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Insights into the activity control of the kallikrein-related peptidase 6: small-molecule modulators and allosterism

机译:洞察Kallikrein相关肽酶6的活性控制:小分子调节剂和变色症

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The activity of kallikrein-related peptidase 6 (KLK6) is deregulated in various diseases such as cancer and neurodegenerative diseases. KLK6 is thus considered as an attractive therapeutical target. In this short report, we depict some novel findings on the regulation of the KLK6 activity. Namely, we identified mechanism-based inhibitors (suicide substrates) from an in-house library of 6-substituted coumarin-3-carboxylate derivatives. In addition, a molecular dynamics study evidenced the allosteric behavior of KLK6 similar to that previously observed for some trypsin-like serine proteases. This allosteric behavior together with the coumarinic scaffold bring new opportunities for the design of KLK6 potent activity modulators, useful as therapeutics or activity-based probes.
机译:Kallikrein相关的肽酶6(KLK6)的活性在各种疾病中取消注入癌症和神经变性疾病。 因此,KLK6被认为是有吸引力的治疗目标。 在这次简短的报告中,我们描绘了关于KLK6活动的监管的一些新发现。 即,我们鉴定了来自6取代的香豆素-3-羧酸酯衍生物的内部文库的机制基抑制剂(自杀基质)。 此外,分子动力学研究证明了KLK6类似于以前观察到的一些胰蛋白酶样丝氨酸蛋白酶的变构行为。 这种变构行为与香豆素脚手架一起为KLK6强效活动调制器设计提供了新的机会,可用作治疗剂或基于活性的探针。

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