Abstract
Glioblastoma multiforme
(GBM) is the most common intracranial cancer but despite recent advances in
therapy the overall survival remains about 20 months. Whole genome exon
sequencing studies implicate mutations in the receptor tyrosine kinase pathways
(RTK) for driving tumor growth in over 80% of GBMs. In spite of various RTKs
being mutated or altered in the majority of GBMs, clinical studies have not
been able to demonstrate efficacy of molecular targeted therapies using
tyrosine kinase inhibitors in GBMs. Activation of multiple downstream signaling
pathways has been implicated as a possible means by which inhibition of a
single RTK has been ineffective in GBM. In this study, we sought a combination
of approved drugs that would inhibit in vitro and in vivo growth of GBM
oncospheres. A combination consisting of gefitinib and sunitinib acted
synergistically in inhibiting growth of GBM oncospheres in vitro. Sunitinib was
the only RTK inhibitor that could induce apoptosis in GBM cells. However, the
in vivo efficacy testing of the gefitinib and sunitinib combination in an EGFR
amplified/ PTEN wild type GBM xenograft model revealed that gefitinib alone
could significantly improve survival in animals whereas sunitinib did not show
any survival benefit. Subsequent testing of the same drug combination in a
different syngeneic glioma model that lacked EGFR amplification but was more
susceptible to sunitinib in vitro demonstrated no survival benefit when treated
with gefitinib or sunitinib or the gefitinib and sunitinib combination.
Although a modest survival benefit was obtained in one of two animal models
with EGFR amplification due to gefitinib alone, the addition of sunitinib, to
test our best in vitro combination therapy, did not translate to any additional
in vivo benefit. Improved targeted therapies, with drug properties favorable to
intracranial tumors, are likely required to form effective drug combinations
for GBM.
Source: Evaluation
of tyrosine kinase inhibitor combinations for glioblastoma therapy. Joshi AD,
Loilome W, Siu IM, Tyler B, Gallia GL, Riggins
GJ (griggin1@jhmi.edu). PLoS One.
2012;7(10):e44372.
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