Non-inferiority Study of Rituximab Compared to Ocrelizumab in Relapsing MS

Multiple Sclerosis Clinical Trial

— Noisy Rebels  

Official title:

Non-inferiority Study of Rituximab Compared to Ocrelizumab in Relapsing Multiple Sclerosis

Clinical Trial Details — Status: Recruiting

Administrative data

• NCT number: NCT05834855
• Other study ID #: Anti-CD20 in RMS
• Status: Recruiting
• Phase: Phase 3
• Start date: April 2023
• Est. completion date: May 2027

Study information

• Verified date: April 2023
• Source: Amsterdam UMC, location VUmc
• Contact: Lisa Schoof, Msc
• Phone: 650087853
• Email: l.g.schoof[@]amsterdamumc.nl
• Is FDA regulated: No
• Study type: Interventional

Clinical Trial Summary

Rationale: Ocrelizumab is widely and effectively used to treat relapsing multiple sclerosis (RMS). Phase II studies and data from large patient cohorts indicate that rituximab, another anti-CD20 monoclonal antibody, is probably equally effective and safe as ocrelizumab in the treatment of RMS. An advantage of rituximab is a considerably lower price. Therefore we will start a study aimed at demonstrating non-inferiority of rituximab compared to ocrelizumab in RMS. If non-inferiority of rituximab can be shown, important reductions in the cost of treatment of RMS will be possible, without loss of efficacy. Objective: Evaluating the efficacy and safety of ritixumab compared to ocrelizumab in the treatmens of RMS. Study design: Randomized double blind multi-centre non-inferiority study of rituximab compared to ocrelizumab in 200 patients with RMS. The trial duration will be 30 months Study population: The study population consists of 200 adult RMS patiens with an indication to start anti-CD20 monoclonal antibody treatment. Intervention: Patients will be randomized 1:1 into the standard group (ocrelizumab treatment) or the experimental group (rituximab treatment). Main study parameters: To conclude non-inferiority of rituximab there will be one primary endpoint: the proportion of patients free of inflammatory disease activity (defined as: new or enlarged T2 lesions) between week 24 (M6) and week 96 (M24) of treatment in each arm. Secondary trial endpoints are presence and number of clinical relapses,T2 and contrast enhancing lesion volumes, brain volume and brain volume changes, disease progression (defined as clinically relevant change on any of the measures: EDSS, T25FW, 9HPT, SDMT), biochemical parameters such as lipidomics and neurofilament light (NfL), immunological parameters, safety as measured by the number of (serious) adverse events ((S)AE), quality of life (EQ-5D-L) and treatment satisfaction (TSQM) and patient reported measures of MS impact (MSIS-29) and well-being (questionnaire on physical complaints) Nature and extent of the burden and risk: Patients included in this study will be treated and monitored by MRI, clinical tests and laboratory tests according to existing protocols and will not be exposed to extra or unknown risks. They will have extra annual questionnaires and larger blood samples at some time points. There is extensive experience with both rituximab and ocrelizumab as efficacious and safe treatments of RMS.

Recruitment information / eligibility

• Status: Recruiting
• Enrollment: 200
• Est. completion date: May 2027
• Est. primary completion date: May 2027
• Accepts healthy volunteers: No
• Gender: All
• Age group: 18 Years and older

Eligibility

Inclusion Criteria:

1. Men and women aged 18 years and older

2. A diagnosis of relapsing MS according to the 2017 revised diagnostic criteria

3. Indication to start treatment with anti-CD20 therapy according to the treating neurologist and the relevant label in the Netherlands for treatment of relapsing MS

4. Able to understand written and spoken Dutch or English

5. Capable of giving signed informed consent including compliance with the requirements and restrictions listed in the informed consent form (ICF) and in this protocol.

6. Screening EDSS score = 6.5 . Exclusion Criteria: Medical Conditions

1. A known allergy or other intolerability to RTX, OCR, gadolinium-based MRI contrast agents, or corticosteroids.

2. A diagnosis of primary progressive MS according to the diagnostic criteria.

3. A diagnosis of not-active secondary progressive MS.

4. Chronic infectious diseases such as tuberculosis, VZV, hepatitis virus or HIV, as well as hepatitis B surface antigen positivity and/or hepatitis C PCR positivity verified at screening visit.

5. A history of proven inflammatory bowel disease such as M. Crohn or ulcerative colitis

6. Prior or current psychiatric illness, mental deficiency or cognitive dysfunction influencing the patient ability to make an informed consent or comply with the treatment and follow-up phases of this protocol.

7. Cardiac disease that makes treatment with OCR or RTX contra-indicated as stated by the most recent SmPC

8. Active malignancy or prior history of malignancy that makes treatment with OCR or RTX contra-indicated as stated by the most recent SmPC.

9. WBC < 1.5 x 109/L if not caused by a reversible effect of documented ongoing medication. If caused by a reversible effect of documented ongoing medication the WBC count must be > 1,5 x 109/L before start of study treatment.

10. Platelet (thrombocyte) count < 100 x 109/L

11. ALAT and/or ASAT more than 2 times the upper normal reference limit (ULN)

12. Serum creatinine > 200 µmol/L

13. Serum bilirubin > ULN

14. Serum IgG < LLN

15. Pregnant or breast-feeding women

16. Women of childbearing potential (WOCBP) not able or willing to use highly effective methods of birth control per ICH M3 (R2) that result in failure rate of = 1% per year when used consistently and correctly for the duration of the study OR until 3 months after last dose administered.

17. History of serious or life-threatening infusion reaction to OCR or RTX

18. Treatment with glucocorticoids or ACTH within one month prior to start of study treatment Prior/Concomitant Therapy

19. Previous use of second line MS-therapies cladribine, RTX, alemtuzumab, OCR, ofatumumab, hematopoietic stem cell therapy (HSCT) or other immunosuppression therapies with long lasting effects. Mitoxantrone is allowed if used > 1 year before enrolment. If any of these medications have been used for indications other than MS, patients can be included if the medications have not been used the year before enrolment. Previous treatment with natalizumab is allowed if the reason to switch was disease activity (so not allowed in for example cases that switch from natalizumab to anti-CD20 therapy because of JCV positivity).

20. Concomitant use of systemic immunosuppressive medication (except corticosteroids for symptomatic treatment of relapses). Prior/Concurrent Clinical Study Experience

21. Currently enrolled in another investigational device or drug study, or less than 30 days since ending of another investigational device or drug study (s), or receiving other investigational treatment(s). Patients participating in a purely observational studies will be allowed to participate. Lifestyle

22. Current alcohol or drug dependencies. Diagnostic assessments

23. Presence of metallic objects implanted in the body, that would preclude the ability of the patient to safely have MRI exams.

24. Not willing to undergo MRI scans with i.v. gadolinium injections

Related Conditions & MeSH terms

• Autoimmune Diseases
• Autoimmune Diseases of the Nervous System
• Demyelinating Autoimmune Diseases, CNS
• Demyelinating Diseases
• Multiple Sclerosis
• Multiple Sclerosis, Relapsing-Remitting
• Nervous System Diseases
• Sclerosis

Intervention

Drug:
• Rituximab
Treatment with rituximab

Locations

Country	Name	City	State
Netherlands	Amsterdam UMC, location VUmc	Amsterdam

Sponsors (2)

Lead Sponsor	Collaborator
Amsterdam UMC, location VUmc	Stichting Treatmeds

Country where clinical trial is conducted

Netherlands, 

Outcome

Type	Measure	Description	Time frame	Safety issue
Other	Anti-drug antibodies	Proportion of patients with anti-drug-antibodies during 30 months of treatment	30 months
Other	Infusion reactions	Proportion of patients with immediate and delayed infusion reactions during 30 months of treatment	30 months
Other	Infections	Proportion of patients with infections during 30 months of treatment	30 months
Other	Malignancies	Proportion of patients with malignancies during 30 months of treatment	30 months
Other	Adverse events	Proportion of patients with any SAE/SAR and AESI during 30 months of treatment	30 months
Other	Burden of physical senstations during treatment	Burden of physical sensations prior to, after, and between infusions as measured with wearing-off questionnaire and question 5 of the RAPID3-HAQ2 questionnaire	Baseline, month 6, month 12, month 18, month 24, month 30
Other	Quality of life questionnaires	Quality of life as measured by multiple sclerosis impact scale-29 (MSIS-29)	Baseline, month 6, month 12, month 18, month 24, month 30
Other	Quality of life questionnaires	Quality of life as measured by EuroQol-5 Dimension (EQ-5D)	Baseline, month 6, month 12, month 18, month 24, month 30
Other	Treatment satisfaction	Treatment satisfaction as measured with the Treatment Satisfaction Questionnaire Measurement (TSQM)	Baseline, month 6, month 12, month 18, month 24, month 30
Other	Lymphocytes	Absolute numbers of different lymphocyte subsets prior to infusion during 30 months of treatment	30 months
Other	Neurofilament	Serum levels of neurofilament during 30 months of treatment	30 months
Other	Dynamics of B-cell depletion	B-cell count (thousand/ml) (normal range: 100-300 thousand/ml)	Baseline, week 2, month 6, month 12, month 18, month 24, month 30
Other	Dynamics of B-cell repopulation	B-cell count (thousand/ml) (normal range: 100-300 thousand/ml)	Baseline, week 2, month 6, month 12, month 18, month 24, month 30
Other	Dynamics of ocrelizumab drug concentrations	Dynamics of ocrelizumab drug concentrations (microgram/mL)	Baseline, week 2, month 6, month 12, month 18, month 24, month 30
Other	Immunoglobulins	Serum levels of immunoglobulins	Baseline, week 2, month 6, month 12, month 18, month 24, month 30
Other	Serum levels	Serum levels of chemokines and cytokines, protectins, resolvins, maresins, and lipoxins during 30 months of treatment	30 months
Primary	Proportion of patients free of inflammatory disease activity	Proportion of patients with no new or enlarged T2 lesions on brain MRI between month 6 and month 24	between month 6 and month 24
Secondary	Presence and number of clinical relapses	Clinical relapses during treatment	Baseline, month 6, month 24
Secondary	Contrast enhancing lesions	Proportion of patients with no contrast enhancing lesions on brain MRI	Baseline, month 6, month 24
Secondary	Average number of T2 lesions on brain MRI	The average number of new/enlarged T2 lesions between baseline, month 6 and month 24 on brain MRI	Baseline, month 6, month 24
Secondary	Disability progression during follow-up	Disability progression measured on the Expanded Disability Status Scale (EDSS)	Baseline, month 6, month 24
Secondary	Disability progression during follow-up	Disability progression measured on the timed 25 foot walk test (T25FW)	Baseline, month 6, month 24
Secondary	Disability progression during follow-up	Disability progression measured on the Nine Hole Peg Test (9HPT)	Baseline, month 6, month 24
Secondary	Disability progression during follow-up	Disability progression measured on the Symbol Digit Modalities Test(SDMT)	Baseline, month 6, month 24