Clinical Trial Details
— Status: Not yet recruiting
Administrative data
| NCT number |
NCT05100641 |
| Other study ID # |
CL-GBM-P02-US |
| Secondary ID |
|
| Status |
Not yet recruiting |
| Phase |
Phase 3
|
| First received |
|
| Last updated |
|
| Start date |
January 2024 |
| Est. completion date |
March 2029 |
Study information
| Verified date |
April 2023 |
| Source |
Aivita Biomedical, Inc. |
| Contact |
Jim Langford |
| Phone |
949-872-2555 |
| Email |
jim[@]aivitabiomedical.com |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
This is a multi-center, double-blind, 2:1 randomized phase III trial to determine whether the
addition of AV-GBM-1, a therapeutic, patient-specific dendritic cell vaccine, to standard
therapy increases OS of patients with a recent diagnosis of primary GBM.
The intent is to enroll approximately 726 patients for tumor collection to enroll 690 who are
eligible for treatment at the time of randomization and who have granted consent for
participation. Because of the lack of toxicity, there are no restrictions related to
performance status or blood tests at the time of treatment. The key endpoint is OS from date
of first injection after RT/TMZ; secondary endpoints are PFS from date of first injection,
and OS and PFS from date of randomization prior to RT/TMZ. Date of PFS will be determined by
the principal investigator at each site.
Description:
This is a multi-center, double-blind, 2:1 randomized phase 3 trial to determine whether the
addition of AV-GBM-1 to standard therapy increases OS of patients with a recent diagnosis of
primary GBM.
Patients will sign two treatment-related consents, one for obtaining fresh tumor tissue at
the time of craniotomy for the purpose of establishing a short-term tumor cell line and for
awareness of subsequent leukapheresis procedure, and the other for randomization and
participation in the randomized trial. As required for related medical procedures, patients
will sign medical consents for craniotomy/tumor resection, and for leukapheresis to obtain
monocytes for the MC control arm, or to manufacture DC.
Key eligibility criteria are (1) recovered from maximal safe surgical resection surgery from
which a short-term cell culture has been established, (2) undergone leukapheresis prior to
planned concurrent RT/TMZ, from which a sufficient number of MC have been derived, (3)
screened, stratified and randomized prior to starting RT/TMZ. Patients will be stratified by
age (70 years or greater or less than 70), KPS (90 or 100 vs 70 or 80), MGMT
promotor-methylation (yes or no), and IDH-mutation status (mutated or wild-type), then
randomized 2:1 (AV-GBM-1 vs MC control).
The final products will be manufactured while the patient is being treated with RT/TMZ. After
recovery from RT/TMZ, one of the study agents, either the DC-ATA AV-GBM-1 or autologous MC
control, will be administered weekly for three weeks just prior to starting adjuvant TMZ, and
then every four weeks concurrently with, adjuvant TMZ or second-line therapy per managing
physician. Both products are admixed with adjuvant 500 mcg of GM-CSF by a local pharmacist,
just prior to each injection. The pharmacist, the patient, their health care givers and local
research team will be masked as to whether the patient is receiving AV-GBM-1 or MC control,
which are similar in appearance. Only the AIVITA manufacturing team will be aware of
randomization so that the appropriate product can be manufactured per SOPs.
The first 3 weekly SC injections of study agent will be administered prior to beginning
adjuvant or salvage temozolomide, temozolomide plus bevacizumab, or temozolomide plus tumor
treating fields. Thereafter study agents will be injected about every 28 days for up to 18
additional vaccines (i.e. a total of 21 vaccines over 18 months from the start of
investigational therapy. Depending on the number of study-agent doses available, additional
leukaphereses and manufacturing of more study agent may be required if treatment is to
continue up to 18 months from the start of therapy. In previous trials, 8 total injections
were given over 6 months. In this trial up to 21 doses may be given over 18 months.
In previous trials each patient-specific batch of DC-ATA was divided into 10 aliquots, 8 of
which were intended for injection. The range of cells was from 1 to over 30 million per
aliquot. However, the clinical trials have consistently suggested that 1 to 2 million cells
is a sufficient dose. Therefore, for this trial each patient-specific batch of DC-ATA will be
divided into aliquots containing 2 million DC-ATA cells (prior to cryopreservation), and
after the initial series of three weekly injections, subsequent injections will be
administered up to 18 months from the first injection. If the product is used up, a
cryopreserved cell line can be re-expanded and an additional leukapheresis procedure
performed in order to make more AV-GBM-1 or MC control, if the patient and their physician
wish to continue treatment. For those who were randomized to AV-GBM-1, a GBM cell culture
would be re-established from a cryopreserved sample of the original cell line. If for some
reason the cell line cannot be reestablished, then patients randomized to the AV-GBM-1 arm
would receive injections of their monocytes with GM-CSF to preserve the double-blind
conditions.
Patients who are confirmed to have experienced PD while on study must discontinue AV-GBM-1
treatment.
The intent is to enroll approximately 1,120 patients for tumor collection to have 672
patients who are eligible for treatment at the time of randomization and who have granted
consent for participation. Because of the lack of toxicity, there are no restrictions related
to performance status or blood tests at the time of treatment. The key endpoint is OS from
date of randomization; secondary endpoints are OS and PFS from date of first injection. Date
of PFS will be determined by the principal investigator at each site.
