Molecular insights into the phase transition of lysozyme into amyloid nanostructures: Implications of therapeutic strategies in diverse pathological conditions

IF 15.9 1区 化学 Q1 CHEMISTRY, PHYSICAL Advances in Colloid and Interface Science Pub Date : 2024-05-23 DOI:10.1016/j.cis.2024.103205
Sindhujit Roy , Venkat Ramanan Srinivasan , Subash Arunagiri , Nishant Mishra , Anubhuti Bhatia , Kiran P. Shejale , Kailash Prasad Prajapati , Karunakar Kar , Bibin Gnanadhason Anand
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Abstract

Lysozyme, a well-known bacteriolytic enzyme, exhibits a fascinating yet complex behavior when it comes to protein aggregation. Under certain conditions, this enzyme undergoes flexible transformation, transitioning from partially unfolded intermediate units of native conformers into complex cross-β-rich nano fibrillar amyloid architectures. Formation of such lysozyme amyloids has been implicated in a multitude of pathological and medical severities, like hepatic dysfunction, hepatomegaly, splenic rupture as well as spleen dysfunction, nephropathy, sicca syndrome, renal dysfunction, renal amyloidosis, and systemic amyloidosis. In this comprehensive review, we have attempted to provide in-depth insights into the aggregating behavior of lysozyme across a spectrum of variables, including concentrations, temperatures, pH levels, and mutations. Our objective is to elucidate the underlying mechanisms that govern lysozyme's aggregation process and to unravel the complex interplay between its structural attributes. Moreover, this work has critically examined the latest advancements in the field, focusing specifically on novel strategies and systems, that have been implemented to delay or inhibit the lysozyme amyloidogenesis. Apart from this, we have tried to explore and advance our fundamental understanding of the complex processes involved in lysozyme aggregation. This will help the research community to lay a robust foundation for screening, designing, and formulating targeted anti-amyloid therapeutics offering improved treatment modalities and interventions not only for lysozyme-linked amyloidopathy but for a wide range of amyloid-related disorders.

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溶菌酶相变为淀粉样蛋白纳米结构的分子见解:不同病理条件下治疗策略的意义
溶菌酶是一种著名的细菌溶解酶,在蛋白质聚集方面表现出迷人而复杂的行为。在特定条件下,这种酶会发生灵活的转变,从部分展开的原生构象中间单元过渡到复杂的富含交叉β的纳米纤维淀粉样结构。溶菌酶淀粉样蛋白的形成与多种病理和医学症状有关,如肝功能障碍、肝肿大、脾破裂以及脾功能障碍、肾病、疱疹综合征、肾功能障碍、肾淀粉样变性和全身性淀粉样变性。在这篇综述中,我们试图深入探讨溶菌酶在各种变量下的聚集行为,包括浓度、温度、pH 值和突变。我们的目标是阐明溶菌酶聚集过程的基本机制,并揭示其结构属性之间复杂的相互作用。此外,这项工作还对该领域的最新进展进行了批判性研究,尤其侧重于新的策略和系统,这些策略和系统已被用于延迟或抑制溶菌酶淀粉样蛋白的生成。除此之外,我们还试图探索和推进对溶菌酶聚集所涉及的复杂过程的基本理解。这将有助于研究界为筛选、设计和制定有针对性的抗淀粉样蛋白疗法奠定坚实的基础,不仅为溶菌酶相关淀粉样蛋白病,而且为各种淀粉样蛋白相关疾病提供更好的治疗方法和干预措施。
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来源期刊
CiteScore
28.50
自引率
2.60%
发文量
175
审稿时长
31 days
期刊介绍: "Advances in Colloid and Interface Science" is an international journal that focuses on experimental and theoretical developments in interfacial and colloidal phenomena. The journal covers a wide range of disciplines including biology, chemistry, physics, and technology. The journal accepts review articles on any topic within the scope of colloid and interface science. These articles should provide an in-depth analysis of the subject matter, offering a critical review of the current state of the field. The author's informed opinion on the topic should also be included. The manuscript should compare and contrast ideas found in the reviewed literature and address the limitations of these ideas. Typically, the articles published in this journal are written by recognized experts in the field.
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