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Cited 3 time in webofscience Cited 3 time in scopus
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NO-dependent attenuation of TPA-induced immunoinflammatory skin changes in Balb/c mice by pindolol, heptaminol or ATRA, but not by verapamil SCIE SCOPUS

Title
NO-dependent attenuation of TPA-induced immunoinflammatory skin changes in Balb/c mice by pindolol, heptaminol or ATRA, but not by verapamil
Authors
Chung, JFYoon, CJCheon, SASeo, ESSUNG, HO PARKYang, JSKIM, BUMJUJoo, MYPark, TJKim, KHSood, AKLEE, SANG JOON
Date Issued
2016-07-26
Publisher
Impact Journals
Abstract
Recently a mouse skin carcinogenesis study reported that a beta-blocker carvedilol displayed antitumor-properties via antihyperplastic effects. However, the antihyperplastic mechanism is unclear as the beta-blocker is characterized with multiple pleiotropic effects including stimulation of endothelial NO release and verapamil-like calcium channel blocking activity. To investigate the nature and the origin of the antihyperplastic effects, we tested topical pretreatment with pindolol, heptaminol, ATRA or verapamil against Balb/c mouse ear skin hyperplasia that was induced by TPA. We found that pindolol, heptaminol or ATRA, but not verapamil, inhibited the TPA-induced immunoinflammatory skin changes in an NO-dependent manner, which included epidermal hyperplasia, skin edema and fibrosis. Furthermore, we also observed NO-dependent alleviation of the TPA-induced NK cell depletion in the ear tissues by heptaminol pretreatment. Together our results suggest that stimulation of NO generation from constitutive synthases may be primarily responsible for the reported antihyperplastic and NK cell-preserving effects of the beta-blockers, and that similar effects may be observed in other immunity normalizing compounds that also promote endothelial NO synthesis.
URI
https://oasis.postech.ac.kr/handle/2014.oak/36534
DOI
10.18632/ONCOTARGET.10217
ISSN
1949-2553
Article Type
Article
Citation
Oncotarget, vol. 7, no. 30, page. 47576 - 47585, 2016-07-26
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김기현KIM, KI HEAN
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