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Endogenous TRPV4 Expression of a Hybrid Neuronal Cell Line N18D3 and Its Utilization to Find a Novel Synthetic Ligand

Authors
Yoo, SungjaeChoi, Seung-InLee, SeulSong, JihoYang, ChungmiBang, SangsuKim, Seung UpMin, Kyung HoonHwang, Sun Wook
Issue Date
12월-2017
Publisher
HUMANA PRESS INC
Keywords
TRPV4; N18D3; Sensory neurons; Novel ligand; MLV-0901
Citation
JOURNAL OF MOLECULAR NEUROSCIENCE, v.63, no.3-4, pp.422 - 430
Indexed
SCIE
SCOPUS
Journal Title
JOURNAL OF MOLECULAR NEUROSCIENCE
Volume
63
Number
3-4
Start Page
422
End Page
430
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/81396
DOI
10.1007/s12031-017-0993-y
ISSN
0895-8696
Abstract
Primary sensory afferent neurons detect environmental and painful stimuli at their peripheral termini. A group of transient receptor potential ion channels (TRPs) are expressed in these neurons and constitute sensor molecules for the stimuli such as thermal, mechanical, and chemical insults. We examined whether a mouse sensory neuronal line, N18D3, shows the sensory TRP expressions and their functionality. In Ca2+ imaging and electrophysiology with these cells, putative TRPV4-mediated responses were observed. TRPV4-specific sensory modalities including sensitivity to a specific agonist, hypotonicity, or an elevated temperature were reproduced in N18D3 cells. Electrophysiological and pharmacological profiles conformed to those from native TRPV4 of primarily cultured neurons. The TRPV4 expression in N18D3 was also confirmed by RT-PCR and Western blot analyses. Thus, N18D3 cells may represent TRPV4-expressing sensory neurons. Further, using this cell lines, we discovered a novel synthetic TRPV4-specific agonist, MLV-0901. These results suggest that N18D3 is a reliable cell line for functional and pharmacological TRPV4 assays. The chemical information from the novel agonist will contribute to TRPV4-targeting drug design.
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