中华老年医学杂志
中華老年醫學雜誌
중화노년의학잡지
Chinese Journal of Geriatrics
2011年
9期
770-773
,共4页
李国前%王杰华%杨小霞%洪诸权
李國前%王傑華%楊小霞%洪諸權
리국전%왕걸화%양소하%홍제권
脑缺血%再灌注%基因表达
腦缺血%再灌註%基因錶達
뇌결혈%재관주%기인표체
Brain ischemia%Reperfusion%Gene expression
目的 观察大鼠脑缺血再灌注损伤后脑组织中Bcl-2和Bax的表达及尤瑞克林的影响。 方法 48只SD大鼠,随机分为假手术组、模型组、生理盐水对照组和尤瑞克林治疗组。线栓法制作大鼠大脑中动脉脑缺血再灌注模型,缺血2h后再灌注,24 h后行神经功能评分,采用免疫组织化学法和反转录聚合酶链反应(RT-PCR)法观察脑组织Bcl-2和Bax表达的变化。 结果 大鼠脑缺血再灌注损伤后,模型组和生理盐水对照组Bcl-2阳性细胞数和mRNA的表达分别为[(14.28±2.54)个/HP、0.551±0.068和(16.54±1.84)个/HP、0.585±0.084],比假手术组[(7.58±0.97)个/HP、0.324±0.042]增多(P<0.05);模型组和生理盐水对照组Bax阳性细胞数和mRNA的表达分别为[(24.38±3.58)个/HP、0.540±0.076和(26.74±4.04)个/HP、0.527±0.065],比假手术组[(8.24±1.95)个/HP、0.309±0.037]增多(P<0.05)。尤瑞克林干预后,Bcl-2阳性细胞数和mRNA的表达显著上调[(25.61±3.41)个/HP、0.791±0.096],Bax阳性细胞数和mRNA的表达下调[(18.54±2.38)个/HP、0.359±0.053],与模型组和生理盐水对照组相比,差异均有统计学意义(P<0.05)。 结论尤瑞克林可上调脑组织中Bcl-2的表达,下调Bax的表达,从而抑制细胞凋亡,这可能是其发挥脑保护作用的机制之一。
目的 觀察大鼠腦缺血再灌註損傷後腦組織中Bcl-2和Bax的錶達及尤瑞剋林的影響。 方法 48隻SD大鼠,隨機分為假手術組、模型組、生理鹽水對照組和尤瑞剋林治療組。線栓法製作大鼠大腦中動脈腦缺血再灌註模型,缺血2h後再灌註,24 h後行神經功能評分,採用免疫組織化學法和反轉錄聚閤酶鏈反應(RT-PCR)法觀察腦組織Bcl-2和Bax錶達的變化。 結果 大鼠腦缺血再灌註損傷後,模型組和生理鹽水對照組Bcl-2暘性細胞數和mRNA的錶達分彆為[(14.28±2.54)箇/HP、0.551±0.068和(16.54±1.84)箇/HP、0.585±0.084],比假手術組[(7.58±0.97)箇/HP、0.324±0.042]增多(P<0.05);模型組和生理鹽水對照組Bax暘性細胞數和mRNA的錶達分彆為[(24.38±3.58)箇/HP、0.540±0.076和(26.74±4.04)箇/HP、0.527±0.065],比假手術組[(8.24±1.95)箇/HP、0.309±0.037]增多(P<0.05)。尤瑞剋林榦預後,Bcl-2暘性細胞數和mRNA的錶達顯著上調[(25.61±3.41)箇/HP、0.791±0.096],Bax暘性細胞數和mRNA的錶達下調[(18.54±2.38)箇/HP、0.359±0.053],與模型組和生理鹽水對照組相比,差異均有統計學意義(P<0.05)。 結論尤瑞剋林可上調腦組織中Bcl-2的錶達,下調Bax的錶達,從而抑製細胞凋亡,這可能是其髮揮腦保護作用的機製之一。
목적 관찰대서뇌결혈재관주손상후뇌조직중Bcl-2화Bax적표체급우서극림적영향。 방법 48지SD대서,수궤분위가수술조、모형조、생리염수대조조화우서극림치료조。선전법제작대서대뇌중동맥뇌결혈재관주모형,결혈2h후재관주,24 h후행신경공능평분,채용면역조직화학법화반전록취합매련반응(RT-PCR)법관찰뇌조직Bcl-2화Bax표체적변화。 결과 대서뇌결혈재관주손상후,모형조화생리염수대조조Bcl-2양성세포수화mRNA적표체분별위[(14.28±2.54)개/HP、0.551±0.068화(16.54±1.84)개/HP、0.585±0.084],비가수술조[(7.58±0.97)개/HP、0.324±0.042]증다(P<0.05);모형조화생리염수대조조Bax양성세포수화mRNA적표체분별위[(24.38±3.58)개/HP、0.540±0.076화(26.74±4.04)개/HP、0.527±0.065],비가수술조[(8.24±1.95)개/HP、0.309±0.037]증다(P<0.05)。우서극림간예후,Bcl-2양성세포수화mRNA적표체현저상조[(25.61±3.41)개/HP、0.791±0.096],Bax양성세포수화mRNA적표체하조[(18.54±2.38)개/HP、0.359±0.053],여모형조화생리염수대조조상비,차이균유통계학의의(P<0.05)。 결론우서극림가상조뇌조직중Bcl-2적표체,하조Bax적표체,종이억제세포조망,저가능시기발휘뇌보호작용적궤제지일。
Objective To investigate the effect of urinary kallidinogenase on the expression of Bcl-2 and Bax in cerebral ischemia-reperfusion injury of rats.Methods Forty eight male adult Sprague-Dawley rats were randomly assigned into four groups: sham operation group, model group,normal saline group and urinary kallidinogenase group. The middle cerebral artery occlusion reperfusion model was made by the suture method. After focal cerebral ischemia-reperfusion, the animals were neurologically assessed on a 5 point scale. The levels of Bcl-2 and Bax expression were measured by immunohistochemical and RT-PCR.Results In model and normal saline group, the expressions of positive Bcl-2 neurocytes and mRNA [(14.28±2.54)/HP, 0.551±0.068 and (16.54± 1.84)/HP, 0.585 ± 0.084] were significantly increased compared with the sham operation group [ (7.58 ± 0.97 )/HP、 0.324 ± 0.042] ( P < 0.05 ) ; The expressions of Bax positive neurocytes and mRNA[( 24.38 ± 3.58 )/HP, 0.540±0.076 and (26.74 ±4.04) /HP, 0.527 ± 0.065] were significantly increased than the sham operation group [ (8.24±1.95 )个/HP, 0.309 ± 0.037] (P <0.05). After treatment with urinary kallidinogenase, the expressions of Bcl-2 positive neurocytes and mRNA [(25.61±3.41)/HP, 0.791 ±0.096] were upregulated ( P<0.05), and the expressions of Bax positive neurocytes and mRNA [( 18.54 ± 2.38)/HP, 0.359±0.053] were down regulated (P<0.05), compared with model group and normal saline group.Conclusions Urinary kallidinogenase is significantly related to the upregulation of Bcl-2 expression and the downregulation of Bax expression, which suggest that urinary kallidinogenase could be related with the inhibitory effects on ischemic neurocyte apoptosis.
