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MB-CART19.1 r/r CD19+ B-cell Malignancies (BCM)

Primary Purpose

Acute Lymphoblastic Leukemia Recurrent, B-cell Lymphoma Recurrent, B-cell Lymphoma Refractory

Status

Recruiting

Phase

Phase 1

Locations

Germany

Study Type

Interventional

Intervention

MB-CART19.1

About this trial

This is an interventional treatment trial for Acute Lymphoblastic Leukemia Recurrent

Eligibility Criteria

1 Year - undefined (Child, Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

Male or female patients must have r/r CD19-expressing ALL or NHL/CLL
CD19 expression must be detected on the malignant cells by flow cytometry (leukemia, malignant effusion in NHL) or immunohistochemistry (NHL);
Age ≥ 1 year (if deemed fit by treating investigator);
Absolute CD3+ T cell count ≥100/μl;
ECOG performance score of 0-2 if >16 years old, or Lansky performance score of >50 if ≤16 years old at screening;
No active Hepatitis B, Hepatitis C, HIV1/2;
No childbearing potential or negative pregnancy test at screening and before chemotherapy in women with childbearing potential;
Signed and dated informed consent/assent by patients
and meet the following disease-specific criteria:

ALL:

patients with >5% blasts in BM (M2 or M3) after at least one standard chemotherapy and one salvage regimen who are ineligible for allogeneic stem cell transplant (alloSCT) or have refractory disease activity precluding alloSCT at this time, or
patients who have relapsed post alloSCT at least 100 days posttransplant, with no evidence of active GVHD, and no longer taking immunosuppressive agents for at least 30 days prior to enrollment.
patients with Ph+ ALL if they are intolerant to tyrosine kinase inhibitor (TKI) therapy, or if they have r/r disease after treatment with at least 2 different TKIs.
ALL patients with combined bone marrow and CNS and/or testicular relapse are eligible only if the extramedullary disease has been successfully cleared by conventional therapy at the time of inclusion (e.g. intrathecal chemotherapy, orchiectomy).

Pediatric aggressive NHL (1-17 years):

patients after at least one salvage chemotherapy as bridge to alloSCT or
patients ineligible for alloSCT or
patients who have relapsed post alloSCT at least 100 days posttransplant, with not evidence of active GVHD, and no longer taking immunosuppressive agents for at least 30 days prior to enrollment.
patients with CNS disease (excluding isolated CNS lymphoma) are eligible only if disease has been successfully cleared by intrathecal chemotherapy at the time of inclusion.

Adult NHL:

patients after at least one standard chemotherapy and one salvage regimen as bridge to alloSCT or
patients who are ineligible for alloSCT or
patients who have relapsed post alloSCT at least 100 days posttransplant, with no evidence of active GVHD, and no longer taking immunosuppressive agents for at least 30 days prior to enrollment.
patients with CNS disease (excluding isolated CNS lymphoma) are eligible only if disease has been successfully cleared by intrathecal chemotherapy at the time of inclusion.

CLL:

patients with r/r disease after established and approved treatment options have failed.
patients not eligible or appropriate for conventional alloSCT.

Exclusion Criteria:

Isolated CNS or testicular relapse in ALL;
Isolated CNS lymphomas;
Active solid brain metastases or history of solid brain metastases
Current autoimmune disease, or history of autoimmune disease with potential CNS involvement;
Active clinically significant CNS dysfunction (including but not limited to uncontrolled seizure disorders, cerebrovascular ischemia or hemorrhage, dementia, paralysis);
History of an additional malignancy other than non-melanoma skin cancer or carcinoma in situ unless disease free for ≥3 years;
Pulmonary function: Patients with pre-existing severe lung disease or an oxygen requirement of >28% O2 supplementation or active pulmonary infiltrates on chest X-ray;
Cardiac function: Fractional shortening <28% or left ventricular ejection fraction <50% by echocardiography;
Renal function: GFR ≤29 mL/min/1.73 m2 by CKD-EPI for patients 18 yrs (Levey et al. 2009) or creatinine clearance ≤29 mL/min/1.73 m2 by Schwartz formula (Schwartz et al. 1976) for patients <18 yrs of age;
Liver function: Patients with a serum bilirubin >3 times upper limit of normal or an AST or ALT > 5 times upper limit of normal, unless due to leukemic liver infiltration in the estimation of the investigator;
Rapidly progressive disease that in the estimation of the investigator would compromise ability to complete study therapy;
Pregnant or breast-feeding females;
Medications:
- Systemic chemotherapies, corticosteroids with the exception of physiologic replacement dosing, tyrosine kinase inhibitors (TKI) within 7 days prior to leukapheresis,
- Fludarabine/clofarabine or immunosuppressive drugs and antibodies (e.g. rituximab, calcineurin inhibitors, blinatumomab) or investigational drugs or donor lymphocyte transfusions or radiation therapy within 30 days prior to apheresis,
- Alemtuzumab within 3 months prior to leukapheresis,
- Exception: Intrathecal chemotherapy is allowed prior to treatment, but should be discontinued in ALL and BL 10 days prior to MB-CART19.1 infusion to limit risk of neurotoxicities;
Hypersensitivity against any drug or its ingredients/impurities that is scheduled or likely to be given during trial participation, e.g. as part of the mandatory lymphodepletion protocol, pre-medication for infusion, rescue medication/salvage therapies for treatment related toxicities;
Intake of concomitant medication contraindicated for other reasons than hypersensitivity, e.g. live vaccines and fludarabine;
Contraindication of trial related procedures as judged by the investigator, e.g. lumbar punctures for CSF sampling;
Female patients of child-bearing potential not willing to practice a highly effective form of birth control from the time of enrollment and for 12 months after dosing the IMP;
Male patients of fathering potential not willing to practice a highly effective form of birth control from the time of enrollment and for 12 months after dosing the IMP;
Concurrent participation in another interventional trial that could interact with this trial, e.g. CAR T trials;
Cerebral dysfunction, legal incapacity of adult patients;
Committal to an institution on judicial or official order.

Sites / Locations

Charité - University clinic, pediatric clinic with focus on oncology and hematologyRecruiting
University clinic, clinical for children and youth
Universitätsklinikum ErlangenRecruiting
University medicine Goettingen, Clinic of hematology and medical oncologyRecruiting
Children's Hospital of Dr. von Hauner by Ludwig-Maximilian UniversityRecruiting
Universitätsklinikum Münster - Klink für Kinderheilkunde und Jugendmedizin / Pädiatrische Hämatologie und OnkologieRecruiting
Universitätsklinikum Münster - Medizinische Klinik A / KMT ZentrumRecruiting
Tuebingen University clinic, medical university clinic for internal medicineRecruiting
University clinic for children and youth medicine
University clinic, pediatric hematology and oncologyRecruiting

Arms of the Study

Arm 1

Arm 2

Arm 3

Arm 4

Arm 5

Arm Type

Experimental

Arm Label

Phase I: DL 0: 1x10e5 MB-CART19.1 cells

Phase I: DL 1: 5x10e5 MB-CART19.1 cells

Phase I: DL 2: 1x10e6 MB-CART19.1 cells

Phase I: DL 3: 3x10e6 MB-CART19.1 cells

Phase II - Recommended dose MB-CART19.1

Arm Description

In each dose level of each of the three cohorts three 3 + 3 patients will be treated. A particular dose level will be expanded to 6 patients if one patient out of 3 patients treated at that particular dose level develops DLT. Once this occurs, further dose-escalations are halted until the dose has proven to be safe in the expanded cohort. If 2 or more in a cohort of 6 patients develop DLT no further dose escalation is allowed, and the next lower dose level will be expanded to 6 patients in total. The highest dose among the dose levels tested at which no more than one out of six patients experiences DLT will be considered the MTD.

Dose evaluation will start in Cohorts 1 and 2 with Dose Level 1. In each dose level of each of the three cohorts three 3 + 3 patients will be treated. A particular dose level will be expanded to 6 patients if one patient out of 3 patients treated at that particular dose level develops DLT. Once this occurs, further dose-escalations are halted until the dose has proven to be safe in the expanded cohort. If 2 or more in a cohort of 6 patients develop DLT no further dose escalation is allowed, and the next lower dose level will be expanded to 6 patients in total. The highest dose among the dose levels tested at which no more than one out of six patients experiences DLT will be considered the MTD.

Dose evaluation will start in Cohort 3 with Dose Level 2, sparing Dose Level 1. If Dose Level 2 is not tolerated, Dose Level 1 will be tested. In each dose level of each of the three cohorts three 3 + 3 patients will be treated. A particular dose level will be expanded to 6 patients if one patient out of 3 patients treated at that particular dose level develops DLT. Once this occurs, further dose-escalations are halted until the dose has proven to be safe in the expanded cohort. If 2 or more in a cohort of 6 patients develop DLT no further dose escalation is allowed, and the next lower dose level will be expanded to 6 patients in total. The highest dose among the dose levels tested at which no more than one out of six patients experiences DLT will be considered the MTD.

Phase II will evaluate the efficacy and safety in patients treated with the recommended dose in Cohorts 1 to 3, respectively.

Outcomes

Primary Outcome Measures

Phase I - Determination of the recommended dose of MB-CART19.1

Determined on the basis of the maximum tolerated dose (MTD); MTD is defined as the highest dose level at which < 33% of patients experience Dose Limiting Toxicity (DLT). Safety and toxicity assessment of MB-CART19.1 per adverse events (AE) reporting classified according to CTCAE version 5.0

Phase II - Determination of the Overall Response Rate (ORR)

ORR in ALL patients is defined as the rate of complete remission (CR, CRh); ORR in NHL patients is defined as the rate of overall response (CR or PR)

Secondary Outcome Measures

Phase I - Overall incidence and severity of adverse events

per adverse events (AE) reporting classified according to CTCAE version 5.0

Phase I - Response to treatment for each timepoint

ORR in ALL (Rate of CR/CRh)

Phase I - Response to treatment for each timepoint

Rate MRD-negative CR in ALL

Phase I - Response to treatment for each timepoint

ORR in NHL/CLL (Rate of CR/PR)

Phase I - Occurence of B-cell depletion

Circulating B cell numbers

Phase I - Phenotype and persistence of MB-CART19.1

Blood samples for determination of persistence/phenotyping of infused MB-CART19.1 will be analysed.

Phase II - Overall incidence and severity of adverse events

per adverse events (AE) reporting classified according to CTCAE version 5.0

Phase II - Number of patients with successful MB-CART19.1 production

Number of patients meeting the inclusion criteria and none of the exclusion criteria for who an autologous MB-CART19.1 product can be generated

Phase II - Rate of ALL patients achieving MRD negative CR

Rate MRD-negative CR in ALL

Phase II - Duration of response

Determination of response rate

Phase II - Disease-free survival

Determination of survival and relapse

Phase II - Occurrence of B cell depletion

Circulating B cell numbers in the peripheral blood will be assessed by Flow cytometry.

Phase II - Phenotype and persistence of MB-CART19.1

Blood samples for determination of persistence/phenotyping of infused MB-CART19.1 will be analysed.

Full Information

NCT ID

NCT03853616

First Posted

February 19, 2019

Last Updated

November 30, 2021

Sponsor

Miltenyi Biomedicine GmbH

1. Study Identification

Unique Protocol Identification Number

NCT03853616

Brief Title

MB-CART19.1 r/r CD19+ B-cell Malignancies (BCM)

Official Title

A Phase I/II Safety, Dose Finding and Feasibility Trial of MB-CART19.1 in Patients With Relapsed or Refractory CD19 Positive B Cell Malignancies

Study Type

Interventional

2. Study Status

Record Verification Date

November 2021

Overall Recruitment Status

Recruiting

Study Start Date

November 26, 2018 (Actual)

Primary Completion Date

August 2022 (Anticipated)

Study Completion Date

December 2022 (Anticipated)

3. Sponsor/Collaborators

Responsible Party, by Official Title

Sponsor

Name of the Sponsor

Miltenyi Biomedicine GmbH

4. Oversight

Studies a U.S. FDA-regulated Drug Product

Studies a U.S. FDA-regulated Device Product

Data Monitoring Committee

Yes

5. Study Description

Brief Summary

This is a phase l/ll multi-centric, single arm, prospective open, dose-escalation study in patients with relapsed or refractory CD19-positive B cell malignancies (ALL, NHL, CLL). The trial will include adult and pediatric patients. The trial consists of 2 parts: Part I and Part II. In total approximately 48 patients will be included in Part I of the trial. There will be three individual cohorts, defined by disease biology: pediatric ALL and aggressive pediatric NHL (Cohort 1), adult ALL (Cohort 2) and adult NHL/CLL (Cohort 3).

Detailed Description

The Part I (Phase I) will evaluate the safety of the MB-CART19.1 and determine the recommended dose levels for the Part II (Phase II) efficacy evaluation in each of the three disease cohorts. Dose evaluation will start in Cohorts 1 and 2 with Dose Level 1 and in Cohort 3 with Dose Level 2, sparing Dose Level 1 (see figure 1). Each of the cohorts will evaluate the safety of MB-CART19.1. In each dose level of each of the three cohorts three 3 + 3 patients will be treated. A particular dose level will be expanded to 6 patients if one patient out of 3 patients treated at that particular dose level develops DLT. Once this occurs, further dose-escalations are halted until the dose has proven to be safe in the expanded cohort. If 2 or more in a cohort of 6 patients develop DLT no further dose escalation is allowed, and the next lower dose level will be expanded to 6 patients in total. The highest dose among the dose levels tested at which no more than one out of six patients experiences DLT will be considered the MTD. In Dose Level 3, three additional patients will be treated, if no DLT occurred. Dose Level 0 will be tested only if Dose Level 1 is not tolerable. Cohort 3 will Start with Dose Level 2. If Dose Level 2 is not tolerated, Dose Level 1 will be tested. DLT will be evaluated within 4 weeks after the infusion of MB-CART19.1. An interval of at least 28 days between the treatment of the first and the second patient in each dose level (and in each cohort) is mandatory. Part II (Phase II) will evaluate the efficacy and safety in patients treated with the recommended dose in Cohorts 1 to 3, respectively. After review of completed day 28 safety and efficacy data within Part I (Phase I) by the SMB, the design of Phase II, specifically the number and types of Phase II cohorts and the recommended dose level(s) for Phase II will be determined and thus, the number of patients to be treated will be calculated.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study

Acute Lymphoblastic Leukemia Recurrent, B-cell Lymphoma Recurrent, B-cell Lymphoma Refractory, Chronic Lymphocytic Leukemia Recurrent, Chronic Lymphocytic Leukemia Refractory

7. Study Design

Primary Purpose

Treatment

Study Phase

Phase 1, Phase 2

Interventional Study Model

Sequential Assignment

Masking

None (Open Label)

Allocation

Non-Randomized

Enrollment

48 (Anticipated)

8. Arms, Groups, and Interventions

Arm Title

Phase I: DL 0: 1x10e5 MB-CART19.1 cells

Arm Type

Experimental

Arm Description

Arm Title

Phase I: DL 1: 5x10e5 MB-CART19.1 cells

Arm Type

Experimental

Arm Description

Arm Title

Phase I: DL 2: 1x10e6 MB-CART19.1 cells

Arm Type

Experimental

Arm Description

Arm Title

Phase I: DL 3: 3x10e6 MB-CART19.1 cells

Arm Type

Experimental

Arm Description

Arm Title

Phase II - Recommended dose MB-CART19.1

Arm Type

Experimental

Arm Description

Phase II will evaluate the efficacy and safety in patients treated with the recommended dose in Cohorts 1 to 3, respectively.

Intervention Type

Biological

Intervention Name(s)

MB-CART19.1

Other Intervention Name(s)

CD19-targeting CAR T cells, Anti-CD19 CAR T cells

Intervention Description

MB-CART19.1 consists of autologous CD19 Chimeric Antigen Receptor (CAR) transduced CD4/CD8 enriched T cells targeting CD19-positive tumor cells in b cell malignancies

Primary Outcome Measure Information:

Title

Phase I - Determination of the recommended dose of MB-CART19.1

Description

Time Frame

until day 28 after infusion of MB-CART19.1

Title

Phase II - Determination of the Overall Response Rate (ORR)

Description

ORR in ALL patients is defined as the rate of complete remission (CR, CRh); ORR in NHL patients is defined as the rate of overall response (CR or PR)

Time Frame

28 days after infusion of MB-CART19.1 (and at month 3 in NHL patients not in CR on day 28)

Secondary Outcome Measure Information:

Title

Phase I - Overall incidence and severity of adverse events

Description

per adverse events (AE) reporting classified according to CTCAE version 5.0

Time Frame

throug study completion, an average of 5 years

Title

Phase I - Response to treatment for each timepoint

Description

ORR in ALL (Rate of CR/CRh)

Time Frame

day 28

Title

Phase I - Response to treatment for each timepoint

Description

Rate MRD-negative CR in ALL

Time Frame

day 28, week 12, month 6, 1 year

Title

Phase I - Response to treatment for each timepoint

Description

ORR in NHL/CLL (Rate of CR/PR)

Time Frame

day 28, patients not in CR on day 28: month 3

Title

Phase I - Occurence of B-cell depletion

Description

Circulating B cell numbers

Time Frame

through study completion, an average of 5 years

Title

Phase I - Phenotype and persistence of MB-CART19.1

Description

Blood samples for determination of persistence/phenotyping of infused MB-CART19.1 will be analysed.

Time Frame

days 2, 7, 10, 14, 28, weeks 8, 12, months 6, 12, 24, 36, 48, 60

Title

Phase II - Overall incidence and severity of adverse events

Description

per adverse events (AE) reporting classified according to CTCAE version 5.0

Time Frame

through study completion, an average of 5 years

Title

Phase II - Number of patients with successful MB-CART19.1 production

Description

Number of patients meeting the inclusion criteria and none of the exclusion criteria for who an autologous MB-CART19.1 product can be generated

Time Frame

day 0

Title

Phase II - Rate of ALL patients achieving MRD negative CR

Description

Rate MRD-negative CR in ALL

Time Frame

day 28, week 12, month 6, 1 year

Title

Phase II - Duration of response

Description

Determination of response rate

Time Frame

through study completion, an average of 5 years

Title

Phase II - Disease-free survival

Description

Determination of survival and relapse

Time Frame

at 1 year after MB-CART19.1 infusion in patients not receiving alloSCT

Title

Phase II - Occurrence of B cell depletion

Description

Circulating B cell numbers in the peripheral blood will be assessed by Flow cytometry.

Time Frame

days 7, 10, 14, 28, weeks 8, 12, 16, months 6, 8, 10, 12, 24, 36, 48, 60

Title

Phase II - Phenotype and persistence of MB-CART19.1

Description

Blood samples for determination of persistence/phenotyping of infused MB-CART19.1 will be analysed.

Time Frame

days 2, 7, 10, 14, 28, weeks 8, 12, months 6, 12, 24, 36, 48, 60

10. Eligibility

Sex

All

Minimum Age & Unit of Time

1 Year

Accepts Healthy Volunteers

Eligibility Criteria

Inclusion Criteria: Male or female patients must have r/r CD19-expressing ALL or NHL/CLL CD19 expression must be detected on the malignant cells by flow cytometry (leukemia, malignant effusion in NHL) or immunohistochemistry (NHL); Age ≥ 1 year (if deemed fit by treating investigator); Absolute CD3+ T cell count ≥100/μl; ECOG performance score of 0-2 if >16 years old, or Lansky performance score of >50 if ≤16 years old at screening; No active Hepatitis B, Hepatitis C, HIV1/2; No childbearing potential or negative pregnancy test at screening and before chemotherapy in women with childbearing potential; Signed and dated informed consent/assent by patients and meet the following disease-specific criteria: ALL: patients with >5% blasts in BM (M2 or M3) after at least one standard chemotherapy and one salvage regimen who are ineligible for allogeneic stem cell transplant (alloSCT) or have refractory disease activity precluding alloSCT at this time, or patients who have relapsed post alloSCT at least 100 days posttransplant, with no evidence of active GVHD, and no longer taking immunosuppressive agents for at least 30 days prior to enrollment. patients with Ph+ ALL if they are intolerant to tyrosine kinase inhibitor (TKI) therapy, or if they have r/r disease after treatment with at least 2 different TKIs. ALL patients with combined bone marrow and CNS and/or testicular relapse are eligible only if the extramedullary disease has been successfully cleared by conventional therapy at the time of inclusion (e.g. intrathecal chemotherapy, orchiectomy). Pediatric aggressive NHL (1-17 years): patients after at least one salvage chemotherapy as bridge to alloSCT or patients ineligible for alloSCT or patients who have relapsed post alloSCT at least 100 days posttransplant, with not evidence of active GVHD, and no longer taking immunosuppressive agents for at least 30 days prior to enrollment. patients with CNS disease (excluding isolated CNS lymphoma) are eligible only if disease has been successfully cleared by intrathecal chemotherapy at the time of inclusion. Adult NHL: patients after at least one standard chemotherapy and one salvage regimen as bridge to alloSCT or patients who are ineligible for alloSCT or patients who have relapsed post alloSCT at least 100 days posttransplant, with no evidence of active GVHD, and no longer taking immunosuppressive agents for at least 30 days prior to enrollment. patients with CNS disease (excluding isolated CNS lymphoma) are eligible only if disease has been successfully cleared by intrathecal chemotherapy at the time of inclusion. CLL: patients with r/r disease after established and approved treatment options have failed. patients not eligible or appropriate for conventional alloSCT. Exclusion Criteria: Isolated CNS or testicular relapse in ALL; Isolated CNS lymphomas; Active solid brain metastases or history of solid brain metastases Current autoimmune disease, or history of autoimmune disease with potential CNS involvement; Active clinically significant CNS dysfunction (including but not limited to uncontrolled seizure disorders, cerebrovascular ischemia or hemorrhage, dementia, paralysis); History of an additional malignancy other than non-melanoma skin cancer or carcinoma in situ unless disease free for ≥3 years; Pulmonary function: Patients with pre-existing severe lung disease or an oxygen requirement of >28% O2 supplementation or active pulmonary infiltrates on chest X-ray; Cardiac function: Fractional shortening <28% or left ventricular ejection fraction <50% by echocardiography; Renal function: GFR ≤29 mL/min/1.73 m2 by CKD-EPI for patients 18 yrs (Levey et al. 2009) or creatinine clearance ≤29 mL/min/1.73 m2 by Schwartz formula (Schwartz et al. 1976) for patients <18 yrs of age; Liver function: Patients with a serum bilirubin >3 times upper limit of normal or an AST or ALT > 5 times upper limit of normal, unless due to leukemic liver infiltration in the estimation of the investigator; Rapidly progressive disease that in the estimation of the investigator would compromise ability to complete study therapy; Pregnant or breast-feeding females; Medications: Systemic chemotherapies, corticosteroids with the exception of physiologic replacement dosing, tyrosine kinase inhibitors (TKI) within 7 days prior to leukapheresis, Fludarabine/clofarabine or immunosuppressive drugs and antibodies (e.g. rituximab, calcineurin inhibitors, blinatumomab) or investigational drugs or donor lymphocyte transfusions or radiation therapy within 30 days prior to apheresis, Alemtuzumab within 3 months prior to leukapheresis, Exception: Intrathecal chemotherapy is allowed prior to treatment, but should be discontinued in ALL and BL 10 days prior to MB-CART19.1 infusion to limit risk of neurotoxicities; Hypersensitivity against any drug or its ingredients/impurities that is scheduled or likely to be given during trial participation, e.g. as part of the mandatory lymphodepletion protocol, pre-medication for infusion, rescue medication/salvage therapies for treatment related toxicities; Intake of concomitant medication contraindicated for other reasons than hypersensitivity, e.g. live vaccines and fludarabine; Contraindication of trial related procedures as judged by the investigator, e.g. lumbar punctures for CSF sampling; Female patients of child-bearing potential not willing to practice a highly effective form of birth control from the time of enrollment and for 12 months after dosing the IMP; Male patients of fathering potential not willing to practice a highly effective form of birth control from the time of enrollment and for 12 months after dosing the IMP; Concurrent participation in another interventional trial that could interact with this trial, e.g. CAR T trials; Cerebral dysfunction, legal incapacity of adult patients; Committal to an institution on judicial or official order.

Central Contact Person:

First Name & Middle Initial & Last Name or Official Title & Degree

Alisa Yakushina

Phone

+4916098973562

Alisa.yakushina@miltenyi.com

First Name & Middle Initial & Last Name or Official Title & Degree

Christine Schubert

Phone

+49 2204 8306 6564

christine.schubert@miltenyi.com

Overall Study Officials:

First Name & Middle Initial & Last Name & Degree

Claudia Rössig, Prof. Dr.

Organizational Affiliation

Univeristy Hospital Muenster

Official's Role

Principal Investigator

Facility Information:

Facility Name

Charité - University clinic, pediatric clinic with focus on oncology and hematology

City

Berlin

ZIP/Postal Code

13353

Country

Germany

Individual Site Status

Recruiting

Facility Contact:

First Name & Middle Initial & Last Name & Degree

Annette Kuenkele, Dr.

Phone

+49 30 450 616 178

annette.kuenkele@charite.de

First Name & Middle Initial & Last Name & Degree

Arend von Stackelberg, PD, Dr.

Phone

+49 30 450 666 833

arend.stackelberg@charite.de

Facility Name

University clinic, clinical for children and youth

City

Erlangen

ZIP/Postal Code

91054

Country

Germany

Individual Site Status

Active, not recruiting

Facility Name

Universitätsklinikum Erlangen

City

Erlangen

ZIP/Postal Code

91054

Country

Germany

Individual Site Status

Recruiting

Facility Contact:

First Name & Middle Initial & Last Name & Degree

Andreas Mackensen, Prof.Dr.

Phone

0049 (0)9131 8535 954

andreas.mackensen@uk-erlangen.de

First Name & Middle Initial & Last Name & Degree

Barbara Ferstl, Dr.

Phone

0049 (0)9131 8543 104

barbara.ferstl@uk-erlangen.de

Facility Name

University medicine Goettingen, Clinic of hematology and medical oncology

City

Göttingen

ZIP/Postal Code

37075

Country

Germany

Individual Site Status

Recruiting

Facility Contact:

First Name & Middle Initial & Last Name & Degree

Justin Hasenkamp, Dr.

Phone

+49 55 139 651 82

justin.hasenkamp@med.uni-goettingen.de

First Name & Middle Initial & Last Name & Degree

Gerald Wulf, Prof., Dr.

Phone

+49 55 139 170 577

gerald.wulf@med.uni-goettingen.de

Facility Name

Children's Hospital of Dr. von Hauner by Ludwig-Maximilian University

City

Munich

ZIP/Postal Code

80337

Country

Germany

Individual Site Status

Recruiting

Facility Contact:

First Name & Middle Initial & Last Name & Degree

Tobias Feuchtinger, Prof., Dr.

Phone

+49 89 440 052 759

tobias.feuchtinger@med.uni-muenchen.de

First Name & Middle Initial & Last Name & Degree

Vera Binder, Dr.

Phone

+49 89 440 052 875

vera.binder@med.uni-muenchen.de

Facility Name

Universitätsklinikum Münster - Klink für Kinderheilkunde und Jugendmedizin / Pädiatrische Hämatologie und Onkologie

City

Münster

ZIP/Postal Code

48149

Country

Germany

Individual Site Status

Recruiting

Facility Contact:

First Name & Middle Initial & Last Name & Degree

Claudia Rössig, Prof. Dr.

Phone

0049 (0)251 83 47 741

rossig@ukmuenster.de

First Name & Middle Initial & Last Name & Degree

Birgit Burkhardt, PD Dr.

Phone

0049 (0)251 83 52 840

birgit.burkhardt@ukmuenster.de

Facility Name

Universitätsklinikum Münster - Medizinische Klinik A / KMT Zentrum

City

Münster

ZIP/Postal Code

48149

Country

Germany

Individual Site Status

Recruiting

Facility Contact:

First Name & Middle Initial & Last Name & Degree

Matthias Stelljes, Prof. Dr.

Phone

+49 251 83 52801

matthias.stelljes@ukmuenster.de

First Name & Middle Initial & Last Name & Degree

Jan Henrik Mikesch, Dr.

Phone

+49 251 83 52801

jan-henrik.mikesch@ukmuenster.de

Facility Name

Tuebingen University clinic, medical university clinic for internal medicine

City

Tuebingen

ZIP/Postal Code

72076

Country

Germany

Individual Site Status

Recruiting

Facility Contact:

First Name & Middle Initial & Last Name & Degree

Wolfgang Bethge, Prof., Dr.

Phone

+49 70 712 083 176

wolfgang.bethge@med.uni-tuebingen.de

First Name & Middle Initial & Last Name & Degree

Christoph Faul, Dr.

Phone

+49 70 712 984 087

christoph.faul@med.uni-tuebingen.de

Facility Name

University clinic for children and youth medicine

City

Tuebingen

ZIP/Postal Code

72076

Country

Germany

Individual Site Status

Active, not recruiting

Facility Name

University clinic, pediatric hematology and oncology

City

Würzburg

ZIP/Postal Code

97070

Country

Germany

Individual Site Status

Recruiting

Facility Contact:

First Name & Middle Initial & Last Name & Degree

Paul-Gerhardt Schlegel, Prof., Dr.

Phone

+49 93 120 127 999

schlegel_p@ukw.de

First Name & Middle Initial & Last Name & Degree

Eyrich Matthias, Prof., Dr.

Phone

+49 93 120 127 620

eyrich_m@ukw.de

12. IPD Sharing Statement

Plan to Share IPD

Learn more about this trial

MB-CART19.1 r/r CD19+ B-cell Malignancies (BCM)

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