We found a match
Your institution may have rights to this item. Sign in to continue.
- Title
Transient receptor potential A1 mediates acetaldehyde-evoked pain sensation.
- Authors
Bang, Sangsu; Kim, Kyung Yoon; Yoo, Sungjae; Kim, Yoon Gyoon; Hwang, Sun Wook
- Abstract
Six transient receptor potential (TRP) ion channels expressed in the sensory afferents play an important role as body thermosensors and also as peripheral pain detectors. It is known that a number of natural compounds specifically activate those sensory neuronal TRP channels, and a well-known example is cinnamaldehyde for TRPA1. Here we show that human and mouse TRPA1 are activated by acetaldehyde, an intermediate substance of ethanol metabolism, in the HEK293T cell heterologous expression system and in cultured mouse trigeminal neurons. Acetaldehyde failed to activate other temperature-sensitive TRP channels expressed in sensory neurons. TRPA1 antagonists camphor and gadolinium, and a general TRP blocker ruthenium red inhibited TRPA1 activation by acetaldehyde. Camphor, gadolinium and ruthenium red also suppressed the acute nociceptive behaviors induced by the intradermal administration of acetaldehyde into the mouse footpads. Intradermal co-application of prostaglandin E2 and acetaldehyde greatly potentiated the acetaldehyde-induced nociceptive responses, and this effect was reversed by treatment with the TRPA1 antagonist camphor. These results suggest that acetaldehyde causes nociception via TRPA1 activation. Our data may also help elucidate the mechanisms underlying acetaldehyde-related pathological symptoms such as hangover pain.
- Subjects
ACETALDEHYDE; ION channels; MEMBRANE proteins; ALCOHOL; SENSORY neurons
- Publication
European Journal of Neuroscience, 2007, Vol 26, Issue 9, p2516
- ISSN
0953-816X
- Publication type
Article
- DOI
10.1111/j.1460-9568.2007.05882.x