首页> 外文期刊>Journal of Medicinal Chemistry >Evaluation of P_1'-Diversified Phosphinic Peptides Leads to the Development of Highly Selective Inhibitors of MMP-11
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Evaluation of P_1'-Diversified Phosphinic Peptides Leads to the Development of Highly Selective Inhibitors of MMP-11

机译:P_1'多样化的膦肽的评估导致对MMP-11的高选择性抑制剂的发展。

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摘要

Phosphinic peptides were previously reported to be potent inhibitors of several matrixins (MMPs). To identify more selective inhibitors of MMP-11, a matrixin overexpressed in breast cancer, a series of phosphinic pseudopeptides bearing a variety of P_1'-side chains has been synthesized, by parallel diversification of a phosphinic template. The potencies of these compounds were evaluated against a set of seven MMPs (MMP-2, MMP-7, MMP-8, MMP-9, MMP-11, MMP-13, and MMP-14). The chemical strategy applied led to the identification of several phosphinic inhibitors displaying high selectivity toward MMP-11. One of the most selective inhibitors of MMP-11 in this series, compound 22, exhibits a K_i value of 0.23 μM toward MMP-11, while its potency toward the other MMPs tested is 2 orders of magnitude lower. This remarkable selectivity may rely on interactions of the P_1'-side chain atoms of these inhibitors with residues located at the entrance of the S_1'-cavity of MMP-11. The design of inhibitors able to interact with residues located at the entrance of MMPs' S_1'-cavity might represent an alternative strategy to identify selective inhibitors that will fully differentiate one MMP among the others.
机译:以前已报道膦肽是几种基质蛋白(MMP)的有效抑制剂。为了鉴定在乳腺癌中过度表达的基质蛋白MMP-11的更多选择性抑制剂,通过平行地使膦酸酯模板多样化,已经合成了一系列带有多种P_1'侧链的膦酸酯假肽。针对一组七个MMP(MMP-2,MMP-7,MMP-8,MMP-9,MMP-11,MMP-13和MMP-14)评估了这些化合物的效力。所采用的化学策略导致鉴定出几种对MMP-11具有高选择性的次膦酸酯抑制剂。该系列中最有选择性的MMP-11抑制剂之一化合物22对MMP-11的K_i值为0.23μM,而对其他测试的MMP的效力则低2个数量级。这种显着的选择性可能取决于这些抑制剂的P_1'侧链原子与位于MMP-11 S_1'腔入口处的残基的相互作用。能够与MMP的S_1'腔入口处的残基相互作用的抑制剂的设计可能代表了另一种策略,该方法可以识别选择性抑制剂,从而完全区分一种MMP。

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