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首页> 外文期刊>Angewandte Chemie >Esterase-Sensitive Prodrugs with Tunable Release Rates and Direct Generation of Hydrogen Sulfide
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Esterase-Sensitive Prodrugs with Tunable Release Rates and Direct Generation of Hydrogen Sulfide

机译:具有可调释放速率和直接生成硫化氢的酯酶敏感性前药

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摘要

Prodrugs that release hydrogen sulfide upon esterase-mediated cleavage of an ester group followed by lactonization are described herein. By modifying the ester group and thus its susceptibility to esterase, and structural features critical to the lactonization rate, H2S release rates can be tuned. Such prodrugs directly release hydrogen sulfide without the involvement of perthiol species, which are commonly encountered with existing H2S donors. Additionally, such prodrugs can easily be conjugated to another non-steroidal anti-inflammatory agent, leading to easy synthesis of hybrid prodrugs. As a biological validation of the H2S prodrugs, the anti-inflammatory effects of one such prodrug were examined by studying its ability to inhibit LPS-induced TNF- production in RAW 264.7 cells. This type of H2S prodrugs shows great potential as both research tools and therapeutic agents.
机译:本文描述了在酯酶介导的酯基裂解后内酯化后释放硫化氢的前药。通过修饰酯基及其对酯酶的敏感性以及对内酯化速率至关重要的结构特征,可以调节H2S的释放速率。此类前药可直接释放硫化氢,而不会涉及现有的H2S供体通常遇到的过硫醇物质。另外,这些前药可以容易地与另一种非甾体抗炎剂结合,从而导致容易合成杂合前药。作为H2S前药的生物学验证,通过研究一种这样的前药在RAW 264.7细胞中抑制LPS诱导的TNF生成的能力来检查其抗炎作用。这种H2S前药作为研究工具和治疗剂均显示出巨大的潜力。

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