A pharmacokinetic PET study of NK₁ receptor occupancy

Stefano Zamuner; Eugenii Rabiner; Sofia A. Fernandes; Massimo Bani; Roger N. Gunn; Roberto Gomeni; Emilangelo Ratti; Vincent J. Cunningham

doi:10.1007/s00259-011-1954-2

A pharmacokinetic PET study of NK₁ receptor occupancy

Stefano Zamuner, Eugenii Rabiner, Sofia A. Fernandes, Massimo Bani, Roger N. Gunn, Roberto Gomeni, Emilangelo Ratti, Vincent J. Cunningham

NIHR Maudsley Biomedical Research Centre (BRC)

Research output: Contribution to journal › Article › peer-review

28 Citations (Scopus)

Abstract

Purpose: There is growing recognition of the importance of integrating drug occupancy data acquired by positron emission tomography (PET) with the plasma pharmacokinetics of the drug, in order to establish proper dose selection in subsequent clinical trials. Here we present a study in human subjects of the occupancy of NK1 receptors achieved following different doses of casopitant, a selective NK1 antagonist.

Methods: Two PET scans were carried out in each of eight human subjects, with the PET radioligand [C-11]GR205171, a high-affinity and selective NK1 receptor antagonist. The first scan was under baseline conditions and the second 24 h after a single oral dose of casopitant (2-120 mg). Arterial blood was collected throughout the scans for determination of plasma and whole blood input functions. Venous blood samples were taken prior to and following oral dosing up to 24 h for a pharmacokinetic study of casopitant concentration in plasma.

Results: It was first necessary to establish a suitable kinetic model for the estimation of [C-11]GR205171 NK1 receptor binding parameters in human brain tissue. A three-tissue compartment model with simultaneous estimation of multiple regions sharing common variables across regions was found suitable for the analysis. Because of the injected cold mass of the tracer and the high affinity of [C-11]GR205171 a correction for tracer occupancy effects was also incorporated into the analysis. We then developed a pharmacokinetic-receptor occupancy (PK-RO) model of the relationship between casopitant plasma concentrations and receptor binding, using a population approach.

Conclusion: These results indicate that after chronic dosing, casopitant can achieve a degree of NK1 receptor occupancy higher than those that have previously been tested in studies of clinical depression.

Original language	English
Pages (from-to)	226-235
Number of pages	10
Journal	European Journal of Nuclear Medicine and Molecular Imaging
Volume	39
Issue number	2
DOIs	https://doi.org/10.1007/s00259-011-1954-2
Publication status	Published - Feb 2012

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title = "A pharmacokinetic PET study of NK₁ receptor occupancy",

abstract = "Purpose: There is growing recognition of the importance of integrating drug occupancy data acquired by positron emission tomography (PET) with the plasma pharmacokinetics of the drug, in order to establish proper dose selection in subsequent clinical trials. Here we present a study in human subjects of the occupancy of NK1 receptors achieved following different doses of casopitant, a selective NK1 antagonist. Methods: Two PET scans were carried out in each of eight human subjects, with the PET radioligand [C-11]GR205171, a high-affinity and selective NK1 receptor antagonist. The first scan was under baseline conditions and the second 24 h after a single oral dose of casopitant (2-120 mg). Arterial blood was collected throughout the scans for determination of plasma and whole blood input functions. Venous blood samples were taken prior to and following oral dosing up to 24 h for a pharmacokinetic study of casopitant concentration in plasma. Results: It was first necessary to establish a suitable kinetic model for the estimation of [C-11]GR205171 NK1 receptor binding parameters in human brain tissue. A three-tissue compartment model with simultaneous estimation of multiple regions sharing common variables across regions was found suitable for the analysis. Because of the injected cold mass of the tracer and the high affinity of [C-11]GR205171 a correction for tracer occupancy effects was also incorporated into the analysis. We then developed a pharmacokinetic-receptor occupancy (PK-RO) model of the relationship between casopitant plasma concentrations and receptor binding, using a population approach. Conclusion: These results indicate that after chronic dosing, casopitant can achieve a degree of NK1 receptor occupancy higher than those that have previously been tested in studies of clinical depression.",

author = "Stefano Zamuner and Eugenii Rabiner and Fernandes, {Sofia A.} and Massimo Bani and Gunn, {Roger N.} and Roberto Gomeni and Emilangelo Ratti and Cunningham, {Vincent J.}",

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AU - Zamuner, Stefano

AU - Rabiner, Eugenii

AU - Fernandes, Sofia A.

AU - Bani, Massimo

AU - Gunn, Roger N.

AU - Gomeni, Roberto

AU - Ratti, Emilangelo

AU - Cunningham, Vincent J.

PY - 2012/2

Y1 - 2012/2

N2 - Purpose: There is growing recognition of the importance of integrating drug occupancy data acquired by positron emission tomography (PET) with the plasma pharmacokinetics of the drug, in order to establish proper dose selection in subsequent clinical trials. Here we present a study in human subjects of the occupancy of NK1 receptors achieved following different doses of casopitant, a selective NK1 antagonist. Methods: Two PET scans were carried out in each of eight human subjects, with the PET radioligand [C-11]GR205171, a high-affinity and selective NK1 receptor antagonist. The first scan was under baseline conditions and the second 24 h after a single oral dose of casopitant (2-120 mg). Arterial blood was collected throughout the scans for determination of plasma and whole blood input functions. Venous blood samples were taken prior to and following oral dosing up to 24 h for a pharmacokinetic study of casopitant concentration in plasma. Results: It was first necessary to establish a suitable kinetic model for the estimation of [C-11]GR205171 NK1 receptor binding parameters in human brain tissue. A three-tissue compartment model with simultaneous estimation of multiple regions sharing common variables across regions was found suitable for the analysis. Because of the injected cold mass of the tracer and the high affinity of [C-11]GR205171 a correction for tracer occupancy effects was also incorporated into the analysis. We then developed a pharmacokinetic-receptor occupancy (PK-RO) model of the relationship between casopitant plasma concentrations and receptor binding, using a population approach. Conclusion: These results indicate that after chronic dosing, casopitant can achieve a degree of NK1 receptor occupancy higher than those that have previously been tested in studies of clinical depression.

AB - Purpose: There is growing recognition of the importance of integrating drug occupancy data acquired by positron emission tomography (PET) with the plasma pharmacokinetics of the drug, in order to establish proper dose selection in subsequent clinical trials. Here we present a study in human subjects of the occupancy of NK1 receptors achieved following different doses of casopitant, a selective NK1 antagonist. Methods: Two PET scans were carried out in each of eight human subjects, with the PET radioligand [C-11]GR205171, a high-affinity and selective NK1 receptor antagonist. The first scan was under baseline conditions and the second 24 h after a single oral dose of casopitant (2-120 mg). Arterial blood was collected throughout the scans for determination of plasma and whole blood input functions. Venous blood samples were taken prior to and following oral dosing up to 24 h for a pharmacokinetic study of casopitant concentration in plasma. Results: It was first necessary to establish a suitable kinetic model for the estimation of [C-11]GR205171 NK1 receptor binding parameters in human brain tissue. A three-tissue compartment model with simultaneous estimation of multiple regions sharing common variables across regions was found suitable for the analysis. Because of the injected cold mass of the tracer and the high affinity of [C-11]GR205171 a correction for tracer occupancy effects was also incorporated into the analysis. We then developed a pharmacokinetic-receptor occupancy (PK-RO) model of the relationship between casopitant plasma concentrations and receptor binding, using a population approach. Conclusion: These results indicate that after chronic dosing, casopitant can achieve a degree of NK1 receptor occupancy higher than those that have previously been tested in studies of clinical depression.

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DO - 10.1007/s00259-011-1954-2

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EP - 235

JO - European Journal of Nuclear Medicine and Molecular Imaging

JF - European Journal of Nuclear Medicine and Molecular Imaging

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ER -

A pharmacokinetic PET study of NK₁ receptor occupancy

Abstract

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