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精胺和雷帕霉素揭示了不同的自噬通量反应和货物受体清除特征。

Spermidine and Rapamycin Reveal Distinct Autophagy Flux Response and Cargo Receptor Clearance Profile.

机构信息

Department of Physiological Sciences, Stellenbosch University, Stellenbosch 7600, South Africa.

出版信息

Cells. 2021 Jan 7;10(1):95. doi: 10.3390/cells10010095.

Abstract

Autophagy flux is the rate at which cytoplasmic components are degraded through the entire autophagy pathway and is often measured by monitoring the clearance rate of autophagosomes. The specific means by which autophagy targets specific cargo has recently gained major attention due to the role of autophagy in human pathologies, where specific proteinaceous cargo is insufficiently recruited to the autophagosome compartment, albeit functional autophagy activity. In this context, the dynamic interplay between receptor proteins such as p62/Sequestosome-1 and neighbour of BRCA1 gene 1 (NBR1) has gained attention. However, the extent of receptor protein recruitment and subsequent clearance alongside autophagosomes under different autophagy activities remains unclear. Here, we dissect the concentration-dependent and temporal impact of rapamycin and spermidine exposure on receptor recruitment, clearance and autophagosome turnover over time, employing micropatterning. Our results reveal a distinct autophagy activity response profile, where the extent of autophagosome and receptor co-localisation does not involve the total pool of either entities and does not operate in similar fashion. These results suggest that autophagosome turnover and specific cargo clearance are distinct entities with inherent properties, distinctively contributing towards total functional autophagy activity. These findings are of significance for future studies where disease specific protein aggregates require clearance to preserve cellular proteostasis and viability and highlight the need of discerning and better tuning autophagy machinery activity and cargo clearance.

摘要

自噬通量是指细胞质成分通过整个自噬途径降解的速率,通常通过监测自噬体的清除率来衡量。由于自噬在人类病理学中的作用,最近人们对自噬靶向特定货物的具体方式给予了极大关注,尽管自噬活性正常,但特定的蛋白质货物不能充分招募到自噬体隔室中。在这种情况下,p62/自噬体相关蛋白 1(Sequestosome-1)和 BRCA1 基因 1 邻居(neighbour of BRCA1 gene 1,NBR1)等受体蛋白之间的动态相互作用引起了关注。然而,在不同自噬活性下,受体蛋白的招募以及随后与自噬体的清除程度仍不清楚。在这里,我们通过微图案化技术,剖析了雷帕霉素和亚精胺暴露对受体招募、清除和自噬体周转率的时间依赖性和浓度依赖性影响。我们的结果揭示了一种独特的自噬活性反应谱,其中自噬体和受体的共定位程度不涉及这两种物质的总池,也不以类似的方式运作。这些结果表明,自噬体周转率和特定货物的清除是具有固有特性的不同实体,它们对总功能自噬活性有独特的贡献。这些发现对未来的研究具有重要意义,因为需要清除特定疾病的蛋白质聚集体以维持细胞的蛋白质稳定性和活力,并强调需要区分和更好地调整自噬机制的活性和货物清除。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ad09/7827520/9f55b8208980/cells-10-00095-g001.jpg

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