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首页> 外文期刊>Drug delivery and translational research >Lidocaine permeation from a lidocaine NaCMC/gel microgel formulation in microneedle-pierced skin: vertical (depth averaged) and horizontal permeation profiles
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Lidocaine permeation from a lidocaine NaCMC/gel microgel formulation in microneedle-pierced skin: vertical (depth averaged) and horizontal permeation profiles

机译:利多卡因NaCMC /凝胶微凝胶制剂在微针刺穿皮肤中的利多卡因渗透:垂直(深度平均)和水平渗透曲线

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摘要

Common local anaesthetics such as lidocaine are administered by the hypodermic parenteral route but it causes pain or anxiety to patients. Alternatively, an ointment formulation may be applied which involves a slow drug diffusion process. In addressing these two issues, this paper aims to understand the significance of the 'poke and patch' microneedle (MN) treatment on skin in conjunction to the lidocaine permeation, and in particular, the vertical (depth averaged) and horizontal (e.g. lateral) permeation profiles of the drug in the skin. The instantaneous pharmacokinetics of lidocaine in skin was determined by a skin denaturation technique coupled with Franz diffusion cell measurements of the drug pharmacokinetics. All pharmacokinetic profiles were performed periodically on porcine skin. Three MN insertion forces of 3.9, 7.9 and 15.7 N were applied on the MN to pierce the skin. For the smaller force (3.9 N), post MN-treated skin seems to provide an 'optimum' percutaneous delivery rate. A 10.2-fold increase in lidocaine permeation was observed for a MN insertion force of 3.9 N at 0.25 h and similarly, a 5.4-fold increase in permeation occurred at 0.5 h compared to passive diffusional delivery. It is shown that lidocaine permeates horizontally beyond the area of the MN-treated skin for the smaller MN insertion forces, namely, 3.9 and 7.9 N from 0.25 to 0.75 h, respectively. The lateral diffusion/permeation of lidocaine for larger MN-treated force (namely, 15.7 N in this work) seems to be insignificant at all recorded timings. The MN insertion force of 15.7 N resulted in lidocaine concentrations slightly greater than control (passive diffusion) but significantly less than 3.9 and 7.9 N impact force treatments on skin. We believe this likelihood is due to the skin compression effect that inhibits diffusion until the skin had time to relax at which point lidocaine levels increase.
机译:常见的局部麻醉药(如利多卡因)通过皮下注射途径进行给药,但会给患者带来疼痛或焦虑。或者,可以使用药膏制剂,其涉及缓慢的药物扩散过程。在解决这两个问题时,本文旨在了解“戳和贴”微针(MN)治疗对利多卡因渗透的皮肤治疗的重要性,尤其是垂直(平均深度)和水平(例如侧面)渗透药物在皮肤中的渗透特性。利多卡因在皮肤中的瞬时药代动力学是通过皮肤变性技术结合药物药代动力学的Franz扩散池测量确定的。定期在猪皮肤上进行所有药代动力学分析。在MN上施加3.9、7.9和15.7 N的三个MN插入力以刺穿皮肤。对于较小的力(3.9 N),MN处理后的皮肤似乎提供了“最佳”的经皮输送速率。在0.25 h时,对于3.9 N的MN插入力,观察到利多卡因渗透率增加了10.2倍,与被动扩散递送相比,在0.5 h时,渗透率增加了5.4倍。结果表明,对于较小的MN插入力(分别为0.25和0.75 h的3.9 N和7.9 N),利多卡因水平渗透到MN处理的皮肤区域之外。利多卡因在较大的MN处理力下(本研究中为15.7 N)的横向扩散/渗透在所有记录的时间点似乎都无关紧要。 15.7 N的MN插入力导致利多卡因浓度略高于对照(被动扩​​散),但显着小于3.9和7.9 N的皮肤冲击力治疗。我们认为,这种可能性是由于皮肤压缩作用抑制了扩散,直到皮肤有时间放松,此时利多卡因水平增加。

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