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Clinical Trial Details — Status: Active, not recruiting

Administrative data

NCT number NCT03570892
Other study ID # CCTL019H2301
Secondary ID 2016-002966-29
Status Active, not recruiting
Phase Phase 3
First received
Last updated
Start date May 7, 2019
Est. completion date February 14, 2026

Study information

Verified date March 2024
Source Novartis
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This is a randomized, open label, multicenter phase III trial comparing the efficacy, safety, and tolerability of tisagenlecleucel to Standard Of Care in adult patients with aggressive B-cell Non-Hodgkin Lymphoma after failure of rituximab and anthracycline containing frontline immunochemotherapy.


Recruitment information / eligibility

Status Active, not recruiting
Enrollment 331
Est. completion date February 14, 2026
Est. primary completion date February 13, 2026
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: 1. Histologically confirmed, aggressive B-cell NHL at relapse/progression or PR after front line therapy. Aggressive B-cell NHL is heretofore defined by the following list of subtypes (Swerdlow et al 2016): 1. DLBCL, NOS, 2. FL grade 3B, 3. Primary mediastinal large B cell lymphoma (PMBCL), 4. T cell rich/histiocyte rich large B cell lymphoma (T/HRBCL), 5. DLBCL associated with chronic inflammation, 6. Intravascular large B-cell lymphoma, 7. ALK+ large B-cell lymphoma, 8. B-cell lymphoma, unclassifiable, (with features intermediate between DLBCL and classical Hodgkin's Lymphoma (HL)), 9. High grade B-cell lymphoma with MYC and BCL2 and/or BCL6 rearrangements, 10. High-grade B-cell lymphoma, NOS 11. HHV8+ DLBCL, NOS 12. DLBCL transforming from follicular lymphoma 13. DLBCL transforming from marginal zone lymphoma 14. DLBCL, leg type 2. Relapse or progression within 365 days from last dose of anti CD20 antibody and anthracycline containing first line immunochemotherapy or refractory (have not achieved a CR). 3. Patient is considered eligible for autologous HSCT as per local investigator assessment. Note: Intention to transplant and type of high dose chemotherapy (HDCT) regimen will be documented at the time of study entry 4. Disease that is both active on PET scan (defined as 5-Deauville scorepoint-scale of 4 or 5) and measurable on CT scan, defined as:: 1. Nodal lesions >15 mm in the long axis, regardless of the length of the short axis, and/or 2. Extranodal lesions (outside lymph node or nodal mass, but including liver and spleen) >10 mm in long AND short axis 5. Eastern Cooperative Oncology Group (ECOG) performance status 0 or 1 6. Adequate organ function: Renal function defined as: 1. Serum creatinine of =1.5 x upper limit of normal (ULN), OR estimated glomerular filtration rate (eGFR) = 60 mL/min/1.73 m2 Hepatic function defined as: 2. Alanine Transaminase (ALT) and Aspartate Transiminase (AST) = 5 × ULN 3. Total bilirubin = 1.5 x ULN with the exception of patients with Gilbert syndrome who may be included if their total bilirubin is =3.0 × ULN and direct bilirubin =1.5 × ULN Hematologic Function (regardless of transfusions) defined as: 4. Absolute neutrophil count (ANC) >1000/mm3 5. Absolute lymphocyte count (ALC) >300/mm3 OR Absolute number of CD3+ T cells >150/mm3 (only for patients with non-historical apheresis) 6. Platelets =50000/mm3 7. Hemoglobin >8.0 g/dl Adequate pulmonary function defined as: 8. No or mild dyspnea (= Grade 1) 9. Oxygen saturation measured by pulse oximetry > 90% on room air 10. Forced expiratory volume in 1 s (FEV1) = 50% and/or carbon monoxide diffusion test (DLCO) =50% of predicted level 7. Must have a leukapheresis material of non-mobilized cells available for manufacturing. Exclusion Criteria: 1. Prior treatment with anti-CD19 therapy, T cell therapy, or any prior gene therapy product 2. Treatment with any systemic lymphoma-directed second line anticancer therapy prior to randomization. Only steroids and local irradiation are permitted for disease control 3. Patients with active central nervous system (CNS) involvement by disease under study are excluded, except if the CNS involvement has been effectively treated and local treatment was >4 weeks before randomization 4. Prior allogeneic HSCT 5. Clinically significant active infection 6. Any of the following cardiovascular conditions: - Unstable angina, myocardial infarction, coronary artery bypass graft (CABG), or stroke within 6 months prior to screening, - Left ventricle ejection fraction (LVEF) <45% as determined by echocardiogram (ECHO) or magnetic resonance angiography (MRA) or multigated acquisition (MUGA) at the screening assessment. - New York Heart Association (NYHA) functional class III or IV (Chavey et al 2001), within the past 12 months. - Clinically significant cardiac arrhythmias (e.g., ventricular tachycardia), complete left bundle branch block, high-grade atrioventricular (AV) block (e.g., bifascicular block, Mobitz type II) and third degree AV block unless adequately controlled by pacemaker implantation. - Resting QTcF =450 msec (male) or =460 msec (female) at screening or inability to determine the QTcF interval - Risk factors for Torsades de Pointes (TdP), including uncorrected hypokalemia or hypomagnesemia, history of cardiac failure, or history of clinically significant/ symptomatic bradycardia, or any of the following: - Long QT syndrome, family history of idiopathic sudden death or congenital long QT syndrome - Concomitant medication(s) with a "Known Risk of Torsades de Pointes" per crediblemeds.org that cannot be discontinued or replaced by safe alternative medication. 7. Patients with active neurological autoimmune or inflammatory disorders (e.g., Guillain-Barré Syndrome (GBS), Amyotrophic Lateral Sclerosis (ALS)) and clinically significant active cerebrovascular disorders (e.g. cerebral edema, posterior reversible encephalopathy syndrome (PRES)) Other protocol-defined inclusion and exclusion criteria may apply.

Study Design


Intervention

Drug:
Tisagenlecleucel after optional bridging and lymphodepleting chemotherapy
Investigator's choice of optional platinum-based immunochemotherapy (ie. R-ICE, R-GemOx, R-GDP, R-DHAP) + Lymphodepleting chemotherapy (fludarabine with cyclophosphamide or bendamustine) + Tisagenlecleucel (a second generation CAR-T composed of a CD19 antigen-binding domain, a 4-1BB costimulatory domain and a CD3-? signaling domain)
Platinum-based immunochemotherapy followed in responding patients with high dose chemotherapy and autologous hematopoietic stem cell transplant (HSCT)
Investigator's choice of platinum-based immunochemotherapy (ie. R-ICE, R-GemOx, R-GDP, R-DHAP)+ High dose chemotherapy (ie. BEAM) + autologous HSCT. *Ibrutinib or lenalidomide may be used in patients who are no longer eligible for autologous HSCT after 2 cycles of immunochemotherapy

Locations

Country Name City State
Australia Novartis Investigative Site Darlinghurst New South Wales
Australia Novartis Investigative Site Melbourne Victoria
Australia Novartis Investigative Site Murdoch Western Australia
Austria Novartis Investigative Site Salzburg
Austria Novartis Investigative Site Vienna
Belgium Novartis Investigative Site Leuven
Brazil Novartis Investigative Site Salvador BA
Brazil Novartis Investigative Site Sao Paulo
China Novartis Investigative Site Beijing
China Novartis Investigative Site Beijing
China Novartis Investigative Site Shanghai
France Novartis Investigative Site Lille
France Novartis Investigative Site Montpellier cedex 5
France Novartis Investigative Site Nantes Cedex 1
France Novartis Investigative Site Paris 10
France Novartis Investigative Site Pierre Benite
France Novartis Investigative Site Toulouse
Germany Novartis Investigative Site Berlin
Germany Novartis Investigative Site Hamburg
Germany Novartis Investigative Site Koeln
Germany Novartis Investigative Site Leipzig
Germany Novartis Investigative Site Muenchen
Germany Novartis Investigative Site Regensburg Bavaria
Germany Novartis Investigative Site Ulm
Hong Kong Novartis Investigative Site Hong Kong
Italy Novartis Investigative Site Milano MI
Italy Novartis Investigative Site Roma RM
Italy Novartis Investigative Site Rozzano MI
Japan Kyushu University Hospital Fukuoka city Fukuoka
Japan Hokkaido University Hospital Sapporo city Hokkaido
Japan Tohoku University Hospital Sendai city Miyagi
Netherlands Amsterdam UMC, locatie AMC Amsterdam
Netherlands UMC Utrecht Cancer Center Utrecht
Norway Novartis Investigative Site Oslo
Singapore Novartis Investigative Site Singapore
Singapore Novartis Investigative Site Singapore
Spain Novartis Investigative Site Barcelona Catalunya
Spain Novartis Investigative Site Hospitalet de LLobregat Catalunya
Spain Novartis Investigative Site Madrid
Spain Novartis Investigative Site Madrid
Spain Novartis Investigative Site Salamanca Castilla Y Leon
Switzerland Novartis Investigative Site Zurich
Taiwan Novartis Investigative Site Taipei
United Kingdom Novartis Investigative Site Birmingham
United Kingdom Novartis Investigative Site London
United States Emory University School of Medicine/Winship Cancer Institute SC Atlanta Georgia
United States St Davids South Austin Medical Ctr Austin Texas
United States MUSC Hollings Cancer Center Charleston South Carolina
United States Uni of Chi Medi Ctr Hema and Onco Chicago Illinois
United States Jewish Hospital Cincinnati Ohio
United States The Ohio State University SC Columbus Ohio
United States Baylor Scott and White Res Inst Dallas Texas
United States Sarah Cannon Research Institute Denver Colorado
United States Wayne State University - Karmanos Cancer Institute SC Detroit Michigan
United States Hackensack Univ Medical Center Hackensack New Jersey
United States University of Texas MD Anderson Cancer Center MD Anderson Cancer Center Houston Texas
United States Mayo Clinic Jacksonville Main Centre Jacksonville Florida
United States University of Kansas Cancer Center SC Kansas City Kansas
United States Moores UC San Diego Cancer Center La Jolla California
United States University of California Los Angeles University of California LA Los Angeles California
United States Uni of Wisconsin Carbone Cancer Ctr Madison Wisconsin
United States Sarah Cannon Research Institute . Nashville Tennessee
United States Uni of Nebraska Med Ctr Omaha Nebraska
United States University of Pennsylvania, Abramson Cancer Center Philadelphia Pennsylvania
United States Oregon Health Sciences Univ SC Portland Oregon
United States Methodist Hospital San Antonio Texas
United States UCSF Medical Center San Francisco California

Sponsors (1)

Lead Sponsor Collaborator
Novartis Pharmaceuticals

Countries where clinical trial is conducted

United States,  Australia,  Austria,  Belgium,  Brazil,  China,  France,  Germany,  Hong Kong,  Italy,  Japan,  Netherlands,  Norway,  Singapore,  Spain,  Switzerland,  Taiwan,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Event-free survival (EFS) Event-free survival (EFS) is defined as the time from the date of randomization to the date of the first documented disease progression or stable disease at or after the week 12 (+/- 1 week) assessment, as assessed by Blinded Independent Review Committee (BIRC) per Lugano criteria, or death due to any cause, at any time. 5 years
Secondary EFS as assessed by local investigator EFS as assessed by local investigator 5 years
Secondary Overall Survival (OS) Overall survival (OS) is defined as the time from date of randomization to date of death due to any cause 5 years
Secondary Overall Response Rate (ORR) Overall Response Rate (ORR) as per the Lugano criteria as per BIRC review and local investigator assessment 5 years
Secondary Duration of Response (DOR) Duration of response: time from the date of first documented response of CR or PR to the date of first documented progression (SD or PD at or after the week 12 assessment will be considered progression) or death due to aggressive B-cell NHL. DOR will be summarized by BIRC and local response 5 years
Secondary Time to Response (TTR) Time from the date of randomization to the date of a patient's first achieved a response of CR or PR on or after the Week 12 assessment 5 years
Secondary SF-36v2 Time to definitive deterioration in SF-36v2 24 Months
Secondary FACT-Lym Time to definitive deterioration in FACT-Lym 24 Months
Secondary EQ-VAS Time to definitive deterioration in EQ-VAS 24 Months
Secondary Tisagenlecleucel transgene concentrations qPCR will be used to measure tisagenlecleucel transgene concentrations in peripheral blood and bone marrow 5 years
Secondary Tisagenlecleucel immunogenicity (humoral and cellular) Pre-existing and treatment related immunogenicity (humoral and cellular) of tisagenlecleucel will be characterized. 5 years
Secondary Presence of replication competent lentivirus (RCL) The presence of RCL will be assessed by VSV-qPCR in patients receiving tisagenlecleucel 5 years
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