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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT01292603
Other study ID # BO25341
Secondary ID 2010-021380-32
Status Completed
Phase Phase 1
First received
Last updated
Start date April 18, 2011
Est. completion date November 17, 2017

Study information

Verified date November 2018
Source Hoffmann-La Roche
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This randomized, parallel-group, multi-center study will compare the pharmacokinetics and safety of subcutaneous administration of MabThera (rituximab) versus intravenous MabThera in combination with chemotherapy in previously untreated patients with chronic lymphocytic leukemia (CLL). The study consists of 2 parts. In part 1, patients who have previously received 4 cycles of intravenous MabThera will receive in Cycle 5 intravenous MabThera and in Cycle 6 subcutaneous MabThera. In part 2, patients will be randomized to receive either 6 cycles of intravenous MabThera, or 1 cycle of intravenous MabThera and 5 cycles of subcutaneous MabThera. Additionally, all patients will receive chemotherapy (fludarabine and cyclophosphamide) on Days 1-3 or Days 1-5 of every cycle. The anticipated time on study drug is 24 weeks.


Recruitment information / eligibility

Status Completed
Enrollment 240
Est. completion date November 17, 2017
Est. primary completion date May 7, 2014
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria:

- Adult patients, >/=18 years of age

- Patients with treatment-requiring chronic lymphocytic leukemia (CLL)

- Eastern Cooperative Oncology Group (ECOG) performance status of 0-1

- Life expectancy >6 months

Exclusion Criteria:

- Transformation to aggressive B-cell malignancy

- History of other malignancy unless the patient was treated with curative intent and has been in remission for more than 5 years prior to enrolment

- HIV or Hepatitis B positive unless clearly due to vaccination

- Inadequate liver or renal function

- Any coexisting medical or psychological condition that would preclude participation in the required study procedures

Additional exclusion criterion for Part 1:

- Any previous treatment for CLL except for up to 4 cycles of rituximab IV in combination with FC chemotherapy as first-line treatment for CLL

Additional exclusion criterion for Part 2:

- Any previous treatment for CLL

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Cyclophosphamide
Days 1-3 or Days 1-5 of cycles 1-6
Fludarabine
Days 1-3 or Days 1-5 of cycles 1-6
rituximab [MabThera]
One cycle of intravenous MabThera, followed by 5 cycles of subcutaneous MabThera
rituximab [MabThera]
After 4 cycles of intravenous MabThera without experiencing grade 3 or 4 infusion-related reactions. patients will receive 1 additional cycle of intravenous MabThera and 1 cycle of subcutaneous MabThera.
rituximab [MabThera]
6 cycles of intravenous MabThera

Locations

Country Name City State
Argentina Cemic; Haematology Buenos Aires
Argentina Fundaleu; Haematology Buenos Aires
Argentina HOSPITAL PRIVADO - CENTRO MEDICO DE CÓRDOBA; Dpto Oncología Córdoba
Australia St Vincent'S Hospital; Haematology Fitzroy Victoria
Australia Frankston Hospital; Oncology/Haematology Frankston Victoria
Australia Royal Brisbane and Women'S Hospital; Haematology Herston Queensland
Australia St George Hospital; Department of Haematology Kogarah New South Wales
Australia Ashford Cancer Center Research Kurralta Park South Australia
Australia Queen Elizabeth Hospital; Haematology Woodville South South Australia
Brazil Hospital da Cidade de Passo Fundo; Centro de Pesquisa em Oncologia Passo Fundo RS
Brazil Hospital Mae de Deus Porto Alegre RS
Brazil Hospital das Clinicas - FMUSP Sao Paulo SP
Brazil Hospital Sirio Libanes; Centro de Oncologia Sao Paulo SP
Canada Queen Elizabeth II Health Sciences Centre; Oncology Halifax Nova Scotia
Canada McGill University; Sir Mortimer B Davis Jewish General Hospital; Oncology Montreal Quebec
Canada Centre de sante et de services sociaux Rimouski Neigette Rimouski Quebec
Canada Centre Hospitalier Universitaire de Sherbrooke Sherbrooke Quebec
Chile Centro Internacional de Estudios Clínicos (CIEC) Santiago
Chile Instituto Nacional del Cancer Santiago
Croatia Clinical Hospital Merkur; Dept of Haematology Zagreb
Croatia University Hospital Center Zagreb; Haematology Department Zagreb
Czechia Fakultni nemocnice Brno; Interni hematologicka a onkologicka klinika Brno
Czechia University Hospital and Medical School; IV.Dept. of Internal Medicine and Hematology Hradec Kralove
Czechia Vseobecna Fakultni Nemocnice v Praze, I. Interni Klinika - Klinika Hematoonkologie VFN a 1. LF UK Praha 2
France Centre Francois Baclesse Caen
France Institut J Paolii Calmettes; Onco Hematologie 1 Marseille
France Hopital Saint Louis ; Service d Oncologie Medicale Fougere 6 (Pr Misset) Paris
France Hopital Robert Debre; Hematologie Clinique Reims
France Hopitaux De Brabois; Hematologie Medecine Interne Vandoeuvre Les Nancy
Germany Onkologische Schwerpunktpraxis Kurfürstendamm Berlin
Germany Onkologischer Schwerpunkt am Oskar-Helene-Heim; Dres. Herrenberger, Keitel-Wittig u. Kirsch Berlin
Germany BAG Freiberg-Richter, Jacobasch, Illmer, Wolf; Gemeinschaftspraxis Hämatologie-Onkologie Dresden
Germany Klinikum Frankfurt; Medizinische Klinik I Frankfurt an der Oder
Germany Universitätsklinikum Greifswald Klinik für Innere Medizin C und Poliklinik Greifswald
Germany Onkologische Schwerpunktpraxis Dres. Bernd Gaede, Hans-Ulrich Ehlers, Ulrike Rodewig u.w. Hannover
Germany Gemeinschaftspraxis Dr. Siehl & Dr. Soeling Kassel
Germany Klinik der Uni zu Köln; Klinik für Innere Medizin Köln
Germany K&K Studien GbR Landshut
Germany Onkologische Schwerpunktpraxis Lübeck Lübeck
Germany Gemeinschaftspraxis Fr. Dr. med. Balser & Hr. Dr. med. Weidenbach Marburg
Germany Klinikum Grosshadern der LMU Muenchen
Germany Medizinisches Versorgungszentrum MOP München
Germany Gemeinschaftspraxis Dr. med. Holger Klaproth / Dr. med. Anca Astrid Cura Neunkirchen/Saar
Germany Prosper-Hospital, Medizinische Klinik I Recklinghausen
Greece Laiko General Hospital of Athens; A Propedeutical Clinic of Internal Medicine Athens
Greece Papageorgiou General Hospital of Thessaloniki; Hematology Clinic Thessaloniki
Italy IRST Istituto Scientifico Romagnolo Per Lo Studio E Cura Dei Tumori, Sede Meldola; Oncologia Medica Meldola Emilia-Romagna
Italy ASST GRANDE OSPEDALE METROPOLITANO NIGUARDA; Struttura Complessa di Ematologia Milano Lombardia
Italy Istituto S. Raffaele Monte Tabor; Divisione Ematologia E Utmo Milano Lombardia
Italy Univ. Piemonte Est Amedeo Avogadro; Div.Ematologia- Dip.Clinica Med.Sperim.& Ircad Novara Piemonte
Italy Az. Osp. S. Maria Delle Croci; U.O. Di Ematologia Ravenna Emilia-Romagna
Italy Ospedale Infermi Di Rimini; Unità Operativa di Oncologia e Oncoematologia Rimini Emilia-Romagna
Italy A.O. Universitaria S. Maria Della Misericordia Di Udine; Oncologia; Clinica Ematologica Udine Friuli-Venezia Giulia
Italy Policlinico G. B. Rossi; Divisione Di Ematologia Verona Veneto
Mexico Centro Estatal De Cancerologia De Chihuahua; Servicio De Hematologia Banco De Sangre Chihuahua
Mexico Hospital General De Culiacan; Servicio De Hematologia Culiacan
Mexico Hospital Universitario Dr. Jose E. Gonzalez; Haematology Monterrey
New Zealand Canterbury Health Laboratories; Haematology Christchurch
New Zealand Wellington Hospital; Wellington Blood and Cancer Centre Newtown
Poland Uniwersyteckie Centrum Kliniczne; Klinika Hematologii i Transplantologii Gdansk
Poland Katedra i Klinika Hematoonkologii i Transplantacji Szpiku; Uniwersytetu Medycznego w Lublinie Lublin
Poland Centrum Onkologii - Inst.Im. Marii Sklodowskiej-Curie; Lymphoma Dept. Warszawa
Poland Medical Uni of Wroclaw; Hematology Wroclaw
Portugal Hospital de Santa Maria; Servico de Hematologia e Transplantacao de Medula Lisboa
Portugal IPO do Porto; Servico de Onco-Hematologia Porto
Russian Federation City Clinical Hospital After Botkin; Hematology Moscow
Russian Federation Haematology Research Center; Haematology Moscow
Russian Federation N.N.Blokhin Russian Cancer Research Center; Dept. of Chemotherapy & Hemoblastosis Moscow
Russian Federation Penza Regional Oncology Dispensary Penza
Russian Federation Clinical MSCh No1 Perm
Russian Federation St. Petersburg State Medical University n.a. I.P. Pavlov; Hematology, transfusiology and transplanta Saint-Petersburg
Slovakia National Oncology Inst. ; Dept. of Haematology Bratislava
Slovakia University Hospital; Clinic of Hematology & Transfusiology Bratislava
Spain Hospital Universitari Vall d'Hebron; Servicio de Hematologia Barcelona
Spain Hospital Universitario de la Princesa; Servicio de Hematologia Madrid
Spain Hospital Universitario Puerta de Hierro; Servicio de Hematologia Madrid
Spain Hospital Clinico Universitario de Salamanca;Servicio de Hematologia Salamanca
Spain Hospital Universitario Virgen del Rocio; Servicio de Hematologia Sevilla
Spain Complejo Hospitalario de Toledo- H. Virgen de la Salud; Servicio de Hematología Toledo
Spain Hospital Clinico Universitario de Valencia; Servicio de Onco-hematologia Valencia
Turkey Hacettepe Uni Medical Faculty; Hematology Ankara
Turkey Istanbul University Cerrahpasa Medical Faculty; Hematology Department Istanbul
Turkey Dokuz Eylul Uni ; Hematology Izmir
Turkey Ege University ARGEFAR Izmir

Sponsors (1)

Lead Sponsor Collaborator
Hoffmann-La Roche

Countries where clinical trial is conducted

Argentina,  Australia,  Brazil,  Canada,  Chile,  Croatia,  Czechia,  France,  Germany,  Greece,  Italy,  Mexico,  New Zealand,  Poland,  Portugal,  Russian Federation,  Slovakia,  Spain,  Turkey, 

Outcome

Type Measure Description Time frame Safety issue
Primary Part 1: Subcutaneous Rituximab Dose Resulting in Trough Concentration (Ctrough) Levels Non-Inferior to Intravenous Rituximab Ctrough is defined as the trough or minimum serum concentration. Pharmacokinetic parameters for rituximab were assessed during Cycles 5 (IV rituximab) and 6 (SC rituximab). Rituximab pharmacokinetic (PK) data from Part 1 were integrated into a population PK model using parametric, nonlinear, mixed-effects modelling. Rituximab IV 500 mg/m^2 administered once every 4 weeks was compared to fixed doses of rituximab SC between 1400 mg and 1870 mg. The dose selection was performed on Ctrough concentrations at Cycle 5 (pre-dose Cycle 6). A test of the probability of success was applied to each of the 100 replicates, and the percentage of replicates with a positive test corresponded to the probability of success of the trial. Pre-dose and post-dose (15 minutes to end of infusion) on Day 1 and on Days 2, 5, 11 and 15 of Cycle 5 and Pre-dose, Post-dose on Days 2, 3, 5,11, 15 and 29 of Cycle 6; Pre-dose was taken 2 hours prior rituximab dose
Primary Part 2: Rituximab C Trough Levels at Cycle 5 Ctrough is defined as the trough or minimum serum concentration in a given cycle of treatment. The objective of Part 2 was to demonstrate the comparability of the observed Ctrough of rituximab SC 1600 mg and rituximab IV 500 mg/m2 at Cycle 5, as assessed by a non-inferiority test with a lower boundary of at least 0.8 for the 90% CI. +/- 25hours around the 28th day post the 5th Cycle of Rituximab administration
Secondary Part 2: Observed Area Under the Serum Concentration-Curve (AUC) of Rituximab at Cycle 6 AUC values were calculated by numerical integration using the linear trapezoidal rule. AUC levels were analyzed using the model below: Ln(AUC) = µ + ti + BlTLij + eij wherein, Ln is the natural log, µ denotes the overall mean effect, ti the effect in each treatment group, BlTLij the tumor load at baseline for each patient and eij a random error variable with normal distribution and mean 0. The treatment effect therein was based on a contrast statement in the model to calculate 90 % confidence intervals for ln(AUC SC)- ln(AUC IV). Rituximab IV arm: pre-dose, post-dose and on Days 2, 3, 8 ,15, 29 of Cycle 6; Rituximab SC arm: pre-dose, and on Days 2, 3, 8 ,15, 29 of Cycle 6
Secondary Part 2: Maximum Observed Concentration (Cmax) of Rituximab at Cycle 6 Cmax was obtained directly from the measured concentration-time curves. The concentration-time curve is the result of time points of blood sampling and its measured concentration of rituximab in the blood samplings. Rituximab IV arm: pre-dose, post-dose and on Days 2, 3, 8 ,15, 29 of Cycle 6; Rituximab SC arm: pre-dose, and on Days 2, 3, 8 ,15, 29 of Cycle 6
Secondary Part 2: Time to Cmax (Tmax) of Rituximab at Cycle 6 Multiple blood samples were obtained at pre-dose, post-dose and on Days 2, 3, 8 ,15, 29 of Cycle 6 in Rituximab IV arm, and at pre-dose, and on Days 2, 3, 8 ,15, 29 of Cycle 6 in Rituximab SC arm and time to peak plasma concentration of rituximab was determined. Rituximab IV arm: pre-dose, post-dose and on Days 2, 3, 8 ,15, 29 of Cycle 6; Rituximab SC arm: pre-dose, and on Days 2, 3, 8 ,15, 29 of Cycle 6
Secondary Part 2: Terminal Half-Life of Rituximab at Cycle 6 The terminal half-life (t1/2) of rituximab is defined as the time required for the plasma concentration of rituximab to reach half of its original concentration. Rituximab IV arm: pre-dose, post-dose and on Days 2, 3, 8 ,15, 29 of Cycle 6; Rituximab SC arm: pre-dose, and on Days 2, 3, 8 ,15, 29 of Cycle 6
Secondary Part 1: Percentage of Participants and Nurses Recording a Preference For Either SC or IV Administration In part 1 of the trial, upon completion of dosing in cycle 6, participants and their treating nurses were asked whether they have a preference of dosing route, IV vs SC Days 4 to 5 in Cycle 6
Secondary Part 2: Physician/Nurse Opinion on Time Savings With Rituximab SC Compared With Rituximab IV Physicians and nurses who administered rituximab were asked to answer the following question: " If used in routine practice, on average, how much staff time could be saved with each administration of rituximab SC as compared to rituximab IV? (Please do not consider the time needed for the first IV administration, consider only the subsequent ones)". The number of nurses that responded for both the IV and SC arms was 70. The number of physicians that responded for the IV and SC arms were 78 and 81 respectively. Days 4-5 in Cycle 6
Secondary Part 2: Physician/Nurse Opinion on Convenience of Rituximab SC Compared With Rituximab IV Physicians and nurses who administered rituximab were asked to answer the following question: "Which formulation of rituximab (SC or IV) do you think is more convenient?" with pre-specified responses as below. Percentage of participants with specified answers were reported. The number of nurses that responded for both the IV and SC arms was 70. The number of physicians that responded for the IV and SC arms were 78 and 81 respectively. Days 4-5 in Cycle 6
Secondary Part 1: Percentage of Participants With Anti-Rituximab Antibodies Blood samples for the assessment of antibodies against rituximab (HACAs) were drawn pre-dose at Cycle 5 and Cycle 6 in Part 1 and at each follow up visit until 24 months after the last dose. Predose at Cycles 5 and 6 and at each follow up visit until 24 months after the last dose
Secondary Part 2: Percentage of Participants With Anti-Rituximab Antibodies In Part 2, samples for the HACA assay were collected at each treatment cycle prior to the administration of rituximab and at each follow-up visit until 24 months after the last dose of rituximab. Day 0 of Cycle 1 and Day 1 of Cycles 1, 2, 3, 4, 5, and 6 and at each follow-up visit until 24 months after the last dose of rituximab.
Secondary Part 1: Total Cluster Differentiation19 Positive (CD19+) B-Cell Counts by Visit CD 19 is a surface antigen (protein) present on B-lymphocytes. Day 1 of Cycles 5 and 6 and Follow-up Days 28 and 56 and Follow-up Visits at Months 3, 6, 9, 12, 15,18, 21 and 24
Secondary Part 1: Percentage of Participants With Total B-Cell Depletion by Visit Total B-cell depletion (normal B-cell plus Malignant B-cell depletion) was defined for each individual participant when the sum of CD5-/CD19+ (normal B-cells) and CD5+/CD19+ (malignant B-cells) cell counts decreased below 80 cells/µL. Day 1 pre-dose of Cycles 5 and 6 and Follow-up Days 28 and 56 and Follow-up Visits at Months 3, 6, 9, 12, 15, 18, 21 and 24
Secondary Part 2: Total CD19+ B-Cell Counts by Visit CD 19 is a surface antigen (protein) present on B-lymphocytes. Cycle 1 pre-dose, 60 minutes post-dose, Days 2 and 3 in Cycle 2, day 1 pre-dose in Cycles 3, 4, 5 and 6, Follow-up Days 28 and 56, and Follow-up Visits at Months 3, 6, 9, 12, 15, and 18 and Withdrawal Visit
Secondary Part 2: Percentage of Participants With Total B-Cell Depletion by Visit Total B-cell depletion (normal B-cell plus Malignant B-cell depletion) was defined for each individual participant when the sum of CD5-/CD19+ (normal B-cells) and CD5+/CD19+ (malignant B-cells) cell counts decreased below 80 cells/µL. Cycle 1 Pre-dose, 60 minutes post-dose, Days 2 and 3 in Cycle 2, day 1 in Cycles 3, 4, 5 and 6, Follow-up Days 28 and 56, and Follow-up Visits at Months 3, 6, 9, 12, 15, and 18 and Withdrawal Visit
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