| Literature DB >> 27099175 |
Lishuang Cao1, Aoibhinn McDonnell1, Anja Nitzsche1, Aristos Alexandrou1, Pierre-Philippe Saintot1, Alexandre J C Loucif1, Adam R Brown1, Gareth Young1, Malgorzata Mis2, Andrew Randall3, Stephen G Waxman4, Philip Stanley1, Simon Kirby1, Sanela Tarabar5, Alex Gutteridge1, Richard Butt1, Ruth M McKernan1, Paul Whiting1, Zahid Ali1, James Bilsland6, Edward B Stevens6.
Abstract
In common with other chronic pain conditions, there is an unmet clinical need in the treatment of inherited erythromelalgia (IEM). TheSCN9Agene encoding the sodium channel Nav1.7 expressed in the peripheral nervous system plays a critical role in IEM. A gain-of-function mutation in this sodium channel leads to aberrant sensory neuronal activity and extreme pain, particularly in response to heat. Five patients with IEM were treated with a new potent and selective compound that blocked the Nav1.7 sodium channel resulting in a decrease in heat-induced pain in most of the patients. We derived induced pluripotent stem cell (iPSC) lines from four of five subjects and produced sensory neurons that emulated the clinical phenotype of hyperexcitability and aberrant responses to heat stimuli. When we compared the severity of the clinical phenotype with the hyperexcitability of the iPSC-derived sensory neurons, we saw a trend toward a correlation for individual mutations. The in vitro IEM phenotype was sensitive to Nav1.7 blockers, including the clinical test agent. Given the importance of peripherally expressed sodium channels in many pain conditions, our approach may have broader utility for a wide range of pain and sensory conditions.Entities:
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Year: 2016 PMID: 27099175 DOI: 10.1126/scitranslmed.aad7653
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956