| Literature DB >> 32106419 |
Ping Bai1,2,3, Sha Bai2, Michael S Placzek2, Xiaoxia Lu1, Stephanie A Fiedler2, Brenda Ntaganda2, Hsiao-Ying Wey2, Changning Wang2.
Abstract
The orexin receptor (OX) is critically involved in motivation and sleep-wake regulation and holds promising therapeutic potential in various mood disorders. To further investigate the role of orexin receptors (OXRs) in the living human brain and to evaluate the treatment potential of orexin-targeting therapeutics, we herein report a novel PET probe ([11C]CW24) for OXRs in the brain. CW24 has moderate binding affinity for OXRs (IC50 = 0.253 μM and 1.406 μM for OX1R and OX2R, respectively) and shows good selectivity to OXRs over 40 other central nervous system (CNS) targets. [11C]CW24 has high brain uptake in rodents and nonhuman primates, suitable metabolic stability, and appropriate distribution and pharmacokinetics for brain positron emission tomography (PET) imaging. [11C]CW24 warrants further evaluation as a PET imaging probe of OXRs in the brain.Entities:
Keywords: PET; imaging; orexin receptors; radiotracer
Mesh:
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Year: 2020 PMID: 32106419 PMCID: PMC7179119 DOI: 10.3390/molecules25051018
Source DB: PubMed Journal: Molecules ISSN: 1420-3049 Impact factor: 4.411
Figure 1Structures of orexin receptor radioligands.
Figure 2Structures and physicochemical properties of IPSU and CW24 (n.t. = not tested). IC50 of IPSU, CW24 and suvorexant were measured by a radioligand competition binding assay.
Scheme 1Radiolabeling condition: IPSU (precursor, 0.5 mg), [11C]CH3I, KOH (10 mg), in 1.0 mL DMF, 3 min, 100 °C. Radiochemical yield (RCY): 10–21% (non-decay corrected from trapped [11C]CH3I).
Figure 3(A) The PET/CT imaging of [11C]CW24 focused on mice brain (20‒60 min after intravenous administration (i.v.)); (B) baseline and blocking time-activity curve (TAC) of [11C]CW24 and (C) TAC after normalized the brain uptake curves with the highest uptake time point (20 seconds post-injection).
Figure 4(A) Positron emission tomography (PET)-Magnetic resonance (MR) Imaging (macaque brain). Summed PET images (30–90 min after [11C]CW24 injection) superimposed structural MRI from the same macaque. (B) Time−activity curves for brain regions of interest from baseline and blocking scans are shown (2.0 mg/kg IPSU) (a) hippocampus, (b) nucleus accumbens, (c) thalamus, (d) hypothalamus, (e) putamen and (f) cerebellum.
Figure 5Kinetic modeling results with [11C]CW24 in the macaque brain. (A) The total volume of distribution (VT) images derived from Logan plot with arterial blood data as input function (color bar indicates VT values from 1–2.5 mL/cm3 (blue to red); (B) Regional VT values showed that the expression difference in brain regions; (C) Arterial plasma analysis showed that [11C]CW24 radioactivity was rapidly cleared from blood and [11C]CW24 stability evaluated in plasma over time showed lasting presence of ~47% of parent compound at 30 min.