一氧化氮合酶抑制剂在体内过敏性大鼠模型中的差异效应。
Differential effects of nitric oxide synthase inhibitors in an in vivo allergic rat model.
作者信息
Tulić M K, Wale J L, Holt P G, Sly P D
机构信息
TVW Telethon Institute for Child Health Research and Dept of Paediatrics, University of Western Australia, Perth, Australia.
出版信息
Eur Respir J. 2000 May;15(5):870-7. doi: 10.1034/j.1399-3003.2000.15e10.x.
The in vivo role of nitric oxide in inflammatory cell migration, vascular permeability and the development of hyperresponsiveness to methacholine (MCh) was studied in rats 24 h following ovalbumin (OVA) challenge. The NO synthase (NOS) inhibitors N(G)-mono-methyl-L-arginine (L-NMMA; nonselective), aminoguanidine (two-fold inducible NOS-selective), N(omega)-nitro-L-arginine methyl ester (L-NAME; 2000-fold endothelial cell NOS-selective) or S-methyl-L-thiocitrulline (100-fold neuronal NOS-selective) were administered (100 mg x kg(-1) s.c.) to OVA-sensitized Piebald-Virol-Glaxo rats on 3 consecutive days during which they were challenged with allergen (1% OVA). Responses to inhaled MCh were measured in anaesthetized animals 24 h after OVA challenge. Cellular inflammation and vascular permeability were assessed using bronchoalveolar lavage (BAL) fluid collected 30 min after administration of Evans blue (50 mg x kg(-1) i.v.). OVA challenge in sensitized animals induced hyperresponsiveness to MCh, inflammatory cell influx and increased leakage of Evans blue into the BAL fluid (n=9, p<0.001). Aminoguanidine was effective in inhibiting the allergen-induced cellular influx and microvascular leakage (n=9, p<0.001) without altering responses to MCh. This effect was reserved by L-arginine. L-NAME (n=5, p<0.01) and S-methyl-L-thiocitrulline (n=6, p<0.001) further potentiated the allergen-induced hyperresponsiveness without altering cellular inflammation. L-NMMA attenuated both the OVA-induced cellular influx and Evans blue leakage (n=8, p<0.001) as well as further potentiating the hyperresponsiveness to MCh (p<0.05). From these studies, it is suggested that, in allergic Piebald-Virol-Glaxo rats, nitric oxide production by inducible nitric oxide synthase plays a role in the migration of inflammatory cells and increase in vascular permeability following allergen challenge, whereas nitric oxide produced by the constitutively expressed neuronal nitric oxide synthase limits hyperresponsiveness to methacholine.
在卵清蛋白(OVA)激发24小时后的大鼠中,研究了一氧化氮在炎症细胞迁移、血管通透性以及对乙酰甲胆碱(MCh)高反应性发展中的体内作用。在连续3天对OVA致敏的花斑-维罗-葛兰素大鼠给予一氧化氮合酶(NOS)抑制剂N(G)-单甲基-L-精氨酸(L-NMMA;非选择性)、氨基胍(对诱导型NOS选择性为两倍)、N(ω)-硝基-L-精氨酸甲酯(L-NAME;对内皮细胞NOS选择性为2000倍)或S-甲基-L-硫代瓜氨酸(对神经元NOS选择性为100倍)(100mg·kg⁻¹皮下注射),在此期间用变应原(1%OVA)对其进行激发。在OVA激发24小时后,在麻醉动物中测量对吸入MCh的反应。使用在静脉注射伊文思蓝(50mg·kg⁻¹)30分钟后收集的支气管肺泡灌洗(BAL)液评估细胞炎症和血管通透性。致敏动物中的OVA激发诱导了对MCh的高反应性、炎症细胞流入以及伊文思蓝向BAL液中的渗漏增加(n = 9,p < 0.001)。氨基胍可有效抑制变应原诱导的细胞流入和微血管渗漏(n = 9,p < 0.001),而不改变对MCh的反应。L-精氨酸可逆转这种作用。L-NAME(n = 5,p < 0.01)和S-甲基-L-硫代瓜氨酸(n = 并6,p < 0.001)进一步增强了变应原诱导的高反应性,而不改变细胞炎症。L-NMMA减弱了OVA诱导的细胞流入和伊文思蓝渗漏(n = 8,p < 0.001),并进一步增强了对MCh的高反应性(p < 0.05)。从这些研究表明,在变应性花斑-维罗-葛兰素大鼠中,诱导型一氧化氮合酶产生的一氧化氮在变应原激发后炎症细胞迁移和血管通透性增加中起作用,而组成性表达的神经元型一氧化氮合酶产生的一氧化氮限制了对乙酰甲胆碱的高反应性。 (注:原文中“n = 并6”可能有误,已按正常理解翻译,若有准确信息可进一步修正)
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