庞璐璐, 高艳, 张丽花, 马金秋, 朱思庆, 朱林, 杜丽娜, 金义光. 治疗创伤后应激障碍的粉防己碱鼻用温敏凝胶研究J. 药学学报, 2019,54(9): 1680-1687. doi: 10.16438/j.0513-4870.2019-0510
引用本文: 庞璐璐, 高艳, 张丽花, 马金秋, 朱思庆, 朱林, 杜丽娜, 金义光. 治疗创伤后应激障碍的粉防己碱鼻用温敏凝胶研究J. 药学学报, 2019,54(9): 1680-1687. doi: 10.16438/j.0513-4870.2019-0510
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PANG Lu-lu, GAO Yan, ZHANG Li-hua, MA Jin-qiu, ZHU Si-qing, ZHU Lin, DU Li-na, JIN Yi-guang. Intranasal tetrandrine temperature-sensitive gel for treatment of post-traumatic stress disorderJ. Acta Pharmaceutica Sinica, 2019,54(9): 1680-1687. doi: 10.16438/j.0513-4870.2019-0510
Citation: PANG Lu-lu, GAO Yan, ZHANG Li-hua, MA Jin-qiu, ZHU Si-qing, ZHU Lin, DU Li-na, JIN Yi-guang. Intranasal tetrandrine temperature-sensitive gel for treatment of post-traumatic stress disorderJ. Acta Pharmaceutica Sinica, 2019,54(9): 1680-1687. doi: 10.16438/j.0513-4870.2019-0510
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治疗创伤后应激障碍的粉防己碱鼻用温敏凝胶研究

Intranasal tetrandrine temperature-sensitive gel for treatment of post-traumatic stress disorder

    摘要
  • 摘要: 创伤后应激障碍(post-traumatic stress disorder,PTSD)以传统全身给药方式起效慢,不良反应明显。本文制备了粉防己碱鼻用温敏凝胶(intranasal tetrandrine temperature-sensitive gel,TTG),鼻内给药治疗小鼠PTSD。以泊洛沙姆为基质制备TTG,胶凝温度合适(低于32℃)、胶凝时间短(1.32 min),流变学考察表明TTG具有温度敏感性,小动物活体成像证明TTG鼻腔滞留时间长,蟾蜍上腭纤毛毒性实验表明制剂安全性高。所有动物实验经军事科学院军事医学研究院辐射医学研究所伦理委员会批准且实验均按照相关指导原则和规定进行。用单次延长应激(single prolonged stress,SPS)、足底电击方法建立小鼠PTSD模型,使其产生焦虑、恐惧行为。用高架十字迷宫评价SPS模型小鼠,其中开臂进入次数百分比(percentages of open arm entry numbers,OE)、开臂进入潜伏期(latency of open arm entries,OL)及开臂滞留时间(residence time of open arm entries,OT)均表明模型建立成功。TTG鼻腔给药7天后,SPS小鼠的OE和OT明显增加,OL明显降低;TTG还可明显减少条件恐惧箱中足底电击模型小鼠的不动时间。苏木精-伊红病理切片与c-fos免疫组化结果表明,TTG能明显改善PTSD模型小鼠海马、前额叶皮层及杏仁核部位的病理变化。因此,TTG是一种使用方便、安全有效的抗PTSD药物,为PTSD临床治疗提供新选择。

     

    Abstract: The traditional systemic treatment of post-traumatic stress disorder (PTSD) requires a long time period for an effect and has obvious side effects. In this study, tetrandrine temperature-sensitive gel (TTG) was prepared for treatment of PTSD in mice by nasal administration. TTG was prepared with poloxamer as matrix, the gelation temperature was suitable (<32℃) and the gelation time was short (1.32 min). Rheology experiments demonstrated that TTG has temperature sensitivity. In vivo imaging system of small animals proved that TTG nasal cavity retention time was so long. The cilia toxic test of toad showed that the formulation was safe. Animal experiments were approved by the Ethics Committee of Beijing Institute of Radiation Medicine, Academy of Military Medical Sciences and the experiments were conducted in accordance with relevant guidelines and regulations. The mice were randomly assigned into healthy group, model group and TTG group. The PTSD model of mice was established by single prolonged stress (SPS) and foot-shock method to generate anxiety and fear behavior. On the day 0 of TTG administration, SPS model mice were evaluated by the elevated plus maze (EPM). Percentages of open arm entries number (OE), latency of open arm entries (OL) and the residence time of open arm entries (OT) all indicated that the SPS model was successfully established. On the 7th day of TTG administration, TTG increased the OE and OT, decreased the OL of SPS mice. The feard behavior of mice in the foot-shock model was tested using conditioned fear box, 7 days of TTG treatment can reduce the freezing time of the mice obviously. The pathological changes of hippocampus, prefrontal cortex and amygdala were observed by H&E histological sections and c-fos immunohistochemical expression. The main influenced areas of PTSD were revealed to be the CA1 of hippocampus, prefrontal cortex and amygdala. All of the above indicated that TTG is a convenient, safe and effective drug for PTSD treatment, and will provide a new choice for clinical management of PTSD.

     

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