The PP2A-B55α phosphatase is a master regulator of mitochondrial degradation and biogenesis

IF 12.5 1区综合性期刊 Q1 MULTIDISCIPLINARY SCIENCES

Science Advances Pub Date : 2025-10-03 DOI:10.1126/sciadv.adw7376

Valentina Cianfanelli, Monica Nanni, Samantha Corrà, Sofia Mauri, David Sumpton, Sergio Lilla, Rossella De Cegli, Matteo Bordi, Giacomo Milletti, Caterina Ferraina, Arnaldur Hall, Michele Petraroia, Valentina Clausi, Ezio Giorda, Marco Scarsella, Alessandra Barbiera, Giulia Cadeddu, Marco Colasanti, Tiziana Persichini, Kenji Maeda, Apolinar Maya-Mendoza, Jiri Bartek, Chiara Di Malta, Franco Locatelli, Sara Zanivan, Shehab Ismail, Elena Ziviani, Francesco Cecconi

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Abstract

Mitochondrial homeostasis relies on a tight balance between mitochondrial biogenesis and degradation. Although mitophagy is one of the main pathways involved in the clearance of damaged or old mitochondria, its coordination with mitochondrial biogenesis is poorly characterized. Here, by unbiased approaches including last-generation liquid chromatography coupled to mass spectrometry and transcriptomics, we identify the protein phosphatase PP2A-B55α/PPP2R2A as a Parkin-dependent regulator of mitochondrial number. Upon mitochondrial damage, PP2A-B55α determines the amplitude of mitophagy induction and execution by regulating both early and late mitophagy events. A few minutes after the insult, ULK1 is released from the inhibitory regulation of PP2A-B55α, whereas 2 to 4 hours later, PP2A-B55α promotes the nuclear translocation of TFEB, the master regulator of autophagy and lysosome genes, to support mitophagy execution. Moreover, PP2A-B55α controls a transcriptional program of mitochondrial biogenesis by stabilizing the Parkin substrate and PGC-1α inhibitor PARIS. PP2A-B55α targeting rescues neurodegenerative phenotypes in a fly model of Parkinson’s disease, thus suggesting potential therapeutic application.

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PP2A-B55α磷酸酶是线粒体降解和生物发生的主要调控因子

线粒体稳态依赖于线粒体生物发生和降解之间的紧密平衡。虽然线粒体自噬是参与清除受损或老化线粒体的主要途径之一，但其与线粒体生物发生的协调性尚不清楚。在这里，通过无偏倚的方法，包括上一代液相色谱联用质谱和转录组学，我们确定蛋白磷酸酶PP2A-B55α/PPP2R2A是线粒体数量的帕金森依赖性调节因子。在线粒体损伤时，PP2A-B55α通过调节线粒体自噬的早期和晚期事件来决定线粒体自噬诱导和执行的幅度。损伤几分钟后，ULK1从PP2A-B55α的抑制调控中释放出来，而2至4小时后，PP2A-B55α促进TFEB的核易位，TFEB是自噬和溶酶体基因的主要调控因子，以支持有丝分裂的执行。此外，PP2A-B55α通过稳定Parkin底物和PGC-1α抑制剂PARIS来控制线粒体生物发生的转录程序。PP2A-B55α靶向治疗帕金森病果蝇模型中的神经退行性表型，从而提示潜在的治疗应用。

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来源期刊

Science Advances 综合性期刊-综合性期刊

CiteScore

21.40

自引率

1.50%

发文量

1937

审稿时长

29 weeks

期刊介绍： Science Advances, an open-access journal by AAAS, publishes impactful research in diverse scientific areas. It aims for fair, fast, and expert peer review, providing freely accessible research to readers. Led by distinguished scientists, the journal supports AAAS's mission by extending Science magazine's capacity to identify and promote significant advances. Evolving digital publishing technologies play a crucial role in advancing AAAS's global mission for science communication and benefitting humankind.