Glioblastoma Clinical Trial
Official title:
Autologous Dendritic Cell-Based Adjuvant Immunotherapy of Malignant Gliomas (WHO Grade IV Glioblastoma Multiforme) - Phase II Clinical Trial
Purposes:
The purpose of this phase-II clinical trial is to determine whether or not ADCTA-G, a
biologic "vaccine" preparation of patient's own dendritic cell (DC) for glioblastoma
multiforme (GBM) treatment, is safe and effective in extending the GBM patient's life. The
current conventional multi-modal regimen that may include surgery for tumor resection or
biopsy, temozolomide (TMZ) combined chemo-radiotherapy (CCRT) and TMZ adjuvant chemotherapy
almost always leaves residual GBM cells to cause fatal recurrence, leading to medium
survival period of 8 -15 months and over-all survival rates of about 30% in 2 years and <3%
in 5 years after diagnosis/surgery. Thus, in neurosurgical oncology practice, GBM patients
in the first 2-year period during and after receiving multi-modal therapy are watched
closely for possible GBM tumor recurrence and mortal disease relapse and immediately given
palliative treatments and health care, until death. In this phase-II trial, GBM patient
participants who receive ADCTA-G "vaccine" adjuvant immunotherapy (added to the conventional
multi-modal regimen) will be similarly watched closely by treatments and health care visits
at least biweekly from the date of surgery/diagnosis to 24 months, and if alive followed by
weekly phone calls and scheduled health care visits at least once every 3 months, up to 72
months after surgery. In the trial protocol, ADCT-G in 10 doses is administered after
surgery, over a period of 6 or 8 months, as an adjuvant immunotherapy of the conventional
multimodal regimen. Individual ADCTA-G "vaccine" lot of every participant GBM patient is
manufactured from patient's own monocyte-derived dendritic cells and the patient's own tumor
cell antigens, both of which are prepared by a distinct method of procedures performed
within air particle-free barrier good laboratory practice (GLP) facility. Previous phase
I/II clinical trial of ADCTA-G "vaccine" immunotherapy administered as an adjuvant to the
conventional multimodal regimen, has obtained promising safety and efficacy results for GBM
patients in a clinical center. This phase-II clinical trial in China Medical University
Hospital-Taichung will employ essentially the same clinical protocols and the same distinct
"vaccine" manufacturing method of standard operational procedures (SOP), that is, the
conventional multimodal regimen plus adjuvant immunotherapy using personal ADCTA-G "vaccine"
lot for every GBM patient participants.
Rationale and Background :
Glioblastoma multiforme (GBM) and other WHO grade IV malignant gliomas of the brain are
among the most lethal of human cancers. Despite current intensive multimodal regimen
including the use of temozolomide (TMZ) for combined chemo-radiotherapy (CCRT) and for
subsequent adjuvant chemotherapy, the medium survival period of GBM patients is still 8-16
months after diagnosis and surgery, with prognosis varied according to demographic features
such as age, radiotherapy types and chemotherapy measures.These fatal brain cancers in
general contain cancer cells with mutation in certain genes. Also, the mutated GBM cancer
cells are usually heterogenous; and different GBM patients may have individual sets of
heterogenous glioma cancer cells in which the mutant genes would generate altered antigens
that can be recognized by the patient's adaptive immune system to mount immuno-targeting
responses to reject or kill the GBM tumor cells. However, GBM is still fatal because it is
highly immunosuppressive, i.e. able to anergize the immune effector cells in the body.
Although surgical resection of rapidly expanding tumor bulk will prevent further physical
damages to the brain and curtail the immunosuppression, the already anergized effector T
lymphocytes still require functional restoration. On the other hand, post-surgical TMZ CCRT
and adjuvant chemotherapy may weaken the residual tumor cells, but TMZ will also impair if
not kill the active T lymphocytes in general, including anti-GBM lymphocytes. It is
therefore important to exploit the adaptive immunity system for effective therapy of GBM. To
apply the adaptive immunotherapy, it is best to use each patient's surgical tumor specimen
to prepare the own individual "tumor regression antigens" for loading onto the patient's own
dendritic cells (the "professional" antigen processing and presenting cells of the immune
system). Dendritic cells loaded with tumor-specific antigens, upon maturation and
inoculation ("vaccination"), would migrate/home to the T cell area of lymph nodes and
stimulate proliferation of tumor-specific cytotoxic T lymphocyte that would move out of
lymph node to find the brain tumor lesion to attack and eradicate the residual GBM tumor
cells, resulting in prevention of GBM recurrence.
With fore-mentioned working hypotheses, the investigators carried out translational research
from 1997 to 2002. A special method has been developed for production of an
immunotherapeutic, which is named "autologous dendritic cell/autologous tumor cell antigens
of GBM" (ADCTA-G). For clinical trial purpose, the investigators have established standard
operational procedures (SOP) of the method with the use of clinical Good Manufacturing
Practice (cGMP)-grade cytokines and pharmaceutical reagents. Individual ADCTA-G lots of all
participant GBM patients are manufactured in high efficiency particle arresting (HEPA)
air-filtered, germ-free bio-safety barrier clinical Good Laboratory Practice (cGLP)
facilities. The phase I/II clinical trial was officially approved by Taiwan Department of
Health and performed in a clinical center to demonstrate that ADCTA-G adjuvant immunotherapy
was safe and apparently could prolong the survival for GBM patients.
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Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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