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Melatonin reduces ultraviolet-B induced cell damages and polyamine levels in human skin fibroblasts in culture

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Affiliated Author(s)
이규석류영욱김병천서성일김상표이성용
Alternative Author(s)
Lee, Kyu SukRyoo, Young WookKim, Byung ChunSuh, Seong IlKim, Sang PyoLee, Seong Ryong
Journal Title
Experimental and Molecular Medicine.
ISSN
1226-3613
Issued Date
2003
Abstract
UV radiation is known to cause photoaging of the
skin and is considered one of the leading cause
of developing skin carcinogenesis. Melatonin which
has a highly lipophilic molecular structure facilitating
penetration of cell membranes and serving as
an extra- and intracellular free radical scavenger
has been demonstrated to protect photodamage of
skin affected by UV exposure. In this study, we
have examined the role of melatonin in response
to UVB induced photodamaging process, using
human skin fibroblasts in vitro. Cell survival curves
after UVB irradiation showed dose-dependent
decrease. Only 60% of fibroblasts were survived
at 140 mJ/cm2 UVB irradiation. By pre-cultivation
of cells with melatonin (100 nM), a significant
number of cells remained unaffected. After UVB
irradiation with 70 mJ/cm2, the level of putrescine
was 1.7±0.3 fold increased compared to melatonin
pre-treated group. In Northern analyses, the
transcriptional level of ornithine decarboxylase
(ODC) gene expression was increased by UVB irradiation
and prohibited by melatonin. These results
indicated that melatonin was effectively able
to neutralize membrane peroxidation when present
in relevant concentration during UVB irradiation
and diminishes the UVB-induced increase of polyamine
synthesis and ODC gene expression. Collectively,
ODC response to UVB induced changes
are possibly involves a melatonin or antioxidant
sensitive regulatory pathway in normal human
skin fibroblast.
Keywords: antioxidants; cell death; melatonin; ornithine
decarboxylase; polyamine; ultraviolet rays
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