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Acute inhalation toxicity of smoke of fentanyl and its 1-substituted analogs in Swiss albino mice

机译:芬太尼烟雾及其1-取代的类似物对瑞士白化病小鼠的急性吸入毒性

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Fentanyl (N-(1-phenethyl-4-piperidinyl) propionanilide) is a synthetic, potent narcotic analgesic agent. However, it is known to have several side effects, which led to synthesis and evaluation of its new analogs for the management of pain. We have earlier reported the comparative bioassay of fentanyl and its eight 1-substituted analogs (1-8) in mice. Three compounds, viz., N-(1-(2-phenoxyethyl)-4-piperidinyl)propionanilide (2), N-isopropyl-3-(4-(N-phenylpropionamido)piperidin-1-yl) propanamide (5), and N-t-butyl-3-(4-(N-phenylpropionamido) piperidin-1-yl) propanamide (6) were found to be more effective and less toxic compared to fentanyl. The present study reports the comparative acute inhalation toxicity of smoke of fentanyl and its three analogs, viz., 2, 5, and 6 in mice. Animals were exposed to different concentrations of smoke generated by heating the compounds. Exposure was performed in a head only all glass static exposure assembly for 15 min to determine the median lethal concentration (LC50). The breathing pattern and various respiratory parameters of the animals were also monitored online using a polygraph. Out of three compounds tested, analog 5 was found to be most toxic (LC50 = 2820 mg/m(3)) while 2 was least toxic (LC50 = > 8000 mg/m(3)). All the compounds caused long lasting respiratory depression in a dose-dependent manner, which did not completely resolve even after discontinuation of exposure. Aerodynamic median diameter and geometric standard deviation of smoke particles was determined employing eight-stage Andersen sampler. The particles were found to be within the respirable range. The study, however, concludes that due to possible decomposition of the compounds by heating or its poor absorption by the alveolar surface, the present inhalation technique cannot be employed to generate smoke of fentanyl and its analogs for any medical or surreptitious use.
机译:芬太尼(N-(1-苯乙基-4-哌啶基)丙酰苯胺)是一种合成的有效麻醉镇痛剂。但是,已知具有多种副作用,这导致合成和评估其新的类似物用于治疗疼痛。我们之前已经报道过芬太尼及其八个1-取代的类似物(1-8)在小鼠中的比较生物测定。三种化合物,即N-(1-(2-(苯氧基乙基)-4-哌啶基)丙酰苯胺(2),N-异丙基-3-(4-(N-苯基丙酰胺基)哌啶-1-基)丙酰胺(5)与芬太尼相比,Nt-丁基-3-(4-(N-苯基丙酰胺基)哌啶-1-基)丙酰胺(6)被发现更有效且毒性更低。本研究报告了芬太尼及其三种类似物(即2、5、6)的烟雾对小鼠的急性急性吸入毒性。使动物暴露于通过加热化合物而产生的不同浓度的烟雾。在仅头部全玻璃静电暴露组件中进行暴露15分钟,以确定中位致死浓度(LC50)。还使用测谎仪在线监测​​动物的呼吸模式和各种呼吸参数。在测试的三种化合物中,类似物5的毒性最高(LC50 = 2820 mg / m(3)),而2种的毒性最低(LC50 => 8000 mg / m(3))。所有化合物均以剂量依赖性方式引起持久的呼吸抑制,即使中断暴露后也无法完全解决。烟雾颗粒的空气动力学中值直径和几何标准偏差使用八级安徒生采样器确定。发现该颗粒在可呼吸范围内。然而,该研究得出结论,由于化合物可能因加热而分解,或者由于其被肺泡表面吸收不良,因此,本吸入技术不能用于产生芬太尼及其类似物的烟雾,以用于任何医学或秘密用途。

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