Monomethylated and unmethylated FUS exhibit increased binding to Transportin and distinguish FTLD-FUS from ALS-FUS

Suárez‐Calvet, Marc; Neumann, Manuela; Arzberger, Thomas; Abou‐Ajram, Claudia; Funk, Eva B. E.; Hartmann, Hannelore; Edbauer, Dieter; Kremmer, Elisabeth; Göbl, Christoph; Resch, Moritz; Bourgeois, Benjamin; Madl, Tobias; Reber, Stefan; Jutzi, Daniel; Ruepp, Marc‐David; Mackenzie, Ian R.; Ansorge, Olaf; Dormann, Dorothee; Haass, Christian

doi:10.1007/s00401-016-1544-2

Cited by 78 publications

(93 citation statements)

References 60 publications

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“…For example, whether a particular arginine residue on histone tails is asymmetrically or symmetrically dimethylated can lead to gene repression or activation (13)(14)(15)(16)(17). However, few studies have been conducted to determine the role of MMA marks (18). It has been proposed that MMA marks are used mainly as precursors for dimethylation by the various type I and II PRMTs (17,19).…”

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confidence: 99%

Protein Arginine Methyltransferase Product Specificity Is Mediated by Distinct Active-site Architectures

Jain¹,

Warmack²,

Debler³

et al. 2016

Journal of Biological Chemistry

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In the family of protein arginine methyltransferases (PRMTs) that predominantly generate either asymmetric or symmetric dimethylarginine (SDMA), PRMT7 is unique in producing solely monomethylarginine (MMA) products. The type of methylation on histones and other proteins dictates changes in gene expression, and numerous studies have linked altered profiles of methyl marks with disease phenotypes. Given the importance of specific inhibitor development, it is crucial to understand the mechanisms by which PRMT product specificity is conferred. We have focused our attention on active-site residues of PRMT7 from the protozoan Trypanosoma brucei. We have designed 26 single and double mutations in the active site, including residues in the Glu-Xaa 8 -Glu (double E) loop and the Met-Gln-Trp sequence of the canonical Thr-His-Trp (THW) loop known to interact with the methyl-accepting substrate arginine. Analysis of the reaction products by high resolution cation exchange chromatography combined with the knowledge of PRMT crystal structures suggests a model where the size of two distinct subregions in the active site determines PRMT7 product specificity.

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mentioning

confidence: 99%

Protein Arginine Methyltransferase Product Specificity Is Mediated by Distinct Active-site Architectures

Jain¹,

Warmack²,

Debler³

et al. 2016

Journal of Biological Chemistry

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“…In ALS-FUS but not FTLD-FUS cases, the pathological inclusions contained FUS with asymmetrically dimethylated arginines (ADMA) (Dormann et al 2012). In contrast, unmethylated/monomethylated Arg (UMA/MMA) at RGG3 region of FUS constituted the inclusions observed in FTLD-FUS but not in ALS-FUS cases (Suarez-Calvet et al 2016). Methylations of Arg residues in FUS have been shown to reduce its binding to transportin and thus suppress the nuclear import of FUS (Dormann et al 2012;Suarez-Calvet et al 2016).…”

Section: Pathological Inclusions Containing Fet Proteins In Als Casesmentioning

confidence: 95%

“…While the regulation of the nuclearcytoplasmic shuttling of the FET proteins remains obscure, the nuclear import of the FET proteins is negatively regulated by chemical modifications near the PY-NLS, such as the methylation of Arg (Dormann et al 2012;Belyanskaya et al 2003) and the phosphorylation of Tyr (Leemann-Zakaryan et al 2011). Given that cytoplasmic accumulation of FUS is observed in the ALS-FUS cases, post-translational modifications affecting the function of PY-NLS may also have pathological roles in ALS (Dormann et al 2012;Suarez-Calvet et al 2016). Also, notably, significant concentrations of FUS are observed in the dendritic spines of neurons, where mRNAs are stored for their local translation upon synaptic activity (Fujii et al 2005).…”

Section: Introductionmentioning

confidence: 97%

Aggregation of FET Proteins as a Pathological Change in Amyotrophic Lateral Sclerosis

Furukawa

Tokuda

2016

Advances in Experimental Medicine and Biology

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Amyotrophic lateral sclerosis (ALS) is a fatal motor neuron disease that is characterized by the formation of abnormal inclusions in neurons. While the pathomechanism of ALS remains obscure, a number of proteins have been identified in the inclusion bodies, and the pathological roles of RNA-binding proteins have been increasingly emphasized. Among those, the FET proteins (FUS, EWSR1, TAF15) were recently identified as RNA-binding proteins in pathological inclusions of ALS and other neurodegenerative diseases; moreover, mutations in the genes encoding the FET proteins were found to be associated with familial forms of ALS. FET proteins are normally localized in the nucleus, but the introduction of pathogenic mutations in FET proteins leads to their abnormal redistribution to the cytoplasm, where they form aggregates. While further investigation will be required to understand the intracellular factors controlling the aggregation propensities of FET proteins, they are thought to lose their physiological functions and become toxic through their misfolding/aggregation. Here, we will briefly review recent advances of our understanding of the physiological functions and aggregation behavior of FET proteins in vivo as well as in vitro.

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“…Dabei wurde das 110 kDa große Protein Tr ansportin-1 hinzutitriert, vom dem gezeigt wurde,d ass es den C-Terminus von FUS bindet, [22] aber neueste Erkenntnisse weisen auch auf eine Rolle der RGGRegion bei der Bindung hin. [18,23] …”

Section: Angewandte Chemieunclassified

Verbesserung der Dispersion der chemischen Verschiebungen von unstrukturierten Proteinen durch einen kovalent gebundenen Lanthanoidkomplex

et al. 2016

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Die Erforschung von intrinsischu nstrukturierten Proteinen (IDPs) mit NMR-spektroskopischen Methoden wird oftmals durch starke Überlagerung der Proteinsignale erschwert. Dies führt zu uneindeutigen Zuordnungen dieser Signale und erschwert die Datenanalyse,i nw elcher oftmals eine gute Separierung der Signale die Grundlage der Dateninterpretation bildet. In dieser Arbeit berichten wir von der Mçglichkeit, einen Lanthanoidkomplex kovalent an das Zielprotein zu binden, der zu einer erhçhten Dispersion der Signale führt. Wir zeigen diesen Effekt an Proteinen mit sich wiederholenden Aminosäuresequenzen, welche somit besonders von Signalüberlappung betroffen sind. Die Bindung eines DOTA-basierten Lanthanoidkomplexes an ein Cystein führt zu pseudochemischenV erschiebungen (PCS), die nochi n mehr als 20 Aminosäureresten entfernten Regionen detektierbar sind. Die stark erhçhte Dispersion der beobachteten Signale führt zu einer beträchtlichen Erleichterung in der Zuordnung und Datenauswertung.

show abstract

Monomethylated and unmethylated FUS exhibit increased binding to Transportin and distinguish FTLD-FUS from ALS-FUS

Cited by 78 publications

References 60 publications

Protein Arginine Methyltransferase Product Specificity Is Mediated by Distinct Active-site Architectures

Protein Arginine Methyltransferase Product Specificity Is Mediated by Distinct Active-site Architectures

Aggregation of FET Proteins as a Pathological Change in Amyotrophic Lateral Sclerosis

Verbesserung der Dispersion der chemischen Verschiebungen von unstrukturierten Proteinen durch einen kovalent gebundenen Lanthanoidkomplex

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