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小盘基网柄菌肌球蛋白轻链MlcB的结构为了解肌球蛋白B的IQ模体识别提供了线索。

Structure of the small Dictyostelium discoideum myosin light chain MlcB provides insights into MyoB IQ motif recognition.

作者信息

Liburd Janine, Chitayat Seth, Crawley Scott W, Munro Kim, Miller Emily, Denis Chris M, Spencer Holly L, Côté Graham P, Smith Steven P

机构信息

From the Department of Biomedical and Molecular Sciences and.

the Protein Function Discovery Group, Queen's University, Kingston, Ontario K7L 3N6, Canada.

出版信息

J Biol Chem. 2014 Jun 13;289(24):17030-42. doi: 10.1074/jbc.M113.536532. Epub 2014 May 1.

Abstract

Dictyostelium discoideum MyoB is a class I myosin involved in the formation and retraction of membrane projections, cortical tension generation, membrane recycling, and phagosome maturation. The MyoB-specific, single-lobe EF-hand light chain MlcB binds the sole IQ motif of MyoB with submicromolar affinity in the absence and presence of Ca(2+). However, the structural features of this novel myosin light chain and its interaction with its cognate IQ motif remain uncharacterized. Here, we describe the NMR-derived solution structure of apoMlcB, which displays a globular four-helix bundle. Helix 1 adopts a unique orientation when compared with the apo states of the EF-hand calcium-binding proteins calmodulin, S100B, and calbindin D9k. NMR-based chemical shift perturbation mapping identified a hydrophobic MyoB IQ binding surface that involves amino acid residues in helices I and IV and the functional N-terminal Ca(2+) binding loop, a site that appears to be maintained when MlcB adopts the holo state. Complementary mutagenesis and binding studies indicated that residues Ile-701, Phe-705, and Trp-708 of the MyoB IQ motif are critical for recognition of MlcB, which together allowed the generation of a structural model of the apoMlcB-MyoB IQ complex. We conclude that the mode of IQ motif recognition by the novel single-lobe MlcB differs considerably from that of stereotypical bilobal light chains such as calmodulin.

摘要

盘基网柄菌MyoB是一种I类肌球蛋白,参与膜突起的形成与回缩、皮质张力产生、膜循环以及吞噬体成熟过程。在有无Ca(2+)的情况下,MyoB特异性的单叶EF手型轻链MlcB以亚微摩尔亲和力结合MyoB唯一的IQ模体。然而,这种新型肌球蛋白轻链的结构特征及其与同源IQ模体的相互作用仍未得到表征。在此,我们描述了脱辅基MlcB的核磁共振衍生溶液结构,其呈现出球状四螺旋束结构。与EF手型钙结合蛋白钙调蛋白、S100B和钙结合蛋白D9k的脱辅基状态相比,螺旋1呈现出独特的取向。基于核磁共振的化学位移扰动图谱确定了一个疏水的MyoB IQ结合表面,该表面涉及螺旋I和IV中的氨基酸残基以及功能性N端Ca(2+)结合环,当MlcB处于全蛋白状态时,该位点似乎得以保留。互补的诱变和结合研究表明,MyoB IQ模体的Ile-701、Phe-705和Trp-708残基对于识别MlcB至关重要,这共同促成了脱辅基MlcB-MyoB IQ复合物的结构模型的生成。我们得出结论,新型单叶MlcB识别IQ模体的模式与典型的双叶轻链如钙调蛋白有很大不同。

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