Synthesis and Evaluation of <sup>11</sup>C-LY2795050 as a κ-Opioid Receptor Antagonist Radiotracer for PET Imaging

Zheng, Ming-Qiang; Nabulsi, Nabeel; Kim, Su Jin; Tomasi, Giampaolo; Lin, Shu-fei; Mitch, Charles H.; Quimby, Steven J.; Barth, Vanessa N.; Rash, Karen; Masters, John J.; Navarro, Arturo Anadón; Seest, Eric P.; Morris, Evan D.; Carson, Richard E.; Huang, Yiyun

doi:10.2967/jnumed.112.109512

Cited by 77 publications

(90 citation statements)

References 37 publications

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“…As reported previously, the in vitro binding affinities ( K i ) of [ 11 C]LY2795050 were 0.72 and 25.8 nM, respectively, for KOR and MOR (16) at room temperature (22 °C). In our present work, in non-human primates, in vivo , ED 50 MOR was found to be 119 μg/kg based on occupancy studies with [ 11 C]carfentanil PET and blocking doses of LY2795050.…”

Section: Discussionsupporting

confidence: 69%

“…[ 11 C]LY2795050 was synthesized as previously described (16). Both chemical and radiochemical purity of the [ 11 C]LY2795050 final product were >95 %.…”

Section: Methodsmentioning

confidence: 99%

“…Twenty blood samples (0.5 mL) were drawn at 0.75, 1.5, 2.25, 3, 4, 5, 6, 8, 9, 12, 15, 20, 25, 30, 40, 50, 60, 75, 90, 105, and 120 min after the injection of [ 11 C]LY2795050. Samples drawn at 4, 12, 30, 60 (3.5 mL), and 90 min (1–5 mL) were also analyzed for radioactive metabolites according to published methods (16). Arterial samples were not taken for [ 11 C]carfentanil because there is an accepted reference region (22).…”

Section: Methodsmentioning

confidence: 99%

“…Our group recently reported a new KOR antagonist radioligand [ 11 C]LY2795050 (16). Radioligand competition assays using cloned human KOR, MOR and DOR indicated [ 11 C]LY2795050 displayed in vitro K i values of 0.72, 25.8, and 153 nM, respectively, for KOR, MOR and DOR.…”

Section: Introductionmentioning

confidence: 99%

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Determination of the In Vivo Selectivity of a New κ-Opioid Receptor Antagonist PET Tracer ¹¹C-LY2795050 in the Rhesus Monkey

et al. 2013

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[11C]LY2795050 is a novel kappa-selective antagonist PET tracer. The in vitro binding affinities (Ki) of LY2795050 at the kappa opioid (KOR) and mu opioid (MOR) receptors are 0.72 and 25.8 nM, respectively. Thus, the in vitro KOR/MOR binding selectivity is about 36:1. Our goal in this study was to determine the in vivo selectivity of this new KOR antagonist tracer in the monkey. Methods To estimate ED50 value of LY2795050 at the MOR and KOR sites, two series of blocking experiments were performed in three rhesus monkeys using [11C]LY2795050 and [11C]carfentanil with co-injections of various doses of unlabeled LY2795050. Kinetic modeling was applied to calculate regional binding potential (BPND), and one- and two-site binding curves were fitted to these data to measure [11C]LY2795050 binding selectivity. Results LY2795050 ED50 at MOR was 119 μg/kg based on a one-site model for [11C]carfentanil. The one-site binding model was also deemed sufficient to describe the specific binding of [11C]LY2795050 at KOR. The ED50 at KOR estimated from the one-site model was 15.6 μg/kg. Thus the ED50 ratio for MOR:KOR was 7.6. Conclusion The in vivo selectivity of [11C]LY2795050 for KOR over MOR is 7.6. [11C]LY2795050 has 4.7-fold lower selectivity at KOR over MOR in vivo as compared to in vitro. Nevertheless, based on our finding in vivo, 88 % of the PET-observed specific binding of [11C]LY2795050 under baseline condition will be due to binding of the tracer at the KOR site in a region with similar prevalence of KOR and MOR. We conclude that [11C]LY2795050 is sufficiently selective for KOR over MOR in vivo to be considered an appropriate probe for studying the kappa opioid receptor with PET.

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Section: Discussionsupporting

confidence: 69%

“…[ 11 C]LY2795050 was synthesized as previously described (16). Both chemical and radiochemical purity of the [ 11 C]LY2795050 final product were >95 %.…”

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Determination of the In Vivo Selectivity of a New κ-Opioid Receptor Antagonist PET Tracer ¹¹C-LY2795050 in the Rhesus Monkey

et al. 2013

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“…On the analgesic route of pain circuits, however, not only µ opioid receptors but also κ-receptors appear to be of great relevance not only in relays of the spinothalamic tract conveying signals to higher centers but also as potential modulators of dopamine release in cortical and subcortical brain areas [240]. Most auspicious approach for κ receptor ligands was described in 2003 by Thomas et al [104] [241]. Simultaneously, entrapment in cellular compartments or activation of c-jun terminal kinase 1 (inductor of autophagosome formation) discussed to prolong the action of JDTic is not known for the shorter acting LY2795050 [242].…”

Section: Discussionmentioning

confidence: 99%

Neuropeptide Receptors in Pain Circuitries: Useful Targets for CNS Imaging with Non-Peptide Ligands Suitable for PET?

Pissarek¹

2014

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Association of In Vivo κ-Opioid Receptor Availability and the Transdiagnostic Dimensional Expression of Trauma-Related Psychopathology

et al. 2014

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IMPORTANCE Exposure to trauma increases the risk for developing threat (ie, fear) symptoms, such as reexperiencing and hyperarousal symptoms, and loss (ie, dysphoria) symptoms, such as emotional numbing and depressive symptoms. While preclinical data have implicated the activated dynorphin/κ-opioid receptor (KOR) system in relation to these symptoms, the role of the KOR system in mediating these phenotypes in humans is unknown. Elucidation of molecular targets implicated in threat and loss symptoms is important because it can help inform the development of novel, mechanism-based treatments for trauma-related psychopathology.OBJECTIVE To use the newly developed [ 11 C]LY2795050 radiotracer and high-resolution positron emission tomography to evaluate the relation between in vivo KOR availability in an amygdala-anterior cingulate cortex-ventral striatal neural circuit and the severity of threat and loss symptoms. We additionally evaluated the role of 24-hour urinary cortisol levels in mediating this association. DESIGN, SETTING, AND PARTICIPANTSThis cross-sectional positron emission tomography study under resting conditions was conducted at an academic medical center. Thirty-five individuals representing a broad transdiagnostic and dimensional spectrum of trauma-related psychopathology, ranging from nontrauma-exposed psychiatrically healthy adults to trauma-exposed adults with severe trauma-related psychopathology (ie, posttraumatic stress disorder, major depressive disorder, and/or generalized anxiety disorder).MAIN OUTCOMES AND MEASURES [ 11 C]LY2795050 volume of distribution values in amygdala-anterior cingulate cortex-ventral striatal neural circuit; composite measures of threat (ie, reexperiencing, avoidance, and hyperarousal symptoms) and loss (ie, emotional numbing, major depressive disorder, and generalized anxiety disorder symptoms) symptoms as assessed using the Clinician-Administered PTSD Scale, Hamilton Depression Rating Scale, and Hamilton Rating Scale for Anxiety; and 24-hour urinary cortisol levels.RESULTS [ 11 C]LY2795050 volume of distribution values in an amygdala-anterior cingulate cortex-ventral striatal neural circuit were negatively associated with severity of loss (r = −0.39; 95% CI, −0.08 to −0.66), but not threat (r = −0.03; 95% CI, −0.30 to 0.27), symptoms; this association was most pronounced for dysphoria symptoms (r = −0.45; 95% CI, −0.10 to −0.70). Path analysis revealed that lower [ 11 C]LY2795050 volume of distribution values in this circuit was directly associated with greater severity of loss symptoms and indirectly mediated by 24-hour urinary cortisol levels. CONCLUSIONS AND RELEVANCEResults of this study suggest that KOR availability in an amygdala-anterior cingulate cortex-ventral striatal neural circuit mediates the phenotypic expression of trauma-related loss (ie, dysphoria) symptoms. They further suggest that an activated corticotropin-releasing factor/hypothalamic-pituitary-adrenal axis system, as assessed by 24-hour urinary cortisol levels, may indirectly mediate this associ...

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Synthesis and Evaluation of ¹¹C-LY2795050 as a κ-Opioid Receptor Antagonist Radiotracer for PET Imaging

Cited by 77 publications

References 37 publications

Determination of the In Vivo Selectivity of a New κ-Opioid Receptor Antagonist PET Tracer ¹¹C-LY2795050 in the Rhesus Monkey

Determination of the In Vivo Selectivity of a New κ-Opioid Receptor Antagonist PET Tracer ¹¹C-LY2795050 in the Rhesus Monkey

Neuropeptide Receptors in Pain Circuitries: Useful Targets for CNS Imaging with Non-Peptide Ligands Suitable for PET?

Association of In Vivo κ-Opioid Receptor Availability and the Transdiagnostic Dimensional Expression of Trauma-Related Psychopathology

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Synthesis and Evaluation of 11C-LY2795050 as a κ-Opioid Receptor Antagonist Radiotracer for PET Imaging

Cited by 77 publications

References 37 publications

Determination of the In Vivo Selectivity of a New κ-Opioid Receptor Antagonist PET Tracer 11C-LY2795050 in the Rhesus Monkey

Determination of the In Vivo Selectivity of a New κ-Opioid Receptor Antagonist PET Tracer 11C-LY2795050 in the Rhesus Monkey

Neuropeptide Receptors in Pain Circuitries: Useful Targets for CNS Imaging with Non-Peptide Ligands Suitable for PET?

Association of In Vivo κ-Opioid Receptor Availability and the Transdiagnostic Dimensional Expression of Trauma-Related Psychopathology

Contact Info

Product

Resources

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Synthesis and Evaluation of ¹¹C-LY2795050 as a κ-Opioid Receptor Antagonist Radiotracer for PET Imaging

Determination of the In Vivo Selectivity of a New κ-Opioid Receptor Antagonist PET Tracer ¹¹C-LY2795050 in the Rhesus Monkey

Determination of the In Vivo Selectivity of a New κ-Opioid Receptor Antagonist PET Tracer ¹¹C-LY2795050 in the Rhesus Monkey