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高熔点和低熔点去氧肾上腺素恶唑烷的物理化学特性

Physicochemical characterization of high- and low-melting phenylephrine oxazolidines.

作者信息

Qiu Y, Schoenwald R D, Guillory J K

机构信息

Division of Pharmaceutics, College of Pharmacy, University of Iowa, Iowa City 52242.

出版信息

Pharm Res. 1993 Oct;10(10):1507-15. doi: 10.1023/a:1018939728993.

Abstract

Phenylephrine oxazolidine is a new prodrug of phenylephrine developed for improving ocular absorption and reducing systemic side effects. In the present study, high- and low-melting phenylephrine oxazolidines (HMP and LMP) were characterized in terms of their stereochemistry and crystal properties. It was found that the molecular configuration of the prodrug in the crystals of either HMP or LMP is identical (5R/2R). The two crystals were shown to have the same IR spectra and X-ray diffraction patterns but different crystal habits, thermal properties, solubilities and intrinsic dissolution rates. Single crystal X-ray structure analysis indicates that crystals of both HMP and LMP are orthorhombic and belong to the P2(1)2(1)2(1) space group with four molecules in a unit cell (a = 20.697 A, b = 7.065 A, and c = 9.304 A). The molecules in the crystal are held together by an intermolecular hydrogen bonding interaction between N(3) and O(13). The different physical properties observed for LMP result from crystal imperfections caused by the presence of trace amounts (often at levels < 0.5%) of an unidentified, structurally related synthetic impurity which can be dispersed in the prodrug. It was observed that both HMP and LMP can sustain thermal and mechanical treatment in the solid state. However, LMP was partially converted to HMP when suspended in certain solvents.

摘要

苯肾上腺素恶唑烷是一种新开发的苯肾上腺素前药,用于改善眼部吸收并减少全身副作用。在本研究中,对高熔点和低熔点苯肾上腺素恶唑烷(HMP和LMP)的立体化学和晶体性质进行了表征。发现HMP或LMP晶体中前药的分子构型相同(5R/2R)。两种晶体显示出相同的红外光谱和X射线衍射图谱,但晶体习性、热性质、溶解度和固有溶解速率不同。单晶X射线结构分析表明,HMP和LMP的晶体均为正交晶系,属于P2(1)2(1)2(1)空间群,一个晶胞中有四个分子(a = 20.697 Å,b = 7.065 Å,c = 9.304 Å)。晶体中的分子通过N(3)和O(13)之间的分子间氢键相互作用结合在一起。LMP观察到的不同物理性质是由痕量(通常含量<0.5%)的未鉴定的、结构相关的合成杂质的存在引起的晶体缺陷所致,这些杂质可分散在前药中。观察到HMP和LMP在固态下都能承受热处理和机械处理。然而,LMP悬浮在某些溶剂中时会部分转化为HMP。

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