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Doxycycline inhibits matrix metalloproteinase-9 and laminin degradation after transient global cerebral ischemia

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Affiliated Author(s)
이형김상표이성용박종욱
Alternative Author(s)
Lee, HyungKim, Sang PyoLee, Seong RyongPark, Jong Wook
Journal Title
Neurobiology of Disease
ISSN
0969-9961
Issued Date
2009
Keyword
DoxycyclineMatrix metalloproteinaseNeuroprotectionGlobal ischemia
Abstract
Doxycycline, a tetracycline antibiotic inhibits matrix metalloproteinase (MMP) and reduces neuronal damage
in focal brain ischemia. This study was undertaken to assess if doxycycline reduces delayed neuronal damage
following transient global cerebral ischemia through MMP inhibition. C57BL/6 mice were subjected to
20 min global cerebral ischemia. Doxycycline was administered to mice 30 min before and 2 h after ischemia.
In TUNEL assay, damaged neurons were also apparent in the CA1 and CA2 areas and doxycycline reduced
TUNEL-positive neurons. Gelatin gel and in situ zymography showed upregulation of gelatinase activity after
ischemia. Doxycycline significantly inhibited MMP-9 activity in gel zymography and also suppressed in situ
gelatinase activity. Laminin degradation was remarkable in CA1 and CA2 areas after ischemia and
doxycycline reduced the laminin degradation and neuronal loss. Our data suggest that doxycycline may
provide a neuroprotection against global cerebral ischemia since it reduces perineuronal laminin degradation
by inhibiting MMP-9 activity.
Keywords:
Doxycycline
Matrix metalloproteinase
Neuroprotection
Global ischemia
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