中华急诊医学杂志
中華急診醫學雜誌
중화급진의학잡지
CHINESE JOURNAL OF EMERGENCY MEDICINE
2013年
8期
855-858
,共4页
孙鹏%李倩%张清%徐丽%韩继媛
孫鵬%李倩%張清%徐麗%韓繼媛
손붕%리천%장청%서려%한계원
S100A8%Toll样受体4%线拴法%脑缺血-再灌注%脑损伤%实时定量PCR技术%免度荧光技术%炎症
S100A8%Toll樣受體4%線拴法%腦缺血-再灌註%腦損傷%實時定量PCR技術%免度熒光技術%炎癥
S100A8%Toll양수체4%선전법%뇌결혈-재관주%뇌손상%실시정량PCR기술%면도형광기술%염증
S100A8%Toll-like receptor 4%Thread embolism method%Cerebral ischemia reperfusion%Brain injury%Real time PCR%Immunofluorescence technique%Inflammation
目的 探讨脑缺血-再灌注(I/R)损伤后S100A8的表达变化及其与Toll样受体4(TLR4)的关系.方法 TLR4基因突变型小鼠C3H/HeJ(n=30)随机(随机数字法)分为模型组(n=18)和健康组(n=12),TLR4野生型小鼠C3H/HeN (n =30)随机分为模型组(n=18)和健康健康组组(n=12),采用线栓法制造局灶性脑缺血-再灌注损伤模型,再灌注12 h后进行神经功能缺损评分,通过TTC染色和HE染色评价各组脑组织损伤程度,实时定量PCR技术和免疫荧光成像检测各组S100A8 mRNA和蛋白的表达.结果 与C3H/HeN模型组比较,脑缺血-再灌注损伤12h后,C3H/HeJ模型组神经缺损评分明显减小(P<0.01),脑梗死体积和神经细胞损伤程度也明显减轻(P<0.01).与健康组比较,C3 H/HeJ和C3H/HeN模型组梗死侧脑组织中S100A8mRNA和蛋白表达显著上调,且C3H/HeN模型组脑组织中S100A8表达量较C3H/HeJ模型组增加更为明显(P<0.01),提示S100A8表达与TLR4关系密切.结论 S100A8很有可能通过与TLR4相互作用在脑I/R炎症损伤早期过程中发挥重要作用.
目的 探討腦缺血-再灌註(I/R)損傷後S100A8的錶達變化及其與Toll樣受體4(TLR4)的關繫.方法 TLR4基因突變型小鼠C3H/HeJ(n=30)隨機(隨機數字法)分為模型組(n=18)和健康組(n=12),TLR4野生型小鼠C3H/HeN (n =30)隨機分為模型組(n=18)和健康健康組組(n=12),採用線栓法製造跼竈性腦缺血-再灌註損傷模型,再灌註12 h後進行神經功能缺損評分,通過TTC染色和HE染色評價各組腦組織損傷程度,實時定量PCR技術和免疫熒光成像檢測各組S100A8 mRNA和蛋白的錶達.結果 與C3H/HeN模型組比較,腦缺血-再灌註損傷12h後,C3H/HeJ模型組神經缺損評分明顯減小(P<0.01),腦梗死體積和神經細胞損傷程度也明顯減輕(P<0.01).與健康組比較,C3 H/HeJ和C3H/HeN模型組梗死側腦組織中S100A8mRNA和蛋白錶達顯著上調,且C3H/HeN模型組腦組織中S100A8錶達量較C3H/HeJ模型組增加更為明顯(P<0.01),提示S100A8錶達與TLR4關繫密切.結論 S100A8很有可能通過與TLR4相互作用在腦I/R炎癥損傷早期過程中髮揮重要作用.
목적 탐토뇌결혈-재관주(I/R)손상후S100A8적표체변화급기여Toll양수체4(TLR4)적관계.방법 TLR4기인돌변형소서C3H/HeJ(n=30)수궤(수궤수자법)분위모형조(n=18)화건강조(n=12),TLR4야생형소서C3H/HeN (n =30)수궤분위모형조(n=18)화건강건강조조(n=12),채용선전법제조국조성뇌결혈-재관주손상모형,재관주12 h후진행신경공능결손평분,통과TTC염색화HE염색평개각조뇌조직손상정도,실시정량PCR기술화면역형광성상검측각조S100A8 mRNA화단백적표체.결과 여C3H/HeN모형조비교,뇌결혈-재관주손상12h후,C3H/HeJ모형조신경결손평분명현감소(P<0.01),뇌경사체적화신경세포손상정도야명현감경(P<0.01).여건강조비교,C3 H/HeJ화C3H/HeN모형조경사측뇌조직중S100A8mRNA화단백표체현저상조,차C3H/HeN모형조뇌조직중S100A8표체량교C3H/HeJ모형조증가경위명현(P<0.01),제시S100A8표체여TLR4관계밀절.결론 S100A8흔유가능통과여TLR4상호작용재뇌I/R염증손상조기과정중발휘중요작용.
Objective To study the expression of S100A8 and the relationship between S100A8 and Toll-like receptor 4 (TLR4) in focal cerebral ischemia reperfusion (I/R) injury.Methods C3H/HeJ mice with TLR4 gene mutation (n =30) and C3H/HeN with normal TLR4 gene mice (n =30) were divided into 4 groups at random (random number),namely C3H/HeJ model group (n =18),C3H/HeJ control group (n =12),and C3H/HeN model group (n =18).C3H/HeN control group (n =12).Middle cerebral artery was occluded to make I/R model in mice by using thread embolism method.Brain tissues were collected after ischemia for one hour and reperfusion for 12 hours.Stroke outcome was evaluated by determination of infarct volume of brain tissue and assessment of neurological scores.And brain injury after cerebral I/R was observed by optical microscope after TTC and HE staining.The immunofluorescence technique and RT-PCR were used to determine the protein level and expression of S100A8 mRNA in damaged brain tissues.Results Compared with C3H/HeN model mice,TLR4-deficient model mice (C3H/ He J) had lower infarct volumes and better outcomes of neurological function after resuscitation for 12 hours.Compared with control groups,the expression of S100A8 mRNA and level of S100A8 protein increased greatly in damaged brain tissues of model mice after I/R injury.In addition,model mice with lacked TLR4 (C3H/HeJ) had lower expression of I/R-induced S100A8 mRNA than C3H/HeN mice in model group,indicating that the close relationship between the levels of S100A8 and TLR4.Conclusions S100A8 interaction with TLR4 might be involved in brain damage and in inflammation triggered by I/R injury.
