Optimized Inhibitors of Soluble Epoxide Hydrolase Improve in Vitro Target Residence Time and in Vivo Efficacy | Zendy

Kin Sing Stephen Lee | Zendy; JunYan Liu | Zendy; Karen Wagner | Zendy; Svetlana Pakhomova | Zendy; Hua Dong | Zendy; Christophe Morisseau | Zendy; Samuel H. Fu | Zendy; Jun Yang | Zendy; Peng Wang | Zendy; Arzu Ulu | Zendy; Christina A. Mate | Zendy; Long Nguyen | Zendy; Sung Hee Hwang | Zendy; Matthew L. Edin | Zendy; Alexandria A. Mara | Zendy; Heike Wulff | Zendy; Marcia E. Newcomer | Zendy; Darryl C. Zeldin | Zendy; Bruce D. Hammock | Zendy

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Optimized Inhibitors of Soluble Epoxide Hydrolase Improve in Vitro Target Residence Time and in Vivo Efficacy

Author(s) -

Kin Sing Stephen Lee,

JunYan Liu,

Karen Wagner,

Svetlana Pakhomova,

Hua Dong,

Christophe Morisseau,

Samuel H. Fu,

Jun Yang,

Peng Wang,

Arzu Ulu,

Christina A. Mate,

Long Nguyen,

Sung Hee Hwang,

Matthew L. Edin,

Alexandria A. Mara,

Heike Wulff,

Marcia E. Newcomer,

Darryl C. Zeldin,

Bruce D. Hammock

Publication year - 2014

Publication title -

journal of medicinal chemistry

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.01

H-Index - 261

eISSN - 1520-4804

pISSN - 0022-2623

DOI - 10.1021/jm500694p

Subject(s) - epoxide hydrolase 2 , neuropathic pain , chemistry , pharmacology , in vivo , pharmacokinetics , potency , diabetes mellitus , gabapentin , diabetic neuropathy , in vitro , enzyme , medicine , biochemistry , endocrinology , alternative medicine , microbiology and biotechnology , pathology , biology

Diabetes is affecting the life of millions of people. A large proportion of diabetic patients suffer from severe complications such as neuropathic pain, and current treatments for these complications have deleterious side effects. Thus, alternate therapeutic strategies are needed. Recently, the elevation of epoxy-fatty acids through inhibition of soluble epoxide hydrolase (sEH) was shown to reduce diabetic neuropathic pain in rodents. In this report, we describe a series of newly synthesized sEH inhibitors with at least 5-fold higher potency and doubled residence time inside both the human and rodent sEH enzyme than previously reported inhibitors. These inhibitors also have better physical properties and optimized pharmacokinetic profiles. The optimized inhibitor selected from this new series displayed improved efficacy of almost 10-fold in relieving pain perception in diabetic neuropathic rats as compared to the approved drug, gabapentin, and previously published sEH inhibitors. Therefore, these new sEH inhibitors could be an attractive alternative to treat diabetic neuropathy in humans.

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