Mongolian gerbil에서 유발시킨 전뇌허혈에 의한 해마 polyamine 함량변동 및 신경세포손상에 대한 melatonin의 영향
- Author(s)
- 이성룡; 전재규
- Keimyung Author(s)
- Lee, Seong Ryong; Cheun, Jae Kyu
- Department
- Dept. of Pharmacology (약리학)
Dept. of Anesthesiology & Pain Medicine (마취통증의학)
- Journal Title
- 대한마취과학화지
- Issued Date
- 2001
- Volume
- 40
- Issue
- 5
- Abstract
- Background: We designed this study to examine whether melatonin has a neuroprotective effect
against hippocampal neuronal damage following transient global ischemia in a gerbil. Because polyamine
is known to participate in the process of ischemic neuronal damage, we examined the influence of
melatonin on the polyamine level as well as histology. In particular, we examined the difference between
pre- and post-ischemic treatments of melatonin by using the above mentioned parameters.
Methods: Male Mongolian gerbils (60-80 g) were used in this study. Transient global ischemia
was induced by occlusion of the bilateral common carotid arteries for 3 min with microclips. Melatonin
was administered 1 h before or 1 h after occlusion. The animals were dissected 4 days after the occlusion
for polyamine measurement by a high performance liquid chromatography (HPLC) and histological
evaluation (hematoxylin and eosin staining). A histological examination was performed by a blinded
investigator.
Results: The hippocampal putrescine (PU) level increased compared to sham-operated animals and
the increase of PU was attenuated by melatonin administration (pre- or post-ischemic treatment). Spermidine
(SD) and spermine (SM) levels didn't show significant changes after ischemia. Hippocampal neuronal
damage in the CA1 region was markedly observed in vehicle-treated animals compared to shamoperated
animals. Both pre- and post-ischemic melatonin administration significantly inhibited hippocampal
CA1 neuronal damage compared to corresponding vehicle-treated animals (P < 0.01, respectively).
Conclusions: Melatonin attenuates the polyamine response following transient global ischemia and
may have putative neuroprotective effects against global ischemia-induced neuronal damage. There is
no difference in neuroprotective effects of melatonin between pre- & post-ischemic treatments. (Korean
J Anesthesiol 2001; 40: 664∼670)
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