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Relaxation effect of synthetic ceramide analogues in cat esophageal smooth muscle cells

Authors
Lee, Doo WonPark, Sun YoungRyu, Jung SuKim, Sung HyoIm, Chae UkChoi, Su HangLee, Se EunKo, Sung KwonSohn, Uy Dong
Issue Date
Aug-2008
Publisher
KOREAN JOURNAL OF PHYSIOLOGY & PHARMACOLOGY
Keywords
mitogen-activated protein kinase; smooth muscle; protein kinase C; C-2-ceramide
Citation
KOREAN JOURNAL OF PHYSIOLOGY & PHARMACOLOGY, v.12, no.4, pp 137 - 142
Pages
6
Journal Title
KOREAN JOURNAL OF PHYSIOLOGY & PHARMACOLOGY
Volume
12
Number
4
Start Page
137
End Page
142
URI
https://scholarworks.bwise.kr/cau/handle/2019.sw.cau/23661
DOI
10.4196/kjpp.2008.12.4.137
ISSN
1226-4512
2093-3827
Abstract
Ceramide has emerged as a novel second messenger for intracellular signalling. It is produced from sphingomyelin and is involved in the control of cell differntiation, proliferation, and apoptosis. C-2-ceramide, short chain ceramide, plays a role in mediating contraction of cat esophageal smooth muscle cells. We examined the effect of synthesized ceramide analogues on the C-2-ceramide and ACh-induced contraction in esophageal smooth muscle cells isolated with collagenase. CY3523, CY3525, or CY3723 inhibited C-2-ceramide induced contraction, in a time dependent manne. Each analogue also inhibited the contraction in concentration dependent manners. CY 3523, CY 3525, and CY 3723 had no effect to the contraction induced by PMA. The inhibition with CY3523, CY3525 and CY3723 on the C-2-ceramide induced contraction was recovered by PMA. These analogues decreased the density of MAPK bands (p44/42 or p38) in the western blot. These results suggest that ceramide analogues can inhibit C-2-ceramide induced contraction via PKC and MAPK dependent pathway.
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약학대학 (약학부)
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