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Efficacy and Safety of Carfilzomib in Combination With Ibrutinib vs Ibrutinib in Waldenström's Macroglobulinemia (CZAR-1)

Primary Purpose

Waldenstrom Macroglobulinemia

Status
Recruiting
Phase
Phase 2
Locations
International
Study Type
Interventional
Intervention
Carfilzomib + Ibrutinib
Ibrutinib
Sponsored by
Christian Buske
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for Waldenstrom Macroglobulinemia focused on measuring MYD88 mutation, CXCR4 mutation, Carfilzomib, Ibrutinib, Hematology, Oncology

Eligibility Criteria

18 Years - undefined (Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

Each patient must meet all of the following inclusion criteria to be enrolled in this study:

  • Proven clinicopathological diagnosis of WM as defined by consensus panel one of the Second International Workshop on WM. Histopathology has to occur before randomization within the last 4 months. In addition, pathological specimens have to be sent to the national pathological reference center prior to randomization for the determination of the mutational status of MYD88 and CYCR4. Immunophenotyping will be performed in each center and saved locally. The positivity for CD20 can be assumed from any previous bone marrow immunohistochemistry or flow cytometry analysis performed up to 4 months prior to enrollment. Flow cytometry of bone marrow and blood cells will include at least one double staining and assess the expression of the following antigens: surface immunoglobulin, CD19, CD20, CD5, CD10, CD38 and CD23. Patients are eligible if tumor cells express the following antigens: CD19, CD20, CD38 and if they are negative for CD5, CD10 and CD23 expression. Patients with tumor cells positive for CD5 and/or CD23 and morphologically similar to WM cells may be included after ruling out other low-grade B-cell malignancies.
  • De novo and relapsed/refractory WM independent of the genotype.
  • Determination of mutational status of MYD88 and CXCR4.
  • Patients must have at least one of the following criteria to initiate treatment as partly defined by "Consensus Panel Two" recommendations from the Second International Workshop on Waldenström Macroglobulinemia:

    • Recurrent fever, night sweats, weight loss, fatigue.
    • Hyperviscosity.
    • Lympadenopathy which is either symptomatic or bulky (≥ 5 cm in maximum diameter).
    • Symptomatic hepatomegaly and/or splenomegaly.
    • Symptomatic organomegaly and/or organ or tissue infiltration.
    • Peripheral neuropathy due to WM.
    • Symptomatic cryoglobulinemia.
    • Cold agglutinin anemia.
    • IgM related immune hemolytic anemia and/or thrombocytopenia.
    • Nephropathy related to WM.
    • Amyloidosis related to WM.
    • Hemoglobin ≤ 10 g/dL (patients should not have received red blood cells transfusions for at least 7 days prior to obtaining the screening haemoglobin).
    • Platelet count < 100 x 109/L (caused by BM infiltration of the lymphoma).
    • Serum monoclonal protein > 5 g/dL, even with no overt clinical symptoms.
    • IgM serum concentration ≥ 5g/dl.
    • and other WM associated relevant symptoms.
  • World Health Organization (WHO)/ECOG performance status 0 to 2.
  • Left ventricular ejection fraction ≥ 40% as assessed by transthoracic echocardiogram (TTE).
  • Other criteria

    • Age ≥ than 18 years (male and female).
    • Life expectancy > 3 months.
    • Baseline platelet count ≥ 50 x 109/L, absolute neutrophil count ≥ 0.75 x 109/L. (if not due to BM infiltration by the lymphoma).
    • Meet the following pre-treatment laboratory criteria at the Screening visit conducted within 30 days prior to randomization:
  • ASAT (SGPOT): < 3.0 times the ULN.
  • ALAT (SGPT): < 3.0 times the ULN.
  • Total Bilirubin: < 1.5 times the ULN, unless clearly related to the disease (except if due to Gilbert's syndrome).
  • Serum creatinine: ≤ 2 mg/dl.
  • Women of childbearing potential (WOCBP) must agree to use a highly effective method of birth control for the duration of the therapy up to 6 months after end of therapy. A highly effective method of birth control is defined as those which result in a low failure rate (i.e. less than 1% per year) when used consistently and correctly such as combined (estrogen and progestogen containing) hormonal contraception associated with inhibition of ovulation (oral, intravaginal or transdermal), progestogen-only hormonal contraception associated with inhibition of ovulation (oral, injectable or implantable), intrauterine device (IUD), intrauterine hormone-releasing system (IUS), bilateral tubal occlusion, vasectomized partner or sexual abstinence. A postmenopausal state is defined as no menses for 12 months without an alternative medical cause. Contraception and pregnancy testing are required according the CTFG recommendations.
  • Men must agree not to father a child for the duration of therapy and 6 months after (use of a condom) and must agree to advice a female partner to use a highly effective method of birth control. Males must refrain from sperm donation for at least 6 months after the last dose of treatment.
  • Voluntary written informed consent in the native language of the patient before performance of any study-related procedure not part of normal medical care, with the understanding that consent may be withdrawn by the subject at any time without prejudice to future medical care.

Exclusion Criteria:

The presence of any of the following will exclude a subject from enrolment:

  • Previous treatments with following substances are not allowed including into the trial:

    • Prior exposure to Ibrutinib or BTK inhibitors
    • Prior exposure to Carfilzomib. Prior exposure to other proteasome inhibitors are allowed if the patients were not refractory, that is had a remission duration of ≥ 6 months. Prior Plasmapheresis and short-term administration of corticosteroids ≤ 6 weeks administered at a dose equivalent to ≤ 20 mg/day prednisone is also allowed.
  • Serious medical or psychiatric illness (especially undergoing treatment) likely to interfere with participation in this clinical study.
  • Uncontrolled bacterial, viral or fungal infection.
  • Active HIV, HBV or HCV infection.
  • Known interstitial lung disease.
  • Central Nervous System involvement by lymphoma.
  • History of a non-lymphoid malignancy except for the following: adequately treated local basal cell or squamous cell carcinoma of the skin, cervical carcinoma in situ, superficial bladder cancer, asymptomatic prostate cancer without known metastatic disease and with no requirement for therapy or requiring only hormonal therapy and with normal prostate specific antigen for ≥ 1 year prior to study enrolment visit, other Stage 1 or 2 cancer treated with a curative intent and currently in complete remission, for ≥ 3 years.
  • Uncontrolled illness including, but not limited to:

    • Uncontrolled diabetes mellitus (as indicated by metabolic derangements and/or severe diabetes mellitus related uncontrolled organ complications).
    • Unstable angina pectoris, angioplasty, stenting, or myocardial infarction within 6 months prior to randomization.
    • Clinically significant cardiac arrhythmia that is symptomatic or requires treatment, or asymptomatic sustained ventricular tachycardia.
    • Known pericardial disease.
  • Malabsorption syndrome, disease significantly affecting gastrointestinal function, or resection of the stomach or small bowel, ulcerative colitis, symptomatic inflammatory bowel disease, or partial or complete bowel obstruction.
  • Primary amyloidosis.
  • Recent major surgery within 30 days prior to randomization.
  • Chemotherapy with approved or investigational anticancer therapeutic within 21 days prior to randomization.
  • Focal radiation therapy within 7 days prior to randomization. Radiation therapy to an extended field involving a significant volume of bone marrow within 21 days prior to randomization (i.e. prior radiation must have been to less than 30% of the bone marrow).
  • Contraindication to any of the required concomitant drugs or supportive treatments, including hypersensitivity to antiviral drugs.
  • Infiltrative pulmonary disease, known pulmonary hypertension.
  • Active infection within 14 days prior to randomization requiring systemic antibiotics, antiviral (except antiviral therapy directed at hepatitis B) or antifungal agents. Such infection must be fully resolved prior to initiating study treatment.
  • Pleural effusions requiring thoracentesis within 14 days prior to randomization.
  • Ascites requiring paracentesis within 14 days prior to randomization.
  • Uncontrolled hypertension, defined as an average systolic blood pressure > 159 mmHg or diastolic > 99 mmHg despite optimal treatment (measured following European Society of Hypertension/European Society of Cardiology [ESH/ESC] 2013 guidelines.
  • History of stroke or intracranial hemorrhage within 6 months prior to randomization
  • Known chronic obstructive pulmonary disease (COPD) with a forced expiratory volume in 1 second (FEV1) < 50% of predicted normal.
  • Known severe persistent asthma within the past 2 years (see also https://www.nhlbi.nih.gov/files/docs/guidelines/asthsumm.pdf), or currently has uncontrolled asthma of any classification or at time of screening has an FEV1 of < 50% of predicted normal.
  • Known cirrhosis.
  • Autologous stem cell transplant less than 90 days prior to randomization.
  • Allogeneic stem cell transplant less than 100 days prior to randomization.
  • Vaccination with live attenuated vaccines within 30 days prior to randomization.
  • History or evidence of any other clinically significant disorder, condition or disease (with the exception of those outlined above) that, in the opinion of the investigator or sponsor, if consulted, would pose a risk to subject safely or interfere with the study evaluation, procedures or completion.
  • Women who are pregnant as well as women who are breast-feeding and do not consent to discontinue breast-feeding.
  • Participation in another interventional clinical trial within 30 days before randomization in this study

Sites / Locations

  • Uniklinikum SalzburgRecruiting
  • Medizinische Universität WienRecruiting
  • Vivantes Klinikum am UrbanRecruiting
  • Ev. DiakoniekrankenhausRecruiting
  • Kath. St.-Johannes-Gesellschaft Dortmund gGmbHRecruiting
  • Gemeinschaftspraxis Mohm / Prange-KrexRecruiting
  • OncoResearch Lerchenfeld GmbHRecruiting
  • Onkologisches Ambulanzzentrum HannoverRecruiting
  • Praxis für Hämatologie und Onkologie, onkologische TagesklinikRecruiting
  • Praxis Dr. Vehling-KaiserRecruiting
  • Rotkreuzklinikum MünchenRecruiting
  • Gemeinschaftspraxis Haematologie / OnkologieRecruiting
  • Kliniken Ostalb, Staufenklinikum Schw. GmuendRecruiting
  • Friedrich-Ebert-KrankenhausRecruiting
  • Bruederkrankenhaus St. JosefRecruiting
  • Universitätsmedizin RostockRecruiting
  • Klinikum Mutterhaus Mitte TrierRecruiting
  • University Hospital UlmRecruiting
  • Hämatologisch-Onkologische Schwerpunktpraxis Drs. Schöttker & PretscherRecruiting
  • Alexandra HospitalRecruiting

Arms of the Study

Arm 1

Arm 2

Arm Type

Experimental

Active Comparator

Arm Label

Arm A: Carfilzomib + Ibrutinib

Arm B: Ibrutinib

Arm Description

Patients will be treated with Ibrutinib until evidence of progressive disease or no longer tolerated. Patients will receive in addition Carfilzomib for two years.

Patients will be treated with Ibrutinib until evidence of progressive disease or no longer tolerated.

Outcomes

Primary Outcome Measures

CR/VGPR
Primary endpoint is the rate of CR or VGPR 12 months after the start of treatment using the response criteria updated at the Sixth IWWM (CR/VGPR).

Secondary Outcome Measures

Response rate
The response rates (CR, VGPR, PR, MR) and overall response rate (CR, VGPR, PR, MR) are evaluated 12 and 24 months after the start of treatment.
Best response
Best response (at least achieving a MR) is determined in the time interval from the start of induction therapy to end of follow-up.
Time to best response
Time to best response is defined as the time from the start of induction to best response the patient achieves (CR, VGPR, PR, MR).
Time to first response
Time to first response is defined as the time from the start of induction to first response (MR, PR, VGPR or CR).
Time to treatment failure (TTF)
TTF is defined as the time of start of induction treatment to discontinuation of therapy for any reason including death from any cause, progression, toxicity or add-on of new anti-cancer therapy. Patients alive without progression and relapse will be censored at the latest tumor assessment date.
Remission duration (RD)
Remission duration will be calculated in patients with response (CR, VGPR, PR, MR) from the date of response to the date of progression, relapse or death from any cause. Patients alive without progression and relapse will be censored at the latest tumor assessment date.
Progression Free Survival (PFS)
PFS will be calculated from the date of start of treatment to the following events: the date of progression (as defined in Appendix A) and the date of death if it occurred earlier. Patients alive without progression and relapse will be censored at the latest tumor assessment date.
Cause specific survival (CSS)
Cause specific survival is defined as the period from the start of induction treatment to death from lymphoma or lymphoma related cause; death unrelated to WM is considered as a competing event.
Overall survival (OS)
Overall survival is defined as the period from the start of induction treatment to death from any cause. Patients who have not died until the time of the analysis will be censored at their last contact date.
Rate of Adverse Events (safety)
Number of adverse events and comparison of adverse event rate in both treatment arms.
Changes in Quality of Life
Changes in quality of life will be assessed by the FACT-Lym questionnaire and compared in both treatment arms.

Full Information

First Posted
February 7, 2020
Last Updated
March 21, 2023
Sponsor
Christian Buske
Collaborators
Amgen, Janssen, LP
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1. Study Identification

Unique Protocol Identification Number
NCT04263480
Brief Title
Efficacy and Safety of Carfilzomib in Combination With Ibrutinib vs Ibrutinib in Waldenström's Macroglobulinemia
Acronym
CZAR-1
Official Title
Efficacy and Safety of Carfilzomib in Combination With Ibrutinib vs Ibrutinib Alone in Waldenström's Macroglobulinemia (CZAR-1)
Study Type
Interventional

2. Study Status

Record Verification Date
March 2023
Overall Recruitment Status
Recruiting
Study Start Date
February 18, 2021 (Actual)
Primary Completion Date
February 2028 (Anticipated)
Study Completion Date
February 2028 (Anticipated)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor-Investigator
Name of the Sponsor
Christian Buske
Collaborators
Amgen, Janssen, LP

4. Oversight

Studies a U.S. FDA-regulated Drug Product
No
Studies a U.S. FDA-regulated Device Product
No
Data Monitoring Committee
Yes

5. Study Description

Brief Summary
In Waldenström macroglobulinemia (WM) chemotherapy induces only low CR/VGPR (Complete Remission/ Very Good Partial Response) rates and responses of short duration compared to other indolent lymphomas. Thus, innovative approaches are needed which combine excellent activity and tolerability in WM. Chemotherapy-free approaches are highly attractive for this patient group. Based on its high activity in WM and its low toxicity, Ibrutinib was approved for the treatment of WM by the European Medicines Agency (EMA). However, also Ibrutinib fails to induce CRs and the VGPR rate is 16% in relapsed patients. In addition, activity of Ibrutinib depends on the genotype: compared to MYD88mut/CXCR4WT patients Ibrutinib single agent therapy induces substantially lower response rates in patients with the MYD88mut/CXCR4mut or the MYD88WT/CXCR4WT genotype (major response (at least PR) in 91.7 % compared to 61.9 and 0 %, respectively). Phase II data have indicated that the proteasome inhibitor Carfilzomib is able to overcome the inferior prognosis of Ibrutinib in MYD88mut/CXCR4mut and MYD88WT/CXCR4WT patients, as response rates were high for all genotypes in a phase II study combining Carfilzomib with Rituximab and Dexamethasone. Based on this the investigators hypothesize that addition of Carfilzomib to Ibrutinib will increase the VGPR/CR rate compared to Ibrutinib alone in patients with WM, in particular in patients carrying the CXCR4 mutation. In addition, the investigators hypothesize, that the combination Carfilzomib and Ibrutinib will be also highly active in MYD88 wildtype patients and that this combination will be at least as efficient in treatment naïve patients as in relapsed/refractory patients.
Detailed Description
In Waldenström macroglobulinemia (WM) conventional chemotherapy induces only low Complete Remission (CR) rates and responses of short duration compared to other indolent lymphomas. Thus, innovative approaches are needed which combine excellent activity and tolerability in patients with WM, who are mostly of advanced age. Today, chemotherapy in combination with the anti-CD20 antibody Rituximab is still the backbone of treatment in patients with WM and is recommended as first line in national and international treatment guidelines.With the approval of Ibrutinib by the EMA 2015 for patients with relapsed WM or for patients not eligible for chemotherapy with treatment naïve WM treatment landscape has changed in this lymphoma subtype and there is an urgent need to evaluate to which extent chemotherapy-free approaches add clinical benefit to the patient. Based on its high activity in WM and its low toxicity, Ibrutinib was approved for the treatment of WM by the EMA. However, also Ibrutinib fails to induce CRs and the VGPR (Very Good Partial Response) rate is 16% in relapsed patients. In addition, activity of Ibrutinib depends on the genotype with inferior response rates in MYD88mut/CXCR4mut patients and in patients with unmutated MYD88 and CXCR4 compared to MYD88mut/CXCR4WT patients (major response (at least PR) in 91.7 % compared to 61.9 and 0 %, respectively). Phase II data have indicated that the proteasome inhibitor Carfilzomib is able to overcome the inferior prognosis of Ibrutinib in MYD88mut/CXCR4mut and MYD88WT/CXCR4WT patients, as response rates were high for all genotypes in a phase II study combining Carfilzomib with Rituximab and Dexamethasone. Based on this the investigators hypothesize that addition of Carfilzomib to Ibrutinib will increase the VGPR/CR rate compared to Ibrutinib alone in patients with WM, in particular in patients carrying the CXCR4 mutation. In addition, the investigators hypothesize, that the combination Carfilzomib and Ibrutinib will be also highly active in MYD88 wildtype patients and that this combination will be at least as efficient in treatment naïve patients as in relapsed/refractory patients. The study is an international, phase II, multicenter, open label and randomized trial comparing Carfilzomib in combination with Ibrutinib (treatment Arm A) versus Ibrutinib (treatment arm B) in male or female patients aged ≥ 18 years of de novo and relapsed/refractory WM in need of treatment. The phase II study will consist of an open labeled, stratified 1:1 randomization between Arm A and Arm B. Stratification factors are MYD88 and CXCR4 status (positive vs. negative) and number of prior lines (0 vs. ≥ 1 treatment lines). A stratified central block randomization will be used. The primary objective of the trial is to test the efficacy and toxicity of Carfilzomib and Ibrutinib in patients with treatment naïve or relapsed WM. The aim of this study is to investigate the rate of CR or VGPR 12 months after the start of treatment using the response criteria updated at the Sixth IWWM (CR/VGPR). 99 patients at approximately 25 investigator sites will be recruited. Patients will be followed up after end of treatment. Patients will receive Ibrutinib in both treatment arms until progression, non-tolerated toxicity or until the study duration has reached its maximum of 7 years after the first patient was included into the trial. Follow-up (5 years or until disease progression for patients who discontinue treatment due to toxicity) or survival follow-up (for patients with progression disease) will be performed until the study duration has reached its maximum of 7 years after the first patient was included into the trial.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Waldenstrom Macroglobulinemia
Keywords
MYD88 mutation, CXCR4 mutation, Carfilzomib, Ibrutinib, Hematology, Oncology

7. Study Design

Primary Purpose
Treatment
Study Phase
Phase 2
Interventional Study Model
Parallel Assignment
Masking
None (Open Label)
Allocation
Randomized
Enrollment
99 (Anticipated)

8. Arms, Groups, and Interventions

Arm Title
Arm A: Carfilzomib + Ibrutinib
Arm Type
Experimental
Arm Description
Patients will be treated with Ibrutinib until evidence of progressive disease or no longer tolerated. Patients will receive in addition Carfilzomib for two years.
Arm Title
Arm B: Ibrutinib
Arm Type
Active Comparator
Arm Description
Patients will be treated with Ibrutinib until evidence of progressive disease or no longer tolerated.
Intervention Type
Drug
Intervention Name(s)
Carfilzomib + Ibrutinib
Intervention Description
Carfilzomib: Cycle 1, day 1: 20 mg/m² i.v. Cycle 1, day 8, day 15: 70 mg/m² i.v. Cycle 2 - 12, day 1, day 8, day 15: 70 mg/m² i.v. Cycle 13 - 24, day 1, day 15: 70 mg/m² i.v. Ibrutinib: 420 mg p.o daily until disease progression or non-tolerable toxicities
Intervention Type
Drug
Intervention Name(s)
Ibrutinib
Intervention Description
Ibrutinib: 420 mg p.o daily until disease progression or non-tolerable toxicities
Primary Outcome Measure Information:
Title
CR/VGPR
Description
Primary endpoint is the rate of CR or VGPR 12 months after the start of treatment using the response criteria updated at the Sixth IWWM (CR/VGPR).
Time Frame
12 months
Secondary Outcome Measure Information:
Title
Response rate
Description
The response rates (CR, VGPR, PR, MR) and overall response rate (CR, VGPR, PR, MR) are evaluated 12 and 24 months after the start of treatment.
Time Frame
12/ 24 months
Title
Best response
Description
Best response (at least achieving a MR) is determined in the time interval from the start of induction therapy to end of follow-up.
Time Frame
12 months
Title
Time to best response
Description
Time to best response is defined as the time from the start of induction to best response the patient achieves (CR, VGPR, PR, MR).
Time Frame
12 months
Title
Time to first response
Description
Time to first response is defined as the time from the start of induction to first response (MR, PR, VGPR or CR).
Time Frame
12 months
Title
Time to treatment failure (TTF)
Description
TTF is defined as the time of start of induction treatment to discontinuation of therapy for any reason including death from any cause, progression, toxicity or add-on of new anti-cancer therapy. Patients alive without progression and relapse will be censored at the latest tumor assessment date.
Time Frame
7 years
Title
Remission duration (RD)
Description
Remission duration will be calculated in patients with response (CR, VGPR, PR, MR) from the date of response to the date of progression, relapse or death from any cause. Patients alive without progression and relapse will be censored at the latest tumor assessment date.
Time Frame
7 years
Title
Progression Free Survival (PFS)
Description
PFS will be calculated from the date of start of treatment to the following events: the date of progression (as defined in Appendix A) and the date of death if it occurred earlier. Patients alive without progression and relapse will be censored at the latest tumor assessment date.
Time Frame
7 years
Title
Cause specific survival (CSS)
Description
Cause specific survival is defined as the period from the start of induction treatment to death from lymphoma or lymphoma related cause; death unrelated to WM is considered as a competing event.
Time Frame
7 years
Title
Overall survival (OS)
Description
Overall survival is defined as the period from the start of induction treatment to death from any cause. Patients who have not died until the time of the analysis will be censored at their last contact date.
Time Frame
7 years
Title
Rate of Adverse Events (safety)
Description
Number of adverse events and comparison of adverse event rate in both treatment arms.
Time Frame
7 years
Title
Changes in Quality of Life
Description
Changes in quality of life will be assessed by the FACT-Lym questionnaire and compared in both treatment arms.
Time Frame
7 years

10. Eligibility

Sex
All
Minimum Age & Unit of Time
18 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria: Each patient must meet all of the following inclusion criteria to be enrolled in this study: Proven clinicopathological diagnosis of WM as defined by consensus panel one of the Second International Workshop on WM. Histopathology has to occur before randomization within the last 4 months. In addition, pathological specimens have to be sent to the pathological reference center prior to randomization for the determination of the mutational status of MYD88 and CYCR4. Immunophenotyping will be performed in each center and saved locally. The positivity for CD20 can be assumed from any previous bone marrow immunohistochemistry or flow cytometry analysis performed up to 4 months prior to enrollment. Flow cytometry of bone marrow and blood cells will include at least one double staining and assess the disease specific expressions. De novo and relapsed/refractory WM independent of the genotype. Determination of mutational status of MYD88 and CXCR4. Patients must have at least one of the following criteria to initiate treatment as partly defined by "Consensus Panel Two" recommendations from the Second International Workshop on Waldenström Macroglobulinemia: Recurrent fever, night sweats, weight loss, fatigue (at least one of them). Hyperviscosity. Lympadenopathy which is either symptomatic or bulky (≥ 5 cm in maximum diameter). Symptomatic hepatomegaly and/or splenomegaly. Symptomatic organomegaly and/or organ or tissue infiltration. Peripheral neuropathy due to WM. Symptomatic cryoglobulinemia. Cold agglutinin anemia. IgM related immune hemolytic anemia and/or thrombocytopenia. Nephropathy related to WM. Amyloidosis related to WM. Hemoglobin ≤ 10 g/dL (patients should not have received red blood cells transfusions for at least 7 days prior to obtaining the screening haemoglobin). Platelet count < 100 x 109/L (caused by BM infiltration of the lymphoma). Serum monoclonal protein > 5 g/dL, even with no overt clinical symptoms. IgM serum concentration ≥ 5g/dl. and other WM associated relevant symptoms. World Health Organization (WHO)/ECOG performance status 0 to 2. Left ventricular ejection fraction ≥ 40% as assessed by transthoracic echocardiogram (TTE). Other criteria Age ≥ than 18 years (male and female). Life expectancy > 3 months. Baseline platelet count ≥ 50 x 109/L, absolute neutrophil count ≥ 0.75 x 109/L. (if not due to BM infiltration by the lymphoma). Meet the following pre-treatment laboratory criteria at the Screening visit conducted within 30 days prior to randomization: ASAT (SGPOT): < 3.0 times the ULN. ALAT (SGPT): < 3.0 times the ULN. Total Bilirubin: < 1.5 times the ULN, unless clearly related to the disease (except if due to Gilbert's syndrome). Serum creatinine: ≤ 2 mg/dl. Women of childbearing potential (WOCBP) must agree to use a highly effective method of birth control for the duration of the therapy up to 6 months after end of therapy. A highly effective method of birth control is defined as those which result in a low failure rate (i.e. less than 1% per year) when used consistently and correctly such as combined (estrogen and progestogen containing) hormonal contraception associated with inhibition of ovulation (oral, intravaginal or transdermal), progestogen-only hormonal contraception associated with inhibition of ovulation (oral, injectable or implantable), intrauterine device (IUD), intrauterine hormone-releasing system (IUS), bilateral tubal occlusion, vasectomized partner or sexual abstinence. A postmenopausal state is defined as no menses for 12 months without an alternative medical cause. Contraception and pregnancy testing are required according the CTFG recommendations. Men must agree not to father a child for the duration of therapy and 6 months after (use of a condom) and must agree to advice a female partner to use a highly effective method of birth control. Males must refrain from sperm donation for at least 6 months after the last dose of treatment. Voluntary written informed consent in the native language of the patient before performance of any study-related procedure not part of normal medical care, with the understanding that consent may be withdrawn by the subject at any time without prejudice to future medical care. Exclusion Criteria: The presence of any of the following will exclude a subject from enrolment: Previous treatments with following substances: Prior exposure to Ibrutinib or other BTK inhibitors. Prior exposure to Carfilzomib. Prior exposure to other proteasome inhibitors is allowed if the patients were not refractory, that is, had a remission (at least minor response) duration of ≥ 6 months. Prior plasmapheresis and short-term administration of corticosteroids ≤ 6 weeks administered at a dose equivalent to ≤ 20 mg/day of prednisone is also allowed. Serious medical or psychiatric illness (especially undergoing treatment) likely to interfere with participation in this clinical study. Active HIV, HBV or HCV infection. Central Nervous System involvement by lymphoma. History of a non-lymphoid malignancy except for the following: adequately treated local basal cell or squamous cell carcinoma of the skin, cervical carcinoma in situ, superficial bladder cancer, asymptomatic prostate cancer without known metastatic disease and with no requirement for therapy or requiring only hormonal therapy and with normal prostate specific antigen for ≥ 1 year prior to randomization, other Stage 1 or 2 cancer treated with a curative intent and currently in complete remission, for ≥ 3 years. Uncontrolled illness including, but not limited to: Uncontrolled diabetes mellitus (as indicated by metabolic derangements and / or severe diabetes mellitus related uncontrolled organ complications). Chronic symptomatic congestive heart failure (Class NYHA III or IV) or LVEF < 40%. Unstable angina pectoris, angioplasty, stenting, or myocardial infarction within 6 months prior to randomization. Clinically significant cardiac arrhythmia that is symptomatic or requires treatment, or asymptomatic sustained ventricular tachycardia. Known pericardial disease. Malabsorption syndrome, disease significantly affecting gastrointestinal function, or resection of the stomach or small bowel, ulcerative colitis, symptomatic inflammatory bowel disease, or partial or complete bowel obstruction. Cardiac amyloidosis. Recent major surgery within 30 days prior to randomization. Known cirrhosis (meeting child-pugh stage C). Approved or investigational anticancer treatment within 21 days prior to randomization. Glucocorticoid therapy within 14 days prior to randomization that exceeds a cumulative dose of 160 mg of Dexamethasone or equivalent dose of other corticosteroids. Focal radiation therapy within 7 days prior to randomization. Radiation therapy to an extended field involving a significant volume of bone marrow within 21 days prior to randomization (i.e. prior radiation must have been to less than 30% of the bone marrow). Contraindication to any of the required concomitant drugs or supportive treatments, including hypersensitivity to antiviral drugs. Hypersensitivity to the active substances or to any of the excipients of the investigational medicinal products. Active infection within 14 days prior to randomization requiring systemic antibiotics, antiviral (except antiviral therapy directed at hepatitis B) or antifungal agents. Such infection must be fully resolved prior to randomization. Ascites requiring paracentesis within 14 days prior to randomization. Uncontrolled hypertension, defined as an average systolic blood pressure > 159 mmHg or diastolic > 99 mmHg despite optimal treatment (measured according European Society of Hypertension/European Society of Cardiology [ESH / ESC] 2013 guidelines[65]. History of stroke or intracranial hemorrhage within 6 months prior to randomization. Known interstitial lung disease. Infiltrative pulmonary disease, known pulmonary hypertension. Known chronic obstructive pulmonary disease (COPD) with a forced expiratory volume in 1 second (FEV1) < 50% of predicted normal. Known severe persistent asthma within the past 2 years (see also https://www.nhlbi.nih.gov/files/docs/guidelines/asthsumm.pdf), or currently has uncontrolled asthma of any classification or at time of screening has an FEV1 of < 50% of predicted normal. Autologous or allogeneic stem cell transplant less than 100 days prior to randomization. Vaccination with live attenuated vaccines within 30 days prior to randomization. Patients who require strong or moderate inducers or inhibitors for cytochrome P450, family 3 or subfamily A (CYP3A). Patients who have an uncontrolled bleeding disorder or require an anticoagulant (e.g. warfarin or other vitamin K antagonists; novel oral anticoagulants (NOACs) are allowed) at time of screening. History or evidence of any other clinically significant disorder, condition or disease (with the exception of those outlined above) that, in the opinion of the investigator or sponsor, if consulted, would pose a risk to patient safely or interfere with the study evaluation, procedures or completion. Patient is a woman who is pregnant or breastfeeding (and do not consent to discontinue breast-feeding) or planning to become pregnant while enrolled in this study or within 6 months after the last study treatment. Vulnerable patients, e.g. patients who are incapable of giving informed consent (severe dementia or psychosis, patients kept in detention). Participation in another interventional clinical study within 30 days before randomization in this study.
Central Contact Person:
First Name & Middle Initial & Last Name or Official Title & Degree
Jana Berthold
Phone
0049 731 500
Ext
45961
Email
czar.mw@uniklinik-ulm.de
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Christian Buske, MD
Organizational Affiliation
University of Ulm
Official's Role
Study Chair
Facility Information:
Facility Name
Uniklinikum Salzburg
City
Salzburg
ZIP/Postal Code
5020
Country
Austria
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Richard Greil, MD
Facility Name
Medizinische Universität Wien
City
Wien
ZIP/Postal Code
1090
Country
Austria
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Philipp Staber, MD
Facility Name
Vivantes Klinikum am Urban
City
Berlin
ZIP/Postal Code
10967
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Christian Scholz, MD
Facility Name
Ev. Diakoniekrankenhaus
City
Bremen
ZIP/Postal Code
28239
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Ralf Ulrich Trappe, MD
Facility Name
Kath. St.-Johannes-Gesellschaft Dortmund gGmbH
City
Dortmund
ZIP/Postal Code
44137
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Ralf Georg Meyer, MD
Facility Name
Gemeinschaftspraxis Mohm / Prange-Krex
City
Dresden
ZIP/Postal Code
01307
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Gabriele Prange-Krex, MD
Facility Name
OncoResearch Lerchenfeld GmbH
City
Hamburg
ZIP/Postal Code
22081
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Volkmar Böhme, MD
Facility Name
Onkologisches Ambulanzzentrum Hannover
City
Hanover
ZIP/Postal Code
30171
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Michael Königsmann, MD
Facility Name
Praxis für Hämatologie und Onkologie, onkologische Tagesklinik
City
Landshut
ZIP/Postal Code
84036
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Ursula Vehling-Kaiser, MD
Facility Name
Praxis Dr. Vehling-Kaiser
City
Landshut
ZIP/Postal Code
84130
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Ursula Vehling-Kaiser, MD
Facility Name
Rotkreuzklinikum München
City
Munich
ZIP/Postal Code
80634
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Alexander Hoellein, MD
Facility Name
Gemeinschaftspraxis Haematologie / Onkologie
City
Munich
ZIP/Postal Code
81241
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Matthias Zingerle, MD
Facility Name
Kliniken Ostalb, Staufenklinikum Schw. Gmuend
City
Mutlangen
ZIP/Postal Code
72557
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Holgar Hebart, MD
Facility Name
Friedrich-Ebert-Krankenhaus
City
Neumünster
ZIP/Postal Code
24534
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Stefan Mahlmann, MD
Facility Name
Bruederkrankenhaus St. Josef
City
Paderborn
ZIP/Postal Code
33098
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Tobias Gaska, MD
Facility Name
Universitätsmedizin Rostock
City
Rostock
ZIP/Postal Code
18055
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Sebastian Böttcher, MD
Facility Name
Klinikum Mutterhaus Mitte Trier
City
Trier
ZIP/Postal Code
54290
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Rolf Mahlberg, MD
Facility Name
University Hospital Ulm
City
Ulm
ZIP/Postal Code
89081
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Christian Buske, MD
Facility Name
Hämatologisch-Onkologische Schwerpunktpraxis Drs. Schöttker & Pretscher
City
Würzburg
ZIP/Postal Code
97080
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Björn Schöttker, MD
Facility Name
Alexandra Hospital
City
Athens
ZIP/Postal Code
11528
Country
Greece
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Meletios A. Dimopoulos, MD

12. IPD Sharing Statement

Learn more about this trial

Efficacy and Safety of Carfilzomib in Combination With Ibrutinib vs Ibrutinib in Waldenström's Macroglobulinemia

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