Glioblastoma Multiforme Clinical Trial
Official title:
A Phase I Trial for the Addition of Chloroquine, an Autophagy Inhibitor, to Concurrent Chemoradiation for Newly Diagnosed Glioblastoma
Patients with a glioblastoma (GBM) have a poor prognosis with a median survival of 14.6
months after maximal treatment with a resection and chemoradiation. Since the pivotal trial
evaluating the effect of temozolomide (TMZ), overall survival has not increased.
Treatment of GBM xenografts in vivo with chloroquine (CQ), an antimalarial agent, has been
shown to reduce the hypoxic fraction and sensitizes tumors to radiation. Epidermal growth
factor receptor (EGFR) amplification or mutation is regularly observed GBM and is thought to
be a major contributor to radioresistance. The most common EGFR mutation in GBM (EGFRvIII) is
present in 50-60% of patients whose tumor shows amplification of EGFR. EGFR provides cells
with a survival advantage through autophagy when exposed to stresses such as hypoxia and
nutrient starvation. This effect is even more pronounced in EGFRvIII overexpressing tumors.
Previously, the potential effect CQ has been demonstrated in a small randomized controlled
trial in GBM treated with radiotherapy and carmustine, which showed a trend towards increased
overall survival. However, as the intracellular effects of chloroquine are dose-dependent the
maximum tolerated dose for CQ in combination with concurrent radiotherapy with daily
temozolomide needs to be established.
This trial has been designed as an open label, single center combination phase I trial. The
primary objective is to determine the maximum tolerated dose (MTD) for chloroquine (CQ) in
combination with concurrent radiotherapy with daily temozolomide in patients with a newly
diagnosed GBM.
Eligible patients will receive radiotherapy and chemotherapy according to standard protocol
for newly diagnosed GBM. This consists of 33 daily fractions of 1.8 Gy to the tumor and
surrounding margin in combination with TMZ 75 mg/m² per os daily (po qd) and six adjuvant
cycles of TMZ 150 - 200 mg/m² po qd. Treatment will be combined with daily intake of
escalating doses of chloroquine. Chloroquine will start with week before the start of
radiotherapy and end on the last day of radiotherapy.
The rate of subject entry and escalation to the next dose level will depend upon assessment
of the safety profile of patients entered at the previous dose level. Toxicity will be
evaluated according to the NCI common Terminology Criteria for Adverse Events (CTCAE),
Version 4.0.
The 3 + 3 cohort method is used. A minimum of three patients will be entered at each dose
level. All three will be followed during the concomitant radiotherapy and a 4 week
observation period before escalation to the next dose level.
The start dose is 200mg chloroquine daily. Before opening the next higher dose level all
toxic effects at the preceding dose level will be reviewed and expansion or escalation will
be undertaken as appropriate
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