Multicenter Randomized Double-blind Study Comparing the Efficacy and Safety of Belimumab in the Treatment of Non-infectious Active Cryoglobulinemia Vasculitis Compared to Placebo. TRIBECA STUDY (Treatment nd BElimumab in Cryoglobulinemia Associated Vasculitis)

Sponsor

Assistance Publique - Hôpitaux de Paris (Other)

Overall Status

Not yet recruiting

CT.gov ID

NCT04629144

Collaborator

(none)

Enrollment

Arms

Anticipated Duration (Months)

Study Details

Study Description

Brief Summary

Cryoglobulinemia vasculitis (CV) is a systemic immune-mediated small vessel vasculitis. Rituximab proved effective on main vasculitis signs, with a complete clinical response of 65%. However, CV relapse is noted in up to 40% of patients. Following rituximab, serum Blys concentration significantly increased and may favor relapses. Tribeca is a multicentre randomized controled study comparing safety and efficacy of belimumab to placebo in non infectious cryoglobulinemia vasculitis.

Condition or Disease	Intervention/Treatment	Phase
Vasculitis Cryoglobulinemia	Drug: Belimumab Drug: Placebo	Phase 2

Study Design

Study Type:

Interventional

Anticipated Enrollment :

48 participants

Allocation:

Randomized

Intervention Model:

Parallel Assignment

Masking:

Double (Participant, Care Provider)

Primary Purpose:

Treatment

Official Title:

Multicenter Randomized Double-blind Study Comparing the Efficacy and Safety of Belimumab in the Treatment of Non-infectious Active Cryoglobulinemia Vasculitis Compared to Placebo. TRIBECA STUDY (Treatment nd BElimumab in Cryoglobulinemia Associated Vasculitis)

Anticipated Study Start Date :

Mar 1, 2021

Anticipated Primary Completion Date :

Jun 1, 2024

Anticipated Study Completion Date :

Mar 1, 2025

Arms and Interventions

Arm	Intervention/Treatment
Experimental: Belimumab Belimumab administered subcutaneously 200mg weekly from week 0 to week 24.	Drug: Belimumab Belimumab administered subcutaneously 200mg weekly from week 0 to week 24. Both arms will have the same corticosteroid tapering scheme, with an initial dose of 60 mg/day. The following schedule of reduction of prednisone will apply to both groups as long as the disease is inactive: 60 mg/day week (W)0-W4, 40 mg/day W4-W6 30 mg/day W6-W8, 20 mg/day W8-W10, 15 mg/day W10-W12, 10 mg/day W12-W14, 7.5 mg/day W14-W16, 5 mg/day W16-W18 2.5mg/day W18-W20. Stopping glucocorticoid therapy at W20 At each step, the prednisone dose will be reduced only in the absence of signs of vasculitis activity.
Placebo Comparator: Placebo Placebo of Belimumab administered subcutaneously weekly from week 0 to week 24.	Drug: Placebo Both arms will have the same corticosteroid tapering scheme, with an initial dose of 60 mg/day. The following schedule of reduction of prednisone will apply to both groups as long as the disease is inactive: 60 mg/day week (W)0-W4, 40 mg/day W4-W6 30 mg/day W6-W8, 20 mg/day W8-W10, 15 mg/day W10-W12, 10 mg/day W12-W14, 7.5 mg/day W14-W16, 5 mg/day W16-W18 2.5mg/day W18-W20. Stopping glucocorticoid therapy at W20 At each step, the prednisone dose will be reduced only in the absence of signs of vasculitis activity.

Arm

Intervention/Treatment

Experimental: Belimumab

Belimumab administered subcutaneously 200mg weekly from week 0 to week 24.

Drug: Belimumab

Belimumab administered subcutaneously 200mg weekly from week 0 to week 24. Both arms will have the same corticosteroid tapering scheme, with an initial dose of 60 mg/day. The following schedule of reduction of prednisone will apply to both groups as long as the disease is inactive: 60 mg/day week (W)0-W4, 40 mg/day W4-W6 30 mg/day W6-W8, 20 mg/day W8-W10, 15 mg/day W10-W12, 10 mg/day W12-W14, 7.5 mg/day W14-W16, 5 mg/day W16-W18 2.5mg/day W18-W20. Stopping glucocorticoid therapy at W20 At each step, the prednisone dose will be reduced only in the absence of signs of vasculitis activity.

Placebo Comparator: Placebo

Placebo of Belimumab administered subcutaneously weekly from week 0 to week 24.

Drug: Placebo

Both arms will have the same corticosteroid tapering scheme, with an initial dose of 60 mg/day. The following schedule of reduction of prednisone will apply to both groups as long as the disease is inactive: 60 mg/day week (W)0-W4, 40 mg/day W4-W6 30 mg/day W6-W8, 20 mg/day W8-W10, 15 mg/day W10-W12, 10 mg/day W12-W14, 7.5 mg/day W14-W16, 5 mg/day W16-W18 2.5mg/day W18-W20. Stopping glucocorticoid therapy at W20 At each step, the prednisone dose will be reduced only in the absence of signs of vasculitis activity.

Outcome Measures

Primary Outcome Measures

Complete clinical response rate W24 [Week 24]
The complete clinical response is defined by the remission of all affected organs involved at baseline and the absence of clinical relapse. The skin and articular remissions are evaluated clinically. Renal remission is evaluated biologically (proteinuria <0.5g/24h or proteinuria/creatinuria <50 mg/mmol, ). Neurological remission is evaluated clinically and electrophysiologically. Digestive remission is evaluated clinically, by endoscopy and/or by Xray. Complete remission of all baseline abnormalities is required to define digestive remission. Cardiac remission is evaluated clinically (improvement of chest pains and other cardiac events), electrically (disappearance of abnormalities indicating acute myocardial suffering on EKG) and biologically (normalization of muscular enzymes). Complete remission of all baseline abnormalities is required to define cardiac remission.

Secondary Outcome Measures

Safety W24 [Week 24]
Frequency and severity of adverse clinical events
Safety W48 [Week 48]
Frequency and severity of adverse clinical events
Response W12 [Week 12]
The complete clinical response is defined by the remission of all affected organs involved at baseline and the absence of clinical relapse. Partial clinical response The partial clinical response is defined by the improvement and / or remission of more than half of the organ involvement present at baseline and the absence of clinical relapse. No clinical response Patients with no clinical response at W4 will be defined by worsening of ulcers or cutaneous necrosis, worsening peripheral neurological involvement or by persistence of active renal involvement defined by persistence of proteinuria> 1.5 g / 24h or proteinuria/creatinuria <150 mg/mmol).
Response W24 [Week 24]
The complete clinical response is defined by the remission of all affected organs involved at baseline and the absence of clinical relapse. Partial clinical response The partial clinical response is defined by the improvement and / or remission of more than half of the organ involvement present at baseline and the absence of clinical relapse. No clinical response Patients with no clinical response at W4 will be defined by worsening of ulcers or cutaneous necrosis, worsening peripheral neurological involvement or by persistence of active renal involvement defined by persistence of proteinuria> 1.5 g / 24h or proteinuria/creatinuria <150 mg/mmol).
Response W48 [Week 48]
The complete clinical response is defined by the remission of all affected organs involved at baseline and the absence of clinical relapse. Partial clinical response The partial clinical response is defined by the improvement and / or remission of more than half of the organ involvement present at baseline and the absence of clinical relapse. No clinical response Patients with no clinical response at W4 will be defined by worsening of ulcers or cutaneous necrosis, worsening peripheral neurological involvement or by persistence of active renal involvement defined by persistence of proteinuria> 1.5 g / 24h or proteinuria/creatinuria <150 mg/mmol).
Rate of cryoglobulinemia clearance W12 [Week 12]
cryoglobulinemia clearance
Rate of cryoglobulinemia clearance W24 [Week 24]
cryoglobulinemia clearance
Rate of cryoglobulinemia clearance W48 [Week 48]
cryoglobulinemia clearance
rheumatoid factor activity W12 [Week 12]
negativation of rheumatoid factor activity
rheumatoid factor activity W24 [Week 24]
negativation of rheumatoid factor activity
rheumatoid factor activity W48 [Week 48]
negativation of rheumatoid factor activity
C4 complement level W12 [Week 12]
normalization of C4 complement level
C4 complement level W24 [Week 24]
normalization of C4 complement level
C4 complement level W48 [Week 48]
normalization of C4 complement level
Early failures [Week 4]
Rate of early failures (non clinical response at W4) Patients with no clinical response at W4 will be defined by worsening of ulcers or cutaneous necrosis, worsening peripheral neurological involvement or by persistence of active renal involvement defined by persistence of proteinuria> 1.5 g / 24h or proteinuria/creatinuria <150 mg/mmol,).
Clinical relapse rate W48 [Week 48]
Relapse is defined as de novo appearance or recurrence of a manifestation of cryoglobulinemia vasculitis
Prednisone W24 [Week 24]
Cumulative dose of prednisone
Prednisone W48 [Week 48]
Cumulative dose of prednisone
Quality of life W24 [Week 24]
Quality of life score SF-36. The SF-36 consists of eight scaled scores, which are the weighted sums of the questions in their section. Each scale is directly transformed into a 0-100 scale on the assumption that each question carries equal weight. The lower the score the more disability. The higher the score the less disability i.e., a score of zero is equivalent to maximum disability and a score of 100 is equivalent to no disability. To calculate the scores it is necessary to purchase special software for the commercial version, but no special software is needed for the RAND-36 version. Pricing depends on the number of scores that the researcher needs to calculate. The eight sections are: vitality physical functioning bodily pain general health perceptions physical role functioning emotional role functioning social role functioning mental health
Quality of life W48 [Week 48]
Quality of life score SF-36. The SF-36 consists of eight scaled scores, which are the weighted sums of the questions in their section. Each scale is directly transformed into a 0-100 scale on the assumption that each question carries equal weight. The lower the score the more disability. The higher the score the less disability i.e., a score of zero is equivalent to maximum disability and a score of 100 is equivalent to no disability. To calculate the scores it is necessary to purchase special software for the commercial version, but no special software is needed for the RAND-36 version. Pricing depends on the number of scores that the researcher needs to calculate. The eight sections are: vitality physical functioning bodily pain general health perceptions physical role functioning emotional role functioning social role functioning mental health
Infections [Week 48]
Rate of infections
BVAS activity W12 [Week 12]
BVAS activity score as defined in Flossmann, Oliver, et al. "Development of comprehensive disease assessment in systemic vasculitis." Postgraduate medical journal 84.989 (2008): 143-152.
BVAS activity W24 [Week 24]
BVAS activity score as defined in Flossmann, Oliver, et al. "Development of comprehensive disease assessment in systemic vasculitis." Postgraduate medical journal 84.989 (2008): 143-152.
BVAS activity W48 [Week 48]
BVAS activity score as defined in Flossmann, Oliver, et al. "Development of comprehensive disease assessment in systemic vasculitis." Postgraduate medical journal 84.989 (2008): 143-152.

Other Outcome Measures

Immunomonitoring W4 [Week 4]
deep immunophenotyping, cytokines production, clonal IgM memoryCD21-/low cells) description
Immunomonitoring W24 [Week 24]
deep immunophenotyping, cytokines production, clonal IgM memoryCD21-/low cells) description
Immunomonitoring W48 [Week 48]
deep immunophenotyping, cytokines production, clonal IgM memoryCD21-/low cells) description
renal response W12 [Week 12]
Renal remission is evaluated biologically (proteinuria <0.5g/24h or proteinuria/creatinuria <50 mg/mmol).
renal response W24 [Week 24]
Renal remission is evaluated biologically (proteinuria <0.5g/24h or proteinuria/creatinuria <50 mg/mmol).

Eligibility Criteria

Criteria

Ages Eligible for Study:

18 Years and Older

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

Inclusion Criteria:

Age > 18 years
Written inform consent
Active cryoglobulinemia vasculitis define by positive cryoglobulinemia and a clinically active vasculitis with skin, joint, renal, peripheral nerve, central neurological, digestive, pulmonary and/or cardiac involvement (no histological evidence needed if presence of purpura demonstrated),
Affiliated to National French social security system
Having received Rituximab as induction therapy within 6 weeks
Female subjects of childbearing potential must not become pregnant and so must be sexually inactive by abstinence or use contraceptive methods with a failure rate of < 1%.

Therefore, these women must have a negative serum pregnancy test at screening, and confirmed monthly while in study, out to at least 4 months (5 half lives) post last dose and agree to 1 of the following:

Complete abstinence from intercourse from 2 weeks prior to administration of the 1st dose of study agent until 16 weeks after the last dose of study agent (Sexual inactivity by abstinence must be consistent with the preferred and usual lifestyle of the subject. Periodic abstinence (e.g. calendar, ovulation, symptothermal, post-ovulation methods) and withdrawal are not acceptable methods of contraception) OR
Consistent and correct use of 1 of the following acceptable methods of birth control for 1 month prior to the start of the study agent, during the study, and 16 weeks after the last dose of study agent
Oral contraceptive, either combined or progestogen alone
Injectable progestogen
Implants of levonorgestrel or etonogestrel
Estrogenic vaginal ring
Percutaneous contraceptive patches
Intrauterine device (IUD) or intrauterine system (IUS) with <1% failure rate as stated in the product label
Male partner sterilization (vasectomy with documentation of azoospermia) prior to the female subject's entry into the study, and this male is the sole partner for that subject. For this definition, "documented" refers to the outcome of the investigator's/designee's medical examination of the subject or review of the subject's medical history for study eligibility, as obtained via a verbal interview with the subject or from the subject's medical records
Double barrier method: condom and occlusive cap (diaphragm or cervical/vault caps) plus spermicidal agent (foam/gel/film/cream/suppository) These allowed methods of contraception are only effective when used consistently, correctly and in accordance with the product label. The investigator is responsible for ensuring subjects understand how to properly use these methods of contraception.
HIV negative serology ; negative HBs Ag test and HBc Ab test; HCV negative serology or negative HCV RNA if positive HCV serology
Adequate haematological status:
neutrophils (ANC) >1x109/L;

Exclusion Criteria:

Patient with a vasculitis unrelated to cryoglobulinemia
Patient with non active cryoglobulinemia vasculitis,
Patient with immunosuppressant introduced or increased in the month prior to the inclusion, (except Rituximab)
Patients receiving corticosteroid therapy > 0.5 mg/kg/d > 1 month before the inclusion or > 1 mg/kg/d >2 weeks before inclusion or taking more than 3000 mg methylprednisolone 4 weeks prior to the inclusion visit
Excluded concomitant medications (except Rituximab) :
365 days Prior to Belimumab:
Any biologic investigational agent (e.g., abetimus sodium, anti CD40L antibody, BG9588/ IDEC 131)
Investigational agent applies to any drug not approved for sale in the country in which it is being used
180 Days Prior to Belimumab:
Intravenous cyclophosphamide
If concomitant use with cyclophosphamide, enhanced safety monitoring required.
Serum IgG levels should be measured monthly in this situation
Benlysta should be discontinued in subjects with serum IgG levels <250 mg/dL associated with a severe or serious infection
30 Days Prior to Belimumab (or 7 half lives, whichever is greater)
Any non-biologic investigational agent
Investigational agent applies to any drug not approved for sale in the country in which it is being use
Live vaccines within 30 days prior to baseline or concurrently with belimumab
Have a history of malignant neoplasm within the last 5 years
Have a Progressive multifocal leukoencephalopathy
.
Have evidence of serious suicide risk including any history of suicidal behaviour in the last 6 months and/or any suicidal ideation in the last 2 months or who in the investigator's judgment, pose a significant suicide risk
Have a history of a primary immunodeficiency
Have a significant IgG deficiency (IgG level < 400 mg/dL)
Have a history of major organ transplant or hematopoietic stem cell/marrow transplant or renal transplant.
• Have an IgA deficiency (IgA level < 10 mg/dL
Infection history:
Currently on any suppressive therapy for a chronic infection (such as tuberculosis, pneumocystis, cytomegalovirus,)
Infection requiring hospitalization and/or use of parenteral (IV or IM) antibiotics (antibacterials, antivirals, anti-fungals, or anti-parasitic agents) within 60 days of Day 0.
Have current drug or alcohol abuse or dependence, or a history of drug or alcohol abuse or dependence within 365 days prior to Day 0
Have a historically positive HIV test or test positive at screening for HIV
Hepatitis status:
Serologic evidence of current or past Hepatitis B (HB) infection based on the results of testing for HBsAg and HBcAb as follows:
Patients positive for HBsAg or HBcAb are excluded
Positive test for Hepatitis C RNA
Have a history of a hypersensitivity or an anaphylactic reaction to parenteral administration of Belimumab or Rituximab, corticosteroids or any excipients of the treatments administered during the study
If Women of Child Bearing Potential (WCBP) are included please see special instructions above
Pregnant or breast feeding women
Have any intercurrent significant medical or psychiatric illness that the investigator considers would make the candidate unsuitable for the study
Patients under legal protection or unable to consent
Participation to another interventional study