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Lipid-independent control of endothelial and neuronal TRPC3 channels by light

机译:光对内皮和神经元TRPC3通道的脂质非依赖性控制

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摘要

Lipid-gated TRPC channels are highly expressed in cardiovascular and neuronal tissues. Exerting precise pharmacological control over their activity in native cells is expected to serve as a basis for the development of novel therapies. Here we report on a new photopharmacological tool that enables manipulation of TRPC3 channels by light, in a manner independent of lipid metabolism and with higher temporal precision than lipid photopharmacology. Using the azobenzene photoswitch moiety, we modified GSK1702934A to generate light-controlled TRPC agonists. We obtained one light-sensitive molecule (OptoBI-1) that allows us to exert efficient, light-mediated control over TRPC3 activity and the associated cellular Ca2+ signaling. OptoBI-1 enabled high-precision, temporal control of TRPC3-linked cell functions such as neuronal firing and endothelial Ca2+ transients. With these findings, we introduce a novel photopharmacological strategy to control native TRPC conductances.
机译:脂质门控的TRPC通道在心血管和神经元组织中高度表达。对其天然细胞中的活性进行精确的药理控制,有望作为开发新疗法的基础。在这里,我们报告了一种新的光药理学工具,该工具可以通过光来操纵TRPC3通道,其方式独立于脂质代谢,并且具有比脂质光药理学更高的时间精度。使用偶氮苯光电开关部分,我们修饰了GSK1702934A以产生光控TRPC激动剂。我们获得了一个光敏分子(OptoBI-1),它使我们能够对TRPC3活性和相关的细胞Ca 2 + 信号进行有效的光介导控制。 OptoBI-1可以对TRPC3连接的细胞功能(如神经元放电和内皮Ca 2 + 瞬态)进行高精度的时间控制。有了这些发现,我们介绍了一种新颖的光药理学策略来控制天然TRPC电导。

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