Purpose of this clinical phase 1 trial was to determine if para-chloro-2-\[18F\]fluoroethyletomidate positron emission computed tomography (\[18F\]CETO-positron emission computed tomography(PET)/computed tomography(CT)) can be used in diagnostics of adrenal tumors and if the biochemical/pharmacological states conditions in humans with various illnesses, compared to healthy humans, such as the radio tracer is suitable?
After receiving oral and written information about the study and its potential risks, all participants provided written informed consent. All participants underwent a screening visit 1-28 days before their \[18F\]CETO PET/CT. At the screening visit their medical history was obtained, including besides information of previous disease(s) and medication, also a clinical examination, WHO performance status, height, weight, pulse rate and blood pressure, blood chemistry and haematology. Right before the PET/CT investigation a baseline assessment was performed including: * A physical examination according to Modified Early Warning Score (MEWS) * 12-lead electrocardiogram (ECG) * Any concomitant medications was recorded * Medical history - occurrence of any new symptoms and events since the screening visit * Hematology (International Normalized Ratio (INR) in patients with antiocoagulant treatment). * Pregnancy test in women. * Assessment of injection site monitored by visual inspection (rash and phlebitis) Participants received on average 0,76 mikrograms (range 0,1-1.37 mikrograms) of administered mass of CETO in conjunction to the PET/CT investigation. Potential adverse events were monitored closely during, and after the administration of \[18F\]CETO, with access to emergency medicine resources. Each participant remained for observation at least 3 hours after administration of \[18F\]CETO and the following assessments were performed: * Blood withdrawn for additional post-scan chemical analysis. * Assessment of injection site monitored by visual inspection (rash and phlebitis). * MEWS The ten first participants were evaluated for serious adverse events/adverse events (SAE/AEs) the day after (approximately 24 hours after) performing the \[18F\]CETO PET due to the short half-life of the radionuclide used, fluorine- 18 (T1/2= 109.5 min). Safety reporting was assessed by use of clinical Adverse Events and Common Toxicity Criteria (CTC), laboratory and non-laboratory toxicities.
Study Type
INTERVENTIONAL
Allocation
NA
Purpose
DIAGNOSTIC
Masking
NONE
Enrollment
20
Injection of F18CETO or O15water followed by PET/CT
Uppsala University Hospital
Uppsala, Sweden
Evaluate safety of up to two administrations of [18F]CETO in up to 15 patients in comparison with 5 healthy controls.
Number of patients with treatment-related adverse events as assessed by clinical Adverse Events and Common ToxicityNCI Common Terminology Criteria for Adverse Events v4.0 (CTCAE)
Time frame: Up to 1 day after the [18F]CETO PET/CT for each patient
Evaluate [18F]CETO as a PET- biomarker for the adrenals and to diagnose and visualize primary aldosteronism, cortisol producing adrenocortical adenoma and non-functioning adrenocortical adenoma in up to 15 patients
Arterial blood was collected to determined the fraction of intact \[18F\]CETO in plasma. PET- modelling based on dynamic PET-data and metabolite analysis was performed for scientific purposes. Measurement of Standard Uptake Value (SUV) was determined for the adrenal glands.
Time frame: Up to 24 month
Biodistribution of [18F]CETO
Measurement of SUV for organs was determined.
Time frame: Up to 22 month
Compare uptake of [18F]CETO in normal adrenal glands in patients comparing healthy controls and determine the test - retest variability of [18F]CETO.
Difference in SUV in the adrenal glands between two investigations in the samt participant was determined.
Time frame: Up to 24 month
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