Role of Porous Carriers in the Biopharmaceutical Performance of Solid SMEDDS of Canagliflozin.

Q3 Pharmacology, Toxicology and Pharmaceutics

Recent Patents on Drug Delivery and Formulation Pub Date : 2018-01-01 DOI:10.2174/1872211312666181008111354

Dilpreet Singh, Ashok K Tiwary, Neena Bedi

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引用次数: 6

Abstract

Objective: The aim of the present investigation entails the development of solid SMEDDS for improving the oral bioavailability of canagliflozin using porous carriers. The previous patent (WO2017046730A1) was based on enhanced solubility of canagliflozin through co-crystal formation.

Methods: Preconcentrates were prepared by employing Lauroglycol (80 mg), Tween 80 (300 mg) and Transcutol P (120 mg) and successfully adsorbed onto various hydrophilic and hydrophobic carriers. The prepared solid SMEDDS were characterized for various parameters to determine the optimized formulation. In vitro, ex vivo and in vivo studies were carried out to determine drug release kinetics, permeation and absorption rate, respectively. Stability of the formulation was investigated at 45°C/75% RH.

Results: The solid preconcentrates prepared with hydrophobic carriers exhibited desired attributes in a uniform range. Neusilin adsorbed solid SMEDDS (S(N)SMEDDS) portrayed enhanced amorphization in XRD and DSC studies and found to be physically compatible in FTIR studies. SEM revealed colloidal particles having spherical morphology with negligible aggregation. Ex vivo permeation rate of the drug across excised intestinal segments (duodenum, jejunum, ileum and colon) was observed to be 3.72, 5.85, 4.51 and 3.0-fold, respectively, as compared to pure drug. TEM of reconstituted SMEDDS indicated nano-sized globules with negligible coalescence. Enhanced in vitro dissolution rate of optimized solid SMEDDS manifested in bioavailability enhancement of 167.54% and 188.98%, as compared to pure drug and marketed product. These studies further substantiate the lymphatic uptake of SMEDDS through chylomicron flow blocking approach. Establishment of Level A IVIVC showed a uniform correlation between the in vitro dissolution efficiency and in vivo pharmacokinetic parameters.

Conclusion: The present investigation reveals the immense potential of solid SMEDDS in augmenting the oral bioavailability profile of poorly water-soluble drug canagliflozin.

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多孔载体对卡格列净固体SMEDDS生物制药性能的影响。

目的:开发固体SMEDDS，以提高卡格列净的口服生物利用度。之前的专利(WO2017046730A1)是基于通过共晶形成来增强canagliflozin的溶解度。方法:采用月桂醇(80 mg)、Tween 80 (300 mg)和Transcutol P (120 mg)制备预浓缩物，并成功吸附在各种亲疏水载体上。对制备的固体SMEDDS进行了各种参数表征，确定了最佳配方。分别进行体外、离体和体内研究，测定药物释放动力学、渗透和吸收率。在45°C/75% RH条件下考察了该配方的稳定性。结果:疏水载体制备的固体预浓缩物在均匀范围内具有理想的性质。Neusilin吸附固体SMEDDS (S(N)SMEDDS)在XRD和DSC研究中表现出增强的非晶化，在FTIR研究中发现其物理相容性。扫描电镜显示，胶体颗粒呈球形，聚集可忽略不计。经切除肠段(十二指肠、空肠、回肠和结肠)的体外渗透率分别为纯药的3.72倍、5.85倍、4.51倍和3.0倍。重建的SMEDDS的透射电镜显示纳米级的球状物，聚结可以忽略不计。优化后的固体SMEDDS体外溶出度提高，生物利用度较纯药和市售产品分别提高了167.54%和188.98%。这些研究进一步证实了通过乳糜微粒阻断途径对SMEDDS的淋巴摄取。A级IVIVC的建立表明，体外溶出效率与体内药动学参数呈均匀相关。结论:本研究揭示了固体SMEDDS在提高难水溶性药物卡格列净口服生物利用度方面的巨大潜力。

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

Recent Patents on Drug Delivery and Formulation Pharmacology, Toxicology and Pharmaceutics-Pharmaceutical Science

CiteScore

2.30

自引率

0.00%

发文量

期刊介绍： Recent Patents on Drug Delivery & Formulation publishes review and research articles, drug clinical trial studies and guest edited thematic issues on recent patents on drug delivery and formulation. A selection of important and recent patents on drug delivery and formulation is also included in the journal. The journal is essential reading for all researchers involved in the fields of drug delivery and formulation. The journal also covers recent research (where patents have been registered) in fast emerging therapeutic areas/targets & therapeutic agents related to drug delivery and formulations.