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The Precision Control of Autophagic Flux and Vesicle Dynamics—A Micropattern Approach

机译:自噬通量和囊泡动力学的精确控制-一种微模式方法

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摘要

Autophagy failure is implicated in age-related human disease. A decrease in the rate of protein degradation through the entire autophagy pathway, i.e., autophagic flux, has been associated with the onset of cellular proteotoxity and cell death. Although the precision control of autophagy as a pharmacological intervention has received major attention, mammalian model systems that enable a dissection of the relationship between autophagic flux and pathway intermediate pool sizes remain largely underexplored. Here, we make use of a micropattern-based fluorescence life cell imaging approach, allowing a high degree of experimental control and cellular geometry constraints. By assessing two autophagy modulators in a system that achieves a similarly raised autophagic flux, we measure their impact on the pathway intermediate pool size, autophagosome velocity, and motion. Our results reveal a differential effect of autophagic flux enhancement on pathway intermediate pool sizes, velocities, and directionality of autophagosome motion, suggesting distinct control over autophagy function. These findings may be of importance for better understanding the fine-tuning autophagic activity and protein degradation proficiency in different cell and tissue types of age-associated pathologies.
机译:自噬失败与年龄相关的人类疾病有关。通过整个自噬途径,即自噬通量,蛋白质降解速率的降低与细胞蛋白毒素和细胞死亡的发作有关。尽管自噬作为药物干预的精确控制已受到广泛关注,但能够解剖自噬通量与途径中间库大小之间关系的哺乳动物模型系统仍在很大程度上尚未得到开发。在这里,我们利用基于微模式的荧光生命细胞成像方法,允许高度的实验控制和细胞几何形状约束。通过评估实现相似程度的自噬通量的系统中的两个自噬调节剂,我们测量了它们对途径中间池大小,自噬速度和运动的影响。我们的结果揭示了自噬通量增强对途径中间池大小,速度和自噬体运动方向性的不同影响,表明对自噬功能的独特控制。这些发现对于更好地了解与年龄相关的病理学的不同细胞和组织类型中的微调自噬活性和蛋白质降解能力可能具有重要意义。

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