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NCT01014208 Clinical Trial

Ofatumumab Versus Rituximab Salvage Chemoimmunotherapy Followed by Autologous Stem Cell Transplant in Relapsed or Refractory Diffuse Large B Cell Lymphoma

Lymphoma, Large-Cell, Diffuse Clinical Trial

ORCHARRD

Official title:
Ofatumumab Versus Rituximab Salvage Chemoimmunotherapy Followed by Autologous Stem Cell Transplant (ASCT) in Relapsed or Refractory Diffuse Large B Cell Lymphoma (DLBCL)

Clinical Trial Details — Status: Completed

Administrative data
NCT number NCT01014208
Other study ID # 110928
Secondary ID
Status Completed
Phase Phase 3
First received November 4, 2009
Last updated July 9, 2015
Start date March 2010
Est. completion date November 2014

Study information
Verified date February 2015
Source GlaxoSmithKline
Contact n/a
Is FDA regulated No
Health authority United States: Institutional Review BoardUnited States: Food and Drug Administration
Study type Interventional

Clinical Trial Summary

This study is being conducted to compare the efficacy and safety of ofatumumab in addition to salvage chemotherapy versus rituximab in addition to salvage chemotherapy in CD20 positive DLBCL subjects relapsing, or with persistent disease, after first-line treatment with rituximab combined with an anthracycline-based chemotherapy regimen and be eligible for ASCT.

Description:

As rituximab-based regimens have become standard first-line treatment in CD20 positive DLBCL, the efficacy of rituximab combined with salvage chemotherapy in the second-line setting has decreased and there is a need for new therapies in patients progressing or relapsing after first-line rituximab-based therapy. Replacement of rituximab with ofatumumab in the second-line setting, following progression/relapse after first-line rituximab-containing regimens, offers the potential to overcome relative or complete rituximab resistance and thus improve response rates, the ability to proceed to consolidative HDT/ASCT, and overall survival.

Recruitment information / eligibility
Status Completed
Enrollment 447
Est. completion date November 2014
Est. primary completion date February 2014
Accepts healthy volunteers No
Gender Both
Age group 18 Years and older
Eligibility Inclusion Criteria:

- Subjects with CD20 positive DLBCL or grade 3b follicular lymphoma (FL) at original diagnosis.

- Refractory to, or relapsed following, first-line treatment with rituximab combined with anthracycline- or anthracenedione-based chemotherapy as defined by the protocol.

- CT with involvement of 2 or more clearly demarcated lesions/ nodes with a long axis > 1.5 cm and short axis >= 1.0cm or 1 clearly demarcated lesion/ node with a long axis > 2.0 cm and short axis >= 1.0 cm.

- Baseline FDG-PET scans must demonstrate positive lesions compatible with CT defined anatomical tumor sites.

- Age 18 yrs or older.

- ECOG performance status of 0, 1 or 2.

- Eligible for high dose chemotherapy and ASCT.

- Resolution of toxicities from first-line therapy to a grade that in the opinion of the investigator does not contraindicate study participation.

- Signed written informed consent.

Exclusion Criteria:

- Previous cancer therapy for lymphoma, with the exception of first-line rituximab/ anthracycline- or anthracenedione-based chemotherapy, monotherapy rituximab prior to or combined with first-line chemotherapy, as maintenance therapy, and radiotherapy in a limited field or as a part of the first-line treatment plan.

- Any anti-cancer therapy, except limited field radiotherapy, within 2 weeks prior to start of study therapy.

- Planned post-randomization chronic glucocorticoid use (limited acute use is allowed and defined by the protocol) unless administered as therapy for mild COPD or asthma.

- Clinically significant cardiac disease, active or chronic infections, serious significant diseases, other cancer within last 5 years. History of significant cerebrovascular disease.

- Prior treatment with anti-CD20 monoclonal antibodies with the exception of rituximab.

- Abnormal/ inadequate WBC count, liver, and kidney function.

- Pregnant or lactating women or female patients of child-bearing potential (or male patients with such partners) not willing to use adequate contraception during and up to 1 year following dosing completion.

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment

Related Conditions & MeSH terms

Intervention

Drug:
OFATUMUMAB + DHAP
3 cycles of treatment will be administered. Each cycle will last 21 days. ofatumumab dose: cycle 1, day 1 - 1000 mg; cycle 1, day 8 - 1000 mg; cycle 2, day 1 and cycle 3, day 1 - 1000 mg. DHAP regimen: dexamethasone - 40 mg on days 1, 2, 3, and 4 of dosing cycle; cisplatin - 100 mg/m2/24hrs continuous on day 1 of dosing cycle; cytarabine - 2g/m2 q12 hrs (2 doses) on day 2 of dosing cycle.
RITUXIMAB + DHAP
3 cycles of treatment will be administered. Each cycle will last 21 days. rituximab dose: cycle 1, day 1 - 375 mg/m2; cycle 1, day 8 - 375 mg/m2; cycle 2, day 1 and cycle 3, day 1 - 375 mg/m2. DHAP regimen: dexamethasone - 40 mg on days 1, 2, 3, and 4 of dosing cycle; cisplatin - 100 mg/m2/24hrs continuous on day 1 of dosing cycle; cytarabine - 2g/m2 q12 hrs (2 doses) on day 2 of dosing cycle.

Locations
Country Name City State
Argentina GSK Investigational Site Capital Federal Buenos Aires
Argentina GSK Investigational Site Ciudad Autonoma de Buenos Aires Buenos Aires
Argentina GSK Investigational Site La Plata Buenos Aires
Austria GSK Investigational Site Graz
Austria GSK Investigational Site Innsbruck
Austria GSK Investigational Site Linz
Austria GSK Investigational Site Linz
Austria GSK Investigational Site Salzburg
Austria GSK Investigational Site Wien
Austria GSK Investigational Site Wien
Belgium GSK Investigational Site Brugge
Belgium GSK Investigational Site Bruxelles
Belgium GSK Investigational Site Gent
Belgium GSK Investigational Site Hasselt
Belgium GSK Investigational Site Leuven
Belgium GSK Investigational Site Yvoir
China GSK Investigational Site Beijing
China GSK Investigational Site Beijing
China GSK Investigational Site Beijing
China GSK Investigational Site Beijing
China GSK Investigational Site Beijing
China GSK Investigational Site Beijing
China GSK Investigational Site Beijing
China GSK Investigational Site Chengdu
China GSK Investigational Site Fuzhou Fujian
China GSK Investigational Site Guangzhou Guangdong
China GSK Investigational Site Guangzhou Guangdong
China GSK Investigational Site Guangzhou Guangdong
China GSK Investigational Site Hangzhou Zhejiang
China GSK Investigational Site Jianan Shandong
China GSK Investigational Site Jiang Su Province
China GSK Investigational Site Nanjing Jiangsu
China GSK Investigational Site Shanghai
China GSK Investigational Site Shanghai
China GSK Investigational Site Tianjin
Czech Republic GSK Investigational Site Brno
Czech Republic GSK Investigational Site Hradec Kralove
Denmark GSK Investigational Site Aarhus
Denmark GSK Investigational Site Koebenhavn
Estonia GSK Investigational Site Tallinn
Estonia GSK Investigational Site Tartu
Finland GSK Investigational Site Helsinki
Finland GSK Investigational Site Oulu
Finland GSK Investigational Site Tampere
Germany GSK Investigational Site Aachen Nordrhein-Westfalen
Germany GSK Investigational Site Berlin
Germany GSK Investigational Site Muenster Nordrhein-Westfalen
Germany GSK Investigational Site Ulm Baden-Wuerttemberg
Greece GSK Investigational Site Athens
Greece GSK Investigational Site Athens
Hungary GSK Investigational Site Budapest
Hungary GSK Investigational Site Budapest
Hungary GSK Investigational Site Debrecen
Hungary GSK Investigational Site Gyor
Hungary GSK Investigational Site Kaposvár
Hungary GSK Investigational Site Szeged
Hungary GSK Investigational Site Szombathely
India GSK Investigational Site Ludhiana
India GSK Investigational Site Pune
India GSK Investigational Site Vellore
Ireland GSK Investigational Site Dublin
Ireland GSK Investigational Site Galway
Ireland GSK Investigational Site James Street
Israel GSK Investigational Site Petach-Tikva
Israel GSK Investigational Site Ramat Gan
Japan GSK Investigational Site Aichi
Japan GSK Investigational Site Akita
Japan GSK Investigational Site Fukuoka
Japan GSK Investigational Site Hokkaido
Japan GSK Investigational Site Hyogo
Japan GSK Investigational Site Ibaraki
Japan GSK Investigational Site Kanagawa
Japan GSK Investigational Site Kanagawa
Japan GSK Investigational Site Kyoto
Japan GSK Investigational Site Miyagi
Japan GSK Investigational Site Nagano
Japan GSK Investigational Site Nagasaki
Japan GSK Investigational Site Okayama
Japan GSK Investigational Site Osaka
Japan GSK Investigational Site Tochigi
Japan GSK Investigational Site Tokushima
Japan GSK Investigational Site Tokyo
Japan GSK Investigational Site Tokyo
Japan GSK Investigational Site Tokyo
Japan GSK Investigational Site Tokyo
Korea, Republic of GSK Investigational Site Jellanamdo
Korea, Republic of GSK Investigational Site Seoul
Korea, Republic of GSK Investigational Site Seoul
Netherlands GSK Investigational Site Amersfoort
Netherlands GSK Investigational Site Amsterdam
Netherlands GSK Investigational Site Amsterdam
Netherlands GSK Investigational Site Amsterdam
Netherlands GSK Investigational Site Den Haag
Netherlands GSK Investigational Site Enschede
Netherlands GSK Investigational Site Groningen
Netherlands GSK Investigational Site Hoofddorp
Netherlands GSK Investigational Site Leiden
Netherlands GSK Investigational Site Maastricht
Netherlands GSK Investigational Site Nieuwegein
Netherlands GSK Investigational Site Nijmegen
Netherlands GSK Investigational Site Rotterdam
Netherlands GSK Investigational Site Rotterdam
Netherlands GSK Investigational Site Rotterdam
Netherlands GSK Investigational Site Sittard-geleen
Netherlands GSK Investigational Site Utrecht
Netherlands GSK Investigational Site Zwolle
Norway GSK Investigational Site Oslo
Poland GSK Investigational Site Chorzow
Poland GSK Investigational Site Gdansk
Poland GSK Investigational Site Poznan
Poland GSK Investigational Site Warszawa
Poland GSK Investigational Site Warszawa
Poland GSK Investigational Site Wroclaw
Russian Federation GSK Investigational Site Moscow
Russian Federation GSK Investigational Site St-Petersburg
Russian Federation GSK Investigational Site St. Petersburg
Singapore GSK Investigational Site Singapore
Spain GSK Investigational Site Barcelona
Spain GSK Investigational Site Madrid
Spain GSK Investigational Site Madrid
Spain GSK Investigational Site Madrid
Spain GSK Investigational Site Madrid
Spain GSK Investigational Site Majadahonda (Madrid)
Spain GSK Investigational Site Murcia
Spain GSK Investigational Site Pamplona
Spain GSK Investigational Site Pozuelo de Alarcón/Madrid
Spain GSK Investigational Site Salamanca
Sweden GSK Investigational Site Göteborg
Sweden GSK Investigational Site Lund
Sweden GSK Investigational Site Stockholm
Sweden GSK Investigational Site Uppsala
Thailand GSK Investigational Site Bangkok
Thailand GSK Investigational Site Bangkok
Thailand GSK Investigational Site Bangkok
United Kingdom GSK Investigational Site Birmingham
United Kingdom GSK Investigational Site Blackpool
United Kingdom GSK Investigational Site Bristol
United Kingdom GSK Investigational Site Cambridge
United Kingdom GSK Investigational Site Cheltenham
United Kingdom GSK Investigational Site Edinburgh
United Kingdom GSK Investigational Site Glasgow
United Kingdom GSK Investigational Site Headington, Oxford
United Kingdom GSK Investigational Site Leeds
United Kingdom GSK Investigational Site Liverpool
United Kingdom GSK Investigational Site London
United Kingdom GSK Investigational Site London
United Kingdom GSK Investigational Site London
United Kingdom GSK Investigational Site London
United Kingdom GSK Investigational Site Manchester
United Kingdom GSK Investigational Site Manchester
United Kingdom GSK Investigational Site Newcastle upon Tyne
United Kingdom GSK Investigational Site Northwood
United Kingdom GSK Investigational Site Nottingham
United Kingdom GSK Investigational Site Sheffield
United Kingdom GSK Investigational Site Southampton
United Kingdom GSK Investigational Site Whitchurch, Cardiff
United Kingdom GSK Investigational Site Wolverhampton
United States GSK Investigational Site Chaple Hill North Carolina
United States GSK Investigational Site Charleston South Carolina
United States GSK Investigational Site Chicago Illinois
United States GSK Investigational Site Chicago Illinois
United States GSK Investigational Site Greenville South Carolina
United States GSK Investigational Site Jackson Mississippi
United States GSK Investigational Site Nashville Tennessee
United States GSK Investigational Site New Haven Connecticut
United States GSK Investigational Site New York New York
United States GSK Investigational Site Philadelphia Pennsylvania
United States GSK Investigational Site Providence Rhode Island
United States GSK Investigational Site Sacramento California
United States GSK Investigational Site San Antonio Texas
United States GSK Investigational Site Seattle Washington
United States GSK Investigational Site Syracuse New York
United States GSK Investigational Site Westwood Kansas

Sponsors (1)
Lead Sponsor Collaborator
GlaxoSmithKline

Countries where clinical trial is conducted

United States,  Argentina,  Austria,  Belgium,  China,  Czech Republic,  Denmark,  Estonia,  Finland,  Germany,  Greece,  Hungary,  India,  Ireland,  Israel,  Japan,  Korea, Republic of,  Netherlands,  Norway,  Poland,  Russian Federation,  Singapore,  Spain,  Sweden,  Thailand,  United Kingdom, 

Outcome
Type Measure Description Time frame Safety issue
Primary Progression-free Survival as Assessed by Independent Reviewers Progression-free survival is defined as the interval of time from the randomization date until the date of stable disease (SD; failure to attain the criteria needed for a CR or PR and no fulfillment of the criteria for progressive disease [PD]) after two cycles of salvage chemotherapy, progression, or death, whichever occurs first. Disease progression was based on the assessments of independent reviewers for the disease under study. Disease progression was based on imaging data via the Revised Response Criteria for Malignant Lymphoma (RRCML). From randomization until the date of stable disease after two cycles of salvage chemotherapy, progression, or death (assessed for up to 5 years) No
Secondary Number of Participants With Overall Response (OR) and Complete Response (CR) After Salvage Chemoimmunotherapy OR is defined as the number of participants achieving either a complete response (CR) or a partial response (PR). CR is defined as the complete disappearance of all detectable clinical evidence of disease and disease-related symptoms. PR is defined as at least a 50% decrease from Baseline in the sum of the product of the diameters of target lesions. RRCML was used to assess CR and PR. At completion of up to 3 cycles of salvage chemoimmunotherapy (assessed up to 9 weeks) No
Secondary Number of Participants With Overall Response (OR) and Complete Response (CR) Three Months After Autologous Stem Cell Transplant OR is defined as the number of participants achieving either a complete response (CR) or a partial response (PR). CR is defined as the complete disappearance of all detectable clinical evidence of disease and disease-related symptoms. PR is defined as at least a 50% decrease from Baseline in the sum of the product of the diameters of target lesions. RRCML was used to assess CR and PR. At 3 months after completion of autologous stem cell transplantation (ASCT) (assessed up to 6 months) No
Secondary Event-free Survival Event-free survival is defined as the time from randomization to progressive disease (PD; disease whose course is growth, or spread of the disease), stable disease (SD; failure to attain the criteria needed for a CR or PR and no fulfillment of the criteria for PD) after completion of 2 cycles of therapy, commencement of a new treatment for diffuse large B cell lymphoma (DLBCL) (e.g., radiotherapy), or death from any cause, whichever occurs first. Disease progression was based on the assessments of independent reviewers for the disease under study. Disease progression was based on imaging data via the Revised Response Criteria for Malignant Lymphoma (RRCML). From randomization to progressive disease, stable disease after completion of 2 cycles of therapy, commencement of a new treatment for DLBCL, or death due to any cause (assessed for up to 5 years) No
Secondary Overall Survival (OS) OS is defined as the time from randomization to death due to any cause. Participants who were still alive by the end of the study were censored. From randomization to death due to any cause (assessed for up to 5 years) No
Secondary Number of Participants With the Ability to Mobilize at Least 2 Million Cluster of Differentiation (CD)34+ Cells Per Kilogram From Peripheral Blood Stem cell mobilization is the process of stimulating the hematopoietic stem cells (CD34+) to move out of the bone marrow and into the bloodstream, where they can be collected via a process called apheresis. Successful mobilization is defined as the collection of >2*10^6 CD34+ cells/kg. Only those participants, who commenced harvest, following the administration of rituximab or ofatumumab in combination with DHAP combination chemotherapy, were assessed. The number of participants with adequate harvest of CD34+ stem cells (at least 2*10^6 CD34+ cells/kg) after dosing of salvage therapy in Cycle 2 and Cycle 3 was analyzed. During Cycles 2 and/or 3 (Weeks 4-9) No
Secondary Number of Participants Completing Autologous Stem Cell Transplant (ASCT) The number of participants who completed ASCT is reported. Approximately 4 to 6 weeks following Cycle 3 (assessed up to 3 months) No
Secondary Change From Baseline in Functional Assessment of Cancer Therapy-General (FACT-G) During Treatment The FACT-G was developed by the Functional Assessment of Chronic Illness Therapy (FACIT) group for use in adults in a wide range of oncology clinical trial populations. The 27 items of the FACT-G are scored in the following domains: Physical Well-being (7 items), Social/Family Wellbeing (7 items), Emotional Well-being (6 items), and Functional Well-being (7 items). Participants responded to the items on a five-point Likert scale ranging from 0, "Not at all" to 4, "Very much." The total score ranges from 0 to 108; higher scores indicate a better patient-reported outcome/quality of life. Participants were asked to think back over the past week when responding to the items. Baseline and the end of the treatment period (until approximately 4 to 6 weeks following Cycle 3 [assessed up to 3 months]) No
Secondary Change From Baseline in the Functional Assessment of Cancer Therapy Lymphoma Trial Outcome Index (FACT-Lym TOI) Total Score During Treatment The FACT-Lym TOI is a measure that combines the FACT-Lym subscale (15 items; responses to each item range from 0, "Not at all" to 4, "Very much") with two domains taken from the FACT-G (responses to each item range from "Not at all " to "Very much"): Physical Well-being (7 items: lack of energy, nausea, meeting family needs, pain, side effects, feels ill, spends time in bed) and Functional Well-being (7 items: ability to work, work fulfilment, ability to enjoy life, illness acceptance, ability to sleep well, enjoying things done for fun, satisfaction with quality of life). This index is designed to be sensitive to changes in treatment regimens. The total FACT-Lym TOI score ranges from 0 to 116; higher scores indicate a better patient-reported outcome/quality of life. Participants were asked to think back over the past week when responding to the items. Baseline and the end of the treatment period (until approximately 4 to 6 weeks following Cycle 3 [assessed up to 3 months]) No
Secondary Time to Neutrophil and Platelet Recovery After Each Cycle of Salvage Chemotherapy Neutrophil (absolute neutrophil count [ANC]) recovery is defined as ANC >=0.5*10^9/Liter and increasing, and platelet (PLT) recovery is defined as PLT >=10*10^9/Liter and increasing. For each cycle, time to ANC recovery is defined as the time from the first dose to the first ANC >=0.5*10^9/Liter and increasing after the nadir in the cycle. For each cycle, time to PLT recovery is defined as the time from the first dose to the first PLT >=10*10^9/L and increasing after the nadir in the cycle. From the start of each cycle for a maximum of 5 weeks per cycle (assessed during treatment period of Baseline up to approximately 3 months) No
Secondary Time to Engraftment After High-dose Therapy (HDT)/ASCT Engraftment is defined as 1) three consecutive days when the ANC is =0.5x109/L and 2) an unsupported platelet count of =20x109/L, and the engraftment date is the date that this occurs. If engraftment was not achieved by Day 42 or the last observation, engraftment was deemed to be a failure, and censoring took place at Day 42 or at the last observation. From ASCT up to 42 days post-ASCT (Baseline up to approximately 4.5 months) No
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