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Cytosolic condensates rich in polyserine define subcellular sites of tau aggregation

Evan Lester, Meaghan Van Alstyne, Kathleen L. McCann, Spoorthy Reddy, Li Yi Cheng, Jeff Kuo, James Pratt, Roy Parker

2023Proceedings of the National Academy of Sciences38 citationsDOIOpen Access PDF

Abstract

Tau aggregates are a hallmark of multiple neurodegenerative diseases and can contain RNAs and RNA-binding proteins, including serine/arginine repetitive matrix protein 2 (SRRM2) and pinin (PNN). However, how these nuclear proteins mislocalize and their influence on the prion-like propagation of tau aggregates is unknown. We demonstrate that polyserine repeats in SRRM2 and PNN are necessary and sufficient for recruitment to tau aggregates. Moreover, we show tau aggregates preferentially grow in association with endogenous cytoplasmic assemblies-mitotic interchromatin granules and cytoplasmic speckles (CSs)-which contain SRRM2 and PNN. Polyserine overexpression in cells nucleates assemblies that are sites of tau aggregate growth. Further, modulating the levels of polyserine-containing proteins results in a corresponding change in tau aggregation. These findings define a specific protein motif, and cellular condensates, that promote tau aggregate propagation. As CSs form in induced pluripotent stem cell (iPSC) derived neurons under inflammatory or hyperosmolar stress, they may affect tau aggregate propagation in neurodegenerative disease.

Topics & Concepts

Stress granuleCytoplasmCell biologyNeurodegenerationRNA-binding proteinChemistryProtein aggregationCytosolTau proteinRNAMitosisTauopathyBiologyBiophysicsBiochemistryMessenger RNAGeneTranslation (biology)Alzheimer's diseaseDiseaseMedicineEnzymePathologyAlzheimer's disease research and treatmentsRNA Research and SplicingRNA regulation and disease