A microfluidic in vitro method predicting the fate of peptide drugs after subcutaneous administration

IF 5.3 2区 医学 Q1 PHARMACOLOGY & PHARMACY
Marcus Wanselius , Susanna Abrahmsén-Alami , Belal I. Hanafy , Mariarosa Mazza , Per Hansson
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引用次数: 0

Abstract

For many biopharmaceuticals, subcutaneous (sc) administration is the only viable route. However, there is no in vitro method available accurately predicting the absorption profiles of subcutaneously injected pharmaceuticals. In this work, we show that a recently developed microfluidics method for interaction studies (MIS) has the potential to be useful in this respect. The method utilises the responsiveness of polyelectrolyte microgel networks to oppositely charged molecules as a means to monitor the interaction between peptides and hyaluronic acid (HA), a major constituent of the subcutaneous extracellular matrix. We use the method to determine parameters describing the strength of interaction between peptide and HA as well as the peptide’s aggregation tendency and transport properties in HA networks. The results from MIS studies of the peptide drugs exenatide, pramlintide, vancomycin, polymyxin B, lanreotide, MEDI7219 and AZD2820 are compared with results from measurements with the commercially available SCISSOR system and in vivo absorption and bioavailability data from the literature. We show that both MIS and SCISSOR reveal differences in the peptides’ diffusivity and tendency to aggregate in the presence of HA. We show that MIS is particularly good at discriminating between peptides forming aggregates stabilised by non-electrostatic forces in the presence of HA, and peptides forming complexes stabilised by electrostatic interactions with HA. The method provides two parameters that can be used to quantify the peptides’ aggregation tendency, the one describing the peptide packing density in complexes with HA and the other the apparent diffusivity upon release in a medium of physiological ionic strength and pH. The order of the peptides when ranked by increasing binding strength at pH 7.4 determined with MIS is shown to be in agreement with the order when ranked by the apparent 1st order absorption rate constant (ka) after sc administration in humans: lanreotide (Autogel) < exenatide (IRF) < AZD2820 < pramlintide < lanreotide (IRF) (IRF: Immediate release formulation). A correlation is found between the 1st order release rate constant determined with SCISSOR and ka for lanreotide (Autogel), exenatide and AZD2820. A mechanism relating the magnitude of ka to the peptides’ charge is proposed.

Abstract Image

预测皮下注射多肽药物转归的微流体体外方法。
对于许多生物制药来说,皮下注射是唯一可行的途径。然而,目前还没有一种体外方法能准确预测皮下注射药物的吸收曲线。在这项工作中,我们展示了最近开发的一种用于相互作用研究的微流控方法(MIS)在这方面的应用潜力。该方法利用聚电解质微凝胶网络对带电分子的反应能力,监测肽与透明质酸(HA)(皮下细胞外基质的主要成分)之间的相互作用。我们用这种方法来确定描述肽与透明质酸之间相互作用强度的参数,以及肽在透明质酸网络中的聚集趋势和传输特性。我们将多肽药物艾塞那肽、普拉克林肽、万古霉素、多粘菌素 B、兰瑞奥肽、MEDI7219 和 AZD2820 的 MIS 研究结果与市售 SCISSOR 系统的测量结果以及文献中的体内吸收和生物利用度数据进行了比较。我们发现,MIS 和 SCISSOR 都能揭示肽在有 HA 存在时的扩散性和聚集倾向的差异。我们的研究表明,MIS 尤其擅长区分在 HA 存在下由非静电力稳定形成聚集体的多肽和由与 HA 的静电相互作用稳定形成复合物的多肽。该方法提供了两个可用于量化多肽聚集趋势的参数,一个是描述多肽在与 HA 的复合物中的堆积密度,另一个是在生理离子强度和 pH 值介质中释放时的表观扩散性。用 MIS 测定的多肽在 pH 值为 7.4 时按结合强度递增排序的顺序与在人体 sc 给药后按表观一阶吸收速率常数 (ka) 排序的顺序一致:兰瑞奥肽(Autogel)a、艾塞那肽和 AZD2820。提出了 ka 大小与肽电荷相关的机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
10.70
自引率
8.60%
发文量
951
审稿时长
72 days
期刊介绍: The International Journal of Pharmaceutics is the third most cited journal in the "Pharmacy & Pharmacology" category out of 366 journals, being the true home for pharmaceutical scientists concerned with the physical, chemical and biological properties of devices and delivery systems for drugs, vaccines and biologicals, including their design, manufacture and evaluation. This includes evaluation of the properties of drugs, excipients such as surfactants and polymers and novel materials. The journal has special sections on pharmaceutical nanotechnology and personalized medicines, and publishes research papers, reviews, commentaries and letters to the editor as well as special issues.
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