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基于氨基酸的聚(酯脲)作为恩替卡韦缓释的基质。

Amino Acid-Based Poly(ester urea)s as a Matrix for Extended Release of Entecavir.

作者信息

Abel Alexandra K, Dreger Nathan Z, Nettleton Karissa, Gustafson Tiffany P, Forster Seth P, Becker Matthew L

机构信息

Department of Polymer Science , The University of Akron , Akron , Ohio 44325 , United States.

Department of Pharmaceutical Sciences , Merck & Co., Inc. , 90 E. Scott Ave. , Rahway , New Jersey 07065 , United States.

出版信息

Biomacromolecules. 2020 Feb 10;21(2):946-954. doi: 10.1021/acs.biomac.9b01586. Epub 2020 Jan 27.

Abstract

The use of polymers as excipients for drug delivery has afforded stable formulations that reliably control the release of active pharmaceutical ingredients (APIs). While many materials are available and used, few polymers exhibit the numerous advantages, including amorphous characteristics, noninflammatory properties, and resorbable degradation products, like those of poly(ester urea)s (PEUs). Furthermore, stability issues that arise in various APIs can make formulation optimization difficult. Herein, a series of PEUs were synthesized that vary by the fraction of l-phenylalanine monomer incorporated into the copolymerization. The various PEUs and entecavir monohydrate were dry-mixed at different weight percentages (15, 30, and 50%). Filaments of the PEU formulations were extruded and analyzed quantitatively for drug loading and content uniformity by using μ-CT and UPLC analysis. Drug dissolution profiles from filament segments were monitored over a 4-week period and ultimately showed that the controlled release of entecavir was influenced by the incorporation of the l-phenylalanine within the polymer.

摘要

使用聚合物作为药物递送的辅料已产生了能够可靠控制活性药物成分(API)释放的稳定制剂。虽然有许多材料可供使用,但很少有聚合物具有聚(酯脲)(PEU)那样的众多优点,包括无定形特性、非炎性性质和可吸收的降解产物。此外,各种API中出现的稳定性问题可能会使制剂优化变得困难。在此,合成了一系列因共聚中引入的L-苯丙氨酸单体比例不同而有所差异的PEU。将各种PEU与一水合恩替卡韦以不同重量百分比(15%、30%和50%)进行干混。通过μ-CT和UPLC分析对PEU制剂的长丝进行挤压并定量分析药物负载和含量均匀性。在4周的时间内监测长丝片段的药物溶出曲线,最终表明聚合物中L-苯丙氨酸的引入影响了恩替卡韦的控释。

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