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Spatial regulation of coalesced protein assemblies: Lessons from yeast to diseases

机译:融合蛋白装配体的空间调控:从酵母到疾病的经验教训

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ABSTRACT Organisms rely on correctly folded proteins to carry out essential functions. Protein?quality control?factors guard proteostasis and prevent protein misfolding. When quality control fails and in response to diverse stresses, many proteins start to accumulate at specific deposit sites that maintain cellular organization and?protect the functionality of coalescing proteins. These transitions involve dedicated proteins that promote coalescence and are facilitated by endo-membranes and cytoskeletal platforms. Moreover, several proteins make use of weak multivalent interactions or conformational templating to drive the formation of large-scale assemblies. Formation of such assemblies is often associated with a change in biochemical activity that can be used by cells to execute biochemical decisions in a localized manner during development and adaption. Since all assembly types impact cell physiology, their localization and dynamics need to be tightly regulated. Interestingly, at least some of the regulatory mechanisms are shared by functional membrane-less organelles and assemblies of terminally aggregated proteins. Furthermore, constituents of functional assemblies can aggregate and become non-functional during aging. Here we present the current knowledge as to how coalescing protein assemblies are spatially organized in cells and we postulate that failures in their spatial confinement might underscore certain aspects of aging and neurodegenerative diseases.
机译:摘要生物体依靠正确折叠的蛋白质来执行基本功能。蛋白质质量控​​制因素可保护蛋白质稳定并防止蛋白质错误折叠。当质量控制失败并响应各种压力时,许多蛋白质开始在特定的沉积位点积聚,这些沉积位点可维持细胞组织并保护聚结蛋白质的功能。这些过渡涉及促进结缔并由内膜和细胞骨架平台促进的专用蛋白质。而且,几种蛋白质利用弱的多价相互作用或构象模板来驱动大规模装配体的形成。这种装配体的形成通常与生化活性的改变有关,细胞可以利用其发生变化以在发育和适应过程中以局部方式执行生化决定。由于所有组装类型都会影响细胞生理,因此必须严格调节其定位和动力学。有趣的是,至少一些调节机制被功能性无膜细胞器和末端聚集蛋白的装配体所共有。此外,功能组件的组成会在老化过程中聚集并失去功能。在这里,我们介绍了有关凝聚蛋白组装在细胞中如何在空间上组织的最新知识,并且我们假设它们在空间上的局限性可能强调衰老和神经退行性疾病的某些方面。

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