Selective NaV1.7 Antagonists with Long Residence Time Show Improved Efficacy against Inflammatory and Neuropathic Pain | Zendy

Girish Bankar | Zendy; Samuel J. Goodchild | Zendy; Sarah Howard | Zendy; Karen Nelkenbrecher | Zendy; Matthew Waldbrook | Zendy; Michelle Dourado | Zendy; Noah Gregory Shuart | Zendy; Sophia Lin | Zendy; Clint Young | Zendy; Zhiwei Xie | Zendy; Kuldip Khakh | Zendy; Elaine Chang | Zendy; Luis Sojo | Zendy; Andrea Lindgren | Zendy; Sultan Chowdhury | Zendy; Shan Decker | Zendy; Michael Grimwood | Zendy; JeanChristophe Andrez | Zendy; Christoph M. Dehnhardt | Zendy; Jodie Pang | Zendy; Jae H. Chang | Zendy; Brian S. Safina | Zendy; Daniel P. Sutherlin | Zendy; J. P. Johnson | Zendy; David H. Hackos | Zendy; Carole Robinette | Zendy; Charles J. Cohen | Zendy

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Selective NaV1.7 Antagonists with Long Residence Time Show Improved Efficacy against Inflammatory and Neuropathic Pain

Author(s) -

Girish Bankar,

Samuel J. Goodchild,

Sarah Howard,

Karen Nelkenbrecher,

Matthew Waldbrook,

Michelle Dourado,

Noah Gregory Shuart,

Sophia Lin,

Clint Young,

Zhiwei Xie,

Kuldip Khakh,

Elaine Chang,

Luis Sojo,

Andrea Lindgren,

Sultan Chowdhury,

Shan Decker,

Michael Grimwood,

JeanChristophe Andrez,

Christoph M. Dehnhardt,

Jodie Pang,

Jae H. Chang,

Brian S. Safina,

Daniel P. Sutherlin,

J. P. Johnson,

David H. Hackos,

Carole Robinette,

Charles J. Cohen

Publication year - 2018

Publication title -

cell reports

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 6.264

H-Index - 154

eISSN - 2639-1856

pISSN - 2211-1247

DOI - 10.1016/j.celrep.2018.08.063

Subject(s) - neuropathic pain , analgesic , pharmacology , sodium channel , potency , medicine , chronic pain , chemistry , anesthesia , biochemistry , sodium , in vitro , organic chemistry , psychiatry

Selective block of Na V 1.7 promises to produce non-narcotic analgesic activity without motor or cognitive impairment. Several Na V 1.7-selective blockers have been reported, but efficacy in animal pain models required high multiples of the IC 50 for channel block. Here, we report a target engagement assay using transgenic mice that has enabled the development of a second generation of selective Nav1.7 inhibitors that show robust analgesic activity in inflammatory and neuropathic pain models at low multiples of the IC 50 . Like earlier arylsulfonamides, these newer acylsulfonamides target a binding site on the surface of voltage sensor domain 4 to achieve high selectivity among sodium channel isoforms and steeply state-dependent block. The improved efficacy correlates with very slow dissociation from the target channel. Chronic dosing increases compound potency about 10-fold, possibly due to reversal of sensitization arising during chronic injury, and provides efficacy that persists long after the compound has cleared from plasma.

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