Assessment of Primary and Metastatic Brain Tumor Hypoxia With Fluoromisonidazole, FDG and Water



Status:Recruiting
Conditions:Cancer, Brain Cancer
Therapuetic Areas:Oncology
Healthy:No
Age Range:18 - Any
Updated:8/15/2018
Start Date:August 2011
End Date:December 2021
Contact:John M Hoffman, MD
Email:john.hoffman@hci.utah.edu
Phone:801-581-4064

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Assessment of Primary and Metastatic Brain Tumor Hypoxia With 18F-Fluoromisonidazole, [18F]Fluoro-2-deoxy-D-glucose (FDG) and [15O]Water (H215O)

Purpose of Study This exploratory clinical study will investigate FMISO (fluoromisonidazole)
in patients with (1) newly diagnosed primary malignant brain tumors (WHO [World Health
Organization] Grade III or IV glial-based tumors) who have not had a complete surgical
resection and by contrast MRI (Magnetic resonance imaging) have residual tumor > 1.0 cm in
diameter and will be receiving radiotherapy or (2) newly diagnosed brain metastasis (> 1.0 cm
in diameter who will be receiving radiotherapy. The ability to accurately assess tumor
hypoxia and accurately determine the amount/degree of tumor hypoxia could potentially change
patient management once validated as tumor hypoxia is known to be associated with a poor
prognosis [Eyler 2008].

Malignant Brain Tumors (Primary and Metastatic) Despite significant advances in the
understanding of brain tumor biology and genetics as well as improvements in surgical
techniques, radiotherapy administration, and chemotherapy methods, many brain tumors remain
incurable. Many brain tumors are highly infiltrative neoplasms, and are therefore unlikely to
be cured by local treatments such as surgery, focal radiotherapy, radiosurgery or
brachytherapy.

Rationale and Goals of Study The preliminary efficacy of the radiopharmaceutical,
1H-1-(3-[18F]-fluoro-2-hydroxy-propyl)-2-nitro-imidazole [18F]-fluoromisonidazole,
[18F]FMISO, FMISO (fluoromisonidazole), a radiopharmaceutical that directly assess tumor
hypoxia using Positron Emission Tomography(PET) will be assessed.

This preliminary/exploratory clinical study will investigate [F-18]FMISO in 30 evaluable
patients with newly diagnosed primary brain tumor or brain metastasis. We expect that up to
35 -40 total patients may be enrolled in this study. This will assure that 30 evaluable
patients (patients who have complete imaging results and blood metabolism data available for
data analysis). In certain patients the blood metabolism data is not acceptable for final
analysis typically due to difficulty in drawing it rapidly enough due to the vein collapsing
during the rapid sampling required.

When possible we will also correlate FMISO uptake with the typical in-vitro test used to
assess proliferation, Ki-67 (protein) and other experimental assessments of hypoxia. This
correlation will be made whenever possible in those patients where tumor tissue is obtained
as part of standard care.

OBJECTIVES:

Primary Objective of Study - Synopsis The primary objective of this study is to determine the
association of FMISO PET (positron emission tomography) uptake (hypoxic volume [HV]), highest
tumor:blood ratio [T/Bmax]), FDG ([18F]-2 fluoro-2-deoxy-d-glucose) uptake, and tumor blood
flow/perfusion determined with H2O (water) and MRI and correlate these variables with overall
survival (OS) and time to progression (TTP) in participants with newly diagnosed primary
brain tumors or brain metastases.

The Hypotheses to be Tested

Three exploratory hypotheses will be studied. These include:

1. The first hypothesis to be tested is that increased FMISO PET uptake (hypoxic volume
[HV], highest tumor:blood ratio [T/Bmax]) is correlated with a shorter overall survival
and a shorter time to progression. An exploratory evaluation assessing combinations of
PET imaging variables such as hypoxic volume [HV], highest tumor:blood ratio [T/Bmax],
FDG-SUV, FDG quantitative parameters and blood flow as well as MR (magnetic resonance)
perfusion and blood volume will be assessed to see if they correlate with survival and
time to progression.

2. A second hypothesis to be tested is that FMISO is safe and non toxic in the dose
administered in this study in patients with primary and metastatic brain tumors. This
will be assessed in the first 10 patients enrolled in the study. Even though there have
been numerous published studies using FMISO in humans in several different tumor types
little human safety data has been published. Laboratory tests (except urinalysis) will
be repeated at approximately 24 hours in the first 10 and compared to the screening
values.

3. A third exploratory hypothesis to be tested is that FMISO uptake (hypoxic volume [HV],
highest tumor:blood ratio [T/Bmax]) will correlate with increased FDG uptake and
possibly with reduced blood flow/perfusion as determined with H215O PET imaging and MRI

Inclusion Criteria:

1. Adult patients. The patient must have a newly diagnosed primary malignant brain tumors
(WHO Grade III or IV glial-based tumors) and not have had a complete surgical
resection and by contrast MRI (obtained within 14 days prior to the FMISO study)

2. Patients must be 18 years or older for inclusion in this research study.

3. Patients must document their willingness to be followed until death or time of
progression.

4. All patients must sign a written informed consent and HIPAA authorization in
accordance with institutional guidelines.

5. Female patients who are not postmenopausal or surgically sterile will undergo a serum
pregnancy test prior to the research PET scans.

6. Pre-treatment laboratory tests for patients receiving [18F]FMISO must be performed
within 21 days prior to study entry.

Exclusion Criteria:

1. Patients with known allergic or hypersensitivity reactions to previously administered
radiopharmaceuticals.

2. Patients who are pregnant or lactating or who suspect they might be pregnant.

3. Adult patients who require monitored anesthesia for PET scanning.

4. Patients who are too claustrophobic to undergo MRI or PET imaging

5. Patients who cannot undergo MRI imaging due to MRI exclusion criteria
We found this trial at
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Salt Lake City, Utah 84112
Principal Investigator: John M Hoffman, MD
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Salt Lake City, UT
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