一氧化氮阿司匹林对血小板聚集功能的影响

目的研究一种能缓慢释放一氧化氮的新型阿司匹林(BPI-1096)对血小板聚集功能的影响。方法正常人富血小板血浆与药物在37℃条件下温育10 min后,采用比浊法测定不同诱导剂作用下血小板聚集率。结果不同浓度条件下BPI-1096能够不同程度地降低由二磷酸腺苷、血小板活化因子、肾上腺素及瑞斯托霉素诱导的血小板聚集(P<0.05),对花生四烯酸诱导的血小板聚集虽有降低但是无统计学意义;在相同浓度条件下BPI-1096与阿司匹林抑制血小板聚集率的作用无显著性差异;在不同浓度条件下BPI-1096对血小板聚集率不存在明显的浓度效应关系。结论BPI-1096作为一种新型的一氧化氮阿司匹林,能够显著抑制二磷酸腺苷、血小板活化因子、瑞斯托霉素及肾上腺素等多种诱导条件下体外血小板聚集功能,作用强度与传统阿司匹林疗效相当,其对血小板的抑制作用强度无明显的浓度效应关系。

一氧化氮阿司匹林(NCX-4016)体外抗氧化作用

目的:探讨一氧化氮阿司匹林(NCX-4016)的体外抗氧化低密度脂蛋白的效应。方法:健康成人空腹12 h新鲜混合静脉血,离心取血浆。采用密度梯度超速离心法分离低密度脂蛋白(LDL),鉴定其纯度并检测其浓度。以Cu2+体外诱导LDL氧化,制备LDL体外氧化模型,采用紫外分光光度计于234 nm监测LDL氧化过程中共轭二烯键(CD)的形成情况。将NCX-4016加入反应体系,观察药物对反应体系内形成动力曲线的影响以及对LDL氧化的作用,同时以硫代巴比妥酸反应活性物(TBRAS)测定诱导LDL氧化前后过氧化脂质生成量的影响。结果:NCX-4016能够降低CD的最大生成量、延长潜伏期,降低LDL氧化产物丙二醛(MDA)的含量,并具有浓度依赖效应关系(P<0．05)。在相同浓度条件下NCX-4016的抗LDL氧化效应显著高于阿司匹林(P<0．05)。结论: NCX-4016对Cu2+诱导的LDL的氧化具有明显抑制作用。

一氧化氮释放型阿司匹林对荷瘤小鼠前列腺癌血管形成的抑制作用

目的探讨一氧化氮释放型阿司匹林(NO-ASA)对小鼠皮下种植前列腺癌的生长及肿瘤血管形成的抑制作用。方法皮下荷前列腺癌小鼠体内注射NO-ASA后监测肿瘤生长情况;处死小鼠后以ELISA法检测小鼠血清VEGF的表达,实时定量PCR法检测肿瘤中VEGF mRNA的表达,免疫组化法检测肿瘤中CD34的表达并量化微血管数目,以未注射NO-ASA的皮下荷前列腺癌小鼠为对照。受精鸡胚尿囊膜(HET-CAM)试验检测NO-ASA在体外对血管形成的影响。结果小鼠体内注射NO-ASA后皮下种植的前列腺癌的生长受到抑制,小鼠血清以及肿瘤组织的VEGF表达明显降低,肿瘤组织中的CD34表达减少,与对照组相比差异有统计学意义(P<0.05,P<0.01)。NO-ASA对受精鸡卵尿囊膜上的血管生长也有明显抑制作用。结论 NO-ASA可抑制前列腺癌肿瘤生长和血管形成。

一氧化氮供体偶联的阿司匹林衍生物Ⅱ_6抗血栓作用及其机制研究

目的观察一氧化氮供体偶联的阿司匹林衍生物Ⅱ6对血栓形成的影响,并探讨其作用机制。方法以阿司匹林为对照,观察Ⅱ6经口给药对大鼠下腔静脉血栓和脑血栓形成的影响,采用放射免疫法分析Ⅱ6对大鼠血浆、主动脉条和ECV304细胞上清液中血栓素B2(TXB2)和6-酮-前列腺素F1α(6-Keto-PGF1α)含量的影响,用G riess法测定Ⅱ6对ECV304细胞外液和大鼠血浆中一氧化氮(NO)释放的影响。结果化合物Ⅱ6可减轻实验动物血栓的重量,降低TXB2的生成,提高大鼠血清和ECV304细胞上清液中NO的含量。结论Ⅱ6具有较好的抗血栓作用,其作用机制可能与抑制TXA2的释放,增加NO含量有关。

释放一氧化氮型阿司匹林防治肿瘤的作用

目的介绍释放一氧化氮型阿司匹林(NO-ASA)在防治肿瘤方面的最新进展。方法查阅国内外文献资料进行整理和归纳。结果NO-ASA防治肿瘤作用靶点较广泛,对人结肠癌和其它癌细胞株有抑制作用,还可以作为抗癌药顺铂的辅助治疗药。结论NO-ASA是一种有希望作为抗结肠癌和其它癌的防治药。

Nitric oxide-releasing aspirin but not conventional aspirin improves healing of experimental colitis

AIM:To determine the effect of non-selective cyclooxygenase (COX) inhibitors,selective COX-2 inhibitors and nitric oxide (NO)-releasing aspirin in the healing of ulcerative colitis.METHODS:Rats with 2,4,6 trinitrobenzenesulfonic acid (TNBS)-induced colitis received intragastric (ig) treatment with vehicle,aspirin (ASA) (a nonselective COX inhibitor),celecoxib (a selective COX-2 inhibitor) or NO-releasing ASA for a period of ten days.The area of colonic lesions,colonic blood flow (CBF),myeloperoxidase (MPO) activity and expression of proinflammatory markers COX-2,inducible form of nitric oxide synthase (iNOS),IL-1β and tumor necrosis factor (TNF)-α were assessed.The effects of glyceryl trinitrate (GTN),a NO donor,and 2-(4-carboxyphenyl)-4,5-dihydro-4,4,5,5-tetramethyl-1H-imidazolyl-1-oxy-3-oxide,onopotassium salt (carboxy-PTIO),a NO scavenger,administered without and with ASA or NO-ASA,and the involvement of capsaicin-sensitive afferent nerves in the mechanism of healing the experimental colitis was also determined.RESULTS:Rats with colitis developed macroscopic and microscopic colonic lesions accompanied by a significant decrease in the CBF,a significant rise in colonic weight,MPO activity and plasma IL-1β and TNF-α levels.These effects were aggravated by ASA and 5-(4-chlorophenyl)-1-(4-methoxyphenyl)3-(trifluoromethyl)-1H-pyrazole (SC-560),but not celecoxib and counteracted by concurrent treatment with a synthetic prostaglandin E 2 (PGE 2) analog.Treatment with NO-ASA dose-dependently accelerated colonic healing followed by a rise in plasma NO x content and CBF,suppression of MPO and downregulation of COX-2,iNOS,IL-1β and TNF-α mRNAs.Treatment with GTN,the NO donor,significantly inhibited the ASA-induced colonic lesions and increased CBF,while carboxy-PTIO or capsaicin-denervation counteracted the NO-ASAinduced improvement of colonic healing and the accompanying increase in the CBF.These effects were restored by co-treatment with calcitonin gene related peptide (CGRP) and NO-ASA in capsaicin-denervated animals.CONCLUSION:NO-releasing ASA,in contrast to ASA,COX-1 inhibitors,and SC-560,accelerated the healing of colitis via a mechanism involving NO mediated improvement of microcirculation and activation of sensory nerves releasing CGRP.