Silencing of TRPV4-expressing sensory neurons attenuates temporomandibular disorders pain.
Abstract
Identification of potential therapeutic targets is needed for temporomandibular disorders
(TMD) pain, the most common form of orofacial pain, because current treatments lack
efficacy. Considering TMD pain is critically mediated by the trigeminal ganglion (TG)
sensory neurons, functional blockade of nociceptive neurons in the TG may provide
an effective approach for mitigating pain associated with TMD. We have previously
shown that TRPV4, a polymodally-activated ion channel, is expressed in TG nociceptive
neurons. Yet, it remains unexplored whether functional silencing of TRPV4-expressing
TG neurons attenuates TMD pain. In this study, we demonstrated that co-application
of a positively charged, membrane-impermeable lidocaine derivative QX-314 with the
TRPV4 selective agonist GSK101 suppressed the excitability of TG neurons. Moreover,
co-administration of QX-314 and GSK101 into the TG significantly attenuated pain in
mouse models of temporomandibular joint (TMJ) inflammation and masseter muscle injury.
Collectively, these results suggest TRPV4-expressing TG neurons represent a potential
target for TMD pain.
Type
Journal articleSubject
Temporomandibular JointTrigeminal Ganglion
Animals
Mice
Temporomandibular Joint Disorders
Facial Pain
TRPV Cation Channels
Sensory Receptor Cells
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https://hdl.handle.net/10161/28696Published Version (Please cite this version)
10.1177/17448069231185696Publication Info
Dias, Fabiana C; Wang, Zilong; Scapellato, Garrett; & Chen, Yong (2023). Silencing of TRPV4-expressing sensory neurons attenuates temporomandibular disorders
pain. Molecular pain, 19. pp. 17448069231185696. 10.1177/17448069231185696. Retrieved from https://hdl.handle.net/10161/28696.This is constructed from limited available data and may be imprecise. To cite this
article, please review & use the official citation provided by the journal.
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Show full item recordScholars@Duke
Yong Chen
Associate Professor in Neurology
Dr. Yong Chen is an Associate Professor of Neurology at the Duke University School
of Medicine. He is also affiliated with Duke Anesthesiology-Center for Translational
Pain Medicine (CTPM) and Duke-Pathology.
The Chen lab mainly studies sensory neurobiology of pain and itch, with a focus on
TRP ion channels and neural circuits. The main objective of our lab is to identify
molecular and cellular mechanisms underlying chronic pain and chronic-disease associated
itch, using a combi

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