Efficacy and Safety Study of Lomustine/Temozolomide Combination Therapy vs. Standard Therapy for Glioblastoma Patients (CeTeG)

Overview
Related items

The prognosis of patients with newly diagnosed glioblastoma is dismal despite recent therapeutic improvements Using standard therapy with temozolomide (TMZ) and radiotherapy (60 Gy), the median overall survival time (mOS) is 14.6 months (Stupp et al., 2005). Since in a previous non-randomized bicentric phase II trial, primary combination chemotherapy with lomustine (CCNU) and TMZ was highly effective (mOS 23 months; UKT-03 trial; Herrlinger et al., 2006; Glas et al., 2009) the proposed trial further investigates the efficacy of CCNU/TMZ in a randomized multicenter phase III setting against standard therapy. In case the projected phase III trial confirms the phase II data, CCNU/TMZ combination would be significantly better than TMZ monotherapy and would thus be the new standard treatment for newly diagnosed GBM patients with a methylated MGMT promotor. Thus, this trial has the potential to profoundly change the standard therapy of this most aggressive brain tumor. Since in the previous trial only patients with a methylated MGMT (mMGMT) promoter had a benefit from CCNU/TMZ (mOS in the mMGMT group 34 months, in the non-mMGMT group 12.5 months; Glas et al., 2009) while patients with a non-methylated MGMT did not have any benefit, the trial is restricted to mMGMT patients.The CeTeG trial randomizes in a 1:1 fashion newly diagnosed GBM patients (18-70 years) for either standard TMZ therapy (concomitant and 6 courses à 4 weeks of adjuvant TMZ therapy) or experimental CCNU/TMZ therapy (6 courses à 6 weeks). Both arms include standard radiotherapy (RT) of the tumor site (30 x 2 Gy). Assuming that CCNU/TMZ therapy increases the median overall survival (mOS) from 48.9% (standard TMZ) to 70% (CCNU/TMZ; 75% in the previous phase II trial, Glas et al., 2009), 2 x 68 patients have to be accrued. Patients will be accrued over 24 months and each patient will be followed for at least 24 months adding up to a total minimal duration of the time from first patient in until the end of the follow-up time of 48 months. The primary endpoint is overall survival; secondary endpoints include progression-free survival, response rate, acute and late toxicity, and quality of life.

SEEK ID: https://fdm.digital-medicine.org/projects/4

Public web page: https://clinicaltrials.gov/study/NCT01149109

Organisms: No Organisms specified

NFDI4Health PIs: No PIs for this Trial Project

Trial Project start date: 1st Oct 2010

Trial Project end date: 6th Apr 2017

Extended Metadata (Nfdi4Health MDS 3.3)

Expand All Collapse All

Resource classification(*)

Type of the resource : Study

Title(s)/name(s) of the Project

Title/name : Phase III trial of CCNU/temozolomide (TMZ) combination therapy vs. standard TMZ therapy for newly diagnosed MGMT-methylated glioblastoma patients (CeTeG)
Language of the title/name : English

Acronym(s) of the Project

Acronym : CeTeG
Language of the acronym : English

Description(s) of the Project

Description : he prognosis of patients with newly diagnosed glioblastoma is dismal despite recent therapeutic improvements Using standard therapy with temozolomide (TMZ) and radiotherapy (60 Gy), the median overall survival time (mOS) is 14.6 months (Stupp et al., 2005). Since in a previous non-randomized bicentric phase II trial, primary combination chemotherapy with lomustine (CCNU) and TMZ was highly effective (mOS 23 months; UKT-03 trial; Herrlinger et al., 2006; Glas et al., 2009) the proposed trial further investigates the efficacy of CCNU/TMZ in a randomized multicenter phase III setting against standard therapy. In case the projected phase III trial confirms the phase II data, CCNU/TMZ combination would be significantly better than TMZ monotherapy and would thus be the new standard treatment for newly diagnosed GBM patients with a methylated MGMT promotor. Thus, this trial has the potential to profoundly change the standard therapy of this most aggressive brain tumor. Since in the previous trial only patients with a methylated MGMT (mMGMT) promoter had a benefit from CCNU/TMZ (mOS in the mMGMT group 34 months, in the non-mMGMT group 12.5 months; Glas et al., 2009) while patients with a non-methylated MGMT did not have any benefit, the trial is restricted to mMGMT patients.The CeTeG trial randomizes in a 1:1 fashion newly diagnosed GBM patients (18-70 years) for either standard TMZ therapy (concomitant and 6 courses à 4 weeks of adjuvant TMZ therapy) or experimental CCNU/TMZ therapy (6 courses à 6 weeks). Both arms include standard radiotherapy (RT) of the tumor site (30 x 2 Gy). Assuming that CCNU/TMZ therapy increases the median overall survival (mOS) from 48.9% (standard TMZ) to 70% (CCNU/TMZ; 75% in the previous phase II trial, Glas et al., 2009), 2 x 68 patients have to be accrued. Patients will be accrued over 24 months and each patient will be followed for at least 24 months adding up to a total minimal duration of the time from first patient in until the end of the follow-up time of 48 months. The primary endpoint is overall survival; secondary endpoints include progression-free survival, response rate, acute and late toxicity, and quality of life.
Language of the description : English

Keyword(s) describing the Project

Keyword(*) : Lomustine

Keyword(*) : Temozolomide

Keyword(*) : MGMT promotor status

Keyword(*) : overall survival

Language(s) of the project : English

Contributor(s) of the Project

Is it a personal or organisational contribution?(*) : Personal
Details about the contributing organisation(s)/institution(s)/group(s)
Contributor type(*) : Not specified
Funding identifier(s) : Not specified
Name of the organisation/institution/group(*) : Rheinische Friedrich-Wilhelms-University Bonn represented by the Faculty of Medicine of the University of Bonn represented by the Dean of the Faculty of Medicine, Clinical Neuro-Oncology
Details about the contributing person(s)
Contributor type(*) : Principal investigator
Given name(*) : Ulrich
Family name(s)(*) : Herrlinger
Digital identifier(s)
Identifier(*) : Not specified
Scheme(*) : Not specified
Email address : Not specified
Phone number : Not specified
Organisation(s) associated with the contributor
Name(*) : Not specified
Address : Not specified
Web page : Not specified
Digital identifier(s)
Identifier(*) : Not specified
Scheme(*) : Not specified

Alternative identifiers

Type of the registry(*) : NCT (ClinicalTrials.gov)
Identifier(*) : NCT01149109

Characteristics of the Project

Is it an interventional or non-interventional Project? : Interventional
Specification of the type of the Project
Interventional Project type : []
Non-interventional Project type : []
Primary health condition(s) or disease(s) considered in the Project
Primary health condition or disease name(*) : Glioblastoma
Terminology/classification(*) : Not specified
Code of the health condition or disease : Not specified
Groups of diseases or conditions(*)
Which groups of diseases or conditions were the data collected on? : Not applicable
On which diseases or conditions were the data collected? : []
Collects mortality data? : Not specified
Administrative information about the Project
Status of the ethics committee approval : Not specified
Overall Project status : Completed: Recruitment, data collection, and data quality management completed normally
Participants enrolled by invitation? : Not applicable
Start date : 1 October 2010
End date : 6 April 2017
Mono- or multicentric? : Multicentric
Number of centers : 12
One or more data providers? : Not specified
Number of data providers : Not specified
Primary subject(*) : Person
Eligibility criteria for Project participants
Eligibility criteria: Minimum age
Minimum eligible age(*) : 18
Unit of age(*) : Years
Eligibility criteria: Maximum age
Maximum eligible age(*) : 70
Unit of age(*) : Years
Eligible gender : Male, Female, Diverse
Inclusion criteria : written informed consent patients have to be in a cognitive state that allows them to understand the rationale and necessity of study therapy and procedures. newly diagnosed histologically proven GBM or gliosarcoma WHO Grad IV methylated MGMT promoter in the tumor estimated life expectancy of at least 12 weeks Karnofsky Performance Score (KPS) ≥ 70% patient compliance and geographic proximity that allow adequate follow up male and female patients with reproductive potential must use an approved contraceptive method pre-menopausal female patients with childbearing potential: a negative serum pregnancy test must be obtained prior to treatment start Adequate organ function as described below: Adequate bone marrow reserve: white blood cell (WBC) count > 3000/µl, granulocyte count >1500/µl, platelets > 100000/µl, haemoglobin ≥ 10 g/dl Adequate liver function bilirubin < 1.5 times above upper limit of normal range (ULN), ALT and AST < 3 times ULN creatinine < 1.5 times ULN Adequate blood clotting: PT and PTT within normal limits Negative HIV test
Exclusion criteria : prior malignancy prior chemotherapy prior radiotherapy to the brain concurrent administration of any other anti-tumor therapy allergy or other intolerability of temozolomide, CCNU, dacarbazine or other nitrosourea derivatives unable to undergo MRI past medical history of diseases with poor prognosis known HIV infection, active Hepatitis B or C infection any active infection female patients that are pregnant or breastfeeding patients with reproductive potential who do not accept to use contraception treatment in another clinical trial any psychological, cognitive, familial, sociological or geographical condition potentially hampering compliance with the study protocol and follow-up scheduled visits (at the discretion of investigator)
Population of the Project(*)
Coverage : National
Country(ies) : Germany
Region(s) and/or city(ies) : Berlin, Bochum, Bonn, Cologne, Dresden, Duesseldorf Frankfurt, Leipzig, Mannheim, Münster, München, Regensburg,
Interventions of the Project
Name of the intervention(*) : Not specified
Type of the intervention : Not specified
Additional information about the intervention : Not specified
Name(s) of the arm(s) associated with the given intervention : Not specified
Exposures of the Project
Name of the exposure : Not specified
Type of the exposure : Not specified
Additional information about the exposure : Not specified
Name(s) of the group(s) associated with the given exposure : Not specified
Outcome measures in the Project
Name of the outcome measure(*) : overall survival
Description of the outcome measure : Not specified
Type of the outcome measure : Primary
Time point(s) of assessment : after follow up (4 years)
Name of the outcome measure(*) : progression free survival
Description of the outcome measure : Not specified
Type of the outcome measure : Secondary
Time point(s) of assessment : after follow up (4 years)
Name of the outcome measure(*) : best response rate determined by MRI
Description of the outcome measure : Not specified
Type of the outcome measure : Secondary
Time point(s) of assessment : after follow up (4 years)
Name of the outcome measure(*) : frequency of delay of the next Lomustine/Temozolomide or Temozolomide course
Description of the outcome measure : Not specified
Type of the outcome measure : Secondary
Time point(s) of assessment : during treatment period (2 years)
Name of the outcome measure(*) : acute toxicity during radiotherapy and chemotherapy according to CTC AE V3.0
Description of the outcome measure : Not specified
Type of the outcome measure : Secondary
Time point(s) of assessment : during treatment period (2 years)
Name of the outcome measure(*) : Quality of live
Description of the outcome measure : Not specified
Type of the outcome measure : Secondary
Time point(s) of assessment : including follow up (4 years)
Name of the outcome measure(*) : Evaluation of late neurotoxicity
Description of the outcome measure : Not specified
Type of the outcome measure : Secondary
Time point(s) of assessment : after follow up (4 years)
Additional information about the Project : Not specified
Additional assessments/measurements in the Project : []
Data sharing strategy of the Project(*)
Is it planned to share the data?(*) : Not specified
Supporting documents available in addition to the data : []
When and for how long will the data be available? : Not specified
Criteria for data access : Not specified
Additional information about data sharing : Not specified
DataSHIELD/Opal infrastructure available? : Not specified
Link to data request application : Not specified
Web page with additional information about data sharing : Not specified
Record linkage possible? : Not specified
Non-interventional aspects of the Project
Temporal design : Prospective
Target follow-up duration of the Project
Target follow-up duration(*) : 2
Unit of time(*) : Years
Number of follow-ups conducted : Not specified
Biosamples retained in a biorepository : []
Specific types of retained biosamples : Not specified
Interventional aspects of the Project
Numerical phase : Phase-3
Masking of intervention(s) assignment
Masking implemented? : false
Who is masked? : []
Additional information about masking : Not specified
Type of allocation of participants to an arm : Randomized
Off-label use of a drug product : No

Efficacy and Safety Study of Lomustine/​Temozolomide Combination Therapy vs. Standard Therapy for Glioblastoma Patients (CeTeG)

Related items

Efficacy and Safety Study of Lomustine/Temozolomide Combination Therapy vs. Standard Therapy for Glioblastoma Patients (CeTeG)