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首页> 外文期刊>Nature Communications >Cellular delivery and photochemical release of a caged inositol-pyrophosphate induces PH-domain translocation in cellulo
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Cellular delivery and photochemical release of a caged inositol-pyrophosphate induces PH-domain translocation in cellulo

机译:关进笼中的肌醇焦磷酸的细胞传递和光化学释放诱导纤维素中PH结构域的移位。

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Inositol pyrophosphates, such as diphospho-myo-inositol pentakisphosphates (InsP7), are an important family of signalling molecules, implicated in many cellular processes and therapeutic indications including insulin secretion, glucose homeostasis and weight gain. To understand their cellular functions, chemical tools such as photocaged analogues for their real-time modulation in cells are required. Here we describe a concise, modular synthesis of InsP7 and caged InsP7. The caged molecule is stable and releases InsP7 only on irradiation. While photocaged InsP7 does not enter cells, its cellular uptake is achieved using nanoparticles formed by association with a guanidinium-rich molecular transporter. This novel synthesis and unprecedented polyphosphate delivery strategy enable the first studies required to understand InsP7 signalling in cells with controlled spatiotemporal resolution. It is shown herein that cytoplasmic photouncaging of InsP7 leads to translocation of the PH-domain of Akt, an important signalling-node kinase involved in glucose homeostasis, from the membrane into the cytoplasm.
机译:肌醇焦磷酸酯,如二磷酸-肌-肌醇五磷酸酯(InsP 7 )是重要的信号分子家族,与许多细胞过程和治疗指征有关,包括胰岛素分泌,葡萄糖稳态和体重增加。为了了解它们的细胞功能,需要化学工具(例如光笼式类似物)对其细胞进行实时调节。在这里,我们描述了InsP 7 和笼状InsP 7 的简洁模块化合成。笼状分子是稳定的,仅在照射时才释放InsP 7 。虽然光笼InsP 7 不会进入细胞,但其细胞摄取是通过与富含胍的分子转运蛋白缔合而形成的纳米颗粒实现的。这种新颖的合成方法和前所未有的多磷酸盐递送策略使人们能够进行首次研究,以了解具有受控时空分辨率的细胞中的InsP 7 信号传导。本文显示InsP 7 的胞质光解开导致Akt的PH结构域从膜进入细胞质,Akt的PH结构域是参与葡萄糖稳态的重要信号节点激酶。

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