Species differences in metabolism of soluble epoxide hydrolase inhibitor, EC1728, highlight the importance of clinically relevant screening mechanisms in drug development

Cindy B. McReynolds; Jun Yang; Alonso Guedes; Christophe Morisseau; Roberto Garcia; Heather Knych; Caitlin Tearney; Briana Hamamoto; Sung Hee Hwang; Karen Wagner; Bruce D. Hammock

doi:10.3390/molecules26165034

Species differences in metabolism of soluble epoxide hydrolase inhibitor, EC1728, highlight the importance of clinically relevant screening mechanisms in drug development

Cindy B. McReynolds, Jun Yang, Alonso Guedes, Christophe Morisseau, Roberto Garcia, Heather Knych, Caitlin Tearney, Briana Hamamoto, Sung Hee Hwang, Karen Wagner, Bruce D. Hammock

Veterinary Clinical Sciences

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

2 Scopus citations

Abstract

There are few novel therapeutic options available for companion animals, and medications rely heavily on repurposed drugs developed for other species. Considering the diversity of species and breeds in companion animal medicine, comprehensive PK exposures in the companion animal patient is often lacking. The purpose of this paper was to assess the pharmacokinetics after oral and intravenous dosing in domesticated animal species (dogs, cats, and horses) of a novel soluble epoxide hydrolase inhibitor, EC1728, being developed for the treatment of pain in animals. Results: Intravenous and oral administration revealed that bioavailability was similar for dogs, and horses (42 and 50% F) but lower in mice and cats (34 and 8%, respectively). Additionally, clearance was similar between cats and mice, but >2× faster in cats vs. dogs and horses. Efficacy with EC1728 has been demonstrated in mice, dogs, and horses, and despite the rapid clearance of EC1728 in cats, analgesic efficacy was demonstrated in an acute pain model after intravenous but not oral dosing. Conclusion: These results demonstrate that exposures across species can vary, and investigation of therapeutic exposures in target species is needed to provide adequate care that addresses efficacy and avoids toxicity.

Original language	English (US)
Article number	5034
Journal	Molecules
Volume	26
Issue number	16
DOIs	https://doi.org/10.3390/molecules26165034
State	Published - Aug 2 2021

Bibliographical note

Funding Information:
This work was supported in part by grants from NIEHS/Superfund Research Program P42 (ES004699), NIH/NIEHS R35 (ES030443), NIH/NIGMS T32GM113770 (to CBM). UC Davis Center for Companion Animal Health for the dog studies, and Every Cat Health Foundation (previously Winn Feline Foundation) for the 1 mg/kg IV cat studies.

Funding Information:
Funding: This work was supported in part by grants from NIEHS/Superfund Research Program P42 (ES004699), NIH/NIEHS R35 (ES030443), NIH/NIGMS T32GM113770 (to CBM). UC Davis Center for Companion Animal Health for the dog studies, and Every Cat Health Foundation (previously Winn Feline Foundation) for the 1 mg/kg IV cat studies.

Publisher Copyright:
© 2021 by the authors. Licensee MDPI, Basel, Switzerland.

Keywords

Companion animals
Feline drug metabolism
Pharmacokinetics
Soluble epoxide hydrolase

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McReynolds, C. B., Yang, J., Guedes, A., Morisseau, C., Garcia, R., Knych, H., Tearney, C., Hamamoto, B., Hwang, S. H., Wagner, K., & Hammock, B. D. (2021). Species differences in metabolism of soluble epoxide hydrolase inhibitor, EC1728, highlight the importance of clinically relevant screening mechanisms in drug development. Molecules, 26(16), Article 5034. https://doi.org/10.3390/molecules26165034

McReynolds, CB, Yang, J, Guedes, A, Morisseau, C, Garcia, R, Knych, H, Tearney, C, Hamamoto, B, Hwang, SH, Wagner, K & Hammock, BD 2021, 'Species differences in metabolism of soluble epoxide hydrolase inhibitor, EC1728, highlight the importance of clinically relevant screening mechanisms in drug development', Molecules, vol. 26, no. 16, 5034. https://doi.org/10.3390/molecules26165034

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title = "Species differences in metabolism of soluble epoxide hydrolase inhibitor, EC1728, highlight the importance of clinically relevant screening mechanisms in drug development",

abstract = "There are few novel therapeutic options available for companion animals, and medications rely heavily on repurposed drugs developed for other species. Considering the diversity of species and breeds in companion animal medicine, comprehensive PK exposures in the companion animal patient is often lacking. The purpose of this paper was to assess the pharmacokinetics after oral and intravenous dosing in domesticated animal species (dogs, cats, and horses) of a novel soluble epoxide hydrolase inhibitor, EC1728, being developed for the treatment of pain in animals. Results: Intravenous and oral administration revealed that bioavailability was similar for dogs, and horses (42 and 50% F) but lower in mice and cats (34 and 8%, respectively). Additionally, clearance was similar between cats and mice, but >2× faster in cats vs. dogs and horses. Efficacy with EC1728 has been demonstrated in mice, dogs, and horses, and despite the rapid clearance of EC1728 in cats, analgesic efficacy was demonstrated in an acute pain model after intravenous but not oral dosing. Conclusion: These results demonstrate that exposures across species can vary, and investigation of therapeutic exposures in target species is needed to provide adequate care that addresses efficacy and avoids toxicity.",

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author = "McReynolds, {Cindy B.} and Jun Yang and Alonso Guedes and Christophe Morisseau and Roberto Garcia and Heather Knych and Caitlin Tearney and Briana Hamamoto and Hwang, {Sung Hee} and Karen Wagner and Hammock, {Bruce D.}",

note = "Funding Information: This work was supported in part by grants from NIEHS/Superfund Research Program P42 (ES004699), NIH/NIEHS R35 (ES030443), NIH/NIGMS T32GM113770 (to CBM). UC Davis Center for Companion Animal Health for the dog studies, and Every Cat Health Foundation (previously Winn Feline Foundation) for the 1 mg/kg IV cat studies. Funding Information: Funding: This work was supported in part by grants from NIEHS/Superfund Research Program P42 (ES004699), NIH/NIEHS R35 (ES030443), NIH/NIGMS T32GM113770 (to CBM). UC Davis Center for Companion Animal Health for the dog studies, and Every Cat Health Foundation (previously Winn Feline Foundation) for the 1 mg/kg IV cat studies. Publisher Copyright: {\textcopyright} 2021 by the authors. Licensee MDPI, Basel, Switzerland.",

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AU - McReynolds, Cindy B.

AU - Yang, Jun

AU - Guedes, Alonso

AU - Morisseau, Christophe

AU - Garcia, Roberto

AU - Knych, Heather

AU - Tearney, Caitlin

AU - Hamamoto, Briana

AU - Hwang, Sung Hee

AU - Wagner, Karen

AU - Hammock, Bruce D.

N1 - Funding Information: This work was supported in part by grants from NIEHS/Superfund Research Program P42 (ES004699), NIH/NIEHS R35 (ES030443), NIH/NIGMS T32GM113770 (to CBM). UC Davis Center for Companion Animal Health for the dog studies, and Every Cat Health Foundation (previously Winn Feline Foundation) for the 1 mg/kg IV cat studies. Funding Information: Funding: This work was supported in part by grants from NIEHS/Superfund Research Program P42 (ES004699), NIH/NIEHS R35 (ES030443), NIH/NIGMS T32GM113770 (to CBM). UC Davis Center for Companion Animal Health for the dog studies, and Every Cat Health Foundation (previously Winn Feline Foundation) for the 1 mg/kg IV cat studies. Publisher Copyright: © 2021 by the authors. Licensee MDPI, Basel, Switzerland.

PY - 2021/8/2

Y1 - 2021/8/2

N2 - There are few novel therapeutic options available for companion animals, and medications rely heavily on repurposed drugs developed for other species. Considering the diversity of species and breeds in companion animal medicine, comprehensive PK exposures in the companion animal patient is often lacking. The purpose of this paper was to assess the pharmacokinetics after oral and intravenous dosing in domesticated animal species (dogs, cats, and horses) of a novel soluble epoxide hydrolase inhibitor, EC1728, being developed for the treatment of pain in animals. Results: Intravenous and oral administration revealed that bioavailability was similar for dogs, and horses (42 and 50% F) but lower in mice and cats (34 and 8%, respectively). Additionally, clearance was similar between cats and mice, but >2× faster in cats vs. dogs and horses. Efficacy with EC1728 has been demonstrated in mice, dogs, and horses, and despite the rapid clearance of EC1728 in cats, analgesic efficacy was demonstrated in an acute pain model after intravenous but not oral dosing. Conclusion: These results demonstrate that exposures across species can vary, and investigation of therapeutic exposures in target species is needed to provide adequate care that addresses efficacy and avoids toxicity.

AB - There are few novel therapeutic options available for companion animals, and medications rely heavily on repurposed drugs developed for other species. Considering the diversity of species and breeds in companion animal medicine, comprehensive PK exposures in the companion animal patient is often lacking. The purpose of this paper was to assess the pharmacokinetics after oral and intravenous dosing in domesticated animal species (dogs, cats, and horses) of a novel soluble epoxide hydrolase inhibitor, EC1728, being developed for the treatment of pain in animals. Results: Intravenous and oral administration revealed that bioavailability was similar for dogs, and horses (42 and 50% F) but lower in mice and cats (34 and 8%, respectively). Additionally, clearance was similar between cats and mice, but >2× faster in cats vs. dogs and horses. Efficacy with EC1728 has been demonstrated in mice, dogs, and horses, and despite the rapid clearance of EC1728 in cats, analgesic efficacy was demonstrated in an acute pain model after intravenous but not oral dosing. Conclusion: These results demonstrate that exposures across species can vary, and investigation of therapeutic exposures in target species is needed to provide adequate care that addresses efficacy and avoids toxicity.

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KW - Feline drug metabolism

KW - Pharmacokinetics

KW - Soluble epoxide hydrolase

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Species differences in metabolism of soluble epoxide hydrolase inhibitor, EC1728, highlight the importance of clinically relevant screening mechanisms in drug development

Abstract

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Keywords

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