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Interaction of formin FH2 with skeletal muscle actin. EPR and DSC studies

机译:Formin FH2与骨骼肌肌动蛋白的相互作用。 EPR和DSC研究

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摘要

Formins are highly conserved proteins that are essential in the formation and regulation of the actin cytoskeleton. The formin homology 2 (FH2) domain is responsible for actin binding and acts as an important nucleating factor in eukaryotic cells. In this work EPR and DSC were used to investigate the properties of the mDia1-FH2 formin fragment and its interaction with actin. MDia1-FH2 was labeled with a maleimide spin probe (MSL). EPR results suggested that the MSL was attached to a single SH group in the FH2. In DSC and temperature-dependent EPR experiments we observed that mDia1-FH2 has a flexible structure and observed a major temperature-induced conformational change at 41 °C. The results also confirmed the previous observation obtained by fluorescence methods that formin binding can destabilize the structure of actin filaments. In the EPR experiments the intermolecular connection between the monomers of formin dimers proved to be flexible. Considering the complex molecular mechanisms underlying the cellular roles of formins this internal flexibility of the dimers is probably important for manifestation of their biological functions.Electronic supplementary materialThe online version of this article (doi:10.1007/s00249-013-0922-0) contains supplementary material, which is available to authorized users.
机译:福尔马林是高度保守的蛋白质,在肌动蛋白细胞骨架的形成和调节中必不可少。形式同源2(FH2)域负责肌动蛋白的结合,并作为真核细胞中的重要成核因子。在这项工作中,EPR和DSC用于研究mDia1-FH2甲酰胺片段的性质及其与肌动蛋白的相互作用。 MDia1-FH2用马来酰亚胺旋转探针(MSL)标记。 EPR结果表明,MSL与FH2中的单个SH组相连。在DSC和依赖温度的EPR实验中,我们观察到mDia1-FH2具有柔性结构,并在41°C下观察到了温度引起的主要构象变化。该结果还证实了先前通过荧光方法获得的观察结果,即形成有力的结合会破坏肌动蛋白丝的结构。在EPR实验中,甲醛二聚体的单体之间的分子间连接被证明是灵活的。考虑到Formins的细胞作用所基于的复杂分子机制,二聚体的这种内部灵活性可能对它们生物学功能的表现很重要。电子补充材料本文的在线版本(doi:10.1007 / s00249-013-0922-0)包含补充剂资料,可供授权用户使用。

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