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Brain delivery of vasoactive intestinal peptide (VIP) following nasal administration to rats

机译:鼻腔给药对大鼠的血管活性肠肽(VIP)的脑传递

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摘要

The aim of this work was to study in rats the nasal route for the brain delivery of the vasoactive intestinal peptide (VIP) neuropeptide. After evaluating VIP stability in solutions obtained from nasal washes, the effect of formulation parameters (pH 4-9, 0-1% (w/v) lauroylcarnitine (LC), hypo- or isoosmolality) on the brain uptake of intranasally administered VIP (10(-8)M)/125I-VIP (300,000 cpm/ml) was studied, using an in situ perfusion technique. Brain radioactivity distribution was assessed by quantitative autoradiographic analysis. Results were compared to intravenously administered VIP. With a hypotonic formulation at pH 4 containing 0.1% LC and 1% bovine serum albumin, VIP stability was satisfactory and loss by adsorption was minimal. Using this formulation, around 0.11% of initial radioactivity was found in the brain after 30 min perfusion and was located in the olfactory bulbs, the midbrain and the cerebellum. HPLC analysis of brain and blood extracts demonstrated the presence of intact VIP in brain and its complete degradation in the blood compartment. By intravenous administration, no intact VIP was found either in brain or in blood. In conclusion, intact VIP could be delivered successfully to the brain using the intranasal route for administration.
机译:这项工作的目的是在大鼠中研究鼻腔输送血管活性肠肽(VIP)神经肽的途径。在评估通过鼻洗液获得的VIP稳定性后,制剂参数(pH 4-9、0-1%(w / v)月桂酰肉碱(LC),低渗或等渗摩尔浓度)对经鼻内施用VIP的大脑摄取的影响(使用原位灌注技术研究了10(-8)M)/ 125I-VIP(300,000 cpm / ml)。通过定量放射自显影分析评估脑放射性分布。将结果与静脉注射的VIP进行比较。在pH值为4的低渗制剂中,含有0.1%LC和1%牛血清白蛋白的VIP稳定性令人满意,吸附损失最小。使用这种配方,在灌注30分钟后,在大脑中发现了约0.11%的初始放射性,并位于嗅球,中脑和小脑中。大脑和血液提取物的HPLC分析表明,完整的VIP存在于大脑中,并且在血液室中完全降解。通过静脉内给药,在大脑或血液中均未发现完整的VIP。总之,可以使用鼻内给药途径将完整的VIP顺利递送至大脑。

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