Glioblastoma Clinical Trial
Official title:
A Safety Study of Fingolimod With Radiation and Temozolomide in Newly Diagnosed High Grade Glioma
A recent prospective multicenter study by Dr. Grossman demonstrated that 40% of patients with
high grade glioma undergoing radiation and chemotherapy developed severe and persistent
lymphopenia (CD4 counts <200 cells/mm3). This lymphopenia lasted for twelve months following
radiation treatment and on multivariate analysis was associated with shorter survival. Our
group has data that strongly suggests that this lymphopenia is secondary to the inadvertent
radiation of circulating lymphocytes as they pass through the radiation beam. Investigators
propose the use of FDA approved for multiple sclerosis, fingolimod to signal lymphocytes to
leave the circulation prior to the initiation of radiation. It is a functional antagonist of
the sphingosine-1-phosphate receptor (S1PR) pathway and prevents lymphocyte egress from
secondary lymphoid organs.
Oral fingolimod will be given 1 week prior to the initiation of concurrent radiation and
temozolomide and will be discontinued immediately upon completion of the six weeks of
therapy. The primary objective is to evaluate if fingolimod can be safely combined with
radiation and temozolomide. Secondary endpoint is total lymphocyte counts (TLC) for the
proposed study participants. Investigators expect that patients receiving radiation and
temozolomide plus fingolimod have a recovery of lymphocyte counts to 80% of baseline within
four months, reference to historical control in which sustained lymphopenia lasted for twelve
months.
Five evaluable patients with newly diagnosed high grade gliomas who will undergo standard
concomitant radiation and temozolomide followed by adjuvant temozolomide will be accrued to
this open-label, single arm, safety study. Oral fingolimod will be given 1 week prior to the
initiation of concurrent radiation and temozolomide and will be discontinued immediately upon
completion of the six weeks of therapy.
The primary objective is to evaluate if fingolimod can be safely combined with radiation and
temozolomide. This standard chemoradiation causes 40% of patients to develop severe
lymphopenia two months after initiation of therapy. Investigators expect that when this is
combined with fingolimod, virtually all patients will have severe lymphopenia two months
after beginning treatment. Investigators will determine if these patients who routinely
receive pneumocystis jiroveci prophylaxis develop other severe opportunistic infections that
would prohibit further evaluation of this novel treatment approach. Primary endpoint is
incidence of greater than or equal to Grade III infections attributable to fingolimod-induced
lymphopenia defined by the NIH/NCI Common Terminology Criteria for Adverse Events (CTCAE)
within four months of starting fingolimod.
The secondary objective is to obtain preliminary information regarding the ability of
fingolimod to reduce radiation-related lymphopenia three months after stopping fingolimod.
The NIH funded Adult Brain Tumor Consortium (ABTC) followed total lymphocyte and CD4 counts
in 96 patients after treatment with radiation and temozolomide. The severe lymphopenia (CD4
count less than 200/mm3) lasted for twelve months in this historical control. Secondary
endpoint is total lymphocyte counts (TLC) for the proposed study participants. These will be
compared with patient level data on TLC from an historical cohort obtained from the ABTC.
Investigators expect that patients receiving radiation and temozolomide plus fingolimod have
a recovery of lymphocyte counts to 80% of baseline within four months, reference to
historical control in which sustained lymphopenia lasted for twelve months.
Investigators will also obtain laboratory analysis on lymphocyte subtypes and cytokine levels
(CD3, CD4, CD8, IL-7, TGF-Beta, etc.). Routine care for high grade gliomas includes weekly
Heme-8 and absolute lymphocyte count. Research blood will be obtained at 2 weeks prior to
chemoradiation and again at weeks 6, 10, 18, 26 and 46. Patients will be on study for
approximately one year.
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