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微针贴片给药鲑鱼降钙素。

Delivery of salmon calcitonin using a microneedle patch.

机构信息

School of Chemical and Biomolecular Engineering, Georgia Institute of Technology, Atlanta, GA 30332-0100, USA.

出版信息

Int J Pharm. 2012 Feb 28;423(2):257-63. doi: 10.1016/j.ijpharm.2011.11.046. Epub 2011 Dec 8.

Abstract

Peptides and polypeptides have important pharmacological properties but only a limited number have been exploited as therapeutics because of problems related to their delivery. Most of these drugs require a parenteral delivery system which introduces the problems of pain, possible infection, and expertise required to carry out an injection. The aim of this study was to develop a transdermal patch containing microneedles (MNs) coated with a peptide drug, salmon calcitonin (sCT), as an alternative to traditional subcutaneous and nasal delivery routes. Quantitative analysis of sCT after coating and drying onto microneedles was performed with a validated HPLC method. In vivo studies were carried out on hairless rats and serum levels of sCT were determined by ELISA. The AUC value of MNs coated with a trehalose-containing formulation (250 ± 83 ng/mL min) was not significantly different as compared to subcutaneous injections (403 ± 253 ng/mL min), but approximately 13 times higher than nasal administration (18.4 ± 14.5 ng/mL min). T(max) (7.5 ± 5 min) values for MN mediated administration were 50% shorter than subcutaneous injections (15 min), possibly due to rapid sCT dissolution and absorption by dermal capillaries. These results suggest that with further optimization of coating formulations, microneedles may enable administration of sCT and other peptides without the need for hypodermic injections.

摘要

肽和多肽具有重要的药理学性质,但由于其传递问题,只有少数被用作治疗药物。这些药物中的大多数需要一种肠胃外给药系统,这会带来疼痛、可能感染以及进行注射所需的专业知识等问题。本研究的目的是开发一种含有微针(MN)的透皮贴剂,MN 表面涂覆有肽类药物鲑鱼降钙素(sCT),作为传统皮下和鼻内给药途径的替代方法。采用经过验证的 HPLC 方法对涂覆和干燥在微针上的 sCT 进行定量分析。在无毛大鼠上进行体内研究,并通过 ELISA 测定血清中 sCT 的水平。与皮下注射(403 ± 253 ng/mL min)相比,含有海藻糖配方的 MN 涂层的 AUC 值(250 ± 83 ng/mL min)没有显著差异,但约为鼻内给药的 13 倍(18.4 ± 14.5 ng/mL min)。MN 介导给药的 T(max)(7.5 ± 5 min)值比皮下注射(15 min)短 50%,这可能是由于 sCT 迅速溶解和被真皮毛细血管吸收。这些结果表明,通过进一步优化涂层配方,微针可能能够无需皮下注射即可给予 sCT 和其他肽类药物。

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