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首页> 外文期刊>Journal of Molecular Biology >Structural Basis for the Selective Inhibition of c-Jun N-Terminal Kinase 1 Determined by Rigid DARPin-DARPin Fusions
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Structural Basis for the Selective Inhibition of c-Jun N-Terminal Kinase 1 Determined by Rigid DARPin-DARPin Fusions

机译:由刚性Darpin-Darpin融合确定的C-JUN N-末端激酶1的选择性依据

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摘要

To untangle the complex signaling of the c-Jun N-terminal kinase (JNK) isoforms, we need tools that can selectively detect and inhibit individual isoforms. Because of the high similarity between JNK1, JNK2 and JNK3, it is very difficult to generate small-molecule inhibitors with this discriminatory power. Thus, we have recently selected protein binders from the designed ankyrin repeat protein (DARPin) library which were indeed isoform-specific inhibitors of JNK1 with low nanomolar potency. Here we provide the structural basis for their isotype discrimination and their inhibitory action. All our previous attempts to generate crystal structures of complexes had failed. We have now made use of a technology we recently developed which consists of rigid fusion of an additional special DARPin, which acts as a crystallization enhancer. This can be rigidly fused with different geometries, thereby generating a range of alternative crystal packings. The structures reveal the molecular basis for isoform specificity of the DARPins and their ability to prevent JNK activation and may thus form the basis of further investigation of the JNK family as well as novel approaches to drug design. (C) 2017 Elsevier Ltd. All rights reserved.
机译:为了解开C-JUM N-末端激酶(JNK)同种型的复杂信号,我们需要选择性地检测和抑制单个同种型的工具。由于JNK1,JNK2和JNK3之间的高相似性,因此具有这种歧视动力的小分子抑制剂是非常困难的。因此,我们最近选择了来自设计的ankyrin重复蛋白(Darpin)文库的蛋白质粘合剂,其实际上是具有低纳米摩尔效力的JNK1的特异性抑制剂。在这里,我们为其同种型歧视及其抑制作用提供了结构依据。我们以前的所有尝试都会产生复合物的晶体结构失败。我们现在已经利用了我们最近开发的技术,该技术包括额外的特殊Darpin的刚性融合,其作为结晶增强剂。这可以与不同的几何形状刚性熔合,从而产生一系列替代的晶体填料。该结构揭示了Darpins的同种型特异性的分子基础及其预防JNK激活的能力,因此可以构成JNK家族的进一步调查的基础,以及新的药物设计方法。 (c)2017 Elsevier Ltd.保留所有权利。

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