首页> 外文期刊>Forensic science international >Validation of Large White Pig as an animal model for the study of cannabinoids metabolism: application to the study of THC distribution in tissues.
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Validation of Large White Pig as an animal model for the study of cannabinoids metabolism: application to the study of THC distribution in tissues.

机译:验证大型白猪作为研究大麻素代谢的动物模型:在组织中四氢大麻酚分布研究中的应用。

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This study presents a new animal model, the Large White Pig, which was tested for studying cannabinoids metabolism. The first step has focused on determination of plasma kinetics after injection of Delta(9)-tetrahydrocannabinol (THC) at different dosages. Seven pigs received THC by intravenous injections (50, 100 or 200 microg/kg). Plasma samples were collected during 48 h. Determination of cannabinoids concentrations were performed by gas chromatography/mass spectrometry. Results showed that plasma kinetics were comparable to those reported in humans. Terminal half-life of elimination was 10.6 h and a volume of distribution of 32 l/kg was calculated. In a second step, this model was used to determine the kinetic profile of cannabinoids distribution in tissues. Eight Large White male pigs received an injection of THC (200 microg/kg). Two pigs were sacrificed 30 min after injection, two others after 2, 6 and 24 h. Different tissues were sampled: liver, kidney, heart, lung, spleen, muscle, fat, bile, blood, vitreous humor and several brain areas. The fastest THC elimination was noted in liver tissue, where it was completely eliminated in 6 h. THC concentrations decreased in brain tissue slower than in blood. The slowest THC elimination was observed for fat tissue, where the molecule was still present at significant concentrations 24 h later. After 30 min, THC concentration in different brain areas was highest in the cerebellum and lowest in the medulla oblongata. THC elimination kinetics noted in kidney, heart, spleen, muscle and lung were comparable with those observed in blood. 11-Hydroxy-THC was only found at high levels in liver. THC-COOH was less than 5 ng/g in most tissues, except in bile, where it increased for 24 h following THC injection. This study confirms, even after a unique administration, the prolonged retention of THC in brain and particularly in fat, which could be at the origin of different phenomena observed for heavy users such as prolonged detection of THC-COOH in urine or cannabis-related flashbacks. Moreover, these results support the interest for this animal model, which could be used in further studies of distribution of cannabinoids in tissues.
机译:这项研究提出了一种新的动物模型,大型白猪,已经过测试以研究大麻素的代谢。第一步集中于确定注射不同剂量的Delta(9)-四氢大麻酚(THC)后的血浆动力学。七头猪通过静脉注射(50、100或200微克/千克)接受四氢大麻酚。在48小时内收集血浆样品。大麻素浓度的测定是通过气相色谱/质谱法进行的。结果表明,血浆动力学与人类报道的相当。消除的最终半衰期为10.6小时,计算得出的分布体积为32 l / kg。第二步,该模型用于确定大麻素在组织中分布的动力学特征。八头大白公猪注射了四氢大麻酚(200微克/千克)。在注射后30分钟处死两只猪,在2、6和24小时后杀死另外两只。采样了不同的组织:肝脏,肾脏,心脏,肺,脾脏,肌肉,脂肪,胆汁,血液,玻璃体液和几个大脑区域。注意到在肝组织中最快的THC消除速度在6小时内被完全消除。脑组织中THC浓度的降低速度比血液中的THC缓慢。在脂肪组织中观察到最慢的THC消除,该分子在24小时后仍以显着浓度存在。 30分钟后,不同大脑区域的THC浓度在小脑中最高,而在延髓中最低。在肾脏,心脏,脾脏,肌肉和肺中发现的THC消除动力学与在血液中观察到的相当。仅在肝脏中发现高水平的11-羟基-THC。除胆汁外,在大多数组织中,THC-COOH均低于5 ng / g,在胆汁中,THC-COOH在注射THC-COOH后24小时内升高。这项研究证实,即使在独特的给药方式下,THC在大脑中,尤其是在脂肪中的保留时间延长,这可能是重度使用者观察到的不同现象的根源,例如长时间检测尿液中的THC-COOH或大麻相关的闪回。 。此外,这些结果支持了这种动物模型的兴趣,该模型可用于进一步研究大麻素在组织中的分布。

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