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NCT02404350 Clinical Trial

Study to Demonstrate the Efficacy (Including Inhibition of Structural Damage), Safety and Tolerability up to 2 Years of Secukinumab in Active Psoriatic Arthritis

Psoriatic Arthritis Clinical Trial

FUTURE5

Official title:
A Phase III, Randomized, Double-blind, Placebo Controlled Multi-center Study of Subcutaneous Secukinumab (150 mg and 300 mg) in Prefilled Syringe to Demonstrate Efficacy (Including Inhibition of Structural Damage), Safety, and Tolerability up to 2 Years in Subjects With Active Psoriatic Arthritis (FUTURE 5)

Clinical Trial Details — Status: Completed

Administrative data
NCT number NCT02404350
Other study ID # CAIN457F2342
Secondary ID 2015-000050-3802
Status Completed
Phase Phase 3
First received
Last updated
Start date August 31, 2015
Est. completion date January 24, 2019

Study information
Verified date April 2020
Source Novartis
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The purpose of this study was to demonstrate efficacy including effect on inhibition of progression of structural damage, safety and tolerability up to 2 years with primary focus at Week 16 (week 24 for structural damage), to support the use of secukinumab pre-filled syringe (PFS) by subcutaneous (s.c.) self-administration with or without loading regimen in subjects with active Psoriatic Arthritis (PsA) despite current or previous NSAID, DMARD therapy and/or previous anti-TNFα therapy. Long term efficacy up to 2 years was based on signs and symptoms of joint/bone structure preservation (X-ray) and improvement in physical function measured by Health Assessment Questionnaire - Disability Index (HAQ-DI©), as well as skin and nail improvement for psoriasis signs.

Description:

This multicenter study uses a randomized, double-blind, placebo-controlled, parallel-group design. A screening period (SCR) running up to 10 weeks before randomization will be used to assess subject eligibility followed by 104 weeks of treatment.

At BSL approximately 990 subjects whose eligibility is confirmed will be randomized to one of four treatment groups in 2:2:2:3 ratio:

- Group 1 - secukinumab 150 mg s.c. without loading regimen

- Group 2 - secukinumab 150 mg s.c. with loading dose regimen

- Group 3 - secukinumab 300 mg s.c. with loading dose regimen

- Group 4 - Placebo s.c. NOTE: Group 4 is split into 2 treatment arms, detailed description below. At randomization, subjects will be stratified on the basis of previous anti-TNF therapy as TNFα inhibitor naïve (TNF-naïve) or TNFα inhibitor inadequate responders (TNF-IR).

At each study treatment visit, one (for secukinumab 150 mg) or two (for secukinumab 300 mg) s.c. injections in the form of PFS will be administered, since secukinumab is available in 1.0 mL (150 mg) PFSs. Placebo to secukinumab is also available in 1.0 mL to match the active drug.

At Week 16, subjects who have been randomized to secukinumab groups at BSL (Groups 1-3) will be classified as either responders (≥20% improvement from BSL in both tender joint count (TJC) and swollen joint counts (SJC)) or non-responders (<20% improvement from BSL TJC or SJC), however they will continue on the same treatment irrespective of their response status.

At Week 16, subjects who have been randomized to placebo at BSL (Group 4) will be classified as either responders (≥20% improvement from BSL in both TJC and SJC) or non-responders (<20% improvement from BSL TJC or SJC):

- Subjects who are non-responders will receive either secukinumab 150 mg or 300 mg s.c. every 4 weeks starting at Week 16 (as dictated by treatment sequence assigned to these subjects at BSL).

- Subjects who are responders will continue to receive placebo every 4 weeks. Starting Week 24, these subjects will receive either secukinumab 150 mg s.c. or 300 mg s.c. every 4 weeks starting at Week 24 (as dictated by treatment sequence assigned to these subjects at BSL).

At Week 24, the assessments to address the primary objective will be performed. As described above, subjects who are still receiving placebo s.c. injection will receive either secukinumab 150 mg s.c. or 300 mg s.c. every 4 weeks starting at Week 24 (as dictated by treatment sequence assigned to these subjects at BSL).

At week 52, based on Investigator's decision, the subjects on a 150 mg dose whose signs and symptoms do not show satisfactory response have the possibility to be allocated to secukinumab 300 mg s.c.

After the Week 52 database lock and analyses have been completed, site personnel and subjects will be unblinded to the original randomized treatment (sequence) assignment at randomization. In addition, treatment will be given open-label in order to eliminate the placebo injection. The subject will continue to receive the same active dose of secukinumab as open-label treatment administered until Week 100.

Recruitment information / eligibility
Status Completed
Enrollment 997
Est. completion date January 24, 2019
Est. primary completion date August 16, 2017
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria:

Diagnosis of PsA classified by CASPAR criteria and with symptoms for at least 6 months with moderate to severe PsA who must have at BSL =3 tender joints out of 78 and =3 swollen joints out of 76 (dactylitis of a digit counts as one joint each).

- Rheumatoid factor (RF) and anti-cyclic citrullinated peptide (anti-CCP) antibodies negative at screening.

- Diagnosis of active plaque psoriasis or nail changes consistent with psoriasis or a documented history of plaque psoriasis.

- Subjects with PsA should have taken NSAIDs for at least 4 weeks prior to randomization with inadequate control of symptoms or at least one dose if stopped due to intolerance to NSAIDs.-Subjects who are regularly taking NSAIDs as part of their PsA therapy are required to be on a stable dose for at least 2 weeks before study randomization and should remain on a stable dose up to Week 24.

- Subjects taking corticosteroids must be on a stable dose of =10 mg/day prednisone or equivalent for at least 2 weeks before randomization and should remain on a stable dose up to Week 24.

- Subjects taking MTX (= 25 mg/week) are allowed to continue their medication if the dose is stable for at least 4 weeks before randomization and should remain on a stable dose up to Week 52.

- Subjects on MTX must be on folic acid supplementation at randomization.

- Subjects who are on a DMARD other than MTX must discontinue the DMARD 4 weeks prior to randomization visit except for leflunomide, which has to be discontinued for 8 weeks prior to randomization unless a cholestyramine wash-out has been performed.

- Subjects who have been on a TNFa inhibitor must have experienced an inadequate response to previous or current treatment with a TNFa inhibitor given at an approved dose for at least 3 months or have stopped treatment due to safety/tolerability problems after at least one administration of a TNFa inhibitor.

- Subjects who have previously been treated with TNFa inhibitors (investigational or approved) will be allowed entry into study after appropriate wash-out period prior to randomization

Exclusion Criteria:

Chest X-ray or chest MRI with evidence of ongoing infectious or malignant process. - Subjects taking high potency opioid analgesics.

- Previous exposure to secukinumab or other biologic drug directly targeting IL-17 or IL-17 receptor. - Ongoing use of prohibited psoriasis treatments / medications (e.g., topical corticosteroids, UV therapy) at randomization.

- Any intramuscular or intravenous or intra-articular corticosteroid treatment within 4 weeks before randomization.

- Subjects who have ever received biologic immunomodulating agents except for those targeting TNFa (investigational or approved).

- Previous treatment with any cell-depleting therapies including but not limited to anti- CD20, investigational agents

- Other protocol-defined exclusion criteria do apply

Study Design

Related Conditions & MeSH terms

Intervention

Biological:
Secukinumab
Anti IL-17a monoclonal antibody

Locations
Country Name City State
Argentina Novartis Investigative Site Caba Buenos Aires
Argentina Novartis Investigative Site San Miguel de Tucuman Tucuman
Argentina Novartis Investigative Site Tucuman
Austria Novartis Investigative Site Graz
Austria Novartis Investigative Site Vienna
Austria Novartis Investigative Site Vienna
Austria Novartis Investigative Site Vienna
Canada Novartis Investigative Site Sainte-Foy Quebec
Canada Novartis Investigative Site St. John's Newfoundland and Labrador
Canada Novartis Investigative Site Trois-Rivieres Quebec
Canada Novartis Investigative Site Vancouver British Columbia
Canada Novartis Investigative Site Victoria British Columbia
Canada Novartis Investigative Site Winnipeg Manitoba
Chile Novartis Investigative Site Santiago
Chile Novartis Investigative Site Vitacura Santiago
Czechia Novartis Investigative Site Bruntal Czech Republic
Czechia Novartis Investigative Site Ostrava Czech Republic
Czechia Novartis Investigative Site Praha 11 Czech Republic
Czechia Novartis Investigative Site Praha 2 Czech Republic
Czechia Novartis Investigative Site Praha 4 Czech Republic
Czechia Novartis Investigative Site Praha 4 Czech Republic
Czechia Novartis Investigative Site Uherske Hradiste
Denmark Novartis Investigative Site Odense
Estonia Novartis Investigative Site Tartu
Finland Novartis Investigative Site Hyvinkaa
Germany Novartis Investigative Site Aachen
Germany Novartis Investigative Site Bad Abbach
Germany Novartis Investigative Site Berlin
Germany Novartis Investigative Site Berlin
Germany Novartis Investigative Site Germering
Germany Novartis Investigative Site Gommern
Germany Novartis Investigative Site Gottingen
Germany Novartis Investigative Site Hamburg
Germany Novartis Investigative Site Hamburg
Germany Novartis Investigative Site Herne
Germany Novartis Investigative Site Leipzig
Germany Novartis Investigative Site Lubeck
Germany Novartis Investigative Site Nienburg
Greece Novartis Investigative Site Athens GR
Greece Novartis Investigative Site Athens
Greece Novartis Investigative Site Athens
Greece Novartis Investigative Site Patras
Greece Novartis Investigative Site Thessaloniki GR
Guatemala Novartis Investigative Site Guatemala City
Guatemala Novartis Investigative Site Guatemala City
Hungary Novartis Investigative Site Budapest
Hungary Novartis Investigative Site Budapest
Hungary Novartis Investigative Site Eger
Hungary Novartis Investigative Site Kistarcsa
Hungary Novartis Investigative Site Szekesfehervar
Hungary Novartis Investigative Site Veszprem
India Novartis Investigative Site Ahmedabad Gujarat
India Novartis Investigative Site Mumbai Maharashtra
India Novartis Investigative Site Nashik Maharashtra
India Novartis Investigative Site New Delhi
India Novartis Investigative Site Pune Maharashtra
India Novartis Investigative Site Secunderabad Andhra Pradesh
Ireland Novartis Investigative Site Dublin 4
Israel Novartis Investigative Site Ashkelon
Israel Novartis Investigative Site Haifa
Israel Novartis Investigative Site Kfar Saba
Israel Novartis Investigative Site Petach Tikva
Israel Novartis Investigative Site Ramat Gan
Israel Novartis Investigative Site Tel Aviv
Italy Novartis Investigative Site Brescia BS
Italy Novartis Investigative Site Palermo PA
Italy Novartis Investigative Site Pavia PV
Italy Novartis Investigative Site Potenza PZ
Italy Novartis Investigative Site Udine UD
Latvia Novartis Investigative Site Liepaja
Latvia Novartis Investigative Site Riga
Latvia Novartis Investigative Site Riga
Latvia Novartis Investigative Site Riga LV
Latvia Novartis Investigative Site Valmiera
Lithuania Novartis Investigative Site Kaunas LT
Lithuania Novartis Investigative Site Kaunas LT
Lithuania Novartis Investigative Site Klaipeda
Lithuania Novartis Investigative Site Siauliai
Lithuania Novartis Investigative Site Vilnius
Lithuania Novartis Investigative Site Vilnius
Mexico Novartis Investigative Site Merida Yucatan
Mexico Novartis Investigative Site Metepec Estado De Mexico
Mexico Novartis Investigative Site Mexicali Baja California
Mexico Novartis Investigative Site Mexico Distrito Federal
Mexico Novartis Investigative Site San Luis Potosi
Netherlands Novartis Investigative Site Maastricht
Netherlands Novartis Investigative Site Rotterdam
Netherlands Novartis Investigative Site Schiedam
Netherlands Novartis Investigative Site Utrecht
Philippines Novartis Investigative Site Manila Metro Manila
Philippines Novartis Investigative Site Manila
Philippines Novartis Investigative Site Quezon City
Russian Federation Novartis Investigative Site Chelyabinsk
Russian Federation Novartis Investigative Site Chelyabinsk
Russian Federation Novartis Investigative Site Ekaterinburg
Russian Federation Novartis Investigative Site Ekaterinburg
Russian Federation Novartis Investigative Site Kazan
Russian Federation Novartis Investigative Site Kemerovo
Russian Federation Novartis Investigative Site Moscow
Russian Federation Novartis Investigative Site Nizhniy Novgorod
Russian Federation Novartis Investigative Site Nizhny Novgorod
Russian Federation Novartis Investigative Site Orenburg
Russian Federation Novartis Investigative Site Rostov on Don
Russian Federation Novartis Investigative Site Saint-Petersburg
Russian Federation Novartis Investigative Site Smolensk
Russian Federation Novartis Investigative Site St-Petersburg
Russian Federation Novartis Investigative Site Yaroslavl
Spain Novartis Investigative Site Alicante Comunidad Valenciana
Spain Novartis Investigative Site Baracaldo Vizcaya
Spain Novartis Investigative Site Barcelona
Spain Novartis Investigative Site Barcelona Catalunya
Spain Novartis Investigative Site Barcelona Catalunya
Spain Novartis Investigative Site Bilbao Pais Vasco
Spain Novartis Investigative Site Cordoba Andalucia
Spain Novartis Investigative Site Madrid
Spain Novartis Investigative Site Sabadell Barcelona
Spain Novartis Investigative Site Sant Joan Despi Barcelona
Spain Novartis Investigative Site Santiago de Compostela Galicia
Spain Novartis Investigative Site Valencia Comunidad Valenciana
Spain Novartis Investigative Site Vigo Pontevedra
Sweden Novartis Investigative Site Stockholm
Thailand Novartis Investigative Site Bangkok
Thailand Novartis Investigative Site Bangkoknoi Bangkok
Thailand Novartis Investigative Site Chiang Mai
Thailand Novartis Investigative Site Khon Kaen THA
Thailand Novartis Investigative Site Songkhla Hat Yai
United Kingdom Novartis Investigative Site Basingstoke Hampshire
United Kingdom Novartis Investigative Site Bath
United Kingdom Novartis Investigative Site Bradford West Yorkshire
United Kingdom Novartis Investigative Site Christchurch Dorset
United Kingdom Novartis Investigative Site Dundee
United Kingdom Novartis Investigative Site Eastbourne
United Kingdom Novartis Investigative Site Edinburgh
United Kingdom Novartis Investigative Site Glasgow
United Kingdom Novartis Investigative Site Inverness Invernesshire
United Kingdom Novartis Investigative Site Leicester
United Kingdom Novartis Investigative Site London
United Kingdom Novartis Investigative Site London
United Kingdom Novartis Investigative Site London
United Kingdom Novartis Investigative Site London England
United Kingdom Novartis Investigative Site Manchester
United Kingdom Novartis Investigative Site Oxford
United Kingdom Novartis Investigative Site Portsmouth
United Kingdom Novartis Investigative Site Salford Manchester
United Kingdom Novartis Investigative Site Stoke on Trent Staffordshire
United Kingdom Novartis Investigative Site Truro Cornwall
United Kingdom Novartis Investigative Site Wigan
United States Novartis Investigative Site Aurora Colorado
United States Novartis Investigative Site Brandon Florida
United States Novartis Investigative Site Brooklyn New York
United States Novartis Investigative Site Coeur d'Alene Idaho
United States Novartis Investigative Site Denver Colorado
United States Novartis Investigative Site Duncansville Pennsylvania
United States Novartis Investigative Site Jackson Tennessee
United States Novartis Investigative Site Kingsport Tennessee
United States Novartis Investigative Site Mesquite Texas
United States Novartis Investigative Site Oklahoma City Oklahoma
United States Novartis Investigative Site Oklahoma City Oklahoma
United States Novartis Investigative Site Portland Oregon
United States Novartis Investigative Site Rochester New York
United States Novartis Investigative Site Seattle Washington
United States Novartis Investigative Site Seattle Washington
United States Novartis Investigative Site Seattle Washington
United States Novartis Investigative Site Shreveport Louisiana
United States Novartis Investigative Site Spokane Washington
United States Novartis Investigative Site Tampa Florida
United States Novartis Investigative Site Upland California
United States Novartis Investigative Site Wexford Pennsylvania
United States Novartis Investigative Site Wyomissing Pennsylvania
Vietnam Novartis Investigative Site Hanoi
Vietnam Novartis Investigative Site Ho Chi Minh
Vietnam Novartis Investigative Site Ho Chi Minh VNM

Sponsors (1)
Lead Sponsor Collaborator
Novartis Pharmaceuticals

Countries where clinical trial is conducted

United States,  Vietnam,  Argentina,  Austria,  Canada,  Chile,  Czechia,  Denmark,  Estonia,  Finland,  Germany,  Greece,  Guatemala,  Hungary,  India,  Ireland,  Israel,  Italy,  Latvia,  Lithuania,  Mexico,  Netherlands,  Philippines,  Russian Federation,  Spain,  Sweden,  Thailand,  United Kingdom, 

References & Publications (1)

Mease P, van der Heijde D, Landewé R, Mpofu S, Rahman P, Tahir H, Singhal A, Boettcher E, Navarra S, Meiser K, Readie A, Pricop L, Abrams K. Secukinumab improves active psoriatic arthritis symptoms and inhibits radiographic progression: primary results fr — View Citation

Outcome
Type Measure Description Time frame Safety issue
Primary Percentage of Participants With Active Psoriatic Arthritis (PsA) Achieving an American College of Rheumatology Response 20 (ACR20) at Week 16 ACR20 response was defined as having a positive clinical response to treatment (individual improvement) in disease activity if the participant had at least 20% improvement based on tender 78-joint count, swollen 76-joint count and at least 20% improvement in 3 of the following 5 measures: participant's assessment of PsA pain, patient's global assessment of disease activity, physician's global assessment of disease activity, participant's self-assessed disability (Health Assessment Questionnaire Disability Index (HAQ-DI) score), and acute phase reactant evaluated as (high sensitivity c-reactive protein (hsCRP) or erythrocyte sedimentation rate (ESR)). Week 16
Secondary Change From Baseline to Week 24 With Secukinumab Compared With Placebo for Joint/Bone Structural Damage (Using Van Der Heijde Modified Total Sharp Score (mTSS)) PsA modified vdH-mTSS scoring method was used to assess bone erosion & joint space narrowing (JSN) in hands & feet; that included the 2nd through 5th distal interphalangeal (DIP) joints of each hand. Maximum score for erosions was 5 in joints of the hands and 10 in joints of the feet with 0=no erosions, 1=discrete erosion, 2=large erosion not passing the mid-line, and 3=large erosion passing the mid-line. JSN is: 0=normal, 1=asymmetrical or minimal narrowing up to a maximum of 25%, 2 = definite narrowing with loss of up to 50% of the normal space, 3 = definite narrowing with loss of 50-99% of the normal space, and 4 = absence of a joint space. Maximum erosion score is 320 (200 for the hands and 120 for the feet), and the max total JSN score is 208 (160 for the hands and 48 for the feet). Total radiographic score (hands & feet combined) ranges from 0 to 528, where higher scores indicate more articular damage Baseline, Week 24
Secondary Count and Percentage of Patients Achieving Psoriatic Area and Severity Index 75 (PASI75) Response The efficacy of secukinumab 150 mg (with or without loading regimen), or 300 mg (with loading regimen) at Week 16 compared with placebo based on the proportion of patients achieving Psoriatic Area and Severity Index 75 (PASI75) response. Week 16
Secondary Count and Percentage of Patients Achieving Psoriatic Area and Severity Index 90 (PASI90) Response The efficacy of secukinumab 150 mg (with or without loading regimen), or 300 mg (with loading regimen) at Week 16 compared with placebo based on the proportion of patients achieving Psoriatic Area and Severity Index 90 (PASI90) response. 16 weeks
Secondary Count and Percentage of Patients Achieving an ACR50 Response ACR 50 Response is a measure based on American College of Rheumatology criteria of at least a 50% improvement in the number of tender and swollen joints, and a 50% improvement in at least 3 of the following: the patient's global assessment of disease status; the patient's assessment of pain; the patient's assessment of function measured using the Stanford Health Assessment Questionnaire the physician's global assessment of disease status; serum C-reactive protein levels. 16 weeks
Secondary Change From Baseline in HAQ-DI© Score The change (within treatment) on secukinumab 150 mg (with or without loading regimen), or 300 mg (with loading regimen), at Week 16 compared with placebo for the disease activity assessed by the changes in The Health Assessment Questionnaire disability index (HAQ-DI) relative to baseline. 16 weeks
Secondary Change From Baseline in Disease Activity Score for 28 Joints (DAS28-CRP) (Utilizing High Sensitivity C-Reactive Protein (hsCRP)) The improvement on secukinumab 150 mg (with or without loading regimen), or 300 mg (with loading regimen) at Week 16 compared with placebo for the disease activity assessed by the changes in Disease Activity Score for 28 joints (DAS28-CRP) (utilizing High sensitivity C-Reactive Protein (hsCRP)) relative to baseline.
Scores range from 0 (no difficulty) to 3 (unable to do)		 16 weeks
Secondary Count and Percentage of Patients With Enthesitis in the Subset of Patients Who Had Enthesitis at Baseline The efficacy of secukinumab pooled regimen (150 mg with or without loading regimen, and 300 mg with loading regimen) at Week 16 compared with placebo based on the proportion of patients with enthesitis in the subset of patients who had enthesitis at baseline 16 weeks
Secondary Count and Percentage of Participants With Dactylitis in the Subset of Patients Who Have Dactylitis at Baseline The efficacy of secukinumab pooled regimen (150 mg with or without loading regimen, and 300 mg with loading regimen) at Week 16 compared with placebo based on the proportion of patients with dactylitis in the subset of patients who have dactylitis at baseline 16 weeks
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