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高分子前药。十三。17β-雌二醇和雌二醇-17β-戊酸与聚天冬酰胺聚合物的亲水性缀合物。

Macromolecular prodrugs. XIII. Hydrosoluble conjugates of 17β-estradiol and estradiol-17β-valerate with polyaspartamide polymer.

机构信息

University of Zagreb, Faculty of Pharmacy and Biochemistry, Zagreb, Croatia.

出版信息

Acta Pharm. 2011 Dec;61(4):465-72. doi: 10.2478/v10007-011-0039-x.

Abstract

Two hydrosoluble conjugates of 17β-estradiol (ED) and estradiol-17β-valerate (EV) with polyaspartamide polymer were prepared and characterized. ED and EV were first chemically modified and bound to poly[α,β-(N-2-hydroxyethyl-DL-aspartamide)]-poly[α,β-(N-2-aminoethyl-DL-aspartamide)] (PAHA), a hydrosoluble polyaspartamide-type copolymer bearing both hydroxyl and amino groups. ED was first converted to 17-hemisuccinate (EDS) and then bound to PAHA. In the resulting conjugate PAHA-EDS, the estradiol moiety was linked to the polymer through a 2-aminoethylhemisuccinamide spacer. On the other hand, EV was first converted to estradiol-17β-valerate-3-(benzotriazole-1-carboxylate), which readily reacted with amino groups in PAHA affording the polymer-drug conjugate PAHA-EV. In the prepared conjugate PAHA-EV, the estradiol moiety was covalently bound to the polyaspartamide backbone by carbamate linkage, through an ethylenediamine spacer. The polymer-drug conjugates were designed and prepared with the aim to increase water-solubility, bioavailability and to improve drug delivery of the lipophilic estrogen hormone.

摘要

两种 17β-雌二醇(ED)和雌二醇-17β-戊酸酯(EV)与聚天冬酰胺聚合物的水溶性缀合物被制备并进行了表征。ED 和 EV 首先经过化学修饰并与聚[α,β-(N-2-羟乙基-DL-天冬酰胺)]-聚[α,β-(N-2-氨基乙基-DL-天冬酰胺)](PAHA)结合,后者是一种同时具有羟基和氨基的水溶性聚天冬酰胺型共聚物。ED 首先转化为 17-琥珀酸半酯(EDS),然后与 PAHA 结合。在得到的缀合物 PAHA-EDS 中,雌二醇部分通过 2-氨基乙基琥珀酸半酰胺间隔物与聚合物相连。另一方面,EV 首先转化为雌二醇-17β-戊酸酯-3-(苯并三唑-1-羧酸盐),它可与 PAHA 中的氨基迅速反应,得到聚合物-药物缀合物 PAHA-EV。在制备的缀合物 PAHA-EV 中,雌二醇部分通过氨基甲酸酯键,通过乙二胺间隔物,共价结合到聚天冬酰胺主链上。这些聚合物-药物缀合物的设计和制备旨在增加亲脂性雌激素激素的水溶性、生物利用度和改善药物传递。

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