国际医药卫生导报
國際醫藥衛生導報
국제의약위생도보
INTERNATIONAL MEDICINE & HEALTH GUIDANCE NEWS
2014年
11期
1536-1539
,共4页
失血性休克%乌司他丁%线粒体
失血性休剋%烏司他丁%線粒體
실혈성휴극%오사타정%선립체
Hemorrhagic shock%Ulinastatin%Mitochondria
目的 探讨乌司他丁对失血性休克诱导的神经元线粒体功能障碍的影响.方法 18只大鼠随机分为对照组、休克+生理盐水组和休克+乌司他丁组,在失血性休克造模后相应予以生理盐水或乌司他丁治疗.透射电镜检测神经元线粒体超微结构;JC-1探针流式细胞仪探测线粒体膜电位(△ψm)变化;荧光素-荧光素酶试剂盒测定ATP含量;过氧化脂质(lipid hydroperoxide,LPO)试剂盒检测血清LPO含量.结果 与对照组比较,生理盐水组神经元线粒体肿胀、嵴结构模糊消失,低线粒体膜电位神经元比例增加(P<0.05),神经元ATP含量降低(P<0.05),血清LPO水平显著增加(P<0.05);而在乌司他丁处理组中以上改变均得到明显改善(P<0.05).结论 乌司他丁通过抑制氧化应激而减少失血性休克诱导的神经元线粒体损伤,改善线粒体功能.
目的 探討烏司他丁對失血性休剋誘導的神經元線粒體功能障礙的影響.方法 18隻大鼠隨機分為對照組、休剋+生理鹽水組和休剋+烏司他丁組,在失血性休剋造模後相應予以生理鹽水或烏司他丁治療.透射電鏡檢測神經元線粒體超微結構;JC-1探針流式細胞儀探測線粒體膜電位(△ψm)變化;熒光素-熒光素酶試劑盒測定ATP含量;過氧化脂質(lipid hydroperoxide,LPO)試劑盒檢測血清LPO含量.結果 與對照組比較,生理鹽水組神經元線粒體腫脹、嵴結構模糊消失,低線粒體膜電位神經元比例增加(P<0.05),神經元ATP含量降低(P<0.05),血清LPO水平顯著增加(P<0.05);而在烏司他丁處理組中以上改變均得到明顯改善(P<0.05).結論 烏司他丁通過抑製氧化應激而減少失血性休剋誘導的神經元線粒體損傷,改善線粒體功能.
목적 탐토오사타정대실혈성휴극유도적신경원선립체공능장애적영향.방법 18지대서수궤분위대조조、휴극+생리염수조화휴극+오사타정조,재실혈성휴극조모후상응여이생리염수혹오사타정치료.투사전경검측신경원선립체초미결구;JC-1탐침류식세포의탐측선립체막전위(△ψm)변화;형광소-형광소매시제합측정ATP함량;과양화지질(lipid hydroperoxide,LPO)시제합검측혈청LPO함량.결과 여대조조비교,생리염수조신경원선립체종창、척결구모호소실,저선립체막전위신경원비례증가(P<0.05),신경원ATP함량강저(P<0.05),혈청LPO수평현저증가(P<0.05);이재오사타정처리조중이상개변균득도명현개선(P<0.05).결론 오사타정통과억제양화응격이감소실혈성휴극유도적신경원선립체손상,개선선립체공능.
Objective To investigate protective effect of Ulinastatin on hemorrhagic shock-induced neuron mitochondrial dysfunction.Methods 18 rats were randomly divided into control group,shock+normal saline (NS) group and shock+Ulinastatin group.Rats were received homologous NS or Ulinastatin treatment after hemorrhagic shock induction.Ultrastructure of neuron mitochondria was detected by electron microscope; change of mitochondrial membrane potential (△ ψm) by JC-1 mitochondrial membrane potential kit; content of ATP by fluorescein-luciferase assay kit; lipid hydroperoxide (LPO) in serum by LPO assay kit.Results Compared with control group,mitochondrial swelling with poorly defined cristas,remarkably increased number of platelets with low mitochondrial membrane potential (△ ψm) (P < 0.05),decreased ATP content (P < 0.05),and increased serum LPO level (P < 0.05) were detected in NS group.These alterations mentioned were marked improved by Ulinastatin treatment (P < 0.05).Conclusion Ulinastatin treatment can improve hemorrhagic shock-induced neuron mitochondrial injury and dysfunction via depression oxidative stress.