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首页> 外文期刊>Science China Life Sciences >Regulation of lysosomal ion homeostasis by channels and transporters
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Regulation of lysosomal ion homeostasis by channels and transporters

机译:通过通道和转运蛋白调节溶酶体离子稳态

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Lysosomes are the major organelles that carry out degradation functions. They integrate and digest materials compartmentalized by endocytosis, phagocytosis or autophagy. In addition to more than 60 hydrolases residing in the lysosomes, there are also ion channels and transporters that mediate the flux or transport of H+, Ca2+, Na+, K+, and Cl- across the lysosomal membranes. Defects in ionic exchange can lead to abnormal lysosome morphology, defective vesicle trafficking, impaired autophagy, and diseases such as neurodegeneration and lysosomal storage disorders. The latter are characterized by incomplete lysosomal digestion and accumulation of toxic materials inside enlarged intracellular vacuoles. In addition to degradation, recent studies have revealed the roles of lysosomes in metabolic pathways through kinases such as mechanistic target of rapamycin (mTOR) and transcriptional regulation through calcium signaling molecules such as transcription factor EB (TFEB) and calcineurin. Owing to the development of new approaches including genetically encoded fluorescence probes and whole endolysosomal patch clamp recording techniques, studies on lysosomal ion channels have made remarkable progress in recent years. In this review, we will focus on the current knowledge of lysosome-resident ion channels and transporters, discuss their roles in maintaining lysosomal function, and evaluate how their dysfunction can result in disease.
机译:溶酶体是执行降解功能的主要细胞器。它们整合并消化通过内吞,吞噬或自噬分隔的物质。除了溶酶体中存在60多种水解酶外,还存在离子通道和转运蛋白,它们介导H + ,Ca 2 + ,Na + ,K + 和Cl -穿过溶酶体膜。离子交换缺陷可导致溶酶体形态异常,囊泡运输不良,自噬受损以及神经退行性疾病和溶酶体贮积病等疾病。后者的特征是不完全的溶酶体消化和有毒物质在扩大的细胞内液泡内积累。除降解外,最近的研究还显示了溶酶体在激酶等雷帕霉素(mTOR)的机械靶标以及通过钙信号分子如转录因子EB(TFEB)和钙调神经磷酸酶的转录调控中的代谢途径中的作用。由于新方法的发展,包括基因编码的荧光探针和完整的溶酶体膜片钳记录技术,近年来对溶酶体离子通道的研究取得了显着进展。在这篇综述中,我们将重点关注溶酶体中离子通道和转运蛋白的最新知识,讨论它们在维持溶酶体功能中的作用,并评估其功能障碍如何导致疾病。

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