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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT05639114
Other study ID # CVAY736F12301
Secondary ID 2022-002691-3620
Status Recruiting
Phase Phase 3
First received
Last updated
Start date March 2, 2023
Est. completion date January 16, 2029

Study information

Verified date June 2024
Source Novartis
Contact Novartis Pharmaceuticals
Phone 1-888-669-6682
Email novartis.email@novartis.com
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The trial will evaluate efficacy, safety and tolerability of two regimens of ianalumab compared to placebo, given as monthly or quarterly subcutaneous (s.c.) injection on top of standard-of-care (SoC) treatment in participants with active systemic lupus erythematosus (SLE).


Description:

A randomized, double-blind, parallel group, placebo-controlled multicenter phase 3 study to evaluate efficacy, safety and tolerability of two regimens of ianalumab on top of standard-of-care therapy in patients with systemic lupus erythematosus (SIRIUS-SLE 1)


Recruitment information / eligibility

Status Recruiting
Enrollment 406
Est. completion date January 16, 2029
Est. primary completion date January 19, 2027
Accepts healthy volunteers No
Gender All
Age group 12 Years and older
Eligibility Inclusion Criteria: - Male and female participants aged 12 years or older at the time of screening, or limited to 18 years or older in European Economic Area countries and other countries where inclusion of participants below 18 years is not allowed. - Diagnosis of systemic lupus erythematosus meeting the 2019 European League Against Rheumatism/American College of Rheumatology (EULAR/ACR) SLE classification criteria at least 6 months prior to screening. - Elevated serum titers at screening of anti-nuclear antibodies = 1:80 as determined by a central laboratory with a SLE-typical fluorescence pattern. - Currently receiving CS and/or anti-malarial treatment and/or another disease-modifying antirheumatic drug (DMARD) as specified in the protocol. - SLEDAI-2K criteria at screening: SLEDAI-2K score = 6 points, excluding points attributed to "fever", "lupus headache", "alopecia", and "organic brain syndrome" - BILAG-2004 disease activity level at screening of at least 1 of the following: - BILAG-2004 level 'A' disease in = 1 organ system, Or - BILAG-2004 level 'B' disease in = 2 organ systems - Weigh at least 35 kg at screening Exclusion Criteria: - Prior treatment with ianalumab - History of receiving following treatment: I) high dose CS, calcineurin inhibitors, JAK or other kinase inhibitors or other DMARD (except as listed in inclusion criteria) administered within 12 weeks prior to screening. II) cyclophosphamide or biologics such as immunoglobulins (intravenous or s.c.), plasmapheresis, anti-type I interferon receptor biologic agents, anti-CD40 agents, CTLA4-Fc Ig or B-cell activating factor (BAFF)-targeting agents administered within 24 weeks prior to screening; belimumab administered within 12 weeks prior to screening. III) any B cell-depleting therapies, other than ianalumab administered within 36 weeks prior to randomization or as long as B cell count is less than the lower limit of normal or baseline value prior to receipt of B cell-depleting therapy (whichever is lower). IV) Traditional Chinese medicines administered within 30 days prior to randomization. - Active viral, bacterial or other infections requiring intravenous or intramuscular treatment for clinically significant infection - Chronic infection with hepatitis B virus (HBV) or hepatitis C virus (HCV) - Evidence of active tuberculosis infection - History of primary or secondary immunodeficiency, including a positive human immunodeficiency virus (HIV) test result at screening - Any one of the following abnormal laboratory values prior to randomization - Platelets < 25000/mm^3 (< 25 x 10^3/µL) - Hemoglobin (Hgb) < 8.0 g/dL (< 5 mmol/L), or < 7.0 g/dL (< 4.3 mmol/L) if related to participant's SLE such as in active hemolytic anaemia - Absolute neutrophil count (ANC) (< 0.8 x 10^3/ µL) - Severe organ dysfunction or life-threatening disease at screening - Presence of severe lupus kidney disease as defined by proteinuria above 2 g/day or equivalent using spot urine protein creatinine ratio, or serum creatinine greater than 2.0 mg/dL (176.84 µmol/L), or requiring immune-suppressive induction or maintenance treatment at screening - Receipt of live/attenuated vaccine within a 4-week period before first dosing - Any uncontrolled, co-existing serious disease, which in the opinion of the investigator will place the participant at risk for participation or interfere with evaluation for SLE-related symptoms - Non-lupus conditions such as asthma, gout or urticaria, requiring intermittent or chronic treatment with systemic CS - History of malignancy of any organ system other than localized basal cell carcinoma of the skin or in situ cervical cancer - Pregnant or nursing (lactating) women. - Women of child-bearing potential (WOCBP), defined as all women physiologically capable of becoming pregnant, unless they are using highly effective methods of contraception while on study treatment and for 6 months after stopping of investigational drug. - Any surgical, medical, psychiatric or additional physical condition that may jeopardize participation in this study

Study Design


Intervention

Drug:
Ianalumab
ianalumab s.c. monthly or quarterly
Placebo
placebo s.c. monthly

Locations

Country Name City State
Brazil Novartis Investigative Site Barretos Sao Paulo
Brazil Novartis Investigative Site Belo Horizonte MG
Brazil Novartis Investigative Site Brasilia DF
Brazil Novartis Investigative Site Curitiba PR
Brazil Novartis Investigative Site Niteroi RJ
Brazil Novartis Investigative Site Rio de Janeiro RJ
Brazil Novartis Investigative Site Salvador
Brazil Novartis Investigative Site Salvador BA
Brazil Novartis Investigative Site Sao Paulo SP
Brazil Novartis Investigative Site São Paulo SP
Brazil Novartis Investigative Site Vitoria ES
Bulgaria Novartis Investigative Site Plovdiv
Bulgaria Novartis Investigative Site Ruse
Canada Novartis Investigative Site Rimouski Quebec
Canada Novartis Investigative Site Vancouver British Columbia
China Novartis Investigative Site Baotou Inner Mongolia
China Novartis Investigative Site Beijing
China Novartis Investigative Site Beijing
China Novartis Investigative Site Chang Chun Jilin
China Novartis Investigative Site Chengdu Sichuan
China Novartis Investigative Site Guangzhou Guangdong
China Novartis Investigative Site Guangzhou Guangdong
China Novartis Investigative Site Haikou Hainan
China Novartis Investigative Site Linyi Shandong
China Novartis Investigative Site Nanchang Jiangxi
China Novartis Investigative Site Nanjing Jiangsu
China Novartis Investigative Site Pingxiang Jiangxi
China Novartis Investigative Site Shanghai
China Novartis Investigative Site Shanghai
China Novartis Investigative Site Shantou Guangdong
China Novartis Investigative Site Suzhou Jiangsu
China Novartis Investigative Site Urumqi Xinjiang
China Novartis Investigative Site Wuhan
China Novartis Investigative Site Zhejiang
China Novartis Investigative Site Zhuzhou Hunan
Czechia Novartis Investigative Site Brno
Czechia Novartis Investigative Site Praha 2
Czechia Novartis Investigative Site Uherske Hradiste
Guatemala Novartis Investigative Site Guatemala
Guatemala Novartis Investigative Site Guatemala City
Guatemala Novartis Investigative Site Guatemala City
Hungary Novartis Investigative Site Gyula
Hungary Novartis Investigative Site Szekesfehervar Fejer
Israel Novartis Investigative Site Haifa
Israel Novartis Investigative Site Ramat Gan
Japan Novartis Investigative Site Bunkyo ku Tokyo
Japan Novartis Investigative Site Chuo ku Tokyo
Japan Novartis Investigative Site Fuchu Tokyo
Japan Novartis Investigative Site Fukuoka
Japan Novartis Investigative Site Gifu
Japan Novartis Investigative Site Ichikawa Chiba
Japan Novartis Investigative Site Kawasaki-city Kanagawa
Japan Novartis Investigative Site Kurashiki Okayama
Japan Novartis Investigative Site Meguro Tokyo
Japan Novartis Investigative Site Miyazaki-city Miyazaki
Japan Novartis Investigative Site Nagoya Aichi
Japan Novartis Investigative Site Nagoya Aichi
Japan Novartis Investigative Site Ono Hyogo
Japan Novartis Investigative Site Sapporo city Hokkaido
Japan Novartis Investigative Site Yokohama Kanagawa
Japan Novartis Investigative Site Yokohama-city Kanagawa
Poland Novartis Investigative Site Bydgoszcz
Poland Novartis Investigative Site Bydgoszcz
Poland Novartis Investigative Site Bytom
Poland Novartis Investigative Site Lodz
Poland Novartis Investigative Site Rzeszow
Poland Novartis Investigative Site Warszawa
Poland Novartis Investigative Site Warszawa
Poland Novartis Investigative Site Wroclaw Dolnoslaskie
Portugal Novartis Investigative Site Braga
Portugal Novartis Investigative Site Leiria
Portugal Novartis Investigative Site Lisboa
Portugal Novartis Investigative Site Lisboa
Portugal Novartis Investigative Site Lisboa
Singapore Novartis Investigative Site Singapore
Singapore Novartis Investigative Site Singapore
Singapore Novartis Investigative Site Singapore
Slovakia Novartis Investigative Site Bratislava
Slovakia Novartis Investigative Site Bratislava
Slovakia Novartis Investigative Site Kosice
Slovakia Novartis Investigative Site Piestany
South Africa Novartis Investigative Site Cape Town
South Africa Novartis Investigative Site Pretoria
South Africa Novartis Investigative Site Stellenbosch
Spain Novartis Investigative Site Badalona Catalunya
Spain Novartis Investigative Site Barcelona Catalunya
Spain Novartis Investigative Site Barcelona Catalunya
Spain Novartis Investigative Site El Palmar Murcia
Spain Novartis Investigative Site Elche Alicante
Spain Novartis Investigative Site La Laguna Santa Cruz De Tenerife
Spain Novartis Investigative Site Madrid
Spain Novartis Investigative Site Merida Extremadura
Spain Novartis Investigative Site Pamplona Navarra
Spain Novartis Investigative Site San Sebastian de los Reyes Madrid
Spain Novartis Investigative Site Santander Cantabria
Spain Novartis Investigative Site Santiago De Compostela Galicia
Spain Novartis Investigative Site Valladolid Castilla Y Leon
Spain Novartis Investigative Site Vigo Pontevedra
Spain Novartis Investigative Site Vitoria Gasteiz Pais Vasco
Thailand Novartis Investigative Site Bangkok
Thailand Novartis Investigative Site Bangkok
Thailand Novartis Investigative Site Chiang Mai
Thailand Novartis Investigative Site Songkhla Hat Yai
Turkey Novartis Investigative Site Ankara
Turkey Novartis Investigative Site Aydin
Turkey Novartis Investigative Site Etlik / Ankara
Turkey Novartis Investigative Site Izmir
Turkey Novartis Investigative Site Konya
United States University of Colorado University of Colorado Denver Aurora Colorado
United States Ochsner Clinic Foundation Baton Rouge Louisiana
United States Providence Medical Center Burbank California
United States Clinical Research of West Florida Clearwater Florida
United States STAT Research Inc . Dayton Ohio
United States Henry Ford Health Detroit Michigan
United States GNP Research Hollywood Florida
United States University of California San Diego . La Jolla California
United States Novartis Investigative Site Las Vegas Nevada
United States Parris and Associates Rheumatology Lawrenceville Georgia
United States Accurate Clinical Research Research League City Texas
United States Keck School of Medicine Keck Medicine of USC Los Angeles California
United States Ramesh C Gupta MD Memphis TN Memphis Tennessee
United States Paramount Med Rsrch and Consult LLC . Middleburg Heights Ohio
United States Lake Cumberland Rheumatology and In New Albany Indiana
United States Epic Medical Research Red Oak Texas
United States Millennium Clinical Trials Simi Valley California
United States Robert A Hozman MD SC Skokie Illinois

Sponsors (1)

Lead Sponsor Collaborator
Novartis Pharmaceuticals

Countries where clinical trial is conducted

United States,  Brazil,  Bulgaria,  Canada,  China,  Czechia,  Guatemala,  Hungary,  Israel,  Japan,  Poland,  Portugal,  Singapore,  Slovakia,  South Africa,  Spain,  Thailand,  Turkey, 

Outcome

Type Measure Description Time frame Safety issue
Primary Proportion of participants on monthly ianalumab achieving Systemic Lupus Erythematosus Responder Index -4 (SRI-4) SRI-4 response is defined as:
Systemic Lupus Erythematosus Disease Activity Index - 2000 (SLEDAI-2K) reduction from baseline of = 4 points
No British Isles Lupus Assessment Group-2004 (BILAG-2004) worsening, defined as = 1 new A or = 2 new B items compared to baseline
No worsening in Physician Global Assessment of Disease Activity (PhGA), defined as an increase of = 0.3 from baseline on a 0 to 3 visual analog scale
Week 60
Secondary Proportion of participants on monthly or quarterly ianalumab with no moderate or severe British Isles Lupus Assessment Group (BILAG) flare Moderate BILAG flare is defined as 2 or more new BILAG-2004 B items compared to the previous visit; severe BILAG flare is defined as (1 or more new BILAG-2004 A items compared to the previous visit) Baseline to Week 60
Secondary Proportion of participants on monthly or quarterly ianalumab maintaining between Week 36 and Week 60 a reduced corticosteroid (CS) dose of predniso(lo)ne = 5 mg/day or = baseline dose, whichever is lower Maintaining reduced CS dose from Week 36 to Week 60 Week 36 to Week 60
Secondary Proportion of participants on monthly or quarterly ianalumab achieving BILAG-based Composite Lupus Assessment (BICLA) BICLA response is defined as:
Reduction of all baseline BILAG-2004 A to B/C/D and baseline B to C/D and no worsening in other organ systems defined as = 1 new A or = 2 new B items compared to baseline
No worsening from baseline in SLEDAI-2K defined as an increase from baseline of > 0 points
No worsening in PhGA defined as an increase of = 0.3 from baseline on a 0 to 3 PhGA visual analog scale
Week 60
Secondary Proportion of participants on monthly or quarterly ianalumab achieving Lupus Low Disease Activity State (LLDAS) LLDAS response is defined as:
SLEDAI-2K = 4, with no activity in major organ systems (renal, central nervous system (CNS), cardiopulmonary, vasculitis, fever).
No new lupus disease activity compared with the previous assessment, defined as any new SLEDAI-2K component that was not present at the previous assessment
PhGA (scale 0-3) = 1
Current predniso(lo)ne (or equivalent) dose = 7.5 mg daily
Well tolerated standard maintenance doses of immunosuppressive drugs and approved biological agents
Week 60
Secondary Time to first occurrence of SRI-4 (participants on ianalumab monthly or quarterly) Time to first occurrence of SRI-4 from baseline to Week 60 Baseline to Week 60
Secondary Proportion of participants on monthly or quarterly ianalumab achieving SRI-4 at Week 60 while maintaining between Week 36 and Week 60 a reduced corticosteroid dose of predniso(lo)ne = 5 mg/day or = baseline dose, whichever is lower Achieving SRI-4 at Week 60 while maintaining between Week 36 and Week 60 a reduced CS dose of predniso(lo)ne = 5 mg/day or = baseline dose, whichever is lower Week 36 to Week 60
Secondary Proportion of participants on monthly or quarterly ianalumab achieving SRI-6 SRI-6 response is defined as:
SLEDAI-2K reduction from baseline of = 6 points
No BILAG-2004 worsening, defined as = 1 new A or = 2 new B items compared to baseline
No worsening in PhGA, defined as an increase of = 0.3 from baseline on a 0 to 3 visual analog scale
Week 60
Secondary Proportion of participants on monthly or quarterly ianalumab achieving Short Form 36 (SF-36) Bodily Pain response Achieving SF-36 Bodily Pain response Week 60
Secondary Proportion of participants on quarterly ianalumab achieving SRI-4 SRI-4 response is defined as:
SLEDAI-2K reduction from baseline of = 4 points
No BILAG-2004 worsening, defined as = 1 new A or = 2 new B items compared to baseline
No worsening in PhGA, defined as an increase of = 0.3 from baseline on a 0 to 3 visual analog scale
Week 60
Secondary Proportion of participants on monthly or quarterly ianalumab with Adverse Events (AEs) and Serious Adverse Events (SAEs) To evaluate safety and tolerability of ianalumab s.c. monthly or quarterly Baseline to Week 60
Secondary Number of participants with adverse events To evaluate safety and tolerability of ianalumab s.c. monthly or quarterly Baseline to Week 60
Secondary Proportion of participants with anti-ianalumab antibodies in serum (ADA assay) over time Immunogenicity of ianalumab s.c. monthly or quarterly Baseline to Week 164
Secondary Ianalumab concentration in serum during the treatment and follow-up Ianalumab concentration in serum Baseline to week 164
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