Effect of Pathogenic Mutations on the Formation of High-Order Dynamin 2 Assemblies in Living Cells

IF 2.9 3区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY Biochemistry Biochemistry Pub Date : 2024-10-10 DOI:10.1021/acs.biochem.4c0026210.1021/acs.biochem.4c00262
Per Niklas Hedde, Songning Zhu, Barbara Barylko, Chi-Li Chiu, Luke T. Nelson, Michelle A. Digman, Joseph P. Albanesi, Nicholas G. James* and David M. Jameson*, 
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Abstract

Mutations in dynamin 2 (DNM2) have been associated with two distinct movement disorders: Charcot-Marie-Tooth neuropathies (CMT) and centronuclear myopathy (CNM). Most of these mutations are clustered in the pleckstrin homology domain (PHD), which engages in intramolecular interactions that limit dynamin self-assembly and GTPase activation. CNM mutations interfere with these intramolecular interactions and suppress the formation of the autoinhibited state. CMT mutations are located primarily on the opposite surface of the PHD, which is specialized for phosphoinositide binding. It has been speculated that the distinct locations and interactions of residues mutated in CMT and CNM explain why each set of mutations causes either one disease or the other, despite their close proximity within the PHD sequence. We previously reported that at least one CMT-causing mutant, lacking residues 555DEE557 (ΔDEE), displays the same inability to undergo autoinhibition as observed in CNM-linked mutants. Here, we show that both the DNM2ΔDEE and CNM-linked DNM2A618T mutants form larger and more stable structures on the plasma membrane than that of wild-type DNM2 (DNM2WT). However, DNM2A618T forms cytoplasmic inclusions at concentrations lower than those of either DNM2WT or DNM2ΔDEE, suggesting that CNM-linked mutations confer more severe gain-of-function properties than the ΔDEE mutation.

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致病突变对活细胞中高阶 Dynamin 2 组装形成的影响
dynamin 2(DNM2)的突变与两种不同的运动障碍有关:Charcot-Marie-Tooth 神经病(CMT)和中心核肌病(CNM)。这些突变大多集中在pleckstrin 同源结构域(PHD),该结构域参与分子内相互作用,从而限制了达因明的自组装和 GTPase 激活。CNM 突变会干扰这些分子内相互作用,抑制自抑制状态的形成。CMT 突变主要位于 PHD 的反面,专门用于磷脂结合。有人推测,CMT 和 CNM 中突变残基的不同位置和相互作用解释了为什么每一组突变都会导致一种疾病或另一种疾病,尽管它们在 PHD 序列中非常接近。我们以前曾报道过,至少有一种缺乏 555DEE557 (ΔDEE) 残基的 CMT 致病突变体显示出与 CNM 相关突变体中观察到的相同的自抑制能力。在这里,我们发现与野生型 DNM2(DNM2WT)相比,DNM2ΔDEE 突变体和 CNM 连接的 DNM2A618T 突变体在质膜上形成的结构更大、更稳定。然而,与 DNM2WT 或 DNM2ΔDEE 相比,DNM2A618T 在浓度较低时也会形成细胞质内含物,这表明与 CNM 相连的突变体比ΔDEE 突变体具有更严重的功能增益特性。
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来源期刊
Biochemistry Biochemistry
Biochemistry Biochemistry 生物-生化与分子生物学
CiteScore
5.50
自引率
3.40%
发文量
336
审稿时长
1-2 weeks
期刊介绍: Biochemistry provides an international forum for publishing exceptional, rigorous, high-impact research across all of biological chemistry. This broad scope includes studies on the chemical, physical, mechanistic, and/or structural basis of biological or cell function, and encompasses the fields of chemical biology, synthetic biology, disease biology, cell biology, nucleic acid biology, neuroscience, structural biology, and biophysics. In addition to traditional Research Articles, Biochemistry also publishes Communications, Viewpoints, and Perspectives, as well as From the Bench articles that report new methods of particular interest to the biological chemistry community.
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