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Role of Phosphorylation on the Structural Dynamics and Function of Types III and IV Intermediate Filaments

机译:磷酸化作用对III型和IV型中间丝的结构动力学和功能的作用

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摘要

Phosphorylation of types III and IV intermediate filaments (IFs) is known to regulate their organization and function. Phosphorylation of the amino-terminal head domain sites on types III and IV IF proteins plays a key role in the assembly/disassembly of IF subunits into 10 nm filaments, and influences the phosphorylation of sites on the carboxyl-terminal tail domain. These phosphorylation events are largely under the control of second messenger-dependent protein kinases and provide the cells a mechanism to reorganize the IFs in response to the changes in second messenger levels. In mitotic cells, Cdk1, Rho kinase, PAK1 and Aurora-B kinase are believed to regulate vimentin and glial fibrillary acidic protein phosphorylation in a spatio-temporal manner. In neurons, the carboxyl-terminal tail domains of the NF-M and NF-H subunits of heteropolymeric neurofilaments (NFs) are highly phosphorylated by proline-directed protein kinases. The phosphorylation of carboxyl-terminal tail domains of NFs has been suspected to play roles in forming cross-bridges between NFs and microtubules, slowing axonal transport and promoting their integration into cytoskeleton lattice and, in doing so, to control axonal caliber and stabilize the axon. The role of IF phosphorylation in disease pathobiology is discussed.
机译:已知III型和IV型中间丝(IF)的磷酸化可调节其组织和功能。 III型和IV型IF蛋白上氨基末端头部结构域位点的磷酸化在IF亚基组装/拆卸成10 nm细丝中起关键作用,并影响羧基末端尾部结构域上位点的磷酸化。这些磷酸化事件在很大程度上受第二信使依赖性蛋白激酶的控制,并为细胞提供了一种机制,以响应于第二信使水平的变化而重组IF。在有丝分裂细胞中,Cdk1,Rho激酶,PAK1和Aurora-B激酶被认为以时空方式调节波形蛋白和神经胶质纤维酸性蛋白的磷酸化。在神经元中,脯氨酸定向蛋白激酶将杂聚神经丝(NFs)NF-M和NF-H亚基的羧基末端尾域高度磷酸化。怀疑NFs的羧基末端尾结构域的磷酸化在NFs和微管之间形成跨桥,减慢轴突运输并促进它们整合到细胞骨架晶格中发挥作用,并在此过程中控制轴突口径并稳定轴突。 。讨论了IF磷酸化在疾病病理生物学中的作用。

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