RT Journal Article
SR Electronic
T1 Characterization of <sup>18</sup>F-FPyKYNE-Losartan for Imaging AT<sub>1</sub> Receptors
JF Journal of Nuclear Medicine
JO J Nucl Med
FD Society of Nuclear Medicine
SP 1612
OP 1617
DO 10.2967/jnumed.115.170951
VO 57
IS 10
A1 Maryam Hachem
A1 Mario Tiberi
A1 Basma Ismail
A1 Chad R. Hunter
A1 Natasha Arksey
A1 Tayebeh Hadizad
A1 Rob S. Beanlands
A1 Robert A. deKemp
A1 Jean N. DaSilva
YR 2016
UL http://jnm.snmjournals.org/content/57/10/1612.abstract
AB Most physiologic effects of the renin angiotensin system (RAS) are mediated via the angiotensin (Ang) type 1 receptor (AT1R). The 18F-FPyKYNE derivative of the clinically used AT1R blocker losartan exhibits high binding selectivity for kidney AT1R and rapid metabolism in rats. The aim of this study was to further assess the binding profile of this novel PET agent for imaging AT1R in rats and pigs. Methods: In vitro binding assays were performed with 18F-FPyKYNE-losartan in rat kidneys. Male Sprague–Dawley rats were used to assess dosimetry, antagonistic efficacy via blood pressure measurements, and presence of labeled metabolites in kidneys. Test–retest PET imaging, blocking with AT1R antagonist candesartan (10 mg/kg), and plasma metabolism analysis were performed in female Yorkshire pigs. Results: 18F-FPyKYNE-losartan bound with high affinity (dissociation constant of 49.4 ± 18.0 nM and maximal binding of 348 ± 112 fmol/mm2) to rat kidney AT1R. It bound strongly to plasma proteins in rats (97%), and its labeled metabolites displayed minimal interference on renal AT1R binding. FPyKYNE-losartan fully antagonized the Ang II pressor effect, albeit with 4-fold potency reduction (the effective dose inhibiting 50% of the Ang II–induced maximal pressor response of 25.5 mg/kg) relative to losartan. PET imaging exhibited high kidney-to-blood contrast and slow renal clearance, with an SUV of 14.1 ± 6.2. Excellent reproducibility was observed in the calculated test–retest variability (7.2% ± 0.75%). Only hydrophilic-labeled metabolites were present in plasma samples, and renal retention was reduced (−60%) at 10–15 min after blockade with candesartan. Conclusion: 18F-FPyKYNE-losartan has a favorable binding profile and displays high potential for translational work in humans as an AT1R PET imaging agent.