A Study to Evaluate the Benefit of Venetoclax Plus Rituximab Compared With Bendamustine Plus Rituximab in Participants With Relapsed or Refractory Chronic Lymphocytic Leukemia (CLL)

Phase 3

Completed

• Conditions: Chronic Lymphocytic Leukemia
• Interventions: Drug: Bendamustine; Drug: Venetoclax; Drug: Rituximab

• Registration Number: NCT02005471
• Lead Sponsor: Hoffmann-La Roche

Brief Summary

The purpose of this open-label, multicenter, randomized, Phase III study is to evaluate the benefit of venetoclax in combination with rituximab compared with bendamustine in combination with rituximab in participants with relapsed or refractory CLL. Participants will be randomly assigned in 1:1 ratio to receive either venetoclax + rituximab (Arm A) or bendamustine + rituximab (Arm B).

Detailed Description

Not available

Study Timeline

• Study First Submitted: 2013-12-04
• Study First Submitted QC: 2013-12-04
• Study First Posted: 2013-12-09
• Study Start: 2014-03-17
• Primary Completion: 2017-05-08
• Results First Submitted: 2018-05-03
• Results First Submitted QC: 2018-09-28
• Results First Posted: 2018-10-01
• Study Completion: 2022-08-03
• Status Verified: 2023-09
• Last Update Submitted: 2023-09-22
• Last Update Posted: 2023-10-17

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 389

Inclusion Criteria

• Diagnosis of CLL per diagnostic criteria for relapsed or refractory CLL per the international workshop on chronic lymphocytic leukemia (iwCLL) guidelines
• Previously treated with 1-3 lines of therapy (example: completed greater than or equal to [>/=] 2 treatment cycles per therapy), including at least one standard chemotherapy-containing regimen
• Participants previously treated with bendamustine only if their duration of response was >/= 24 months
• Eastern Cooperative Oncology Group (ECOG) performance score of less than or equal to (</=) 1
• Adequate bone marrow function
• Adequate renal and hepatic function
• Participants must use effective birth control throughout study until at least 30 days after study treatment or 1 year after rituximab treatment, whichever is later; female participants must not be pregnant or breast-feeding
• For participants with the 17p deletion, previously treated with 1-3 lines of therapy, including at least one prior standard chemotherapy-containing regimen or at least one prior alemtuzumab-containing therapy

Inclusion Criteria R/C Substudy:

• Participants randomized to Arm A or Arm B with a confirmed disease progression of CLL per iwCLL criteria
• Participants who have not received new anti-CLL therapy following disease progression in Arm A or Arm B
• Adequate renal and hepatic function per laboratory reference range

Exclusion Criteria

• Transformation of CLL to aggressive non-Hodgkin lymphoma or central nervous system (CNS) involvement by CLL
• Undergone an allogenic stem cell transplant
• A history of significant renal, neurologic, psychiatric, endocrine, metabolic, immunologic, cardiovascular or hepatic disease
• Hepatitis B or C or known human immunodeficiency virus (HIV) positive
• Receiving warfarin treatment
• Received an anti-CLL monoclonal antibody within 8 weeks prior to the first dose of study drug
• Received any anti-cancer or investigational therapy within 28 days prior to the first dose of study drug or has not recovered to less than Grade 2 clinically significant adverse effect(s)/toxicity(ies) of any previous therapy
• Received cytochrome P450 3A4 (CYP3A4) inhibitors (such as fluconazole, ketoconazole and clarithromycin) or inducers (such as rifampin, carbamazapine, phenytoin, St. John's Wort) within 7 days prior to the first dose of venetoclax
• History of prior venetoclax treatment
• Participants with another cancer, history of another cancer considered uncured on in complete remission for <5 years, or currently under treatment for another suspected cancer except non-melanoma skin cancer or carcinoma in situ of the cervix that has been treated or excised and is considered resolved
• Malabsorption syndrome or other condition that precludes enteral route of administration
• Other clinically significant uncontrolled condition(s) including, but not limited to, systemic infection (viral, bacterial or fungal)
• Vaccination with a live vaccine within 28 days prior to randomization
• Consumed grapefruit or grapefruit products, seville oranges (including marmalade containing seville oranges), or star fruit within 3 days prior to the first dose of study treatment
• A cardiovascular disability status of New York Heart Association Class >/=3. Class 3 is defined as cardiac disease in which participants are comfortable at rest but have marked limitation of physical activity due to fatigue, palpitations, dyspnea, or anginal pain
• Major surgery within 30 days prior to the first dose of study treatment
• A participant who is pregnant or breastfeeding
• Known allergy to both xanthine oxidase inhibitors and rasburicase

Exclusion Criteria R/C Substudy:

• Transformation of CLL to aggressive NHL (e.g., Richter's transformation, prolymphocytic leukemia, or DLBCL) or CNS involvement by CLL
• Evidence of other clinically significant uncontrolled condition(s) including, but not limited to, uncontrolled systemic infection (viral, bacterial, or fungal)
• Development of other malignancy since enrollment into the study, with the exception of curatively treated basal cell carcinoma or squamous cell carcinoma of the skin or carcinoma in situ of the cervix
• Uncontrolled autoimmune hemolytic anemia or immune thrombocytopenia
• History of severe (i.e., requiring permanent discontinuation of prior rituximab therapy) prior allergic or anaphylactic reactions to rituximab
• Known HIV positivity
• Positive test results for chronic hepatitis B infection (defined as positive hepatitis B surface antigen [HbsAg] serology)
• Positive test results for hepatitis C virus (HCV; HCV antibody serology testing)
• Requires the use of warfarin (due to potential drug interactions that may potentially increase the exposure of warfarin)
• Has not recovered to less than Grade 2 clinically significant adverse effect(s)/toxicity(ies) of any previous therapy
• Received potent CYP3A4 inhibitors (such as fluconazole, ketoconazole, and clarithromycin) within 7 days prior to the first dose of study treatment
• Received potent CYP3A4 inducers (such as rifampin, carbamazepine, phenytoin, St. John's wort) within 7 days prior to the first dose of study treatment
• Consumed grapefruit or grapefruit products, Seville oranges (including marmalade containing Seville oranges), or star fruit within 3 days prior to the first dose of study treatment
• A cardiovascular disability status of New York Heart Association Class >/= 3
• A significant history of renal, neurologic, psychiatric, endocrine, metabolic, immunologic, cardiovascular, or hepatic disease that, in the opinion of the investigator, would adversely affect the participants's participation in this study or interpretation of study outcomes
• Major surgery within 30 days prior to the first dose of study treatment
• A participant who is pregnant or breastfeeding
• Malabsorption syndrome or other condition that precludes enteral route of administration
• Known allergy to both xanthine oxidase inhibitors and rasburicase
• Vaccination with a live vaccine within 28 days prior to randomization

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Bendamustine + Rituximab	Bendamustine	Participants will receive bendamustine 70 milligrams per meter square (mg/m\^2) via intravenous (IV) infusion on Days 1 and 2 of each 28-day cycle for 6 cycles, in combination with rituximab 375 mg/m\^2 via IV infusion on Day 1 of Cycle 1 followed by 500 mg/m\^2 on Day 1 of Cycles 2-6.
Bendamustine + Rituximab	Rituximab	Participants will receive bendamustine 70 milligrams per meter square (mg/m\^2) via intravenous (IV) infusion on Days 1 and 2 of each 28-day cycle for 6 cycles, in combination with rituximab 375 mg/m\^2 via IV infusion on Day 1 of Cycle 1 followed by 500 mg/m\^2 on Day 1 of Cycles 2-6.
Venetoclax + Rituximab	Venetoclax	Participants will be initially placed on a venetoclax 5 weeks ramp-up period, and will receive an initial dose of 20 milligrams (mg) via tablet orally once daily (QD). Then the dose will be incremented weekly up to a maximum dose of 400 mg. Participants will then continue receiving venetoclax 400 mg QD from Week 6 (Day 1 of Cycle 1 of combination therapy) onwards, as directed by the investigator, in combination with rituximab 375 mg/m\^2 via IV infusion on Day 1 of Cycle 1 followed by 500 mg/m\^2 on Day 1 of Cycles 2-6.
Venetoclax + Rituximab	Rituximab	Participants will be initially placed on a venetoclax 5 weeks ramp-up period, and will receive an initial dose of 20 milligrams (mg) via tablet orally once daily (QD). Then the dose will be incremented weekly up to a maximum dose of 400 mg. Participants will then continue receiving venetoclax 400 mg QD from Week 6 (Day 1 of Cycle 1 of combination therapy) onwards, as directed by the investigator, in combination with rituximab 375 mg/m\^2 via IV infusion on Day 1 of Cycle 1 followed by 500 mg/m\^2 on Day 1 of Cycles 2-6.
Bendamustine + Rituximab Crossover Substudy	Venetoclax	Participants entering the Crossover Substudy will have a 5-week venetoclax dose ramp-up period to reach the target dose of 400 mg QD. Following the venetoclax ramp-up period, Participants will receive 6 cycles of rituximab consisting of a single infusion on the first day of each 28-day cycle. Participants will continue to take their daily dose of venetoclax during the rituximab cycles. Participants who have not progressed following the completion of the 6 cycles will continue to receive venetoclax monotherapy until disease progression or for a maximum of 2 years from Cycle 1 Crossover Day 1 of the Substudy.
Bendamustine + Rituximab Crossover Substudy	Rituximab	Participants entering the Crossover Substudy will have a 5-week venetoclax dose ramp-up period to reach the target dose of 400 mg QD. Following the venetoclax ramp-up period, Participants will receive 6 cycles of rituximab consisting of a single infusion on the first day of each 28-day cycle. Participants will continue to take their daily dose of venetoclax during the rituximab cycles. Participants who have not progressed following the completion of the 6 cycles will continue to receive venetoclax monotherapy until disease progression or for a maximum of 2 years from Cycle 1 Crossover Day 1 of the Substudy.
Venetoclax + Rituximab Re-Treatment	Venetoclax	Participants entering the Re-Treatment Substudy will have a 5-week venetoclax dose ramp-up period to reach the target dose of 400 mg QD. Following the venetoclax ramp-up period, Participants will receive 6 cycles of rituximab consisting of a single infusion on the first day of each 28-day cycle. Participants will continue to take their daily dose of venetoclax during the rituximab cycles. Participants who have not progressed following the completion of the 6 cycles will continue to receive venetoclax monotherapy until disease progression or for a maximum of 2 years from Cycle 1 Re-Treatment Day 1 of the Substudy.
Venetoclax + Rituximab Re-Treatment	Rituximab	Participants entering the Re-Treatment Substudy will have a 5-week venetoclax dose ramp-up period to reach the target dose of 400 mg QD. Following the venetoclax ramp-up period, Participants will receive 6 cycles of rituximab consisting of a single infusion on the first day of each 28-day cycle. Participants will continue to take their daily dose of venetoclax during the rituximab cycles. Participants who have not progressed following the completion of the 6 cycles will continue to receive venetoclax monotherapy until disease progression or for a maximum of 2 years from Cycle 1 Re-Treatment Day 1 of the Substudy.

Primary Outcome Measures

Name	Time	Method
Percentage of Participants With PD as Assessed by the Investigator Using Standard International Workshop on Chronic Lymphocytic Leukemia (iwCLL) Guidelines or Death	Baseline up to PD or death from any cause, whichever occurred first (up to approximately 8 years 5 months)	Assessment of response was performed by the investigator according to the iwCLL guidelines. PD was defined as occurrence of one of the following events: appearance of any new extra nodal lesion; new palpable lymph node (greater than \[\>\] 1.5 centimeters \[cm\]); unequivocal progression of non-target lesion; an increase of greater than or equal to (\>/=) 50 percent (%) compared to baseline in splenomegaly, hepatomegaly, number of blood lymphocytes with lymphocyte count \>/=5000 per microliter (mcL), or in longest diameter of any extra nodal lesion; transformation to a more aggressive histology; decrease of \>/=50% compared to baseline in platelet or neutrophil count; or decrease in hemoglobin level by \>2 grams per deciliter (g/dL) or to less than \[\<\] 10 g/dL. Percentages are rounded off.
Progression-Free Survival (PFS) as Assessed by the Investigator Using Standard iwCLL Guidelines	Baseline up to PD or death, whichever occurred first (up to approximately 8 years 5 months)	PFS was defined as the time from randomization until first occurrence of PD/relapse as assessed by the investigator using iwCLL guidelines, or death from any cause, whichever occurred first. PD: occurrence of one of the following: new lesion; new palpable lymph node (\>1.5 cm); unequivocal progression of non-target lesion; increase of \>/=50% in splenomegaly, hepatomegaly, blood lymphocytes with count \>/=5000/mcL, longest diameter of any lesion; transformation to more aggressive histology; decrease of \>/=50% in platelet or neutrophil count, or hemoglobin level by \>2 g/dL or to \<10 g/dL. Participants who had not progressed, relapsed, or died at the time of analysis, were censored on the date of last assessment. In case of no disease assessment after baseline, PFS was censored at the time of randomization+1 day. The median PFS was estimated using Kaplan-Meier method and the 95% confidence interval (CI) was computed using method of Brookmeyer and Crowley.

Secondary Outcome Measures

Name	Time	Method
Event-Free Survival (EFS) as Assessed by the Investigator Using iwCLL Guidelines	Baseline up to PD/relapse, start of a new anti-CLL therapy, or death from any cause, whichever occurred first (approximately 8 years 5 months)	EFS was defined as the time from date of randomization until the date of PD/relapse, start of a new non-protocol-specified anti-CLL therapy, or death from any cause, whichever occurred first, as assessed by the investigator. PD: occurrence of one of the following: new lesion; new palpable lymph node (\>1.5 cm); unequivocal progression of non-target lesion; increase of \>/=50% in splenomegaly, hepatomegaly, blood lymphocytes with count \>/=5000/mcL, longest diameter of any lesion; transformation to more aggressive histology; decrease of \>/=50% in platelet or neutrophil count, or hemoglobin level by \>2 g/dL or to \<10 g/dL. Participants without any of the specified event at the time of analysis were censored at the date of last adequate response assessment. In case of no post-baseline response assessment, participants were censored at the randomization date. The median EFS was estimated using Kaplan-Meier method and the 95% CI was computed using method of Brookmeyer and Crowley.
Percentage of Participants With PD or Death Among Participants With Best Overall Response of CR, CRi, nPR, or PR as Assessed by the Investigator Using iwCLL Guidelines	From time of achieving best overall response until PD or death from any cause, whichever occurred first (up to approximately 8 years 5 months)	Percentage of participants with PD as assessed by the investigator according to the iwCLL guidelines or death from any cause during the study was reported. PD was defined as occurrence of one of the following events: appearance of any new extra nodal lesion; new palpable lymph node (\>1.5 cm); unequivocal progression of non-target lesion; an increase of \>/=50% compared to baseline in splenomegaly, hepatomegaly, number of blood lymphocytes with lymphocyte count \>/=5000/mcL, or in longest diameter of any extra nodal lesion; transformation to a more aggressive histology; decrease of \>/=50% compared to baseline in platelet or neutrophil count; or decrease in hemoglobin level by \>2 g/dL or to \<10 g/dL. CR, CRi, nPR, and PR have been defined in previous outcomes, and are not repeated here due to space constraint. Percentage is rounded off.
Duration of Responses (DOR) as Assessed by the Investigator Using iwCLL Guidelines	From time of achieving best overall response until PD or death from any cause, whichever occurred first (up to approximately 8 years 5 months)	DOR was defined as the time from first occurrence of a documented response of CR, CRi, nPR, or PR until PD/relapse, as assessed by the investigator according to the iwCLL guidelines, or death from any cause. PD: occurrence of one of the following: new lesion; new palpable lymph node (\>1.5 cm); unequivocal progression of non-target lesion; increase of \>/=50% in splenomegaly, hepatomegaly, blood lymphocytes with count \>/=5000/mcL, longest diameter of any lesion; transformation to more aggressive histology; decrease of \>/=50% in platelet or neutrophil count, or hemoglobin level by \>2 g/dL or to \<10 g/dL. Participants without PD or death after response were censored at the last date of adequate response assessment. The median DOR was estimated using Kaplan-Meier method and the 95% CI was computed using method of Brookmeyer and Crowley. CR, CRi, nPR, and PR have been defined in previous outcomes, and are not repeated here due to space constraint.
Percentage of Participants With Start of New Anti-CLL Treatment or Death as Assessed by the Investigator	Baseline up to start of new ani-CLL therapy or death, whichever occurred first (up to approximately 8 years 5 months)	Percentage of participants with start of new non-protocol-specified anti-CLL therapy, as assessed by the investigator, or death from any cause, during the study, was reported. Percentage is rounded off.
Percentage of Participants With Minimal Residual Disease (MRD) Negativity in Peripheral Blood	EoCTR visit (8 to 12 weeks after C6D1); Cycle length = 28 days	MRD-negativity was defined as the presence of \<1 malignant B-cell per 10000 normal B-cells in a sample of at least 200000 B-cells, as assessed by the allele specific oligonucleotide polymerase chain reaction (ASO-PCR) and/or flow cytometry technique. Percentage of participants with MRD-negativity was reported. The 95% CI was computed using Pearson-Clopper method. Percentage is rounded off.
Percentage of Participants With PD or Death as Assessed by the Independent Review Committee (IRC) Using Standard iwCLL Guidelines	Baseline up to PD or death, whichever occurred first (up to approximately 3 years)	Assessment of response was performed by the IRC according to the iwCLL guidelines. PD was defined as occurrence of one of the following events: appearance of any new extra nodal lesion; new palpable lymph node (\>1.5 cm); unequivocal progression of non-target lesion; an increase of \>/=50% compared to baseline in splenomegaly, hepatomegaly, number of blood lymphocytes with lymphocyte count \>/=5000/mcL, or in longest diameter of any extra nodal lesion; transformation to a more aggressive histology; decrease of \>/=50% compared to baseline in platelet or neutrophil count; or decrease in hemoglobin level by \>2 g/dL or to \<10 g/dL. No new IRC data was generated post the primary analysis.
PFS as Assessed by the IRC Using Standard iwCLL Guidelines	Baseline up to PD or death, whichever occurred first (up to approximately 3 years)	PFS was defined as the time from randomization until first occurrence of PD/relapse as assessed by the IRC using iwCLL guidelines, or death from any cause, whichever occurred first. PD: occurrence of one of the following: new lesion; new palpable lymph node (\>1.5 cm); unequivocal progression of non-target lesion; increase of \>/=50% in splenomegaly, hepatomegaly, blood lymphocytes with count \>/=5000/mcL, longest diameter of any lesion; transformation to more aggressive histology; decrease of \>/=50% in platelet or neutrophil count, or hemoglobin level by \>2 g/dL or to \<10 g/dL. Participants who had not progressed, relapsed, or died at the time of analysis, were censored on the date of last assessment. In case of no disease assessment after baseline, PFS was censored at the time of randomization+1 day. The median PFS was estimated using Kaplan-Meier method and the 95% CI was computed using method of Brookmeyer and Crowley. No new IRC data was generated post the primary analysis.
PFS as Assessed by the IRC Using Standard iwCLL Guidelines in Participants With 17p Deletion as Identified by FISH Test	Baseline up to PD or death, whichever occurred first (up to approximately 3 years)	PFS was defined as the time from randomization until first occurrence of PD/relapse as assessed by the IRC using iwCLL guidelines, or death from any cause, whichever occurred first. PD: occurrence of one of the following: new lesion; new palpable lymph node (\>1.5 cm); unequivocal progression of non-target lesion; increase of \>/=50% in splenomegaly, hepatomegaly, blood lymphocytes with count \>/=5000/mcL, longest diameter of any lesion; transformation to more aggressive histology; decrease of \>/=50% in platelet or neutrophil count, or hemoglobin level by \>2 g/dL or to \<10 g/dL. Participants who had not progressed, relapsed, or died at the time of analysis, were censored on the date of last assessment. In case of no disease assessment after baseline, PFS was censored at the time of randomization+1 day. The median PFS was estimated using Kaplan-Meier method and the 95% CI was computed using method of Brookmeyer and Crowley. No new IRC data was generated post the primary analysis.
Percentage of Participants With Best Overall Response of CR, CRi, nPR, or PR as Assessed by the IRC Using iwCLL Guidelines	Baseline up to last FUV (up to approximately 3 years)	Response was assessed by IRC according to iwCLL guidelines and was confirmed by repeat assessment \>/=4 weeks after initial documentation. CR: peripheral blood lymphocytes \<4000/mcL; absence of any new lesion, nodal disease, lymphadenopathy, hepatomegaly, splenomegaly, constitutional symptoms; neutrophils \>1500/mcL, platelets \>100000/mcL, hemoglobin \>11.0 g/dL without need for transfusion or exogenous growth factors; normocellular bone marrow with \<30% lymphocytes; no lymphoid nodules. CRi: fulfilling all CR criteria but persistent cytopenia. PR: \>/=50% reduction in 2 of following: peripheral blood lymphocytes, lymphadenopathy, spleen and/or liver enlargement; 1 of following: neutrophils \>1500/mcL, platelets \>100000/mcL, hemoglobin \>11.0 g/dL or \>/=50% improvement without need for transfusion or exogenous growth factors. nPR: fulfilling all CR criteria but presence of lymphoid nodules. 95% CI was computed using Pearson-Clopper method.No new IRC data was generated post primary analysis.
Percentage of Participants With MRD Negativity in Bone Marrow	EoCTR visit (8 to 12 weeks after C6D1); Cycle length = 28 days	MRD-negativity was defined as the presence of \<1 malignant B-cell per 10000 normal B-cells in a sample of at least 200000 B-cells, as assessed flow cytometry technique. Percentage of participants with MRD-negativity was reported. The 95% CI was computed using Pearson-Clopper method. Percentages are rounded off.
Percentage of Participants With Best Overall Response of Complete Response (CR), CR With Incomplete Bone Marrow Recovery (CRi), Nodular Partial Response (nPR), or Partial Response (PR) as Assessed by the Investigator Using iwCLL Guidelines	Baseline up to approximately 8 years 5 months	Response was assessed by investigator according to iwCLL guidelines and was confirmed by repeat assessment \>/=4 weeks after initial documentation. CR: peripheral blood lymphocytes \<4000/mcL; absence of any new lesion, nodal disease, lymphadenopathy, hepatomegaly, splenomegaly, and constitutional symptoms; neutrophils \>1500/mcL, platelets \>100000/mcL, hemoglobin \>11.0 g/dL without need for transfusion or exogenous growth factors; normocellular bone marrow with \<30% lymphocytes; no lymphoid nodules. CRi: fulfilling all CR criteria but persistent cytopenia. PR: \>/=50% reduction in two of following: peripheral blood lymphocytes, lymphadenopathy, spleen and/or liver enlargement; and 1 of following: neutrophils \>1500/mcL, platelets \>100000/mcL, hemoglobin \>11.0 g/dL or \>/=50% improvement without need for transfusion or exogenous growth factors. nPR: fulfilling all CR criteria but presence of lymphoid nodules. 95% CI was computed using Pearson-Clopper method.Percentages are rounded off.
Percentage of Participants Who Died	Baseline up to approximately 8 years 5 months	Percentage of participants who died from any cause, during the study, was reported. Percentage is rounded off.
Time to New Anti-CLL Treatment (TTNT) as Assessed by the Investigator	Baseline up to start of new ani-CLL therapy or death, whichever occurred first (up to approximately 8 years 5 months)	TTNT was defined as the time from randomization until start of new non-protocol-specified anti-CLL treatment or death from any cause. Participants without the event at the time of analysis were censored at the last visit date for this outcome measure analysis. The median TTNT was estimated using Kaplan-Meier method and the 95% CI was computed using method of Brookmeyer and Crowley.
Change From Baseline in HRQoL as Measured by Quality of Life Questionnaire Associated CLL Module (QLQ-CLL16) Multi-Item Scales Score	Baseline, D1 of Cycles 1, 2, 3, 4, 5, 6, STC/EW visit (up to C6D28), EoCTR visit (8 to 12 weeks after C6D1), and FUVs (every 12 weeks after EoCTR up to 3 years); Cycle length = 28 days	The EORTC QLQ-CLL16 module is designed for participants with Stage 0 to Stage 4 CLL. It is composed of 16 questions and there are four multi-item scales on Fatigue (2 items), Treatment-related side effects (TRSE, 4 items), Disease-related symptoms (DRS, 4 items), and Infection (4 items); and two single-item scales on social activities and future health worries. Multi-item scales score are reported and the total score for each multi-item scale was transformed to result in a total score range of 0 to 100, where higher score = poor HRQoL.
Number of Participants With Adverse Events (AEs) and Serious Adverse Events (SAEs)	From signing of informed consent form up to approximately 8 years 5 months	An AE was defined as any untoward medical occurrence in a participant administered with Mircera and which does not necessarily have a causal relationship with Mircera. A Serious Adverse Event (SAE) is any significant hazard, contraindication, side effect that is fatal or life threatening; requires in-patient hospitalization or prolongation of existing hospitalization; results in persistent or significant disability/incapacity; is a congenital anomaly/birth defect; is medically significant or requires intervention to prevent one or other of the outcomes listed above. AEs were assessed using National Cancer Institute Common Terminology Criteria for Adverse Events, version 4.0 (NCI CTCAE, v4.0)
Percentage of Participants With Overall Response of CR, Cri, nPR, or PR at End of Combination Treatment Visit as Assessed by the Investigator Using iwCLL Guidelines	End of combination treatment response (EoCTR) visit (8 to 12 weeks after Cycle [C] 6 Day [1]); Cycle length = 28 days	Response was assessed by investigator according to iwCLL guidelines and was confirmed by repeat assessment \>/=4 weeks after initial documentation. CR: peripheral blood lymphocytes \<4000/mcL; absence of any new lesion, nodal disease, lymphadenopathy, hepatomegaly, splenomegaly, and constitutional symptoms; neutrophils \>1500/mcL, platelets \>100000/mcL, hemoglobin \>11.0 g/dL without need for transfusion or exogenous growth factors; normocellular bone marrow with \<30% lymphocytes; no lymphoid nodules. CRi: fulfilling all CR criteria but persistent cytopenia. PR: \>/=50% reduction in 2 of following: peripheral blood lymphocytes, lymphadenopathy, spleen and/or liver enlargement; and 1 of following: neutrophils \>1500/mcL, platelets \>100000/mcL, hemoglobin \>11.0 g/dL or \>/=50% improvement without need for transfusion or exogenous growth factors. nPR: fulfilling all CR criteria but presence of lymphoid nodules. 95% CI was computed using Pearson-Clopper method. Percentages are rounded off.
Percentage of Participants With Overall Response of CR, Cri, nPR, or PR at End of Combination Treatment Visit as Assessed by the IRC Using iwCLL Guidelines	EoCTR visit (8 to 12 weeks after C6D1); Cycle length = 28 days	Response was assessed by the IRC according to the iwCLL guidelines and was confirmed by repeat assessment \>/=4 weeks after initial documentation. CR: peripheral blood lymphocytes \<4000/mcL; absence of any new lesion, nodal disease, lymphadenopathy, hepatomegaly, splenomegaly, and constitutional symptoms; neutrophils \>1500/mcL, platelets \>100000/mcL, hemoglobin \>11.0 g/dL without need for transfusion or exogenous growth factors; normocellular bone marrow with \<30% lymphocytes; no lymphoid nodules. CRi: fulfilling all CR criteria but persistent cytopenia. PR: \>/=50% reduction in two of the following: peripheral blood lymphocytes, lymphadenopathy, spleen and/or liver enlargement; and one of the following: neutrophils \>1500/mcL, platelets \>100000/mcL, hemoglobin \>11.0 g/dL or \>/=50% improvement without need for transfusion or exogenous growth factors. nPR: fulfilling all CR criteria but presence of lymphoid nodules. The 95% CI was computed using Pearson-Clopper method.
Overall Survival (OS)	Baseline up to approximately 8 years 5 months	OS was defined as the time from the date of randomization to the date of death from any cause. Participants alive at the time of the analysis were censored at the date when they were last known to be alive as documented by the investigator. The median OS was estimated using Kaplan-Meier method and the 95% CI was computed using method of Brookmeyer and Crowley.
Percentage of Participants With PD or Death as Assessed by the Investigator Using Standard iwCLL Guidelines in Participants With 17p Deletion as Identified by Fluorescence In-situ Hybridization (FISH) Test	Baseline up to PD or death, whichever occurred first (up to approximately 8 years 5 months)	Assessment of response was performed by the investigator according to the iwCLL guidelines. PD was defined as occurrence of one of the following events: appearance of any new extra nodal lesion; new palpable lymph node (\>1.5 cm); unequivocal progression of non-target lesion; an increase of \>/=50% compared to baseline in splenomegaly, hepatomegaly, number of blood lymphocytes with lymphocyte count \>/=5000/mcL, or in longest diameter of any extra nodal lesion; transformation to a more aggressive histology; decrease of \>/=50% compared to baseline in platelet or neutrophil count; or decrease in hemoglobin level by \>2 g/dL or to \<10 g/dL. Percentages are rounded off.
PFS as Assessed by the Investigator Using Standard iwCLL Guidelines in Participants With 17p Deletion as Identified by FISH Test	Baseline up to PD or death, whichever occurred first (up to approximately 8 years 5 months)	PFS was defined as the time from randomization until first occurrence of PD/relapse as assessed by the investigator using iwCLL guidelines, or death from any cause, whichever occurred first. PD: occurrence of one of the following: new lesion; new palpable lymph node (\>1.5 cm); unequivocal progression of non-target lesion; increase of \>/=50% in splenomegaly, hepatomegaly, blood lymphocytes with count \>/=5000/mcL, longest diameter of any lesion; transformation to more aggressive histology; decrease of \>/=50% in platelet or neutrophil count, or hemoglobin level by \>2 g/dL or to \<10 g/dL. Participants who had not progressed, relapsed, or died at the time of analysis, were censored on the date of last assessment. In case of no disease assessment after baseline, PFS was censored at the time of randomization+1 day. The median PFS was estimated using Kaplan-Meier method and the 95% CI was computed using method of Brookmeyer and Crowley.
Percentage of Participants With PD or Death as Assessed by the IRC Using Standard iwCLL Guidelines in Participants With 17p Deletion as Identified by FISH Test	Baseline up to PD or death, whichever occurred first (up to approximately 3 years)	Assessment of response was performed by the IRC according to the iwCLL guidelines. PD was defined as occurrence of one of the following events: appearance of any new extra nodal lesion; new palpable lymph node (\>1.5 cm); unequivocal progression of non-target lesion; an increase of \>/=50% compared to baseline in splenomegaly, hepatomegaly, number of blood lymphocytes with lymphocyte count \>/=5000/mcL, or in longest diameter of any extra nodal lesion; transformation to a more aggressive histology; decrease of \>/=50% compared to baseline in platelet or neutrophil count; or decrease in hemoglobin level by \>2 g/dL or to \<10 g/dL. No new IRC data was generated post the primary analysis.
Percentage of Participants With PD/Relapse, Start of a New Anti-Chronic Lymphocytic Leukemia (CLL) Therapy, or Death as Assessed by the Investigator Using iwCLL Guidelines	Baseline up to PD/relapse, start of a new anti-CLL therapy, or death from any cause, whichever occurred first (approximately 8 years 5 months)	Percentage of participants with PD/relapse, death from any cause, or start of a new non-protocol-specified anti-CLL therapy as assessed by the investigator, during the study, was reported. PD was defined as occurrence of one of the following events: appearance of any new extra nodal lesion; new palpable lymph node (\>1.5 cm); unequivocal progression of non-target lesion; an increase of \>/=50% compared to baseline in splenomegaly, hepatomegaly, number of blood lymphocytes with lymphocyte count \>/=5000/mcL, or in longest diameter of any extra nodal lesion; transformation to a more aggressive histology; decrease of \>/=50% compared to baseline in platelet or neutrophil count; or decrease in hemoglobin level by \>2 g/dL or to \<10 g/dL. Percentages are rounded off.
Plasma Venetoclax Concentrations	Pre-dose (0 hour, anytime before venetoclax administration) and 4 hours post-dose on D1 of Cycles 1 and 4; Cycle length = 28 days
Change From Baseline in Monroe Dunaway (MD) Anderson Symptom Inventory (MDASI) Core Symptom Severity, Module Symptom Severity, and Interference Scores	Baseline, Days 1, 8, and 15 of Cycles 1, 2, and 3; Cycle length = 28 days	MDASI is a 25-item validated questionnaire consisting of 2 parts. Part 1: 19-items divided into 2 scales, Core Symptom Severity (average of Questions 1 to 13; total 13 items: pain, fatigue, nausea, disturbed sleep, distress, shortness of breath, remembering things, lack of appetite, drowsiness, dry mouth, sadness, vomiting, and numbness) and Module Symptom Severity (average of Questions 14 to 19; total 6 items: night sweats, fevers and chills, lymph node swelling, diarrhea, bruising easy or bleeding, and constipation). Part 2: 6-items to assess Interference (symptom distress) (average of Questions 20 to 25; total 6 items: general activity, walking, work, mood, relations with other people, and enjoyment of life). Each item was rated from 0 to 10, with lower scores indicating better outcome. Total score for Core Symptom Severity, Module Symptom Severity, and Interference are reported which range from 0 to 10, with lower scores indicating better health-related quality of life (HRQoL).
Change From Baseline in HRQoL as Measured by European Organization for Research and Treatment of Cancer Core Quality of Life Questionnaire (EORTC QLQ-C30) Functional Scales Score and Global Health Status/Global Quality-of-Life (QoL) Scale Score	Baseline, D1 of Cycles 1, 2, 3, 4, 5, 6, STC/EW visit (up to C6D28), EoCTR visit (8 to 12 weeks after C6D1), and FUVs (every 12 weeks after EoCTR up to 3 years); Cycle length = 28 days	EORTC QLQ-C30 is a validated self-report measure consisting of 30 questions incorporated into 5 functional scales (Physical, Role, Cognitive, Emotional, and Social), 3 symptom scales (fatigue, pain, nausea, and vomiting), a global health status/global QoL scale, and single items (dyspnea, appetite loss, sleep disturbance, constipation, and diarrhea). Most questions used 4-point scale (1='Not at all' to 4='Very much'), while 2 questions used 7-point scale (1='very poor' to 7='Excellent'). Scores were averaged, transformed to 0-100 scale; where higher score for functional scales=poor level of functioning; higher score for global health status/global QoL=better HRQoL.
Number of Participants With Grade 3 or Higher Tumor Lysis Syndrome (TLS) and Infusion-related Reactions (IRRs)	From signing of informed consent form up to approximately 8 years 5 months	An AE was defined as any untoward medical occurrence in a participant administered with Mircera and which does not necessarily have a causal relationship with Mircera. A SAE is any significant hazard, contraindication, side effect that is fatal or life threatening; requires in-patient hospitalization or prolongation of existing hospitalization; results in persistent or significant disability/incapacity; is a congenital anomaly/birth defect; is medically significant or requires intervention to prevent one or other of the outcomes listed above. TLS and IRRs were graded using the National Cancer Institute Common Terminology Criteria for Adverse Events (CTCAE v4.0). Grade 1 = Mild; Grade 2 = Moderate; Grade 3 = Severe or medically significant; Grade 4 = Life-threatening; Grade 5 = Death. A higher grade indicates a worse outcome.

Trial Locations

Locations (111)

Cliniques Universitaires Saint-Luc; Hematology; 🇧🇪 Bruxelles, Belgium

Huntsman Cancer Institute; University of Utah; 🇺🇸 Salt Lake City, Utah, United States

Royal Adelaide Hospital; 🇦🇺 Adelaide, South Australia, Australia

Rigshospitalet; 🇩🇰 København Ø, Denmark

Istituto Tumori Giovanni Paolo II IRCCS Ospedale Oncologico Bari; 🇮🇹 Bari, Puglia, Italy

Azienda Ospedaliera Universitaria Careggi; 🇮🇹 Florence, Toscana, Italy

CHU Poitiers - Hopital La Miletrie; 🇫🇷 Poitiers, France

Centre Henri Becquerel; 🇫🇷 Rouen, France

Institut Universitaire du Cancer - Oncopole Toulouse (IUCT-O); 🇫🇷 Toulouse, France

Klinik Ottakring; 🇦🇹 Wien, Austria

ZNA Antwerpen; Department Hematology; 🇧🇪 Antwerpen, Belgium

CHU UCL Mont-Godinne; 🇧🇪 Mont-godinne, Belgium

AZ Delta (Campus Rumbeke); 🇧🇪 Roeselare, Belgium

Henry Ford Health System; 🇺🇸 Detroit, Michigan, United States

Memorial Sloan Kettering Cancer Center; Clinical Trials Office; 🇺🇸 New York, New York, United States

Princess Alexandra Hospital; 🇦🇺 Woolloongabba, Queensland, Australia

UZ Leuven; Department Hematology; 🇧🇪 Leuven, Belgium

Slade Health Pharmacy; 🇦🇺 Mount Waverley, Victoria, Australia

Fakultni nemocnice Hradec Kralove; 🇨🇿 Hradec Kralove, Czechia

The Perth Blood Institute; 🇦🇺 Nedlands, Western Australia, Australia

LKH - Universitätsklinikum der PMU Salzburg; 🇦🇹 Salzburg, Austria

Fakultni nemocnice Brno; 🇨🇿 Brno, Czechia

AZ Groeninge; 🇧🇪 Kortrijk, Belgium

Juravinski Cancer Clinic; 🇨🇦 Hamilton, Ontario, Canada

Saskatoon City Hospital;Saskatchewan Cancer Centre; 🇨🇦 Saskatoon, Saskatchewan, Canada

Fakultní nemocnice Olomouc; 🇨🇿 Olomouc, Czechia

Szegedi Tud.Egyetem Szent-Gyorgyi Albert Klin.Kozp.; 🇭🇺 Szeged, Hungary

Centre Hospitalier Lyon Sud; 🇫🇷 Pierre Benite, France

Vseobecna fakultni nemocnice v Praze; 🇨🇿 Praha 2, Czechia

Fakultni nemocnice Kralovske Vinohrady; 🇨🇿 Praha, Czechia

Hôpital de Brabois Adultes; 🇫🇷 Vandoeuvre-les-nancy, France

Hopital Claude Huriez - CHU Lille; 🇫🇷 Lille, France

Fakultni nemocnice Ostrava; 🇨🇿 Ostrava - Poruba, Czechia

Herlev Hospital; 🇩🇰 Herlev, Denmark

Odense Universitetshospital; 🇩🇰 Odense C, Denmark

Konkuk University Medical Center; 🇰🇷 Seoul, Korea, Republic of

Sjællands Universitetshospital, Roskilde; 🇩🇰 Roskilde, Denmark

Sygehus Lillebælt, Vejle; 🇩🇰 Vejle, Denmark

Hôpital Morvan; 🇫🇷 Brest, France

Centre Hospitalier Départemental Les Oudairies; 🇫🇷 La Roche sur Yon, France

CHU Nantes - Hôtel Dieu; Service Assistance Medicale à la Procreation; 🇫🇷 Nantes, France

Hopital Robert Debre; 🇫🇷 Paris, France

Severance Hospital, Yonsei University Health System; 🇰🇷 Seoul, Korea, Republic of

Hopital Saint Eloi; 🇫🇷 Montpellier, France

CHU Tours - Hôpital Bretonneau; 🇫🇷 Tours, France

Universitätsklinikum "Carl Gustav Carus" der Technischen Universität Dresden; 🇩🇪 Dresden, Germany

Orszagos Onkologiai Intezet; 🇭🇺 Budapest, Hungary

Debreceni Egyetem Klinikai Központ; B?rgyógyászati Klinika; 🇭🇺 Debrecen, Hungary

SP ZOZ Zespol Szpitali Miejskich w Chorzowie; 🇵🇱 Chorzow, Poland

Azienda Ospedaliero Universitaria Ospedali Riuniti; 🇮🇹 Torrette Di Ancona, Marche, Italy

Ospedale San Raffaele; 🇮🇹 Milano, Lombardia, Italy

Asst Grande Ospedale Metropolitano Niguarda; SC Farmacia Ospedale; 🇮🇹 Milano, Lombardia, Italy

Seoul National University Bundang Hospital; 🇰🇷 Seongnam-si, Korea, Republic of

The Catholic University of Korea Seoul St. Mary?s Hospital; 🇰🇷 Seoul, Korea, Republic of

Akademiska Sjukhuset; 🇸🇪 Uppsala, Sweden

Singleton Hospital; Pharmacy Department; 🇬🇧 Swansea, United Kingdom

North Shore Hospital; Haematolgy; 🇳🇿 Auckland, New Zealand

Amsterdam UMC Location AMC; 🇳🇱 Amsterdam, Netherlands

Hospital Universitari Vall d'Hebron; 🇪🇸 Barcelona, Spain

Skånes Universitetssjukhus; 🇸🇪 Lund, Sweden

Middlemore Hospital; 🇳🇿 Auckland, New Zealand

Christchurch Hospital NZ; 🇳🇿 Christchurch, New Zealand

Baxter Healthcare; 🇳🇿 Mount Wellington, New Zealand

FSBSI "Russian Oncological Scientific Center n.a. N.N. Blokhin"; 🇷🇺 Moscow, Moskovskaja Oblast, Russian Federation

SRI of Hematology and Transfusiology; 🇷🇺 Sankt-peterburg, Sankt Petersburg, Russian Federation

Universitaetsklinikum Freiburg; 🇩🇪 Freiburg, Germany

Universitätsklinikum Tübingen; 🇩🇪 Tübingen, Germany

Hospital Clinic i Provincial de Barcelona; Hematology; 🇪🇸 Barcelona, Spain

University of California San Diego Medical Center; 🇺🇸 La Jolla, California, United States

Perlmutter Cancer Center NYU Langone Health; 🇺🇸 New York, New York, United States

Concord Repatriation General Hospital; 🇦🇺 Concord, New South Wales, Australia

St George Hospital; 🇦🇺 Kogarah, New South Wales, New South Wales, Australia

Royal Hobart Hospital; 🇦🇺 Hobart, Tasmania, Australia

Frankston Hospital; 🇦🇺 Frankston, Victoria, Australia

Flinders Medical Centre; 🇦🇺 Bedford Park, South Australia, Australia

CHU de Rennes - Hopital de Pontchaillo; 🇫🇷 Rennes, France

Somogy Megyei Kaposi Mor Oktato Korhaz; 🇭🇺 Pecs, Hungary

Azienda Socio Sanitaria Territoriale Papa Giovanni XXIII (Presidio Papa Giovanni XXIII); 🇮🇹 Bergamo, Lombardia, Italy

Azienda Ospedaliero Universitaria San Martino; 🇮🇹 Genova, Liguria, Italy

Samodzielny Publiczny Szpital Kliniczny nr 1; 🇵🇱 Zabrze, Poland

North-West Federal Medical Research Center n.a. V.A. Almazov; 🇷🇺 St. Petersburg, Sankt Petersburg, Russian Federation

Hospital Clinico Universitario de Salamanca; 🇪🇸 Salamanca, Spain

Hospital Universitario 12 de Octubre; 🇪🇸 Madrid, Spain

Bristol Haematology and Oncology centre; 🇬🇧 Bristol, United Kingdom

Southampton General Hospital; 🇬🇧 Southampton, United Kingdom

The Christie; 🇬🇧 Manchester, United Kingdom

Jewish General Hospital; 🇨🇦 Montreal, Quebec, Canada

Azienda Ospedaliera Città della Salute e della Scienza di Torino; Radiology; 🇮🇹 Torino, Abruzzo, Italy

Albert Schweitzer Ziekenhuis, Dordwijk; Internal Medicine, Hemato-Oncology; 🇳🇱 Dordrecht, Netherlands

Wojewódzkie Wielospecjalistyczne Centrum Onkologii i Traumatologii im. M. Kopernika w Lodzi; 🇵🇱 Lodz, Poland

Kemerovo Regional Clinical Hospital; 🇷🇺 Kemerovo, Russian Federation

BHI of Omsk region Clinical Oncology Dispensary; 🇷🇺 Omsk, Russian Federation

Erasmus Medisch Centrum; 🇳🇱 Rotterdam, Netherlands

UMC Utrecht; 🇳🇱 Utrecht, Netherlands

Foothills Medical Centre; Centre Dept of Medical Clinical Neuroscience; 🇨🇦 Calgary, Alberta, Canada

Monash Medical Centre; Haematology; 🇦🇺 Melbourne, Victoria, Australia

Peter MacCallum Cancer Center; 🇦🇺 North Melbourne, Victoria, Australia

Medisch Spectrum Twente; 🇳🇱 Enschede, Netherlands

Leids Universitair Medisch Centrum; Cardiology; 🇳🇱 Leiden, Netherlands

Royal Melbourne Hospital; 🇦🇺 Parkville, Victoria, Australia

National Taiwan University Hospital; 🇨🇳 Taipei, Taiwan

Medizinische Universität Wien; 🇦🇹 Wien, Austria

Uniwersyteckie Centrum Kliniczne; 🇵🇱 Gdansk, Poland

The Canberra Hospital; 🇦🇺 Garran, Australian Capital Territory, Australia

Azienda Ospedaliera Di Padova; 🇮🇹 Padova, Veneto, Italy

Complejo Hospitalario de Navarra; 🇪🇸 Pamplona, Navarra, Spain

Amsterdam UMC, Locatie VUMC; Neurology; 🇳🇱 Amsterdam, Netherlands

Szpital Wojewodzki w Opolu; 🇵🇱 Opole, Poland

MTZ Clinical Research Sp. z o.o.; 🇵🇱 Warszawa, Poland

Semmelweis Egyetem; 🇭🇺 Budapest, Hungary

Medizinische Universität Innsbruck; 🇦🇹 Innsbruck, Austria