新型中枢神经系统靶向半合成青霉素。

Drug design and delivery Pub Date : 1990-03-01
E Pop, T Loftsson, N Bodor
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引用次数: 0

摘要

设计并合成了一系列新型半合成青霉素。该化合物具有作为分子的组成部分的吡啶-二氢吡啶氧化还原体系作为6位取代基。药物的二氢吡啶(前药)形式的酯,由于其明显的亲脂性,很容易穿透生物膜,包括血脑屏障,并产生极性吡啶离子(前药)的酯(通过酶氧化二氢吡啶部分)。由此产生的离子预计会迅速从外周排出,但会被“锁定”在中枢神经系统中;随后的酶裂解的酯功能预计释放游离酸吡啶盐(药物)在中枢神经系统中持续的方式。本文介绍了该新型药物的设计方法、合成、一些重要理化性质的研究、稳定性测定以及初步体内分布和效价评价。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Novel central nervous system targeted semisynthetic penicillins.

A novel series of semisynthetic penicillins was designed and synthesized. The compounds have as an integral part of the molecule a pyridinium <--> dihydropyridine redox system as a substituent at the 6-position. Esters of the dihydropyridine (pro-prodrug) forms of the drugs were expected, because of their pronounced lipophilic character, to easily penetrate biological membranes, including the blood-brain barrier, and to give rise to esters of polar pyridinium ions (prodrug) (via enzymic oxidation of the dihydropyridine moiety). The resulting ions were expected to be rapidly excreted from the periphery, but to be "locked" in the central nervous system; subsequent enzymic cleavage of the ester function was expected to release the free acid-pyridinium salts (drug) in the central nervous system in a sustained manner. The design approach, synthesis, study of some important physicochemical properties, stability determinations and preliminary in vivo distribution and potency evaluations of the novel drugs are described.

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