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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT01200758
Other study ID # BO22334
Secondary ID 2010-021377-36
Status Completed
Phase Phase 3
First received
Last updated
Start date February 15, 2011
Est. completion date October 31, 2017

Study information

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

Clinical Trial Summary

This two-stage, multi-center, randomized, controlled, open-label study will investigate the pharmacokinetics, efficacy and safety of rituximab SC versus rituximab IV in participants with previously untreated follicular non-Hodgkin's lymphoma. Participants will be randomized to receive 375 milligrams per meter square (mg/m^2) rituximab as IV infusion or 1400 milligrams (mg) rituximab SC. In addition, participants will receive standard chemotherapy. Participants who achieved a complete or partial response (PR) after 8 treatment cycles, will receive maintenance treatment for a further maximum number of 12 cycles. Maintenance treatment cycles will be repeated every 8 weeks. This is a two-stage study. Stage 1 was designed to confirm the chosen rituximab SC dose resulting in comparable rituximab serum Ctrough levels compared with rituximab IV, when given as part of induction treatment every 3 weeks. Enrollment for Stage 2 started after the rituximab SC dose was established in Stage 1. Stage 2 aimed to further investigate the efficacy and safety of rituximab SC compared with rituximab IV. The anticipated time on study treatment is 96 weeks.


Recruitment information / eligibility

Status Completed
Enrollment 410
Est. completion date October 31, 2017
Est. primary completion date June 12, 2012
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria:

- Cluster of differentiation 20 (CD20)-positive, follicular Non-Hodgkin's lymphoma grade 1, 2, 3a. A tumor biopsy must have been performed within 6 months before study entry with material available for central review

- No prior treatment

- Eastern Cooperative Oncology Group (ECOG) performance status 0-2

Exclusion Criteria:

- Grade 3b follicular lymphoma

- Transformation to high-grade lymphoma secondary to follicular lymphoma

- Types of Non-Hodgkin's lymphoma other than follicular lymphoma

- Presence or history of central nervous system (CNS) disease

- Corticoid therapy during the last 4 weeks, except prednisone treatment less than (<) 20 milligrams per day (mg per day)

- Known active bacterial, viral, fungal, or mycobacterial, or any major episode of infections requiring hospitalization or treatment with IV antibiotics within 4 weeks of start of study medication, or oral antibiotics within 2 weeks prior to start of study medication

Study Design


Intervention

Drug:
Rituximab SC
First cycle of rituximab IV infusion (375 mg/m^2) + 7 cycles of rituximab SC (1400 mg; rituximab induction) in administered every 3 weeks. Participants achieving at least PR entered rituximab SC (1400 mg) maintenance therapy once every 8 weeks for 24 months.
Rituximab IV
Eight cycles of rituximab IV infusion (375 mg/m^2; rituximab induction) administered every 3 weeks. Participants achieving at least PR during induction, entered rituximab IV maintenance therapy (375 mg/m^2) once every 8 weeks for 24 months.
Cyclophosphamide
Eight cycles of cyclophosphamide (750 mg/m^2 IV) administered every 3 weeks.
Doxorubicin
Eight cycles of doxorubicin (50 mg/m^2 IV) administered every 3 weeks.
Vincristine
Eight cycles of doxorubicin (1.4 mg/m^2 IV) administered every 3 weeks.
Prednisone/Prednisolone
Eight cycles of prednisone/prednisolone (100 mg/day or 40 mg/m^2/day IV/orally) administered Days 1 to 5 of every 21 days cycle.

Locations

Country Name City State
Australia Gosford Hospital; Cancer Care Services Gosford New South Wales
Australia Royal Brisbane and Women's Hospital Herston Queensland
Australia Gold Coast Hospital; Haematology Department Southport Queensland
Australia Wollongong Hospital; Cancer Services Wollongong New South Wales
Australia Queen Elizabeth Hospital; Haematology Woodville South South Australia
Belgium UZ Antwerpen Edegem
Belgium CHU Sart-Tilman Liège
Belgium Sint Augustinus Wilrijk Wilrijk
Bosnia and Herzegovina University Clinical Center of the Republic of Srpska, Clinic for Internal Disease, Hematology Dept Banja Luka
Bosnia and Herzegovina University Clinical Center Sarajevo, Clinic for Hematology Sarajevo
Bosnia and Herzegovina University Clinical Centre Tuzla, Clinic for Oncology, Hematology and Radiotherapy Tuzla
Brazil Nucleo de Hematologia e Transplante de Medula Ossea de Minas Gerais Belo Horizonte MG
Brazil Hospital das Clinicas - UFRGS Porto Alegre RS
Brazil Hospital Sao Lucas - PUCRS Porto Alegre RS
Brazil Hospital das Clinicas - FMUSP Sao Paulo SP
Brazil Santa Casa de Misericordia de Sao Paulo; Hematologia e Hemoterapia Sao Paulo SP
Bulgaria UMHAT Dr Georgi Stranski; Hematology Pleven
Bulgaria Umhat S. George; Hematology Plovdiv
Bulgaria Specialised Hospital For Treatment Of Hematological Diseases; Hematology Sofia
Bulgaria Mhat Sveta Marina; Dept. of Haematology Varna
Canada Queen Elizabeth II Health Sciences Centre; Oncology Halifax Nova Scotia
Canada Cite de La Sante de Laval; Hemato-Oncologie Laval Quebec
Canada CHU de Quebec - Hopital de l'Enfant-Jesus; Unite de Recherche en Hematologie et Oncologie Quebec
Canada Centre de sante et de services sociaux Rimouski Neigette Rimouski Quebec
Canada Centre Hospitalier Universitaire de Sherbrooke Sherbrooke Quebec
Canada Centre hospitalier regional de Trois-Rivieres Trois-Rivieres Quebec
Colombia Fundacion Cardioinfantil Bogota
Colombia Centro Medico Imbanaco Cali
Colombia Hospital Pablo Tobon Uribe Medellin-Antioquia
Colombia Oncólogos de Occidente Pereira
Croatia UHC Rijeka Rijeka
Croatia University Hospital Center Zagreb; Haematology Department Zagreb
Denmark Aarhus Universitetshospital, Hæmatologisk Afdeling R Århus
Denmark Herlev Uni Hospital; Hæmatologisk Afdeling L 121 Herlev
Denmark Rigshospitalet; Hæmatologisk Klinik København Ø
Denmark Odense Universitetshospital; Hæmatologisk Afdeling Odense C
Denmark Sygehus Syd Roskilde; Onkologisk/haematologisk ambulatorium Roskilde
Denmark Vejle Hospital; Dept of Medicine, Division of Hematology Vejle
Finland Helsinki University Central Hospital; Dept of Oncology Helsinki
France Polyclinique Bordeaux Nord Aquitaine; Chimiotherapie Radiotherapie Bordeaux
France Hopital Henri Mondor; Hematologie Clinique Creteil
France Chu Site Du Bocage;Hematologie Clinique Dijon
France Clinique Victor Hugo; Chimiotherapie Le Mans
France Institut J Paolii Calmettes; Onco Hematologie 1 Marseille
France Hopital Saint Eloi; Hematologie Oncologie Medicale Montpellier
France Hopital Hotel Dieu Et Hme;Hopital De Jour Nantes
France Hopital Saint Louis ; Service d Oncologie Medicale Fougere 6 (Pr Misset) Paris
France Hopital De Haut Leveque; Hematologie Clinique Pessac
France Ch Lyon Sud; Hemato Secteur Jules Courmont Pierre Benite
France Hopital De La Miletrie; Hematologie Et Oncologie Medicale Poitiers
France Hopital Bretonneau; Hematologie Therapie Cellulaire Tours
Georgia Chemotherapy and Immunotherapy Clinic Medulla Tbilisi
Georgia Institute of Hematology and Transfusiology Tbilisi
Georgia M.Zodelava's Hematology Center Tbilisi
Georgia Mediclub Tbilisi
Germany Onkologische Schwerpunktpraxis Kurfürstendamm Berlin
Germany Klinikum Darmstadt GmbH; Med. Klinik V; Onkologie & Hämatologie Darmstadt
Germany Gemeinschaftspraxis Dr. med. J. Mohm und Dr. med. G. Prange-Krex; Fachaerzte fuer Innere Medizin Dresden
Germany PIOH PD Dr. R. Schnell - Dr. H. Schulz - Dr. M. Hellmann Frechen
Germany Universitätsklinikum Gießen und Marburg GmbH Standort Gießen Medizinische Klinik I Giessen
Germany Universitätsklinikum Greifswald Klinik für Innere Medizin C und Poliklinik Greifswald
Germany Internistisch-Onkologische Gemeinschaftspraxis; Dres. Rohrberg, Hurtz, Schma usw. Halle
Germany Medizinische Hochschule; Zentrum Innere Medizin; Abt. Hämatologie u. Onkologie Hannover
Germany St. Vincentius Kliniken Ag; Medizinische Klinik Abt. 2 Karlsruhe
Germany UKSH Klinik für Innere Medizin II, Hämatologie und Internistische Onkologie Kiel
Germany Gemeinschaftspraxis PD Dr. med. Marcel Reiser und Dr. med. Ildiko Kátay Koeln
Germany Onkologische Gemeinschaftspraxis Magdeburg
Germany Gemeinschaftspraxis Fr. Dr. med. Balser & Hr. Dr. med. Weidenbach Marburg
Germany Medizinisches Versorgungszentrum MOP München
Germany Praxis Dr.med. Jens Uhlig Naunhof
Germany Praxis Dr. Clemens Müller-Naendrup (Onkologische Schwerpunktpraxis im MVZ 2 GmbH) Olpe
Germany Prosper-Hospital, Medizinische Klinik I Recklinghausen
Germany Praxis Dr. Fenchel Saalfeld
Germany Caritas Kilinik St. Theresia; Abt. Innere Medizin Saarbruecken
Germany Praxis für Hämatologie & Onkologie Saarbruecken
Greece Attiko Hospital; Haematology Clinic Athens
Greece Laiko General Hospital of Athens; A Propedeutical Clinic of Internal Medicine Athens
Italy A.O. Spedali Civili Di Brescia-P.O. Spedali Civili;U.O. Ematologia Brescia Lombardia
Italy Uni Degli Studi Di Genova; 1A Divisione Di Ematologia Genova Liguria
Italy Irccs Istituto Europeo Di Oncologia (IEO); Emato-Oncologia Milano Lombardia
Italy A.O. Universitaria Federico II Di Napoli; Oncologia Ed Endocrinologia Clinica Napoli Campania
Italy Azienda Ospedaliera Ospedale S.Carlo; Ematologia Potenza Basilicata
Italy AUSL - IRCCS Santa Maria Nuova; U.O. Day Hospital di Oncologia Reggio Emilia Emilia-Romagna
Italy Ospedale S. Eugenio; Divisione Di Ematologia Roma Lazio
Italy IRCCS Ospedale Casa Sollievo Della Sofferenza; Ematologia E Trapianto Di Midollo Osseo San Giovanni Rotondo Puglia
Italy Ospedale Ca Foncello; Ematologia Treviso Veneto
Italy Ospedale Di Vicenza; Nefrologia, Ematologia Vicenza Veneto
Macedonia, The Former Yugoslav Republic of University Clinic for Hematology; HSCT Department Skopje
Macedonia, The Former Yugoslav Republic of University Clinic of Hematology Skopje, Hospital Care Department Skopje
Malaysia Ampang Hospital; Department of Haematology Ampang
Malaysia University Malaya Medical Center; Hematology Unit of Department of Internal Medicine Kuala Lumpur FED. Territory OF Kuala Lumpur
Malaysia Sarawak General Hospital; Department of Radiotherapy, Oncology and Palliative care Sarawak
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
Mexico Centro de Estudios Clinicos de Queretaro (CECLIQ) Queretaro
New Zealand Canterbury Health Laboratories; Haematology Christchurch
New Zealand Palmerston North Hospital; Regional Cancer Treatment Service Palmerston North
Peru Hospital Maria Auxiliadora Lima
Peru Instituto;Oncologico Miraflores Lima
Peru Oncosalud Sac; Oncología Lima
Romania Spitalul Clinic Judetean de Urgenta Brasov,Clinica de Hematologie Brasov
Romania Fundeni Clinical Inst. ; Hematology Dept Bucharest
Romania Institutul Regional de Oncologie Iasi; Clinica de Hematologie Iasi
Romania Spitalul Clinic Judetean de Urgenta Sf. Spiridon Iasi, Clinica de Hematologie Iasi
Romania Spitalul Clinic Judetean de Urgenta Targu-Mures; compartiment Hematologie Targu-mures
Romania Spitalul Clinic municipal de Urgenta Timisoara; Clinica de Hematologie Timisoara
Russian Federation Clinical Oncology Dispensary of Ministry of Health of Tatarstan Kazan
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 St. Petersburg State Medical University n.a. I.P. Pavlov; Hematology, transfusiology and transplanta Saint-Petersburg
Russian Federation Research Inst. of Hematology & Blood Transfusion ; Hematology St Petersburg
Russian Federation Russian Scientific Center of Radiology and Surgical Technologies; Dept of Radiology St.Petersburg, Pesochny
Serbia Institute of Hematology Belgrade
Serbia Clinical Center Vojvodine; Clinic for Hematology Novi Sad
Singapore National Cancer Centre; Medical Oncology Singapore
Singapore National University Hospital; National University Cancer Institute, Singapore (NCIS) Singapore
Singapore Singapore General Hospital; Department of Haematology Singapore
Slovakia National Cancer Inst. ; Dept. of Chemotherapy Bratislava
Slovakia St. Elisabeths Cancer Center Bratislava
South Africa National Hospital; Oncotherapy Dept Bloemfontein
South Africa King Edward VIII; Department of Haematology Congella
South Africa Durban Oncology Center Durban
South Africa University of Witwatersrand/Johannesburg Hospital; Dept. of ocnology Johannesburg
South Africa Cancercare Kraaifontein
Spain Hospital Clínic i Provincial; Servicio de Hematología y Oncología Barcelona
Spain Hospital del Mar; Servicio de Hematologia Barcelona
Spain Hospital Duran i Reynals; Servicio de Hematologia Barcelona
Spain Hospital Universitari Vall d'Hebron; Servicio de Hematologia Barcelona
Spain Hospital Universitario Puerta del Mar; Servicio de Hematologia Cádiz Cadiz
Spain Hospital Ramon y Cajal; Servicio de Hematologia Madrid
Spain Hospital Universitario de la Princesa; Servicio de Hematologia Madrid
Spain Hospital Universitario Virgen de Arrixaca; Servicio de Hematologia Murcia
Spain Hospital Clinico Universitario de Salamanca;Servicio de Hematologia Salamanca
Spain Hospital Universitario Virgen del Rocio; Servicio de Hematologia Sevilla
Spain Hospital Universitario la Fe; Servicio de Oncologia Valencia
Thailand National Cancer Inst. Bangkok
Thailand Siriraj Hospital; Division of Hematology, Department of Medicine Bangkok
Thailand Srinagarind Hospital, Khon Kaen Uni ; Dept of Medicine Khon Kaen
Turkey Adana Baskent University Hospital; Medical Oncology Adana
Turkey Bilim University School of Medicine; Hematology Istanbul
Turkey Istanbul University Cerrahpasa Medical Faculty; Hematology Department Istanbul
Turkey Dokuz Eylul Uni ; Hematology Izmir
Turkey Ege Uni Medical School; Hematology Izmir
United Kingdom Ninewells Hospital & Medical School; Ward 34 Dundee
United Kingdom Maidstone & Tonbridge Wells Hospital; Kent Oncology Center Maidstone
United Kingdom Derriford Hospital; Department of Haematology Plymouth
United Kingdom Queen's Hospital; Oncology Romford
United Kingdom Southampton General Hospital Southampton
United Kingdom Pinderfields General Hospital; Dept of Haematology Wakefield
United Kingdom New Cross Hospital; Dept. Of Haematology Wolverhampton

Sponsors (1)

Lead Sponsor Collaborator
Hoffmann-La Roche

Countries where clinical trial is conducted

Australia,  Belgium,  Bosnia and Herzegovina,  Brazil,  Bulgaria,  Canada,  Colombia,  Croatia,  Denmark,  Finland,  France,  Georgia,  Germany,  Greece,  Italy,  Macedonia, The Former Yugoslav Republic of,  Malaysia,  Mexico,  New Zealand,  Peru,  Romania,  Russian Federation,  Serbia,  Singapore,  Slovakia,  South Africa,  Spain,  Thailand,  Turkey,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Stage I: Trough Serum Concentrations (Ctrough) of IV and SC Rituximab Stage I: Cycle (Cy) 7 Day (D) 21 (within 2 hours predose on Cy8) of induction treatment (1 Cy=3 weeks)
Primary Stage II: Percentage of Participants With Overall Response at the End of Induction Treatment Assessed Using International Working Group Response Criteria for Non-Hodgkin Lymphoma (NHL) Overall Response comprised complete response (CR), CR unconfirmed (CRu), or PR. A participant was defined as a responder if they sustained a CR, CRu or PR at the end of induction treatment. Response assessment was based on clinical examination and computed tomography (CT) scans. Assessment of tumor response was performed according to the International Working Group response criteria for NHL. CR: complete disappearance of all detectable clinical and radiographic evidence of disease and disappearance of all disease-related symptoms if present before therapy; CRu: CR along with regression in lymph node mass by more than (>) 75% in the sum of the products of greatest diameters (SPD); PR: Greater than or equal to (=) 50% decrease in SPD of 6 largest dominant nodes or nodal masses. The 95% CI was estimated for one sample binomial using Pearson-Clopper. Stage II: Baseline up to end of induction treatment Cy8 (24 weeks) (1 Cy=3 weeks)
Secondary Stage I: Percentage of Participants With Overall Response at the End of Induction Treatment Assessed Using International Working Group Response Criteria for NHL Overall Response comprised CR, CRu, or PR. A participant was defined as a responder if they sustained a CR, CRu or PR at the end of induction treatment. Response assessment was based on clinical examination and CT scans. Assessment of tumor response was performed according to the International Working Group response criteria for NHL. CR: complete disappearance of all detectable clinical and radiographic evidence of disease and disappearance of all disease-related symptoms if present before therapy; CRu: CR along with regression in lymph node mass by >75% in the SPD; PR: =50% decrease in SPD of 6 largest dominant nodes or nodal masses. The 95% CI was estimated for one sample binomial using Pearson-Clopper. Stage I: Baseline up to end of induction treatment Cy8 (24 weeks) (1 Cy=3 weeks)
Secondary Stage I and II (Pooled): Percentage of Participants With Overall Response at the End of Induction Treatment Assessed Using International Working Group Response Criteria for NHL Overall Response comprised of CR, CRu, or PR. A participant was defined as a responder if they sustained a CR, CRu or PR at the end of induction treatment. Response assessment was based on clinical examination and CT scans. Assessment of tumour response was performed according to the International Working Group response criteria for NHL. CR: complete disappearance of all detectable clinical and radiographic evidence of disease and disappearance of all disease-related symptoms if present before therapy; CRu: CR along with regression in lymph node mass by >75% in SPD; PR: =50% decrease in SPD of 6 largest dominant nodes or nodal masses. The 95% CI for the response rates was estimated for one sample binomial using Pearson-Clopper. Stage I and II: Baseline up to end of induction treatment Cy8 (24 weeks) (1 Cy=3 weeks)
Secondary Stage I: Percentage of Participants With Complete Response at the End of Induction Treatment Assessed Using International Working Group Response Criteria for NHL Complete Response was comprised CR and CRu. A participant was defined as a responder if they sustained a CR or CRu at the end of induction treatment. Response assessment was based on clinical examination and CT scans. Assessment of tumor response was performed according to the International Working Group response criteria for NHL. CR: complete disappearance of all detectable clinical and radiographic evidence of disease and disappearance of all disease-related symptoms if present before therapy; CRu: CR along with regression in lymph node mass by >75% in SPD. The 95% CI for the response rates was estimated for one sample binomial using Pearson-Clopper. Stage I: Baseline up to end of induction treatment Cy8 (24 weeks) (1 Cy=3 weeks)
Secondary Stage II: Percentage of Participants With Complete Response at the End of Induction Treatment Assessed Using International Working Group Response Criteria for NHL Complete Response comprised of CR and CRu. A participant was defined as a responder if they sustained a CR or CRu at the end of induction treatment. Response assessment was based on clinical examination and CT scans. Assessment of tumor response was performed according to the International Working Group response criteria for NHL. CR: complete disappearance of all detectable clinical and radiographic evidence of disease and disappearance of all disease-related symptoms if present before therapy; CRu: CR along with regression in lymph node mass by >75% in SPD. The 95% CI for the response rates was estimated for one sample binomial using Pearson-Clopper. Stage II: Baseline up to end of induction treatment Cy8 (24 weeks) (1 Cy=3 weeks)
Secondary Stage I and II (Pooled): Percentage of Participants With Complete Response at the End of Induction Treatment Assessed Using International Working Group Response Criteria for NHL Complete Response comprised of CR and CRu. A participant was defined as a responder if they sustained a CR or CRu at the end of induction treatment. Response assessment was based on clinical examination and CT scans. Assessment of tumor response was performed according to the International Working Group response criteria for NHL. CR: complete disappearance of all detectable clinical and radiographic evidence of disease and disappearance of all disease-related symptoms if present before therapy; CRu: CR along with regression in lymph node mass by >75% in SPD. The 95% CI for the response rates was estimated for one sample binomial using Pearson-Clopper. Stage I and II: Baseline up to end of induction treatment Cy8 (24 weeks) (1 Cy=3 weeks)
Secondary Stage I and II (Pooled): Percentage of Participants With Complete Response at the End of Maintenance Treatment Assessed Using International Working Group Response Criteria for NHL Complete Response comprised of CR and CRu. A participant was defined as a responder if they sustained a CR or CRu at the end of induction treatment. Response assessment was based on clinical examination and CT scans. Assessment of tumor response was performed according to the International Working Group response criteria for NHL. CR: complete disappearance of all detectable clinical and radiographic evidence of disease and disappearance of all disease-related symptoms if present before therapy; CRu: CR along with regression in lymph node mass by >75% in SPD. The 95% CI for the response rates was estimated for one sample binomial using Pearson-Clopper. Stage I and II: Baseline up to 57 days after last maintenance dose (last maintenance dose: maintenance Cy12/Study Cy20 [30 months]) (up to data cutoff of 31 Oct 2017 [up to 6 years]) (1 Cy=8 weeks)
Secondary Stage I and II (Pooled): Percentage of Participants With Overall Response at the End of Maintenance Treatment Assessed Using International Working Group Response Criteria for NHL Overall Response comprised of CR, CRu, or PR . A participant was defined as a responder if they sustained a CR, CRu or PR at the end of induction treatment. Response assessment was based on clinical examination and CT scans. Assessment of tumor response was performed according to the International Working Group response criteria for NHL. CR: complete disappearance of all detectable clinical and radiographic evidence of disease and disappearance of all disease-related symptoms if present before therapy; CRu: CR along with regression in lymph node mass by >75% in SPD. The 95% CI for the response rates was estimated for one sample binomial using Pearson-Clopper. Stage I and II: Baseline up to 57 days after last maintenance dose (last maintenance dose: maintenance Cy12/Study Cy20 [30 months]) (up to data cutoff of 31 Oct 2017 [up to 6 years]) (1 Cy=8 weeks)
Secondary Stage I and II (Pooled): Percentage of Participants With Disease Progression/Relapse or Death Disease progression: =50% increase from nadir in the SPD of any previously identified abnormal node or appearance of any new lesion during or at the end of therapy or =50% increase in the greatest diameter of any previously identified node >1 cm in its short axis or in the SPD of more than one node. Baseline, D1 of all cycles (Cy 1-20) (1 Cy=3 weeks for Cy1-8 & 8 weeks for Cy9-20), at early withdrawal, at follow-up, every 12 weeks for 96 weeks or until documented disease progression/relapse or death (up to median of 27 months; up to data cutoff of 31 Oct 2017 [up to 6 years]) Baseline up to disease progression or death up to data cutoff of 31 Oct 2017 (up to 6 years) (See detailed timeframe in Outcome Measure description)
Secondary Stage I and II (Pooled): Progression-Free Survival (PFS) Assessed Using International Working Group Response Criteria for NHL PFS was defined as the time from randomization to disease progression/relapse or death due to any cause. If the specified event (disease progression/relapse, death) did not occur, PFS was censored at the last tumor assessment date showing no disease progression, either during treatment or follow-up. Disease progression: =50% increase from nadir in the SPD of any previously identified abnormal node or appearance of any new lesion during or at the end of therapy or =50% increase in the greatest diameter of any previously identified node >1 cm in its short axis or in the SPD of more than one node. PFS analysis was performed using Kaplan - Meier curves. Baseline, D1 of all cycles (Cy 1-20) (1 Cy=3 weeks for Cy1-8 & 8 weeks for Cy9-20), at early withdrawal, at follow-up, every 12 weeks for 96 weeks or until documented disease progression/relapse or death (up to median of 27 months; up to data cutoff of 31 Oct 2017 [up to 6 years]) Baseline up to disease progression or death up to data cutoff of 31 Oct 2017 (up to 6 years) (See detailed timeframe in Outcome Measure description)
Secondary Stage I and II (Pooled): Percentage of Participants With Disease Progression/Relapse, New Anti-Lymphoma Treatment or Death Assessed Using International Working Group Response Criteria for NHL Disease progression: =50% increase from nadir in the SPD of any previously identified abnormal node or appearance of any new lesion during or at the end of therapy or =50% increase in the greatest diameter of any previously identified node >1 cm in its short axis or in the SPD of more than one node. Baseline, D1 of all cycles (Cy 1-20) (1 Cy=3 weeks for Cy1-8 & 8 weeks for Cy9-20), at early withdrawal, at follow-up, every 12 weeks for 96 weeks or until documented disease progression/relapse or death (up to a median of 27 months; up to data cutoff of 31 Oct 2017 [up to 6 years]) Baseline up to disease progression or death up to data cutoff of 31 Oct 2017 (up to 6 years) (See detailed timeframe in Outcome Measure description)
Secondary Stage I and II (Pooled): Event-Free Survival Assessed Using International Working Group Response Criteria for NHL Event-free survival was defined as the time from randomization to disease progression/relapse, death or initiation of new NHL therapy. If the specified event (progression/relapse, death or new anti-lymphoma treatment) did not occur, event-free survival was censored at the last tumor assessment date either during treatment or follow up. Event-free survival analysis was performed using Kaplan-Meier curves. Baseline, D1 of all cycles (Cy 1-20) (1 Cy=3 weeks for Cy1-8 & 8 weeks for Cy9-20), at early withdrawal, at follow-up, every 12 weeks for 96 weeks or until documented disease progression/relapse or death (up to a median of 27 months; up to data cutoff of 31 Oct 2017 [up to 6 years]) Baseline up to disease progression or death up to data cutoff of 31 Oct 2017 (up to 6 years) (See detailed timeframe in Outcome Measure description)
Secondary Percentage of Participants Who Died Baseline up to death (up to data cutoff of 31 Oct 2017 [up to 6 years])
Secondary Overall Survival (OS) OS was defined as the time from randomization to death due to any cause. Participants without event were censored at the time of last follow-up information for survival, ie, at the last time known to be alive. Baseline up to death (up to data cutoff of 31 Oct 2017 [up to 6 years])
Secondary Stage I: Observed Area Under the Serum Concentration-Time Curve (AUC) of Rituximab AUC is a measure of the serum concentration of the drug over time. It is used to characterize drug absorption. Predose (within 2 hr) and 24 hrs postdose on Cy 7 (D1,3,7,15), predose (0 hr) on Cy 8 D1 (1 Cy=3 weeks); additionally within 15 minutes after end of infusion (infusion duration=30 minutes) on Cy 7 D1 for rituximab IV (up to data cutoff of 11 Apr 2012 [up to 26 months]) Stage I (Induction): Predose (within 2 hour [hr]) up to data cutoff of 11 Apr 2012 [up to 26 months]) (See detailed timeframe in Outcome Measure description)
Secondary Stage I: Maximum Serum Concentrations (Cmax) of IV and SC Rituximab Predose (within 2 hr) and 24 hrs postdose on Cy7 (D1,3,7,15), predose (0 hr) on Cy8 D1 (1 Cy=3 weeks); additionally within 15 minutes after end of infusion (infusion duration=30 minutes) on Cy7 D1 for rituximab IV (up to data cutoff of 11 Apr 2012 [up to 26 months]) Stage I (Induction): Predose (within 2hr) up to data cutoff of 11 Apr 2012 [up to 26 months]) (See detailed timeframe in Outcome Measure description)
Secondary Stage I and II (Pooled): Ctrough of Rituximab at Each Induction Treatment Cycle Stage I and II (Induction): Rituximab IV: Predose (within 2 hr) on D1 of Cy1-8 (1 Cy=3 weeks & 4 weeks for Cy8); Rituximab SC: Predose (within 2 hr) on D1 of Cy1 & Cy3-8 (1 Cy=3 weeks and 4 weeks for Cy8), predose (within 2 hr) on D0 of Cy2 (up to data cutoff of 31 Oct 2013 [up to 32 months]) Stage I and II (Pooled): Predose (within 2hr) up to data cutoff of 31 Oct 2013 [up to 32 months]) (See detailed timeframe in Outcome Measure description)
Secondary Stage I and II (Pooled): Ctrough of Rituximab at Each Maintenance Treatment Cycle Stage I and II (maintenance): D29 of Cy8 (induction; 1 Cy=4 weeks), predose (within 2 hr) on D1 of Cy9 to 19 (maintenance Cy1 to 12 [1 Cy=8 weeks]; up to data cutoff of 11 Jan 2016 [up to 6 years]) Stage I and II (maintenance): Predose (within 2hr) up to data cutoff of 11 Jan 2016 [up to 6 years]) (See detailed timeframe in Outcome Measure description)
Secondary Stage I and II (Pooled): Rituximab Levels 12 Weeks, 24 Weeks, and 36 Weeks After the Last Rituximab Administration 12 weeks, 24 weeks, and 36 weeks after the last rituximab administration (up to data cutoff of 11 Jan 2016 [up to 6 years])
Secondary Percentage of Participants With B-Cell Depletion by Cycle for Induction Phase Depletion is defined as a cluster of differentiation (CD) 19 value <80 cells per cubic millimeter (cells/mm^3). Stage I and II (induction): for rituximab IV - D1 of Cy 1 to 8 (1 Cy=3 weeks); for rituximab SC - D1 of Cy 1 and Cy 3 to 8, D0 of Cy 2
Secondary Percentage of Participants With B-Cell Depletion by Cycle for Maintenance Phase Depletion is defined as a CD19 value <80 cells/mm^3. Stage I and II (maintenance): D1 of Cy 9 to 20 (1 Cy=8 weeks) (up to data cutoff of 11 Jan 2016 [up to 6 years])
Secondary Stage I and II (Pooled): Percentage of Participants Positive for Human Anti-Chimeric Antibodies (HACAs) to Rituximab Levels of HACA in serum were detected at Day 1 of each cycle up to Cycle 8 and at follow-up visit. Stage I and II: Baseline: pre-dose (72 hours prior) D1 of Cy1, Cy 3-20, D0 of Cy2 (1 Cy=3 weeks for Cy1-8 & 8 weeks for Cy9-20), post-baseline: every 12 weeks after last rituximab administration until 96 weeks (a median of 27 months; up to data cutoff of 11 Jan 2016 [up to 6 years]) Stage I and II: Baseline, post-baseline (See detailed timeframe in Outcome Measure description)
Secondary Stage I and II (Pooled): Percentage of Participants Positive for Human Anti-Human Antibodies (HAHAs) to Rituximab Levels of HAHA in serum were detected at Day 1 of each cycle up to Cycle 8 and at follow-up visit. Stage I and II: Baseline: pre-dose (72 hours prior) D1 of Cy1, Cy 3-20, D0 of Cy2 (1 Cy=3 weeks for Cy1-8 & 8 weeks for Cy9-20), post-baseline: every 12 weeks after last rituximab administration until 96 weeks (a median of 27 months; up to data cutoff of 11 Jan 2016 [up to 6 years]) Stage I and II: Baseline, post-baseline (See detailed timeframe in Outcome Measure description)
Secondary Stage I and II (Pooled): Percentage of Responses Showing Time Saved of Staff as Per Physician/Nurse Opinions With Each Administration of Rituximab SC as Compared to Rituximab IV at the End of Cy 8, 15 and 20 All investigator physicians and nurses involved in this study were asked to provide the staff time that could be saved with each administration of rituximab SC as compared with rituximab IV to participants in routine practice afetr Cy 8, 15, 20 and categorized as less than (<) 1 hr, at least 1 hr but <2 hrs, at least 2 hrs but <3 hrs, at least 3 hrs but <4 hrs, >/=4 hrs. Staff were asked not to consider the time needed for the first IV administration. Analysis was done in all participants to show a comparison on the time saved by staffs when administered via SC and IV. After Cycle 8 of induction treatment (24 weeks) and during the maintenance part of the study after 12 months (i.e., Cycle 15), and after the end of the maintenance treatment, (i.e., Cycle 20) (1 Cycle=4 weeks for Cycle 8 and 8 weeks for Cycles 15 and 20)
Secondary Percentage of Responses Who Showed Rituximab SC Formulation Convenient as Compared to Rituximab IV Formulation as Assessed by Physician/Nurse Opinion All investigator physicians and nurses involved in this study were asked to complete question i.e. "Which formulation of rituximab (SC or IV) do you think is more convenient?" based on their experience with the rituximab SC and IV formulations across all participants and presented as rituximab SC is much more convenient; rituximab SC is a little more convenient; both formulations are equally convenient; rituximab IV is a little more convenient; and rituximab IV is much more convenient. After Cycle 8 of induction treatment (24 weeks) and during the maintenance part of the study after 12 months (i.e., Cycle 15), and after the end of the maintenance treatment, (i.e., Cycle 20) (1 Cycle=4 weeks for Cycle 8 and 8 weeks for Cycles 15 and 20)
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