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溶酶体离子通道在溶酶体功能障碍中的作用。

The role of lysosomal ion channels in lysosome dysfunction.

机构信息

Department of Biomedical and Pharmaceutical Sciences, Center for Environmental Health Sciences, University of Montana, Missoula, MT, USA.

出版信息

Inhal Toxicol. 2021 Feb;33(2):41-54. doi: 10.1080/08958378.2021.1876188. Epub 2021 Feb 25.

Abstract

Lysosomes offer a unique arrangement of degradative, exocytic, and signaling capabilities that make their continued function critical to cellular homeostasis. Lysosomes owe their function to the activity of lysosomal ion channels and transporters, which maintain concentration gradients of H, K, Ca, Na, and Cl across the lysosomal membrane. This review examines the contributions of lysosomal ion channels to lysosome function, showing how ion channel function is integral to degradation and autophagy, maintaining lysosomal membrane potential, controlling Ca signaling, and facilitating exocytosis. Evidence of lysosome dysfunction in a variety of disease pathologies creates a need to understand how lysosomal ion channels contribute to lysosome dysfunction. For example, the loss of function of the TRPML1 Ca lysosome channel in multiple lysosome storage diseases leads to lysosome dysfunction and disease pathogenesis while neurodegenerative diseases are marked by lysosome dysfunction caused by changes in ion channel activity through the TRPML1, TPC, and TMEM175 ion channels. Autoimmune disease is marked by dysregulated autophagy, which is dependent on the function of multiple lysosomal ion channels. Understanding the role of lysosomal ion channel activity in lysosome membrane permeability and NLRP3 inflammasome activation could provide valuable mechanistic insight into NLRP3 inflammasome-mediated diseases. Finally, this review seeks to show that understanding the role of lysosomal ion channels in lysosome dysfunction could give mechanistic insight into the efficacy of certain drug classes, specifically those that target the lysosome, such as cationic amphiphilic drugs.

摘要

溶酶体提供了独特的降解、外排和信号转导能力,使其持续的功能对细胞内稳态至关重要。溶酶体的功能归功于溶酶体离子通道和转运体的活性,它们维持着 H、K、Ca、Na 和 Cl 跨溶酶体膜的浓度梯度。这篇综述考察了溶酶体离子通道对溶酶体功能的贡献,展示了离子通道功能如何与降解和自噬、维持溶酶体膜电位、控制 Ca 信号以及促进外排等过程密不可分。各种疾病病理中溶酶体功能障碍的证据表明,需要了解溶酶体离子通道如何导致溶酶体功能障碍。例如,多种溶酶体贮积病中 TRPML1 Ca 溶酶体通道的功能丧失导致溶酶体功能障碍和疾病发病机制,而神经退行性疾病则以 TRPML1、TPC 和 TMEM175 离子通道的离子通道活性变化引起的溶酶体功能障碍为特征。自身免疫性疾病的特点是自噬失调,这依赖于多种溶酶体离子通道的功能。了解溶酶体离子通道活性在溶酶体膜通透性和 NLRP3 炎性小体激活中的作用,可以为 NLRP3 炎性小体介导的疾病提供有价值的机制见解。最后,本综述旨在表明,了解溶酶体离子通道在溶酶体功能障碍中的作用,可以为某些药物类别的疗效提供机制见解,特别是那些靶向溶酶体的药物,如阳离子两亲性药物。

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