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探索瘦素的折叠构象:对穿线途径的见解。

Exploring the folding landscape of leptin: Insights into threading pathways.

作者信息

da Silva Fernando Bruno, Simien Jennifer M, Viegas Rafael G, Haglund Ellinor, Leite Vitor Barbanti Pereira

机构信息

Centre of New Technologies, University of Warsaw, Banacha 2c, Warsaw, Poland; Institute of Biosciences, Humanities and Exact Sciences (IBILCE), São Paulo State University (UNESP), São José do Rio Preto, SP, Brazil.

Department of Chemistry, University of Hawaii at Manoa, Honolulu, Hawaii 96822, United States.

出版信息

J Struct Biol. 2024 Mar;216(1):108054. doi: 10.1016/j.jsb.2023.108054. Epub 2023 Dec 6.

DOI:10.1016/j.jsb.2023.108054
PMID:38065428
Abstract

The discovery of new protein topologies with entanglements and loop-crossings have shown the impact of local amino acid arrangement and global three-dimensional structures. This phenomenon plays a crucial role in understanding how protein structure relates to folding and function, affecting the global stability, and biological activity. Protein entanglements encompassing knots and non-trivial topologies add complexity to their folding free energy landscapes. However, the initial native contacts driving the threading event for entangled proteins remains elusive. The Pierced Lasso Topology (PLT) represents an entangled topology where a covalent linker creates a loop in which the polypeptide backbone is threaded through. Compared to true knotted topologies, PLTs are simpler topologies where the covalent-loop persists in all conformations. In this work, the PLT protein leptin, is used to visualize and differentiate the preference for slipknotting over plugging transition pathways along the folding route. We utilize the Energy Landscape Visualization Method (ELViM), a multidimensional projection technique, to visualize and distinguish early threaded conformations that cannot be observed in an in vitro experiment. Critical contacts for the leptin threading mechanisms were identified where the competing pathways are determined by the formation of a hairpin loop in the unfolded basin. Thus, prohibiting the dominant slipknotting pathway. Furthermore, ELViM offers insights into distinct folding pathways associated with slipknotting and plugging providing a novel tool for de novo design and in vitro experiments with residue specific information of threading events in silico.

摘要

具有缠结和环交叉的新蛋白质拓扑结构的发现,已显示出局部氨基酸排列和整体三维结构的影响。这一现象在理解蛋白质结构如何与折叠及功能相关、影响整体稳定性和生物活性方面起着关键作用。包含结和非平凡拓扑结构的蛋白质缠结增加了其折叠自由能景观的复杂性。然而,驱动缠结蛋白质穿线事件的初始天然接触仍然难以捉摸。穿孔套索拓扑结构(PLT)代表一种缠结拓扑结构,其中共价连接子形成一个环,多肽主链穿过该环。与真正的打结拓扑结构相比,PLT是更简单的拓扑结构,共价环在所有构象中都持续存在。在这项工作中,PLT蛋白瘦素被用于可视化和区分在折叠路径上滑结相对于堵塞转变途径的偏好。我们利用能量景观可视化方法(ELViM),一种多维投影技术,来可视化和区分在体外实验中无法观察到的早期穿线构象。确定了瘦素穿线机制的关键接触点,其中竞争途径由未折叠区域中发夹环的形成决定。因此,阻止了占主导地位的滑结途径。此外,ELViM提供了与滑结和堵塞相关的不同折叠途径的见解,为从头设计和体外实验提供了一种新颖的工具,该实验具有计算机模拟中穿线事件的残基特异性信息。

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Exploring the folding landscape of leptin: Insights into threading pathways.探索瘦素的折叠构象:对穿线途径的见解。
J Struct Biol. 2024 Mar;216(1):108054. doi: 10.1016/j.jsb.2023.108054. Epub 2023 Dec 6.
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Topological Reaction Coordinate Captures the Folding Transition State Ensemble in a Pierced Lasso Protein.拓扑反应坐标捕获穿孔套索蛋白中的折叠转变态集合。
J Phys Chem B. 2024 Jan 11;128(1):117-124. doi: 10.1021/acs.jpcb.3c06678. Epub 2023 Dec 20.
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Pierced Lasso Topology Controls Function in Leptin.穿孔套索拓扑结构控制瘦素的功能。
J Phys Chem B. 2017 Feb 2;121(4):706-718. doi: 10.1021/acs.jpcb.6b11506. Epub 2017 Jan 18.
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Pierced Lasso Bundles are a new class of knot-like motifs.穿孔套索束是一类新型的类结基序。
PLoS Comput Biol. 2014 Jun 19;10(6):e1003613. doi: 10.1371/journal.pcbi.1003613. eCollection 2014 Jun.
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Slipknotting upon native-like loop formation in a trefoil knot protein.三叶纽结蛋白中类似天然的环形成的套索。
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Effects of knots on protein folding properties.结对蛋白质折叠性质的影响。
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Engineering covalent loops in proteins can serve as an on/off switch to regulate threaded topologies.在蛋白质中构建共价环可作为一种开/关开关来调节螺旋拓扑结构。
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Experimental detection of knotted conformations in denatured proteins.变性蛋白质中纽结构象的实验检测。
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Topological Twists in Nature.自然界中的拓扑扭转。
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