首页> 外文期刊>Journal of Pharmacological and Toxicological Methods >A method to measure dual NK1/NK2-antagonist activity in dogs.
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A method to measure dual NK1/NK2-antagonist activity in dogs.

机译:一种测量犬双NK1 / NK2-拮抗剂活性的方法。

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The major pulmonary effects of tachykinins are produced by activation of both NK1- and NK2-receptors. A variety of animal models have been used to profile activity of the tachykinins, particularly rodents and guinea pigs, but little information exists regarding methods to evaluate NK1- and NK2-receptor antagonist activity in dogs. This study describes a simple method in dogs to measure NK1- and NK2-receptor agonist and antagonist activity of drugs in the same preparation. We measured pulmonary resistance (RL), dynamic lung compliance (CDyn), minute volume (MV), and mean arterial blood pressure (MAP) before and after challenge with aerosolized NKA (1%) and i.v. SP (100 ng/kg) to quantify responses to the tachykinin challenge. Challenge with NKA produced an increase in RL and a decrease in CDyn, and this bronchospasm was inhibited by the NK2-antagonist SR 48968 (ID50 RL=1.3 mg/kg and ID50 CDyn=1.3 mg/kg, p.o.). The NK1-antagonist, CP 99994 was inactive against NKA-induced bronchospasm at doses up to 10 mg/kg, p.o. When the dogs were challenged with SP, there was a fall in MAP and an increase in MV and both responses were inhibited by CP 99994 (ID50 MV=2.3 mg/kg and ID50 BP=4.5 mg/kg, p.o.), but not by SR 48968 at doses up to 3 mg/kg, p.o. These results identify that NK2-receptors mediate the bronchoconstrictor effect of NKA, and NK1-receptors mediate the hypotension and respiratory stimulation due to SP in dogs. This method offers many advantages for evaluating the effects of tachykinin antagonists including the fact that it is relatively simple to perform and has the capacity to assess both NK1 and NK2 antagonist activity in the same preparation.
机译:通过NK1和NK2受体的激活来产生Tachykinins的主要肺部效应。各种动物模型已被用于概况Tachykinins,特别是啮齿动物和豚鼠的活性,但有关于评估犬NK1和NK2-受体拮抗剂活性的方法存在很少的信息。本研究描述了一种在相同制剂中测量NK1和NK2-受体激动剂和药物的拮抗剂活性的简单方法。在攻击性NKA(1%)和I.V之前,我们测量肺抗性(R1),动态肺顺应性(CDYN),微小体积(MV)和平均动脉血压(MAP),以及攻击前后的攻击前后。 SP(100 ng / kg)量化对Tachykinin挑战的反应。 NKA挑战产生了RL的增加和CDYN的减少,并且通过NK2-拮抗剂SR 48968抑制该支气管痉挛(ID50 R1 = 1.3mg / kg和ID50 cdyn = 1.3mg / kg,p.o.)。 NK1-拮抗剂CP 99994对NKA诱导的支气管痉挛,剂量高达10mg / kg,p.o.当狗用SP挑战时,地图中存在掉落,CP 99994(ID50 mV = 2.3mg / kg和Id50bp = 4.5mg / kg,po)抑制mv和两个反应的增加,但不是SR 48968剂量高达3毫克/千克,PO这些结果鉴定了NK2受体介导NKA的支气管电池效应,NK1受体由于SP在狗中介导低血压和呼吸刺激。该方法提供了评估Tachykinin拮抗剂的影响的许多优点,包括在相对简单的情况下具有相对简单的事实,并且具有在相同的制剂中评估NK1和NK2拮抗剂活性的能力。

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