVID-19) pandemic has caused clinical care and research disruptions nationwide, including for patients enrolled in the TREAT-MS trial. Many patients with MS, as well as their clinicians, are fearful that MS or the MS therapy they are using may increase the risk or severity of COVID-19 infection. Whether a person with early MS is more likely to experience more severe COVID-19 if treated with a higher-efficacy therapy is not known. Further, whether COVID-19-induced disruptions in therapy or other clinical care increase MS disease activity or MS symptoms is not clear but is relevant, particularly since greater MS activity in the early therapeutic course is associated in observational studies with worse long-term outcomes. Moreover, it is unclear if pre-pandemic anxiety and depression, common comorbidities in people with MS, contribute to decisions to delay care, overall or differently depending on therapeutic strategy (higher-efficacy vs. traditional). TREAT-MS provides an optimal cohort in which to investigate the effect of the COVID-19 pandemic on MS outcomes.

COVID-19 Substudy Aim 1. To evaluate if patients enrolled in TREAT-MS delayed or altered their disease-modifying therapy schedule or other MS care, and whether such alterations are associated with a greater degree of breakthrough inflammatory disease activity or the development of new (or worsening baseline) MS symptoms.

COVID-19 Substudy Aim 2: To evaluate if patients with MS treated with higher-efficacy, versus traditional, therapies differ in the risk of severe COVID-19 infection, defined as requiring hospitalization (with or without intubation) or mortality due to COVID-19.

Study Design

Study Type:
Interventional
Anticipated Enrollment :
900 participants
Allocation:
Randomized
Intervention Model:
Parallel Assignment
Masking:
Single (Outcomes Assessor)
Primary Purpose:
Treatment
Official Title:
A Pragmatic Trial to Evaluate the Intermediate-term Effects of Early, Aggressive Versus Escalation Therapy in People With Multiple Sclerosis
Actual Study Start Date :
May 2, 2018
Anticipated Primary Completion Date :
Aug 1, 2025
Anticipated Study Completion Date :
Aug 1, 2025

Arms and Interventions

Arm Intervention/Treatment
Active Comparator: Early Aggressive Therapy

Higher efficacy disease-modifying therapy (Early Aggressive Therapy) for treatment of multiple sclerosis Early Aggressive Therapy choices and maximum allowable doses: Natalizumab (Tysabri), 300 mg intravenously (IV) every 4 weeks Alemtuzumab (Lemtrada), 12 mg IV daily for 5 days; 1 year later: 12 mg IV daily for 3 days Ocrelizumab (Ocrevus), 300 mg IV every 2 weeks (for 2 doses) at initiation; subsequently, 600 mg IV every 6 months Rituximab (Rituxan), 1000 mg IV every 2 weeks (for 2 doses); may repeat every 16-24 weeks Cladribine (Mavenclad), 3.5 mg per kg body weight PO divided into 2 yearly treatment courses (1.75 mg per kg body weight each year); each yearly treatment course is divided into 2 treatment cycles; administer cycle dosage as 1 or 2 tablets once daily over 4-5 consecutive days Ofatumumab (Kesimpta), 20 mg SC weekly for weeks 0, 1 and 2; 20 mg SC monthly starting at week 4

Other: Early Aggressive Therapy or Traditional Therapy
Participants will be stratified by whether they are at higher versus lower risk for long-term disability and then randomized 1:1 to a higher-efficacy versus a traditional, first-line disease-modifying therapy (DMT) class.
Active Comparator: Traditional Therapy

First-line disease-modifying therapy (Traditional Therapy) for treatment of multiple sclerosis Traditional Therapy choices and maximum allowable doses: Glatiramer acetate (Copaxone, Glatopa, and other generics), 20 mg subcutaneously (SC) daily, or 40 mg SC three times a week Intramuscular interferon (Avonex), 30 mcg intramuscularly (IM) weekly Subcutaneous interferon (Betaseron, Extavia, Rebif), 0.25 mg SC every other day (Betaseron, Extavia); 44 mcg SC three times a week (Rebif) Pegylated interferon (Plegridy), 125 mcg SC every 14 days Teriflunomide (Aubagio), 14 mg orally (PO) daily Dimethyl fumarate (Tecfidera and generics), 240 mg PO twice a day Diroximel fumarate (Vumerity), 462 mg PO twice a day Monomethyl fumarate (Bafiertam), 190 mg PO twice a day Fingolimod (Gilenya and generics), 0.5 mg PO daily Siponimod (Mayzent), 1 mg PO daily or 2 mg PO daily Ozanimod (Zeposia), 0.92 mg PO daily Ponesimod (Ponvory), 20 mg PO daily

Other: Early Aggressive Therapy or Traditional Therapy
Participants will be stratified by whether they are at higher versus lower risk for long-term disability and then randomized 1:1 to a higher-efficacy versus a traditional, first-line disease-modifying therapy (DMT) class.

Outcome Measures

Primary Outcome Measures

  1. Time to sustained disability progression [From date of randomization until the date of first documented sustained disability progression, up to 75 months]

    Time to sustained disability progression is measured by the Expanded Disability Status Scale plus (EDSS+): a composite endpoint that includes EDSS change (change at any 6 month time point of > 1.0 point if baseline EDSS is < 5.5 or of > 0.5 if baseline EDSS is > 6.0, that is sustained 6 months later) OR 20% worsening on either of two specific components of the Multiple Sclerosis Functional Composite (MSFC), the timed 25-foot walk test (T25FWT) and the nine hole peg test (9HPT) that is sustained 6 months later.

  2. Change in Overall Burden of MS [up to 48 weeks from enrollment into COVID-19 related substudy]

    The change in overall burden of MS will be defined for the COVID-19 related substudy as the occurrence of breakthrough disease (relapses or new MRI activity) or the development of new (or worsening baseline) MS symptoms, which are (for TREAT-MS) and will continue to be (during the substudy) documented at clinical visits, whether in-person or on tele-visits.

Secondary Outcome Measures

  1. Patient-Determined Disease Steps (PDDS) [up to 75 months]

    PDDS is a self-assessment scale of disability due to MS on a scale from 0 to 8 and will be administered as an electronic patient-reported outcome (PRO).

  2. Multiple Sclerosis Functional Composite (MSFC) Composite Score [up to 75 months]

    The MSFC consists of the timed 25 foot walk test, the 9-hole peg test, and the Paced Auditory Serial Addition Test (PASAT) and a composite MSFC z-score will be evaluated.

  3. Timed 25 Foot Walk Test [up to 75 months]

    Time taken to complete the timed 25 foot walk test, measured twice in units of seconds, will be averaged and evaluated.

  4. Nine-hole Peg Test [up to 75 months]

    Time taken to complete the nine-hole peg test, measured twice for each hand (dominant and non-dominant) in units of seconds, will be averaged for each hand and evaluated.

  5. Paced Auditory Serial Addition Test (PASAT) [up to 75 months]

    The paced auditory serial addition test that measures processing speed will be administered once; number and percent correct will be evaluated.

  6. Low contrast visual acuity [up to 75 months]

    Low-contrast letter acuity (binocular, 2.5% contrast Sloan charts)

  7. Patient-reported incomplete relapse recovery [up to 75 months]

    Among participants identified to have a relapse, relapse recovery will be defined as complete or incomplete based on patient self-report.

  8. Neurologic exam-based incomplete relapse recovery [up to 75 months]

    Among participants identified to have a relapse, relapse recovery will be defined as complete or incomplete based on neurologic examination (those who have increased Functional System scores, corresponding to the relapse symptoms, of 1.0 point or greater for at least 6 months after the relapse onset, without subsequent accrual of worsening in that same Functional System (e.g. more indicative of progression), will be considered to have incomplete relapse recovery).

  9. Cognition using Symbol Digit Modality Test (SDMT) [up to 75 months]

    The SDMT is commonly used in MS to assess processing speed and will be administered orally and used to evaluate changes in cognition throughout the study.

  10. Multiple Sclerosis Impact Scale (MSIS-29) [up to 75 months]

    The MSIS-29 will be used to evaluate the impact of MS on the participants and will be administered as an electronic PRO.Multiple Sclerosis Impact Scale (MSIS-29) is an instrument used for measuring the physical (20 items) and psychological (nine items) impact of multiple sclerosis.

  11. Quality of Life in Neurological Disorders (Neuro-QoL): Anxiety Subscale [up to 75 months]

    The Anxiety Subscale of Neuro-QoL will be administered as an electronic PRO.

  12. Quality of Life in Neurological Disorders (Neuro-QoL): Depression Subscale [up to 75 months]

    The Depression Subscale of Neuro-QoL will be administered as an electronic PRO.

  13. Quality of Life in Neurological Disorders (Neuro-QoL): Fatigue Subscale [up to 75 months]

    The Fatigue Subscale of Neuro-QoL will be administered as an electronic PRO.

  14. Quality of Life in Neurological Disorders (Neuro-QoL): Upper Extremity Function [up to 75 months]

    The Upper Extremity Function Subscale of Neuro-QoL will be administered as an electronic PRO.

  15. Quality of Life in Neurological Disorders (Neuro-QoL): Lower Extremity Function [up to 75 months]

    The Lower Extremity Function Subscale of Neuro-QoL will be administered as an electronic PRO.

  16. Quality of Life in Neurological Disorders (Neuro-QoL): Cognitive Function [up to 75 months]

    The Cognitive Function Subscale of Neuro-QoL will be administered as an electronic PRO.

  17. Quality of Life in Neurological Disorders (Neuro-QoL): Positive Affect/Well-being [up to 75 months]

    The Positive Affect/Well-being Subscale of Neuro-QoL will be administered as an electronic PRO.

  18. Quality of Life in Neurological Disorders (Neuro-QoL): Sleep Disturbance [up to 75 months]

    The Sleep Disturbance Subscale of Neuro-QoL will be administered as an electronic PRO.

  19. Quality of Life in Neurological Disorders (Neuro-QoL): Ability to Participate in Social Roles and Activities [up to 75 months]

    The Ability to Participate in Social Roles and Activities Subscale of Neuro-QoL will be administered as an electronic PRO.

  20. Quality of Life in Neurological Disorders (Neuro-QoL): Satisfaction with Social Roles and Activities [up to 75 months]

    The Satisfaction with Social Roles and Activities Subscale of Neuro-QoL will be administered as an electronic PRO.

  21. Quality of Life in Neurological Disorders (Neuro-QoL): Stigma [up to 75 months]

    The Stigma Subscale of Neuro-QoL will be administered as an electronic PRO.

  22. Employment status [up to 75 months]

    The incidence of change in employment to "disabled" or "looking for work, unemployed," will be evaluated for all participants through an electronic PRO.

  23. Marital status [up to 75 months]

    Incident divorce or separation, among those who previously were married or in a domestic partnership, will be evaluated for all participants through an electronic PRO.

  24. Serious Adverse Events (SAEs) [up to 75 months]

    SAEs (clinically significant infections, malignancies, or the development of other serious comorbidities, as well as unplanned hospitalizations [for non-elective issues, excluding MS relapse] and death)

  25. Adverse event resulting in a decision to change disease-modifying therapy [up to 75 months]

    Adverse events meaningful enough to lead to medication discontinuation

  26. Severe COVID-19 Infection [up to 48 weeks from enrollment into COVID-19 related substudy]

    Severe COVID-19 infection will be defined as an outcome of "hospitalization or death" due to confirmed or suspected COVID-19 infection

Other Outcome Measures

  1. Brain Magnetic Resonance Imaging (MRI) evidence of neurodegeneration [From 6 months after starting 1st therapy up to 75 months after randomization]

    Changes in brain MRI measures of neurodegeneration, including whole brain and normalized gray matter volumes, cortical thickness, subcortical gray matter compartment volumes, and measures of T2 lesion burden.

  2. Number of relapses [up to 75 months]

    The number of relapses (new or worsening neurologic symptoms lasting for 24 hours or more in the absence of fever).

  3. Number of new brain lesions on MRI [up to 75 months]

    The number of new/enlarging T2-weighted hyperintense lesions and T1-weighted hypointense lesions will be quantified on each MRI scan

  4. Retinal layer thickness by Optical Coherence Tomography (OCT) [up to 75 months]

    Retinal nerve fiber layer and ganglion cell/inner plexiform thickness will be evaluated among patients at centers and offices with access to OCT as standard of care

  5. Number of new medications, escalated dosage of medications, and non-pharmacologic interventions for MS-related symptoms [up to 75 months]

    As an exploratory outcome, the number of newly-prescribed or dose-escalated medications used for treating MS symptoms (including pain, weakness, numbness/tingling, trouble walking, cognitive problems, fatigue, depression, anxiety, visual dysfunction, spasticity, vertigo, or bladder/bowel/sexual dysfunction) during the trial will be evaluated using the electronic health record. In addition, non-pharmacologic interventions (and referrals to other healthcare providers) for symptom management will also be captured.

Eligibility Criteria

Criteria

Ages Eligible for Study:
18 Years to 60 Years
Sexes Eligible for Study:
All
Accepts Healthy Volunteers:
No
Inclusion Criteria:

  • Aged 18-60 years

  • Meets 2017 McDonald criteria for relapsing-remitting MS [patients with clinically isolated syndrome (CIS) are not eligible]

  • Must be EITHER John Cunningham (JC) virus antibody negative or low positive (index antibody titer <0.9), OR negative for: Hepatitis B and C, tuberculosis

  • HIV negative

  • No chemotherapy in past year; if patient has prior history of chemotherapy or malignancy, documentation in chart explaining why potential risks of higher-efficacy therapy are justified

Exclusion Criteria:

  • Prior treatment with rituximab, ocrelizumab, ofatumumab, alemtuzumab, mitoxantrone or cladribine

  • Prior treatment with any other MS DMT for more than 6 months

  • Prior treatment with experimental aggressive therapies (e.g., T-cell vaccine, total lymphoid radiation, stem cells)

  • Treatment with teriflunomide within past 2 years (even for ≤ 6 months), unless rapid wash out done (i.e., with cholestyramine or activated charcoal)

  • Treatment in the past 6 months with any MS DMT

  • Prior treatment with any other investigational immune-modulating /suppressing drug for MS not listed above

  • Pregnant or breast-feeding

  • Women of child-bearing age who are planning or strongly considering conception during the study time frame

Contacts and Locations

Locations

Site City State Country Postal Code
1 University of Alabama at Birmingham Birmingham Alabama United States 35233
2 The University of South Alabama Mobile Alabama United States 36604
3 St. Joseph's Hospital & Medical Center - Barrow Neurological Institute Phoenix Arizona United States 85013
4 Dignity Health Medical Foundation Carmichael California United States 95608
5 Cedars-Sinai Medical Center Los Angeles California United States 90048
6 University of California, Los Angeles Los Angeles California United States 90095
7 University of California, San Diego San Diego California United States 92037
8 University of California, San Francisco San Francisco California United States 94158
9 Christiana Care Health Services, Inc. Newark Delaware United States 19713
10 Georgetown University Washington District of Columbia United States 20007
11 University of Florida Gainesville Florida United States 32611
12 University of Miami Miami Florida United States 33136
13 University of South Florida Health Tampa Florida United States 33612
14 Rush University Medical Center Chicago Illinois United States 60612
15 The University of Kansas Medical Center (KUMC) Kansas City Kansas United States 66160
16 University of Louisville Louisville Kentucky United States 40202
17 Norton Neurology MS Services Louisville Kentucky United States 40207
18 University of Maryland, Baltimore Baltimore Maryland United States 21201
19 The Johns Hopkins Hospital Baltimore Maryland United States 21287
20 Massachusetts General Hospital Boston Massachusetts United States 02114
21 University of Massachusetts Medical School Worcester Massachusetts United States 01655
22 University of Michigan Ann Arbor Michigan United States 48109
23 Wayne State University Detroit Michigan United States 48201
24 Mayo Clinic Rochester Minnesota United States 55905
25 Billings Clinic Billings Montana United States 59101
26 Advanced Neurology Specialists Great Falls Montana United States 59405
27 University of Nebraska Medical Center Omaha Nebraska United States 68198
28 Hackensack University Medical Center Hackensack New Jersey United States 07601
29 RWJBarnabas Health Multiple Sclerosis Comprehensive Care Center Livingston New Jersey United States 07039
30 New York University School of Medicine New York New York United States 10016
31 Icahn School of Medicine at Mount Sinai New York New York United States 10029
32 Columbia University Medical Center New York New York United States 10032
33 University of Rochester Medical Center Rochester New York United States 14642
34 Stony Brook University Stony Brook New York United States 11794-8121
35 Novant Health Neurology and Sleep Charlotte North Carolina United States 28207
36 University of Cincinnati Cincinnati Ohio United States 45219
37 OhioHealth Research Institute Columbus Ohio United States 43214
38 Oklahoma Medical Research Foundation Oklahoma City Oklahoma United States 73104
39 Providence Health and Services - Oregon Portland Oregon United States 97225
40 Geisinger Clinic Danville Pennsylvania United States 17822
41 Allegheny Health Network Research Institute Pittsburgh Pennsylvania United States 15212
42 Vanderbilt Comprehensive MS Center Nashville Tennessee United States 37215
43 Baylor Scott and White Health Dallas Texas United States 75246
44 The University of Texas Southwestern Medical Center Dallas Texas United States 75390-8806
45 Central Texas Neurology Consultants Round Rock Texas United States 78681
46 University of Utah Salt Lake City Utah United States 84108
47 The University of Vermont and State Agricultural College Burlington Vermont United States 05405
48 Blacksburg Neurology Christiansburg Virginia United States 24073
49 Neurology Consultants of Tidewater Norfolk Virginia United States 23502
50 Swedish Health Services Seattle Washington United States 98122
51 University of Washington Seattle Washington United States 98133
52 Medical College of Wisconsin Milwaukee Wisconsin United States 53226

Sponsors and Collaborators

  • Johns Hopkins University
  • Patient-Centered Outcomes Research Institute

Investigators

  • Principal Investigator: Ellen M. Mowry, MD, MCR, Johns Hopkins University
  • Principal Investigator: Scott D. Newsome, DO, Johns Hopkins University

Study Documents (Full-Text)

None provided.

More Information

Publications

None provided.
Responsible Party:
Johns Hopkins University
ClinicalTrials.gov Identifier:
NCT03500328
Other Study ID Numbers:
  • IRB00143534
First Posted:
Apr 18, 2018
Last Update Posted:
Jul 19, 2022
Last Verified:
Jul 1, 2022
Studies a U.S. FDA-regulated Drug Product:
No
Studies a U.S. FDA-regulated Device Product:
No
Product Manufactured in and Exported from the U.S.:
No
Additional relevant MeSH terms:
Multiple Sclerosis
Multiple Sclerosis, Relapsing-Remitting
Sclerosis

Study Results

No Results Posted as of Jul 19, 2022