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大鼠肢体缺血/再灌注后肺损伤及一氧化氮合酶的变化与意义
作者姓名:Zhang YB  Zhang LY  Men XL  Dong SY  Yang QH  Yao RL
作者单位:华北煤炭医学院病理生理教研室,河北,唐山,063000
摘    要:目的:研究大鼠肢体缺血/再灌注后急性肺损伤时,内皮型一氧化氮合酶(eNOS)和诱导型一氧化氮合酶(i-NOS)的表达及其在急性肺损伤发生中的作用。方法:雄性Wistar大鼠于后肢根部阻断血流后松解(4h/4h),分别给予L-Arg和氨基胍(AG)预先干预,分为control、IR、L-Arg和AG组,免疫组织化学方法检测肺组织中iNOS和eNOS的表达,同时检测肺组织中MDA、MPO、W/D和NO2^-/NO3^-值,肺组织形态学观察以评价肺损伤的程度。结果:与control组比较,I/R组eNOS表达降低,iNOS表达增强,MDA、MPO、W/D和NO2^-/NO3^-值增加。肺组织充血、炎细胞浸润,肺泡腔渗液;与I/R组比较,L-Arg组eNOS、iNOS表达无明显变化,NO2^-/NO3^-增加。MDA、MPO、W/D降低,肺组织损伤有减轻趋势,AG组eNOS表达无明显变化,iNOS活性降低,NO2^-/NO3^-减少,MDA、MPO、W/D增加,肺组织损伤有加重趋势。结论:肢体缺血/再灌注急性肺损伤过程中,iNOS表达增加,NO生成增多,在肺损伤发生中有一定的保护作用。

关 键 词:一氧化氮  一氧化氮合酶  缺血/再灌注  急性肺损伤
文章编号:1000-6834(2006)04-0484-04
收稿时间:2005-03-07
修稿时间:2005-03-072006-03-24

Expression NOS in acute lung injury following limb ischemia/reprefusion and its significance in rats
Zhang YB,Zhang LY,Men XL,Dong SY,Yang QH,Yao RL.Expression NOS in acute lung injury following limb ischemia/reprefusion and its significance in rats[J].Chinese Journal of Applied Physiology,2006,22(4):484-487.
Authors:Zhang Yi-Bing  Zhang Lian-Yuan  Men Xiu-Li  Dong Shu-Yun  Yang Quan-Hui  Yao Rui-Li
Institution:North China Coal Medical College, Tangshan 063000, China
Abstract:Aim: To investigate the expression and role of inducible NOS(iNOS) and endothelial NOS(eNOS) in acute lung injury following limb ischemia/reperfusion(4h/4h). Methods: Wistar rats were randomized into four groups:control group, ischemia/reperfusion (I/R) group, L-Arginine(L-Arg) pretreatment group, Aminoguanidine(AG)pretreatment group. The lung tissue of each group was subjected to assay of content of MDA, MPO,W/D andNO2-/NO3-. The expression of iNOS and eNOS was examined with immunohistological staining. The pulmonary morphologic changes were observed under microscope respectively. Results: The acute lung injury existed after limb ischemia/reperfusion. The eNOS downregulation and iNOS upregulation among I/R, L-Arg and AG groups were observed contrasted to the control group. There was no expressional and statistical difference of iNOS between I/R group and L-Arg group. The expression of eNOS was similar between IR and AG buti NOS expression was downregulated in AG The parameters of MDA, MPO, W/D and NO2-/NO3- in pulmonarytissue were significantly increased in I/R groups compared with those of the control group. The parameters of L-Arg and AG pretreatment groups in comparison with those of the I/R group showed significantly difference. Based on the results of pulmonary pathology, the congestion and infiltration of inflammatory cells existed obviously in IR group. L-Arg played definite role in militating lung injury and AG might make lung injury aggravated. Conclusion: The NO definite production from iNOS is possible to play a compensitivly protective role in acute lung injury following limb ischemia/reperfusion and antagonist of iNOS may aggravate the lung injury.
Keywords:nitric oxide (NO)  nitric oxide synthase (NOS)  ischemia/reperfusion  acute lung injury
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