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Molecular overlap in the regulation of SK channels by small molecules and phosphoinositides

机译:小分子和磷酸肌醇调节SK通道中的分子重叠

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摘要

Phosphatidylinositol 4,5-bisphosphate (PIP2) directly interacts with the small-conductance Ca2+-activated K+ 2-a (SK2-a) channel/calmodulin complex, serving as a critical element in the regulation of channel activity. We report that changes of protein conformation in close proximity to the PIP2 binding site induced by a small-molecule SK channel modulator, NS309, can effectively enhance the interaction between the protein and PIP2 to potentiate channel activity. This novel modulation of PIP2 sensitivity by small-molecule drugs is likely not to be limited in its application to SK channels, representing an intriguing strategy to develop drugs controlling the activity of the large number of PIP2-dependent proteins.
机译:磷脂酰肌醇4,5-二磷酸(PIP2)与小电导Ca 2 + 活化的K + 2-a(SK2-a)通道/钙调蛋白复合物直接相互作用,在调节频道活动方面起着至关重要的作用。我们报告说,由小分子SK通道调节剂NS309诱导的PIP2结合位点附近蛋白质构象的变化可以有效增强蛋白和PIP2之间的相互作用以增强通道活性。小分子药物对PIP2敏感性的这种新的调节作用可能不限于将其应用于SK通道,这代表了开发控制大量PIP2依赖性蛋白活性的药物的有趣策略。

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