The effect of drug ionization on lipid-based formulations for the oral delivery of anti-psychotics

IF 3.4 Q2 CHEMISTRY, MEDICINAL ADMET and DMPK Pub Date : 2020-07-17 DOI:10.5599/admet.830
Tahlia R. Meola, K. Paxton, P. Joyce, H. B. Schultz, C. Prestidge
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引用次数: 6

Abstract

Lipid-based formulations (LBFs) are well-known to improve the oral bioavailability of poorly water-soluble drugs (PWSDs) by presenting the drug to the gastrointestinal environment in a molecularly dispersed state, thus avoiding the rate-limiting dissolution step. Risperidone and lurasidone are antipsychotics drugs which experience erratic and variable absorption, leading to a low oral bioavailability. The aim of this research was to develop and investigate the performance of risperidone and lurasidone when formulated as an emulsion and silica-lipid hybrid (SLH). Lurasidone and risperidone were dissolved in Capmul® MCM at 100% and 80% their equilibrium solubility, respectively, prior to forming a sub-micron emulsion. SLH microparticles were fabricated by spray-drying a silica stabilised sub-micron emulsion to form a solid powder. The performances of the formulations were evaluated in simulated intestinal media under digesting conditions, where the emulsion and SLH provided a 17-fold and 23-fold increase in LUR solubilisation, respectively. However, the performance of RIS was reduced by 2.2-fold when encapsulated within SLH compared to pure drug. Owing to its pKa, RIS adsorbed to the silica and thus, dissolution was significantly hindered. The results reveal that LBFs may not overcome the challenges of all PWSDs and physiochemical properties must be carefully considered when predicting drug performance.
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药物电离对口服抗精神病药物脂基制剂的影响
众所周知,脂基制剂(LBFs)通过将药物以分子分散状态呈现在胃肠道环境中,从而避免了限速溶出步骤,从而提高了低水溶性药物(PWSDs)的口服生物利用度。利培酮和鲁拉西酮是抗精神病药物,其吸收不稳定和可变,导致口服生物利用度低。本研究的目的是开发和研究利培酮和鲁拉西酮作为乳剂和硅脂混合物(SLH)配制时的性能。鲁拉西酮和利培酮分别以100%和80%的平衡溶解度溶解在Capmul®MCM中,形成亚微米乳剂。通过喷雾干燥二氧化硅稳定的亚微米乳剂来制备SLH微颗粒,形成固体粉末。在消化条件下的模拟肠道培养基中对配方的性能进行了评估,其中乳剂和SLH分别将LUR的增溶性提高了17倍和23倍。然而,与纯药物相比,在SLH内包裹RIS的性能降低了2.2倍。由于其pKa, RIS吸附在二氧化硅上,因此,溶解明显受阻。结果表明,LBFs可能无法克服所有pwsd的挑战,在预测药物性能时必须仔细考虑理化性质。
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来源期刊
ADMET and DMPK
ADMET and DMPK Multiple-
CiteScore
4.40
自引率
0.00%
发文量
22
审稿时长
4 weeks
期刊介绍: ADMET and DMPK is an open access journal devoted to the rapid dissemination of new and original scientific results in all areas of absorption, distribution, metabolism, excretion, toxicology and pharmacokinetics of drugs. ADMET and DMPK publishes the following types of contributions: - Original research papers - Feature articles - Review articles - Short communications and Notes - Letters to Editors - Book reviews The scope of the Journal involves, but is not limited to, the following areas: - physico-chemical properties of drugs and methods of their determination - drug permeabilities - drug absorption - drug-drug, drug-protein, drug-membrane and drug-DNA interactions - chemical stability and degradations of drugs - instrumental methods in ADMET - drug metablic processes - routes of administration and excretion of drug - pharmacokinetic/pharmacodynamic study - quantitative structure activity/property relationship - ADME/PK modelling - Toxicology screening - Transporter identification and study
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