Arginine Methyltransferase PRMT8 Provides Cellular Stress Tolerance in Aging Motoneurons

Simándi, Zoltán; Pajer, Krisztián; Károlyi, Katalin; Sieler, Tatiana; Jiang, Lu; Kolostyák, Zsuzsanna; Sári, Zsanett; Fekécs, Zoltán; Pap, Attila; Patsalos, Andreas; Contreras, Gerardo Alvarado; Rehó, Bálint; Papp, Zoltán; Guo, Xiufang; Horváth, Attila; G, Kiss; Keresztessy, Zsolt; Vámosi, György; Hickman, James J.; Xu, Huaxi; Dormann, Dorothee; Hortobágyi, Tibor; Antal, Miklós; Nógrádi, Antal; Nagy, László

doi:10.1523/jneurosci.3389-17.2018

Cited by 32 publications

(32 citation statements)

References 77 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Methylation of FUS is required to bind the autophagy receptor p62 which in association with other proteins can control the aberrant accumulation of the granules [54]. Other studies have reported methylation as an important modification type in the accumulation and elimination of these toxic granules [55] supporting our predicted association with ALS ( Figure 2C). In a close look, Figure 5C shows FUS with methylation sites affected and non-affected by the ALS mutations, the former with the probability of being more pathogenic than regular methylation sites, measured using rps.…”

Section: Prediction Of New Potential Mutation Sites Associated To Dissupporting

confidence: 86%

A global map of the impact of deletion of Post-Translational Modification sites in genetic diseases

Vellosillo

Mínguez

2020

Preprint

View full text Add to dashboard Cite

BackgroundThere are >200 protein post-translational modification (PTMs) types described in eukaryotes, having diverse species conservation levels, proteome coverage, number of high-throughput experiments and functional roles. From a clinical perspective, a number of diseases have been associated to deregulated PTM sites and missense rare variants are globally enriched in PTMs. We hypothesize that some genetic diseases may be caused by the deregulation of particular functions produced by the removal of a specific PTM type by genomic variants.ResultsWe collected >320,000 human PTMs of 59 types and cross them with >4M missense DNA variants annotated with pathogenic predictions and disease associations. We report >1.74M PTM-variant concurrences in >16,500 proteins that an enrichment analysis distributed in 217 pairwise significant associations between 18 PTM types and 150 genetic diseases. Around 23% of these associations are already described in the literature, 34% have partial evidences based on single variants, related diseases or regulatory evidences, and 43% are novel. Removal of acetylation presents the highest effect, still low studied PTM types like S-glutathionylation or S-nitrosylation show relevance. A network of PTM types and phenotypes associations is also discussed. Using pathogenicity predictions we identified potential PTM sites to produce particular diseases if genomic variants remove them.ConclusionsOur results show an important impact of PTM removal producing genetic diseases and phenotypes that is PTM type specific. We describe for the first time a general scenario of PTM types and genetic diseases direct associations, many of them novel, that provides new capacities to understand and diagnose these disorders.

show abstract

Section: Prediction Of New Potential Mutation Sites Associated To Dissupporting

confidence: 86%

A global map of the impact of deletion of Post-Translational Modification sites in genetic diseases

Vellosillo

Mínguez

2020

Preprint

View full text Add to dashboard Cite

show abstract

“…The PRMT8 protein has critical roles in numerous physiological functions, including in the brain and stem cells, in a variety of animals (9, 10, 12, 22, 23). In zebrafish, for example, PRMT8 has an extra N-terminal sequence, and shows brain-specific expression that is critical for the development of the zebrafish brain.…”

Section: Resultsmentioning

confidence: 99%

“…This enzyme has a unique N-terminal extended region that is involved in plasma membrane localization via myristoylation, and is suggested to regulate PRMT8 enzymatic activity (7, 8). It is a multifunctional protein with arginine methyl transferase and phospholipase D activities (9), localizes to both presynaptic and postsynaptic sites, and plays multiple roles in the brain, including in Purkinje cell morphology, perineuronal net formation in the visual cortex, fear learning in the hippocampus, and neuroprotection against age-related increases in cellular stress (9–12). Type I PRMTs may undergo oligomerization/dimerization through an interaction between the dimerization arm projecting off the β-barrel and the Rossman fold of another subunit (13).…”

Section: Introductionmentioning

confidence: 99%

Deciphering the molecular mechanisms underlying the plasma membrane targeting of PRMT8

et al. 2019

View full text Add to dashboard Cite

Arginine methylation plays crucial roles in many cellular functions including signal transduction, RNA transcription, and regulation of gene expression. Protein arginine methyl-transferase 8 (PRMT8), a unique brain-specific protein, is localized to the plasma membrane. However, the detailed molecular mechanisms underlying PRMT8 plasma membrane targeting remain unclear. Here, we demonstrate that the N-terminal 20 amino acids of PRMT8 are sufficient for plasma membrane localization and that oligomerization enhances membrane localization. The basic amino acids, combined with myristoylation within the N-terminal 20 amino acids of PRMT8, are critical for plasma membrane targeting. We also found that substituting Gly-2 with Ala [PRMT8(G2A)] or Cys-9 with Ser [PRMT8(C9S)] induces the formation of punctate structures in the cytosol or patch-like plasma membrane localization, respectively. Impairment of PRMT8 oligomerization/dimerization by C-terminal deletion induces PRMT8 mis-localization to the mitochondria, prevents the formation of punctate structures by PRMT8(G2A), and inhibits PRMT8(C9S) patch-like plasma membrane localization. Overall, these results suggest that oligomerization/dimerization plays several roles in inducing the efficient and specific plasma membrane localization of PRMT8.

show abstract

“…Arg-methylation appears to be especially relevant in terminally differentiated and long-lived neurons, e.g. motor neurons, which show tissue-specific expression of PRMT8 and require Arg-methylation for a proper stress response and for maintaining motor neuron health during aging (132). Suppression of aberrant RBP phase separation by Arg-methylation may be part of the protective mechanism, and hence it would be interesting to examine whether loss of PRMT8 promotes pathological RBP phase transitions and alters RNP granule dynamics and function in neurons.…”

Section: Arginine Methylation and Phosphorylation As Regulators Of Llmentioning

confidence: 99%

Friend or foe—Post-translational modifications as regulators of phase separation and RNP granule dynamics

Hofweber¹,

Dormann

2019

Journal of Biological Chemistry

Self Cite

287

257

View full text Add to dashboard Cite

Edited by Paul E. FraserRibonucleoprotein (RNP) granules are membrane-less organelles consisting of RNA-binding proteins (RBPs) and RNA. RNA granules form through liquid-liquid phase separation (LLPS), whereby weak promiscuous interactions among RBPs and/or RNAs create a dense network of interacting macromolecules and drive the phase separation. Post-translational modifications (PTMs) of RBPs have emerged as important regulators of LLPS and RNP granule dynamics, as they can directly weaken or enhance the multivalent interactions between phase-separating macromolecules or can recruit or exclude certain macromolecules into or from condensates. Here, we review recent insights into how PTMs regulate phase separation and RNP granule dynamics, in particular arginine (Arg)-methylation and phosphorylation. We discuss how these PTMs regulate the phase behavior of prototypical RBPs and how, as "friend or foe," they might influence the assembly, disassembly, or material properties of cellular RNP granules, such as stress granules or amyloidlike condensates. We particularly highlight how PTMs control the phase separation and aggregation behavior of disease-linked RBPs. We also review how disruptions of PTMs might be involved in aberrant phase transitions and the formation of amyloid-like protein aggregates as observed in neurodegenerative diseases.

show abstract

Arginine Methyltransferase PRMT8 Provides Cellular Stress Tolerance in Aging Motoneurons

Cited by 32 publications

References 77 publications

A global map of the impact of deletion of Post-Translational Modification sites in genetic diseases

A global map of the impact of deletion of Post-Translational Modification sites in genetic diseases

Deciphering the molecular mechanisms underlying the plasma membrane targeting of PRMT8

Friend or foe—Post-translational modifications as regulators of phase separation and RNP granule dynamics

Contact Info

Product

Resources

About