中国医科大学学报
中國醫科大學學報
중국의과대학학보
JOURNAL OF CHINA MEDICAL UNIVERSITY
2010年
3期
191-193,204
,共4页
牛平%陈鑫%王聪杰%刘宝茹%辛志强
牛平%陳鑫%王聰傑%劉寶茹%辛誌彊
우평%진흠%왕총걸%류보여%신지강
塞来昔布%多巴胺能神经元%脂多糖%神经炎症
塞來昔佈%多巴胺能神經元%脂多糖%神經炎癥
새래석포%다파알능신경원%지다당%신경염증
celecoxib%dopaminergic neuron%lipopolysaccharide%neuroinflammation
目的 观察塞来昔布(CB)对脂多糖(LPS)所致大鼠黑质多巴胺能(DA)神经元损伤的保护作用.方法 黑质内注射LPS制作帕金森病(PD)大鼠模型.应用CB对实验动物进行处理.采用行为学、酪氨酸羟化酶(TH)、环氧化酶-2(COX-2)等免疫组化及免疫印迹技术观察CB的神经保护作用.结果 对照组大鼠无行为变化,PD组大鼠平均旋转圈数为196.90±9.52,CB组为109.30±9.38,差异非常显著(P<0.01).TH免疫组化表明,对照组TH阳性神经元数量较多,胞体较大,突起明显;PD组神经元数量明显减少或消失(P<0.01),神经元胞体萎缩,突起不清晰;CB组TH阳性神经元数与PD组相比明显增加(P<0.01),神经元形态变化亦不明显.COX-2免疫组化表明,对照纽黑质偶见COX-2阳性细胞,PD组见大量COX-2阳性细胞;CB组COX-2阳性细胞数与PD组相比明显减少(P<0.01).小胶质细胞特异性抗体(OX-42)免疫组化表明,对照组小胶质细胞多呈静止的"分枝样"状态;PD组多为激活状态,呈典型的"阿米巴样";CB组激活状态的小胶质细胞与PD组相比明显减少,形态为高度分枝状态.Western blotting分析结果相同.结论 CB可防护LPS所致黑质DA能神经元损伤,具有神经保护作用.
目的 觀察塞來昔佈(CB)對脂多糖(LPS)所緻大鼠黑質多巴胺能(DA)神經元損傷的保護作用.方法 黑質內註射LPS製作帕金森病(PD)大鼠模型.應用CB對實驗動物進行處理.採用行為學、酪氨痠羥化酶(TH)、環氧化酶-2(COX-2)等免疫組化及免疫印跡技術觀察CB的神經保護作用.結果 對照組大鼠無行為變化,PD組大鼠平均鏇轉圈數為196.90±9.52,CB組為109.30±9.38,差異非常顯著(P<0.01).TH免疫組化錶明,對照組TH暘性神經元數量較多,胞體較大,突起明顯;PD組神經元數量明顯減少或消失(P<0.01),神經元胞體萎縮,突起不清晰;CB組TH暘性神經元數與PD組相比明顯增加(P<0.01),神經元形態變化亦不明顯.COX-2免疫組化錶明,對照紐黑質偶見COX-2暘性細胞,PD組見大量COX-2暘性細胞;CB組COX-2暘性細胞數與PD組相比明顯減少(P<0.01).小膠質細胞特異性抗體(OX-42)免疫組化錶明,對照組小膠質細胞多呈靜止的"分枝樣"狀態;PD組多為激活狀態,呈典型的"阿米巴樣";CB組激活狀態的小膠質細胞與PD組相比明顯減少,形態為高度分枝狀態.Western blotting分析結果相同.結論 CB可防護LPS所緻黑質DA能神經元損傷,具有神經保護作用.
목적 관찰새래석포(CB)대지다당(LPS)소치대서흑질다파알능(DA)신경원손상적보호작용.방법 흑질내주사LPS제작파금삼병(PD)대서모형.응용CB대실험동물진행처리.채용행위학、락안산간화매(TH)、배양화매-2(COX-2)등면역조화급면역인적기술관찰CB적신경보호작용.결과 대조조대서무행위변화,PD조대서평균선전권수위196.90±9.52,CB조위109.30±9.38,차이비상현저(P<0.01).TH면역조화표명,대조조TH양성신경원수량교다,포체교대,돌기명현;PD조신경원수량명현감소혹소실(P<0.01),신경원포체위축,돌기불청석;CB조TH양성신경원수여PD조상비명현증가(P<0.01),신경원형태변화역불명현.COX-2면역조화표명,대조뉴흑질우견COX-2양성세포,PD조견대량COX-2양성세포;CB조COX-2양성세포수여PD조상비명현감소(P<0.01).소효질세포특이성항체(OX-42)면역조화표명,대조조소효질세포다정정지적"분지양"상태;PD조다위격활상태,정전형적"아미파양";CB조격활상태적소효질세포여PD조상비명현감소,형태위고도분지상태.Western blotting분석결과상동.결론 CB가방호LPS소치흑질DA능신경원손상,구유신경보호작용.
Objective To observe the neuroprotective effect of celecoxib against degeneration of dopaminergic neurons caused by lipopolysaccharide in vivo.Methods The rat model of Parkinson disease(PD)was established by intranigral injection of lipopolysaccharide.Sprague-Dawley rats were randomly divided into control group,PD group,and celecoxib group.Behavioural changes were recorded,and the expressions of tyrosine hydroxylase(TH)and cyclooxygenase-2(COX-2)were determined by immunohistochmistry and Western blot.Results No behavioral change was found in control group.There was significant difference in the number of circling behavior between PD and celecoxib groups(196.90±9.52 vs 109.30±9.38,P<0.01).The number of TH-positive cells and the expression of TH protein in rat substantia nigra were significantly higher in celecoxib group than in PD group(P<0.01).Compared with PD group,the number of COX-2positive cells and the expression of COX-2 protein were significant lower in celecoxib group(P<0.01).Conclusion Celecoxib has neuroprotective effect on the degeneration of dopaminergic neurons caused by lipopolysaccharide in vivo.