Sarcoidosis Clinical Trial
Official title:
Optimizing Acquisition Parameters and Interpretive Methods of FDG-PET/CT With Rb-82 Myocardial Perfusion Imaging for Evaluation of Cardiac Sarcoidosis
In this this investigation, 15 subjects with a high probability of cardiac sarcoidosis based
on clinical criteria and abnormal cardiac FDG uptake on initial, clinically indicted FDG PET
study will be considered for this study. The study will test the following Aims:
Aim 1. Effect of FDG incubation time on visual and quantitative interpretation of FDG uptake.
Changes in incubation time can affect imaging target:background ratios and study
sensitivity/specificity. For the study-directed exam, all patients will undergo sequential
cardiacfocused FDG-PET imaging at 90 and 120 minutes after injection of FDG. Imaging
variables will be evaluated as below.
Aim 2. Reproducibility of FDG and Rb82 PET findings on sequential imaging. It is unknown
whether FDG-positive imaging findings in cardiac sarcoidosis are reproducible. All patients
will undergo study-directed FDG-PET/CT with MPI imaging within approximately 2 weeks from
initial clinical scan.
Sarcoidosis is a systemic disease of unknown etiology characterized by non-caseating
granulomatous inflammation. The pathophysiologic features of cardiac sarcoidosis include
macrophage-induced, T-cell mediated non-caseating granulomatous inflammation, followed by
myocardial scarring/fibrosis with clinical sequelae including arrhythmias, conduction
abnormalities, and contractile dysfunction. These lead to high event rates in patients with
cardiac sarcoidosis, with several studies reporting a prevalence of ventricular tachycardia
ranging from 23% to 38% and an ~ 20% rate of clinical congestive heart failure.
FDG-PET/CT with Rb82 myocardial perfusion imaging (FDG-PET with MPI) is becoming the gold
standard imaging technique for evaluating the degree of inflammation and the response to
immunosuppressive treatment in patients with cardiac sarcoidosis. FDG PET imaging allows for
evaluation of inflammatory macrophage infiltration, while Rb82 MPI allows for determination
of myocardial scar burden. Despite emerging data from our center and others on the clinical
utility of this technique in predicting prognosis, there is little consensus on the
reproducibility of this technique or optimal imaging acquisition techniques and
interpretative strategies.
In this study, patients with a high clinical likelihood of cardiac sarcoidosis will undergo a
study-directed FDG PET/CT with Rb82 myocardial perfusion imaging study approximately 2 weeks
following an initial clinically-directed examination.
The two FDG PET with MPI examinations will be examined for reproducibility of imaging
findings, including: SUVmax, SUVmean, distribution of FDG uptake, extra cardiac FDG uptake,
SUVvolume, SUVvolume:intensity, perfusion defect size/severity/location, LV ejection
fraction, myocardial blood flow.
Strict attention will be paid to ensure patients undergo the same metabolic preparation prior
to the two examinations.
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