Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT00813566 |
| Other study ID # |
HCI31335 |
| Secondary ID |
|
| Status |
Completed |
| Phase |
Phase 1
|
| First received |
|
| Last updated |
|
| Start date |
November 12, 2010 |
| Est. completion date |
February 3, 2015 |
Study information
| Verified date |
April 2022 |
| Source |
University of Utah |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
The standard treatment approach for patients with high-grade primary brain tumors includes
maximum feasible surgical resection, followed by 6 weeks of concurrent cranial irradiation
and daily low-dose temozolomide chemotherapy, followed by 12 cycles of high-dose temozolomide
administered for 5 consecutive days every 4 weeks [Stupp 2005]. Contrast-enhanced MRI is the
current standard for evaluating the success of therapy and monitoring for tumor recurrence.
MRI is typically obtained prior to initial surgery, within 24 hours after surgery, at the
conclusions of cranial irradiation, and then every 8 weeks during temozolomide chemotherapy
until evidence of recurrence. Despite this careful clinical and radiographic surveillance,
and despite decades of research into the histologic and molecular classification of primary
brain tumors, our ability to predict tumor behavior remains very limited. Some gliomas will
result in overall survival times of only months, whereas other histologically-identical
gliomas may yield survivals of years to decades [Carson 2007, Curran 1993, Lamborn 2004].
Current assessment of tumor response to therapy is also poor. Patients with complete
radiographic response after cranial irradiation often progress rapidly post-irradiation. In
contrast, some patients with enhancing masses at the end of chemoradiotherapy may respond
dramatically to further chemotherapy alone, or the masses may even disappear in the absence
of further therapy (so called "tumor pseudoprogression") [Chamberlain 2007]. This confounding
situation demonstrates a need for better assessment of tumor response.
Description:
Positron emission tomography (PET) is a molecular imaging modality that can probe various
aspects of tumor function using a variety of radio-labeled imaging agents ("tracers").
Oncologic PET imaging has seen a dramatic rise in clinical utilization over the past decade
for cancer detection, staging, and evaluating residual or recurrent disease following
therapy. These clinical scans use the tracer [18F]fluoro-2-deoxy-D-glucose (FDG), which
accumulates in cells in proportion to glucose (GLUT) transporter and hexokinase activity. FDG
thus provides a measure of tissue glucose metabolism. Concurrent with this clinical growth, a
number of other PET tracers have received significant attention in research for a variety of
imaging targets. Of special interest are the tracers 3'-deoxy-3'-[18F]fluorothymidine (FLT),
1-[11C]-acetate (ACE), and [15O]water (H2O). The uptake, retention/washout, and ultimate
biodistribution of these tracers are each related to different functional or molecular
processes. As such, each can be used to probe a different aspect of tumor function: FLT
directly assesses tumor proliferation, ACE provides a measure of tumor growth related to
fatty acid and membrane synthesis, and H2O quantifies tumor perfusion.
OBJECTIVES:
This study has two primary objectives: a translational objective in which a new PET imaging
technology will be translated from experimental development (with simulations and in animals)
to the first use in human subjects; and an exploratory objective in which the complementary
value of multiple PET tracers will be investigated. Each of these objective is described
below, where the study design has been carefully setup to fulfill both objectives in the same
study population.
The translational objective of this study is to implement and evaluate a new imaging
technology for rapid, single-scan multi-tracer PET imaging of these tracers. Current PET
technology prohibits imaging of more than one tracer in a single scan since the imaging
signals from each tracer cannot be distinguished by normal techniques; as such, separate
scans with each tracer currently need to be acquired hours or days apart. Our group has
developed techniques and algorithms for recovering individual-tracer images from
rapidly-acquired multi-tracer PET data using dynamic imaging techniques. These methods have
been tested through extensive simulations and verified experimentally in a canine model with
spontaneously-occurring tumors. Refinement of the methods with more advanced algorithms is
ongoing. The patient imaging studies of this protocol will be implemented in two phases. In
Phase A, separate single-tracer imaging of each tracer will be performed. The data from these
scans will be co-registered and combined to "emulate" multi-tracer scans, which will then be
processed by the multi-tracer signal-separation algorithms. This will permit a direct
comparison of imaging biomarkers from multi-tracer vs. single-tracer scans for each tracer.
Such comparison techniques have been established by the investigators and have been accepted
by peer review for testing multi-tracer signal-separation algorithms. Once
statistically-significant evidence is obtained that multi-tracer scans can accurately provide
the same imaging biomarkers as separate single-tracer scans, the imaging will transition to
Phase B-in which actual multi-tracer scans will be performed.
The objectives of this exploratory study is to preliminarily evaluate the complementary value
of FDG, FLT, ACE, and H2O PET in patients with primary glial neoplasms. Multi-tracer PET
profiles with these four tracers will be obtained in 20 patients with primary glial neoplasms
at up to three timepoints: (1) at "baseline" prior to surgery or immediately after surgery
providing a complete surgical resection was not possible and confirmed by a post-operative
contrast MRI scan where residual tumor greater than 1.0 cm in diameter was present and prior
to any tumor-directed therapy; (2) at the conclusions of the initial (~6-8 weeks)
chemoradiotherapy; and (3) at the time of MRI-documented recurrence within 2 years. In
addition, patients with a known primary brain tumor who have previously undergone treatment
and have recurred based on standard clinical and imaging criteria will be eligible for the
study. A number of quantitative and pseudo-quantitative imaging biomarkers for each tracer
will be computed at each imaging timepoint, and the change in each biomarker between
timepoints will also be computed. These data will be compared with clinical endpoints
(survival, time to progression), and with tumor biologic information (histology, WHO grade,
vascularity, Ki-67, vascular endothelial growth factor (VEGF), epidermal growth factor
receptor (EGFR), p53) in cases when tumor tissue becomes available from standard care. These
data will provide pilot information into the potential value of concurrent multiple PET
biomarkers for predicting tumor behavior prior to the start of therapy, for improved
prognostication, for more efficient and effective tumor surveillance, and/or for more
appropriate assignment of patients to conventional, aggressive, or investigational therapies
early in their clinical courses.
The driving hypothesis for the overall line of research is that multiple PET imaging
biomarkers obtained in conjunction can provide improved image-guided personalized care of
patients with primary glial neoplasms. The term "personalized care" is used here to broadly
include the prediction of tumor behavior prior to the start of therapy, tumor surveillance,
prognostication, and individualized assignment of patients to conventional, aggressive, or
investigational therapies early in their clinical courses. This pilot project will obtain
initial data on the value of these PET biomarkers for such image-guided personalized care.
Specific hypotheses to be tested include:
- HYPOTHESIS I a: Rapid, single-scan multi-tracer PET imaging can recover PET imaging
biomarker information of each tracer that are not significantly different from those
obtained from conventional, single-tracer scans of each tracer.
- HYPOTHESIS II b: Multi-tracer PET biomarkers, obtained in conjunction, are better able
to predict tumor aggressiveness than individual-tracer biomarkers or conventional
radiographic imaging.
- HYPOTHESIS III b: Multi-tracer PET biomarkers, obtained in conjunction, are better able
to detect functional changes in tumor state that occur in response to therapy than
individual-tracer biomarkers or conventional radiographic imaging.
- HYPOTHESIS IV b: Characterization of multiple aspects of tumor function (glucose
metabolism, proliferation, membrane growth, and perfusion) provides new insight into
tumor status that can guide selection of the most appropriate therapy.
a Sufficient statistical power is expected to be obtained under this protocol to validate the
extensive simulations and experimental evaluations performed previously and concurrently with
these patient imaging studies.
b Pilot data regarding these three hypotheses will be obtained in this work by studying the
correlation of PET imaging biomarkers with clinical outcomes and tumor biologic information.
Though high statistical power cannot be expected from the limited number of patients in this
pilot study, underlying trends in the data will be identified, permitting the formulation of
formal hypotheses to be tested in future rigorous trials.
