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A Stapled Peptide Mimic of the Pseudosubstrate Inhibitor PKI Inhibits Protein Kinase A

机译:伪底物抑制剂PKI的拟订好的肽模拟物抑制蛋白激酶A。

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摘要

Kinases regulate multiple and diverse signaling pathways and misregulation is implicated in a multitude of diseases. Although significant efforts have been put forth to develop kinase-specific inhibitors, specificity remains a challenge. As an alternative to catalytic inhibition, allosteric inhibitors can target areas on the surface of an enzyme, thereby providing additional target diversity. Using cAMP-dependent protein kinase A (PKA) as a model system, we sought to develop a hydrocarbon-stapled peptide targeting the pseudosubstrate domain of the kinase. A library of peptides was designed from a Protein Kinase Inhibitor (PKI), a naturally encoded protein that serves as a pseudosubstrate inhibitor for PKA. The binding properties of these peptide analogs were characterized by fluorescence polarization and surface plasmon resonance, and two compounds were identified with KD values in the 500–600 pM range. In kinase activity assays, both compounds demonstrated inhibition with 25–35 nM IC50 values. They were also found to permeate cells and localize within the cytoplasm and inhibited PKA activity within the cellular environment. To the best of our knowledge, these stapled peptide inhibitors represent some of the highest affinity binders reported to date for hydrocarbon stapled peptides.
机译:激酶调节多种多样的信号传导途径,并且调节失调与多种疾病有关。尽管为开发激酶特异性抑制剂付出了巨大的努力,但是特异性仍然是一个挑战。作为催化抑制的替代方法,变构抑制剂可以靶向酶表面的区域,从而提供额外的靶多样性。使用依赖cAMP的蛋白激酶A(PKA)作为模型系统,我们试图开发靶向该激酶假底物结构域的烃类固定肽。从蛋白激酶抑制剂(PKI)设计肽库,PKI是一种天然编码的蛋白,可作为PKA的假底物抑制剂。这些肽类似物的结合特性通过荧光偏振和表面等离振子共振来表征,并且鉴定出两种化合物的KD值在500–600 pM范围内。在激酶活性测定中,两种化合物均显示出25-35 nM IC50值的抑制作用。还发现它们渗透细胞并定位于细胞质内,并抑制了细胞环境中的PKA活性。据我们所知,这些固定肽抑制剂代表了迄今为止报道的某些烃固定肽的最高亲和力粘合剂。

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