Induction Therapy With Anti-TNFα vs Cyclophosphamide in Severe Behçet Disease (ITAC)
Primary Purpose
Behcet's Disease, Vasculitis
Status
Completed
Phase
Phase 3
Locations
France
Study Type
Interventional
Intervention
Infliximab
Cyclophosphamide
Sponsored by
About this trial
This is an interventional treatment trial for Behcet's Disease focused on measuring Behcet's Disease, Vasculitis, Biotherapy, immunosuppressant, Infliximab
Eligibility Criteria
Inclusion Criteria:
- Age ≥ 12 years old
- Written inform consent (Informed Consent should be obtained from the legal guardian in accordance with regional laws or regulations for patients 12 to 17 years of age)
- Diagnosis of BD according to international criteria for BD (ICBD) (see Appendix 1).
Life threatening active BD defined as 1 of the following disease categories and according to the validated international definition:
- Major vessel disease: arterial aneurysms or arterial stenosis, myocarditis and/or major deep vein thrombosis (i.e. inferior vena cava, superior vena cava, cardiac cavity thrombosis, pulmonary embolism, supra-hepatic vessels, renal and mesenteric vessels). Diagnosis of major vessel involvement will be done using vascular doppler sonography, echocardiography, angio-CT scan and/or cardiac magnetic resonance imaging (MRI).
- Central nervous system involvement: encephalitis or meningoencephalitis or myelitis. The diagnosis of neuro-Behçet's (CNS involvement) will be based on objective neurological symptoms that were associated with neuroimaging (CNS and/or medullar MRI) findings suggestive of BD-related CNS involvement. Cerebrospinal fluid (CSF) findings showing aseptic inflammation may be associated.
- Chest X-ray results (postero-anterior and lateral) within 12 weeks prior to inclusion with no evidence of active Tuberculosis, active infection, or malignancy
- For female subjects of child-bearing age, a negative pregnancy test
- For subjects with reproductive potential, a willingness to use contraceptive measures adequate to prevent the subject or the subject's partner from becoming pregnant during the study and 6 months after stopping therapy. Adequate contraceptive measures include hormonal methods used for two or more cycles prior to Inclusion (e.g., oral contraceptive pills, contraceptive patch, or contraceptive vaginal ring), barrier methods (e.g., contraceptive sponge, diaphragm used in conjunction with contraceptive foam or jelly, or condom used in conjunction with contraceptive foam or jelly), intrauterine methods (IUD), sterilization (e.g., tubal ligation or a monogamous relationship with a vasectomized partner), and abstinence.
- A potential subject with a positive interferon-gamma release assay (IGRA) (e.g., QuantiFERON®-TB Gold or T-spot TB® Test) or a positive tuberculin skin test (≤6 months) is eligible if her/his chest X-ray does not show evidence suggestive of active tuberculosis (TB) disease and there are no clinical signs and symptoms of pulmonary and/or extra-pulmonary TB disease. These subjects with a latent TB infection who have not already received a prophylactic TB treatment must agree in advance to complete such a treatment course.
- HIV negative serology and negative HBs Ag test (≤1 month)
Exclusion Criteria:
- Evidence of active Tuberculosis
- HIV or active HBV infection (HBs Ag+).
- Pregnancy or lactation
- Have been taking an oral daily dose of a glucocorticoid of more than 20 mg prednisone equivalent for more than 6 weeks continuously prior to the inclusion visit or taking more than 3000 mg methylprednisolone 4 weeks prior to the inclusion visit
- Alcohol or drug dependance
- Severe renal (creatinine clearance <30ml/min/1,73m2) or pre-existing hemorrhagic cystitis or liver insufficiency (hepatic encephalopathy, ascites)
- Heart failure ≥ stage III / IV NYHA,
- History of malignancy within 5 years prior to Inclusion other than carcinoma in situ of the cervix or excised basal cell or squamous cell carcinoma of the skin.
- History of multiple sclerosis and/or demyelinating disorder
- History of severe allergic or anaphylactic reactions to cyclophosphamide or infliximab
Infectious disease:
- Infection requiring treatment with antibiotics within 2 weeks prior to Inclusion
- History of recurrent infection
Laboratory values assessed during Inclusion:
- Hemoglobin < 8 g/dL
- WBC < 2.0 x 103/mm3
- Platelet count < 70 x 103/mm3
Use of the following systemic treatments during the specified periods:
- Treatment with systemic biologic therapy or with cyclophosphamide within 3 months prior to Inclusion
- if on azathioprine, mycophenolate mofetil, or methotrexate at the time of inclusion, these drugs must be withdrawn prior to receiving the cyclophosphamide or infliximab dose on Day 1
- Any live (attenuated) vaccine within 4 weeks prior inclusion; recombinant or killed virus vaccines are permitted.
- Lack of affiliation to a social security benefit plan (as a beneficiary or assignee)
Sites / Locations
- CHRU Amiens
- Hôpital Avicenne
- CHU Bordeaux
- Hôpital Saint André
- CH Ambroise Paré
- CHU Caen
- Henri Mondor Hospital
- CHU Dijon
- CHU Grenoble
- CHU Bicêtre
- CHRU Lille
- Hôpital de la Croix Rousse
- Hôpital Edouard Herriot
- Hôpital de La Timone
- CH Metz
- CHU Bichat
- CHU Tenon
- Hôpital de La Pitié Salpetriere
- Hôpital Foch
- Hôpital Lariboisière
- Hôpital Saint Antoine
- Hôpital Saint Louis
- CHU Poitiers
- Hôpital Bois Guillaume
- CH Saint-Denis
- CHU Purpan
- CH Valenciennes
Arms of the Study
Arm 1
Arm 2
Arm Type
Experimental
Active Comparator
Arm Label
Infliximab
Cyclophosphamide
Arm Description
Infliximab 5mg/kg intravenously at week 0, 2, 6, 12, and 18
Cyclophosphamide 0.7g/m2 up to 1.2g/m2 intravenously at week 0, 4, 8, 12, 16 and 20
Outcomes
Primary Outcome Measures
Complete clinical response
The complete clinical response is defined by the remission of all affected organs involved at baseline with a prednisone ≤ 0.1mg/kg per day
Secondary Outcome Measures
Complete clinical response
The complete clinical response is defined by the remission of all affected organs involved at baseline with a prednisone ≤ 0.1mg/kg per day
Complete clinical response
The complete clinical response is defined by the remission of all affected organs involved at baseline with a prednisone ≤ 0.1mg/kg per day
Remission of CNS and/or cardiovascular involvement
Remission of CNS and/or cardiovascular involvement
Remission of CNS and/or cardiovascular involvement
Percent meeting the target of ≤ 0.1 mg/day/kg of prednisone
Percent meeting the target of ≤ 0.1 mg/day/kg of prednisone
Mean dose of prednisone
Mean dose of prednisone
Mean dose of prednisone
Cumulative dose of prednisone
Cumulative dose of prednisone
Cumulative dose of prednisone
Time to response onset
C-reactive protein
CRP in blood sample
Time to relapse
Relapse will be defined as the reappearance of clinical and/or paraclinical features of active disease or by the occurrence of new lesions at week 48
Rate of relapse
Time to occurrence of worsening
Worsening will be defined as the progression of preexisting lesions) at week 22 and 48
Rate of worsening
Overall survival
Overall survival
Event Free Survival
Event Free Survival
Frequency of adverse clinical events
Incidence of Treatment related Adverse Events
Severity of adverse clinical events
Change in quality of life
Change in quality of life (QOL) (SF-36V2TM Health Survey)
Change in quality of life
Change in quality of life (QOL) (SF-36V2TM Health Survey)
Changes in CNS involvement
Changes in CNS involvement on physical exam, and cerebral and/or medullar MRI.
Changes in CNS involvement
Changes in CNS involvement on physical exam, and cerebral and/or medullar MRI.
Changes in vascular involvement
Changes in vascular involvement on physical exam, vascular Doppler US, and angio-CT imaging and biologically (normalization of C reactive protein)
Changes in vascular involvement
Changes in vascular involvement on physical exam, vascular Doppler US, and angio-CT imaging and biologically (normalization of C reactive protein)
Changes in cardiological involvement
Changes in cardiological involvement on physical exam, echocardiography (normalization of left ventricular function and/or disappearance of cardiac thrombosis), and cardiac magnetic resonance imaging (disappearance of gadolinium enhancement and normalization of left ventricular function) and biologically (normalization of troponin and of C reactive protein)
Changes in cardiological involvement
Changes in cardiological involvement on physical exam, echocardiography (normalization of left ventricular function and/or disappearance of cardiac thrombosis), and cardiac magnetic resonance imaging (disappearance of gadolinium enhancement and normalization of left ventricular function) and biologically (normalization of troponin and of C reactive protein)
Serum concentration measurement of TNFa inhibitor at week 22
Change in Behcet's Disease Current Activity Form
Change in Behcet's Disease Current Activity Form
Full Information
NCT ID
NCT03371095
First Posted
December 7, 2017
Last Updated
June 30, 2023
Sponsor
Assistance Publique - Hôpitaux de Paris
1. Study Identification
Unique Protocol Identification Number
NCT03371095
Brief Title
Induction Therapy With Anti-TNFα vs Cyclophosphamide in Severe Behçet Disease
Acronym
ITAC
Official Title
Multicenter, Randomized, Prospective Trial Comparing the Efficacy and Safety of Infliximab to That of Cyclophosphamide in Severe Behçet's Disease. ITAC : Induction Therapy With Anti-TNFα vs Cyclophosphamide in Severe Behçet Disease
Study Type
Interventional
2. Study Status
Record Verification Date
December 2017
Overall Recruitment Status
Completed
Study Start Date
May 25, 2018 (Actual)
Primary Completion Date
December 24, 2021 (Actual)
Study Completion Date
April 11, 2022 (Actual)
3. Sponsor/Collaborators
Responsible Party, by Official Title
Sponsor
Name of the Sponsor
Assistance Publique - Hôpitaux de Paris
4. Oversight
Studies a U.S. FDA-regulated Drug Product
No
Studies a U.S. FDA-regulated Device Product
No
5. Study Description
Brief Summary
Behçet's disease (BD) is a systemic vasculitis of arterial and venous vessels of any size, involving young patients (from 15 to 45 years). BD significantly increases morbidity and mortality. Therapeutic management of BD depends on the clinical presentation and organ involved. Although colchicine, nonsteroidal antiinflammatory agents and topical treatments are often sufficient for mucocutaneous and joint involvement, more aggressive approach with immunosuppressive agents is warranted for severe manifestations. Early recognition and vigorous use of immunosuppressives with high dose steroids have changed the prognosis of patients with severe BD. BD is a severe systemic vasculitis leading to blindness in up to 20% at 4 years and a 5-year mortality rate of 15% in patients with major vessel or neurological involvement. Cyclophosphamide has been used for life-threatening BD for 40 years. However, the outcome of severe complications of BD is poor. The European League Against Rheumatism (EULAR) recommendation for the management of BD advocated cyclophosphamide plus glucocorticoids for life-threatening manifestations (i.e neurological and/or major vessel involvement). TNFa antagonists have been used with success in severe and/or resistant cases. In addition, the incidence of blindness in BD has been dramatically reduced in the recent years with the use of anti-TNF. However, there is no firm evidence or randomized controlled trials directly addressing the best induction immunosuppressive therapy in severe BD manifestations. The investigators therefore aimed to assess the best induction therapy in severe and difficult to treat BD patients. The investigators hypothesize that up to 70% of the patients with life-threatening manifestations of BD receiving these compounds [anti-TNFa or cyclophosphamide] will achieve a complete remission of BD at 6 months and with less than 0.1 mg/kg/day of prednisone.
ITAC, is the first randomized prospective, head to head study, comparing infliximab, to cyclophosphamide in severe manifestations of BD. There is no firm evidence or randomized controlled trials directly addressing the best induction immunosuppressive therapy in severe BD. Cyclophosphamide failed to demonstrate sustainable remission over 70 % of life threatening BD cases. There is little published information on use of immunosuppressants other than cyclophosphamide for severe BD. TNFa antagonists have been used with success in severe and/or resistant cases. TNFa expression correlates with BD activity and other immunological data provide a strong rationale for targeting BD with biologics. Despite a strong rationale, these compounds are not yet approved in BD, which guarantees the innovative nature of this study that aims selecting or dropping any arm when evidence of efficacy already exists.
6. Conditions and Keywords
Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Behcet's Disease, Vasculitis
Keywords
Behcet's Disease, Vasculitis, Biotherapy, immunosuppressant, Infliximab
7. Study Design
Primary Purpose
Treatment
Study Phase
Phase 3
Interventional Study Model
Parallel Assignment
Masking
None (Open Label)
Allocation
Randomized
Enrollment
53 (Actual)
8. Arms, Groups, and Interventions
Arm Title
Infliximab
Arm Type
Experimental
Arm Description
Infliximab 5mg/kg intravenously at week 0, 2, 6, 12, and 18
Arm Title
Cyclophosphamide
Arm Type
Active Comparator
Arm Description
Cyclophosphamide 0.7g/m2 up to 1.2g/m2 intravenously at week 0, 4, 8, 12, 16 and 20
Intervention Type
Drug
Intervention Name(s)
Infliximab
Intervention Description
Use of infliximab instead of cyclophosphamide
Intervention Type
Drug
Intervention Name(s)
Cyclophosphamide
Intervention Description
Use of cyclophosphamide
Primary Outcome Measure Information:
Title
Complete clinical response
Description
The complete clinical response is defined by the remission of all affected organs involved at baseline with a prednisone ≤ 0.1mg/kg per day
Time Frame
At week 22 after randomization
Secondary Outcome Measure Information:
Title
Complete clinical response
Description
The complete clinical response is defined by the remission of all affected organs involved at baseline with a prednisone ≤ 0.1mg/kg per day
Time Frame
At week 12 after randomization
Title
Complete clinical response
Description
The complete clinical response is defined by the remission of all affected organs involved at baseline with a prednisone ≤ 0.1mg/kg per day
Time Frame
At week 48 after randomization
Title
Remission of CNS and/or cardiovascular involvement
Time Frame
At week 12 after randomization
Title
Remission of CNS and/or cardiovascular involvement
Time Frame
At week 22 after randomization
Title
Remission of CNS and/or cardiovascular involvement
Time Frame
At week 48 after randomization
Title
Percent meeting the target of ≤ 0.1 mg/day/kg of prednisone
Time Frame
At week 22 after randomization
Title
Percent meeting the target of ≤ 0.1 mg/day/kg of prednisone
Time Frame
At week 48 after randomization
Title
Mean dose of prednisone
Time Frame
At week 12 after randomization
Title
Mean dose of prednisone
Time Frame
At week 22 after randomization
Title
Mean dose of prednisone
Time Frame
At week 48 after randomization
Title
Cumulative dose of prednisone
Time Frame
At week 12 after randomization
Title
Cumulative dose of prednisone
Time Frame
At week 22 after randomization
Title
Cumulative dose of prednisone
Time Frame
At week 48 after randomization
Title
Time to response onset
Time Frame
At week 48 after randomization
Title
C-reactive protein
Description
CRP in blood sample
Time Frame
Every 4 weeks
Title
Time to relapse
Description
Relapse will be defined as the reappearance of clinical and/or paraclinical features of active disease or by the occurrence of new lesions at week 48
Time Frame
At week 48 after randomization
Title
Rate of relapse
Time Frame
At week 48 after randomization
Title
Time to occurrence of worsening
Description
Worsening will be defined as the progression of preexisting lesions) at week 22 and 48
Time Frame
At week 48 after randomization
Title
Rate of worsening
Time Frame
At week 48 after randomization
Title
Overall survival
Time Frame
At week 22 after randomization
Title
Overall survival
Time Frame
At week 48 after randomization
Title
Event Free Survival
Time Frame
At week 22 after randomization
Title
Event Free Survival
Time Frame
At week 48 after randomization
Title
Frequency of adverse clinical events
Description
Incidence of Treatment related Adverse Events
Time Frame
At week 22 after randomization
Title
Severity of adverse clinical events
Time Frame
At week 22 after randomization
Title
Change in quality of life
Description
Change in quality of life (QOL) (SF-36V2TM Health Survey)
Time Frame
At week 12 after randomization
Title
Change in quality of life
Description
Change in quality of life (QOL) (SF-36V2TM Health Survey)
Time Frame
At week 22 after randomization
Title
Changes in CNS involvement
Description
Changes in CNS involvement on physical exam, and cerebral and/or medullar MRI.
Time Frame
At week 12 after randomization
Title
Changes in CNS involvement
Description
Changes in CNS involvement on physical exam, and cerebral and/or medullar MRI.
Time Frame
At week 22 after randomization
Title
Changes in vascular involvement
Description
Changes in vascular involvement on physical exam, vascular Doppler US, and angio-CT imaging and biologically (normalization of C reactive protein)
Time Frame
At week 12 after randomization
Title
Changes in vascular involvement
Description
Changes in vascular involvement on physical exam, vascular Doppler US, and angio-CT imaging and biologically (normalization of C reactive protein)
Time Frame
At week 22 after randomization
Title
Changes in cardiological involvement
Description
Changes in cardiological involvement on physical exam, echocardiography (normalization of left ventricular function and/or disappearance of cardiac thrombosis), and cardiac magnetic resonance imaging (disappearance of gadolinium enhancement and normalization of left ventricular function) and biologically (normalization of troponin and of C reactive protein)
Time Frame
At week 12 after randomization
Title
Changes in cardiological involvement
Description
Changes in cardiological involvement on physical exam, echocardiography (normalization of left ventricular function and/or disappearance of cardiac thrombosis), and cardiac magnetic resonance imaging (disappearance of gadolinium enhancement and normalization of left ventricular function) and biologically (normalization of troponin and of C reactive protein)
Time Frame
At week 22 after randomization
Title
Serum concentration measurement of TNFa inhibitor at week 22
Time Frame
At week 12 after randomization
Title
Change in Behcet's Disease Current Activity Form
Time Frame
At week 12 after randomization
Title
Change in Behcet's Disease Current Activity Form
Time Frame
At week 22 after randomization
10. Eligibility
Sex
All
Minimum Age & Unit of Time
12 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria:
Age ≥ 12 years old
Written inform consent (Informed Consent should be obtained from the legal guardian in accordance with regional laws or regulations for patients 12 to 17 years of age)
Diagnosis of BD according to international criteria for BD (ICBD) (see Appendix 1).
Life threatening active BD defined as 1 of the following disease categories and according to the validated international definition:
Major vessel disease: arterial aneurysms or arterial stenosis, myocarditis and/or major deep vein thrombosis (i.e. inferior vena cava, superior vena cava, cardiac cavity thrombosis, pulmonary embolism, supra-hepatic vessels, renal and mesenteric vessels). Diagnosis of major vessel involvement will be done using vascular doppler sonography, echocardiography, angio-CT scan and/or cardiac magnetic resonance imaging (MRI).
Central nervous system involvement: encephalitis or meningoencephalitis or myelitis. The diagnosis of neuro-Behçet's (CNS involvement) will be based on objective neurological symptoms that were associated with neuroimaging (CNS and/or medullar MRI) findings suggestive of BD-related CNS involvement. Cerebrospinal fluid (CSF) findings showing aseptic inflammation may be associated.
Chest X-ray results (postero-anterior and lateral) within 12 weeks prior to inclusion with no evidence of active Tuberculosis, active infection, or malignancy
For female subjects of child-bearing age, a negative pregnancy test
For subjects with reproductive potential, a willingness to use contraceptive measures adequate to prevent the subject or the subject's partner from becoming pregnant during the study and 6 months after stopping therapy. Adequate contraceptive measures include hormonal methods used for two or more cycles prior to Inclusion (e.g., oral contraceptive pills, contraceptive patch, or contraceptive vaginal ring), barrier methods (e.g., contraceptive sponge, diaphragm used in conjunction with contraceptive foam or jelly, or condom used in conjunction with contraceptive foam or jelly), intrauterine methods (IUD), sterilization (e.g., tubal ligation or a monogamous relationship with a vasectomized partner), and abstinence.
A potential subject with a positive interferon-gamma release assay (IGRA) (e.g., QuantiFERON®-TB Gold or T-spot TB® Test) or a positive tuberculin skin test (≤6 months) is eligible if her/his chest X-ray does not show evidence suggestive of active tuberculosis (TB) disease and there are no clinical signs and symptoms of pulmonary and/or extra-pulmonary TB disease. These subjects with a latent TB infection who have not already received a prophylactic TB treatment must agree in advance to complete such a treatment course.
HIV negative serology and negative HBs Ag test (≤1 month)
Exclusion Criteria:
Evidence of active Tuberculosis
HIV or active HBV infection (HBs Ag+).
Pregnancy or lactation
Have been taking an oral daily dose of a glucocorticoid of more than 20 mg prednisone equivalent for more than 6 weeks continuously prior to the inclusion visit or taking more than 3000 mg methylprednisolone 4 weeks prior to the inclusion visit
Alcohol or drug dependance
Severe renal (creatinine clearance <30ml/min/1,73m2) or pre-existing hemorrhagic cystitis or liver insufficiency (hepatic encephalopathy) or urinary obstruction
Heart failure ≥ stage III / IV NYHA,
History of malignancy within 5 years prior to Inclusion other than carcinoma in situ of the cervix or excised basal cell or squamous cell carcinoma of the skin.
History of multiple sclerosis and/or demyelinating disorder
History of severe allergic or anaphylactic reactions to cyclophosphamide or infliximab
Infectious disease:
Infection requiring treatment with intravenous antibiotics within 2 weeks prior to Inclusion
History of recurrent infection
Laboratory values assessed during Inclusion:
Hemoglobin < 8 g/dL
WBC < 2.0 x 103/mm3
Platelet count < 70 x 103/mm3
Use of the following systemic treatments during the specified periods:
Treatment with systemic biologic therapy or with cyclophosphamide within 3 months prior to Inclusion
if on azathioprine, mycophenolate mofetil, or methotrexate at the time of inclusion, these drugs must be withdrawn prior to receiving the cyclophosphamide or infliximab dose on Day 1
Any live (attenuated) vaccine within 4 weeks prior inclusion; recombinant or killed virus vaccines are permitted.
Lack of affiliation to a social security benefit plan (as a beneficiary or assignee), patients affiliated to universal medical coverage (CMU) are eligible for the study
Facility Information:
Facility Name
CHRU Amiens
City
Amiens
Country
France
Facility Name
Hôpital Avicenne
City
Bobigny
Country
France
Facility Name
CHU Bordeaux
City
Bordeaux
Country
France
Facility Name
Hôpital Saint André
City
Bordeaux
Country
France
Facility Name
CH Ambroise Paré
City
Boulogne-Billancourt
Country
France
Facility Name
CHU Caen
City
Caen
Country
France
Facility Name
Henri Mondor Hospital
City
Créteil
Country
France
Facility Name
CHU Dijon
City
Dijon
Country
France
Facility Name
CHU Grenoble
City
Grenoble
Country
France
Facility Name
CHU Bicêtre
City
Le Kremlin-Bicêtre
Country
France
Facility Name
CHRU Lille
City
Lille
Country
France
Facility Name
Hôpital de la Croix Rousse
City
Lyon
Country
France
Facility Name
Hôpital Edouard Herriot
City
Lyon
Country
France
Facility Name
Hôpital de La Timone
City
Marseille
Country
France
Facility Name
CH Metz
City
Metz
Country
France
Facility Name
CHU Bichat
City
Paris
Country
France
Facility Name
CHU Tenon
City
Paris
Country
France
Facility Name
Hôpital de La Pitié Salpetriere
City
Paris
Country
France
Facility Name
Hôpital Foch
City
Paris
Country
France
Facility Name
Hôpital Lariboisière
City
Paris
Country
France
Facility Name
Hôpital Saint Antoine
City
Paris
Country
France
Facility Name
Hôpital Saint Louis
City
Paris
Country
France
Facility Name
CHU Poitiers
City
Poitiers
Country
France
Facility Name
Hôpital Bois Guillaume
City
Rouen
Country
France
Facility Name
CH Saint-Denis
City
Saint-Denis
Country
France
Facility Name
CHU Purpan
City
Toulouse
Country
France
Facility Name
CH Valenciennes
City
Valenciennes
Country
France
12. IPD Sharing Statement
Plan to Share IPD
Undecided
Learn more about this trial
Induction Therapy With Anti-TNFα vs Cyclophosphamide in Severe Behçet Disease
We'll reach out to this number within 24 hrs