Hepatoprotective effect of nitric oxide in experimental model of acute hepatic failure

AIM: To evaluate the effect of nitric oxide (NO) on the development and degree of liver failure in an animal model of acute hepatic failure (AHF).

Intestinal expressions of eNOSmRNA and iNOSmRNA in rats with acute liver failure

AIM: To observe the gene expression change of eNOSmRNA and iNOSmRNA in the small and large intestines with acute liver failure (ALF), and to reveal the biological function of NO on the pathogenesis of ALF and multiple organs dysfunction at the molecular level. METHODS: Sixty male Wistar rats were selected, weighing from 250g to 350g, and divided into 5 groups randomly: SO, ALF (6h, 12h), L-Arg, L-NAME, L-Arg and L-NAME, each group with 10 rats. The dose of L-Arg was 300mg.kg(-1), and L-NAME was 30mg.kg(-1), the reagents diluted by normal saline were injected through tail vein 30 minutes pre and post operation. The rats in the ALF group were respectively sacrificed postoperatively at 6h, 12h, and the rats in the other groups were sacrificed postoperatively at 6h. The tissues of small and large intestines were harvested in 4% paraforaldehyde containing the reagent of DEPC and fixed at 6h, embedded in paraffin, and 4 microm section was cut. The expression of eNOSmRNA and iNOSmRNA in these tissues was determined with in situ hybridization, and analyzed with the imaging analysis system of CMM-3 and SPSS statistical software. RESULTS: The expression of eNOSmRNA in the large intestine and iNOSmRNA in the small and large intestines increased significantly at 6h after ALF, but the expression of iNOSmRNA in the small and large intestines reduced notably at 12h after ALF (P【0.05); the expression of eNOSmRNA in the large intestine and iNOSmRNA in the small and large intestines decreased significantly with the reagents of L-Arg at 6h ALF, but the expression of eNOSmRNA and iNOSmRNA in the small and large intestines decreased totally with the reagents of L-NAME or association with L-Arg 6h ALF. CONCLUSION: The expression of eNOSmRNA in the large intestine increased notably at the early stage of ALF, NO induced by the enzyme of eNOS from the transplantation of eNOSmRNA can protect the function of the large intestine, the high expression of iNOSmRNA is involved in the damaged function of the small and large intestines. NO precursor can reduce the expression of iNOSmRNA in the small and large intestines and the damage to intestines; NOS inhibitor or association with NO pre-cursor can totally lower the expression of eNOSmRNA and iNOSmRNA in the small and large intestines, it cannot notably influence the NOS inhibitor in the gene expression of eNOSmRNA and iNOSmRNA to supply the additional NO precursor.

L-硝基精氨酸对大鼠LPS性肺损伤的实验治疗研究

目的 :观察一氧化氮 (NO)和一氧化氮合酶抑制剂NG-硝基 -L -精氨酸 (L -NA)对LPS性肺损伤的影响。方法 :采用静脉注射脂多糖 (LPS)复制急性肺损伤大鼠模型。将 4 0只SD大鼠随机分为 5组 :空白对照组、LPS模型组、L -NA高剂量 (2 0mg/kg)、中剂量 (10mg/kg)、低剂量 (5mg/kg)治疗组 ,经腹腔注射 ,实验过程中监测大鼠平均动脉压 (MAP) ,定时取静脉血测定血浆中NO2 -/NO3 -含量 ,于规定时间处死大鼠 ,迅速取出肺脏 ,观察LPS引起大鼠急性肺损伤后肺系数、肺水肿情况和肺组织中丙二醛 (MDA)含量、一氧化氮合酶 (NOS)、超氧化物歧化酶(SOD)活性的变化 ,以及L -NA的治疗作用。结果 :L -NA可明显升高MAP ,降低肺系数和肺含水量 ,减少血浆中NO2 -/NO3 -含量 ,可显著降低肺组织中NOS活性 ,减少MDA含量 ,增强SOD活性 ,减轻肺损伤。结论 :L -NA对LPS性肺损伤具有治疗作用 ,且随剂量增大作用增强。

大剂量顺铂所致大鼠急性肾损害过程中内源性血管活性物质的动态变化及其意义

[目的]观察内源性血管活性物质内皮素(ET-1)和一氧化氮(NO)在大剂量顺铂(DDP)所致大鼠急性肾损害过程中的动态变化及其意义。[方法]SD大鼠24只,雌雄各半,依体重随机分组,DDP用药组18只和NS对照组6只。10 mg/kg DDP单次腹腔内注射,等量生理盐水对照。DDP用药前和DDP用药后3、6、48 h分别取大鼠6只,称重后内眦静脉取血,放射免疫法测定血浆ET-1水平,比色法测定血浆NO含量,统计学分析。[结果]大剂量DDP用药后3 h大鼠血ET-1升至(213.68±28.3)ng/mL,与对照组大鼠(157.45±27.7)ng/mL比较差异具有显著性意义(P<0.01)。用药后6 h血浆ET-1较前稍下降,随后持续在较高水平,与对照组比较差异仍有显著性意义(P<0.05)。大剂量DDP用药后3 h,大鼠血浆NO含量开始升高,用药后6 h升至(166.67±84.62)μmol/L,与对照组大鼠(32.85±12.98)μmol/L比较,差异具显著性意义(P<0.01);用药后48 h血NO较前稍微下降,但与对照组比较差异仍具有显著性意义(P<0.01)。[结论]血浆ET-1和NO浓度的变化与大剂量顺铂所致急性肾功能衰竭有关,二者可能在顺铂所致肾毒性损伤早期的发病机制中发挥重要作用。

NO及NO合成酶抑制剂对急性肾衰大鼠内源性内皮素分泌的影响

在甘油致大鼠ARF模型上,分别观察了NO前体L—Arg及NO合成酶抑制剂L—NNA对ARF大鼠肾功能及内源性ET分泌的影响。结果显示:ARF大鼠ET分泌增多,NO合成减少,L—NNA明显增加ARF大鼠P_(ET)水平(P<0.001),肾小管ET免疫反应阳性颗粒明显增多(P<0.001),肾功能更加恶化。L—Arg则使ARF大鼠P_(ET)水平明显降低(P<0.001),肾小管ET免疫反应阳性颗粒明显减少(P<0.001),肾功能得到改善。提示甘油所致ARF时,NO改善肾功能的作用可能与具抑制内源性ET分泌有关。

诱导型一氧化氮合酶在缺血性急性肾衰竭肾小管损伤中的作用及L-精氨酸的疗效观察

目的研究急性肾衰竭(ARF)时诱导型一氧化氮合酶(iNOS)与肾小管损伤的关系及初步探讨L-精氨酸(L-arg)灌注对ARF的治疗作用。方法SD大鼠分为3组:①正常对照组(n=6),假手术;②ARF组(n=18),夹闭双肾动脉50min建立ARF模型;③ARF+L-Arg组(n=18),夹闭双肾动脉50min后,股静脉灌注L-Arg(300mg/kg)。通过内生肌酐清除率(Ccr)测定,肾脏病理学检查i、NOS免疫组化及改良NOS酶组化染色等方法观察iNOS在ARF小管损伤中的作用。结果术后1,3和5d Ccr值自术前(0.9978±0.149)L/d分别下降至(0.194±0.029)L/d、(0.21±0.126)L/d和(0.421±0.31)L/d,治疗组术后1,3和5d Ccr值分别为(0.294±0.056)L/d(、0.923±0.096)L/d和(1.126±0.21)L/d,与未治疗组同期相比有显著性差异(P<0.01)。生理状态下,iNOS在肾内表达较弱,ARF后1,3和5d肾内iNOS表达明显高于正常(P<0.05)。治疗组小管细胞iNOS表达明显减少(P<0.05)。小管细胞的空泡样变性、坏死、管型亦相应减少。结论ARF时局部缺血、低氧可迅速诱导肾小管上皮细胞的iNOS大量表达,这可能是引起小管损伤的重要因素之一。外源性L-Arg能减少小管细胞iNOS的表达,减轻ARF时的肾小管损伤。