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Drebrin 含有一种隐蔽的 F-肌动蛋白成束活性,受 Cdk5 磷酸化调节。

Drebrin contains a cryptic F-actin-bundling activity regulated by Cdk5 phosphorylation.

机构信息

Medical Research Council MRC Centre for Developmental Neurobiology, King's College London, London SE1 1UL, England, UK.

出版信息

J Cell Biol. 2013 Sep 2;202(5):793-806. doi: 10.1083/jcb.201303005. Epub 2013 Aug 26.

Abstract

Drebrin is an actin filament (F-actin)-binding protein with crucial roles in neuritogenesis and synaptic plasticity. Drebrin couples dynamic microtubules to F-actin in growth cone filopodia via binding to the microtubule-binding +TIP protein EB3 and organizes F-actin in dendritic spines. Precisely how drebrin interacts with F-actin and how this is regulated is unknown. We used cellular and in vitro assays with a library of drebrin deletion constructs to map F-actin binding sites. We discovered two domains in the N-terminal half of drebrin-a coiled-coil domain and a helical domain-that independently bound to F-actin and cooperatively bundled F-actin. However, this activity was repressed by an intramolecular interaction relieved by Cdk5 phosphorylation of serine 142 located in the coiled-coil domain. Phospho-mimetic and phospho-dead mutants of serine 142 interfered with neuritogenesis and coupling of microtubules to F-actin in growth cone filopodia. These findings show that drebrin contains a cryptic F-actin-bundling activity regulated by phosphorylation and provide a mechanistic model for microtubule-F-actin coupling.

摘要

布雷布林是一种肌动蛋白丝(F-actin)结合蛋白,在神经突生成和突触可塑性中具有关键作用。布雷布林通过与微管结合+TIP 蛋白 EB3 结合,将动态微管与生长锥丝状伪足中的 F-actin 偶联,并在树突棘中组织 F-actin。布雷布林如何与 F-actin 相互作用以及这种相互作用如何被调节尚不清楚。我们使用包含布雷布林缺失构建体文库的细胞和体外测定法来绘制 F-actin 结合位点。我们在布雷布林的 N 端半部分发现了两个结构域——一个卷曲螺旋结构域和一个螺旋结构域——它们可以独立地与 F-actin 结合,并协同地将 F-actin 束集在一起。然而,这种活性被位于卷曲螺旋结构域中的丝氨酸 142 的 Cdk5 磷酸化所解除的分子内相互作用所抑制。丝氨酸 142 的磷酸模拟和磷酸缺失突变体干扰了神经突的生成以及生长锥丝状伪足中微管与 F-actin 的偶联。这些发现表明布雷布林含有一个受磷酸化调节的隐蔽的 F-actin 束集活性,并为微管-F-actin 偶联提供了一种机制模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4a91/3760615/9edb72515b18/JCB_201303005_Fig1.jpg

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