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α-突触核蛋白半衰期之谜。

The αSynuclein half-life conundrum.

机构信息

UK Dementia Research Institute at University College London, London, United Kingdom.

Department of Biology, University of Padova, Padova, Italy; Centro Studi per la Neurodegenerazione (CESNE), University of Padova, Padova, Italy.

出版信息

Neurobiol Dis. 2024 Jun 15;196:106524. doi: 10.1016/j.nbd.2024.106524. Epub 2024 May 4.

Abstract

αSynuclein (αSyn) misfolding and aggregation frequently precedes neuronal loss associated with Parkinson's Disease (PD) and other Synucleinopathies. The progressive buildup of pathological αSyn species results from alterations on αSyn gene and protein sequence, increased local concentrations, variations in αSyn interactome and protein network. Therefore, under physiological conditions, it is mandatory to regulate αSyn proteostasis as an equilibrium among synthesis, trafficking, degradation and extracellular release. In this frame, a crucial parameter is protein half-life. It provides indications of the turnover of a specific protein and depends on mRNA synthesis and translation regulation, subcellular localization, function and clearance by the designated degradative pathways. For αSyn, the molecular mechanisms regulating its proteostasis in neurons have been extensively investigated in various cellular models, either using biochemical or imaging approaches. Nevertheless, a converging estimate of αSyn half-life has not emerged yet. Here, we discuss the challenges in studying αSyn proteostasis under physiological and pathological conditions, the advantages and disadvantages of the experimental strategies proposed so far, and the relevance of determining αSyn half-life from a translational perspective.

摘要

α-突触核蛋白(αSyn)错误折叠和聚集常常先于帕金森病(PD)和其他突触核蛋白病相关的神经元丢失。病理性αSyn 物种的逐渐积累是由于αSyn 基因和蛋白质序列的改变、局部浓度的增加、αSyn 相互作用组和蛋白质网络的变化所致。因此,在生理条件下,必须调节αSyn 的蛋白质稳态,使其在合成、运输、降解和细胞外释放之间达到平衡。在这种情况下,蛋白质半衰期是一个关键参数。它提供了特定蛋白质周转率的指示,取决于 mRNA 的合成和翻译调控、亚细胞定位、功能以及通过指定的降解途径进行清除。对于αSyn,调节神经元中其蛋白质稳态的分子机制已在各种细胞模型中得到了广泛研究,无论是使用生化方法还是成像方法。然而,目前尚未得出关于αSyn 半衰期的一致估计值。在这里,我们讨论了在生理和病理条件下研究αSyn 蛋白质稳态的挑战,迄今为止提出的实验策略的优缺点,以及从转化角度确定αSyn 半衰期的相关性。

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