α-Synuclein in Parkinson’s disease: causal or bystander?

Riederer, Peter; Berg, Daniela; Casadei, Nicolas; Cheng, Fu Bo; Claßen, Joseph; Dresel, Christian; Jost, Wolfgang H.; Krüger, Rejko; Müller, Thomas; Reichmann, Heinz; Rieß, Olaf; Storch, Alexander; Strobel, Sabrina; Eimeren, Thilo van; Völker, Hans-Ullrich; Winkler, Jürgen; Winklhofer, Konstanze F.; Wüllner, Ullrich; Zunke, Friederike; Monoranu, Camelia‐Maria

doi:10.1007/s00702-019-02025-9

Cited by 100 publications

(68 citation statements)

References 260 publications

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“…Individuals with PD suffer from tremors and impaired posture and movement [172,176]. Genetic risk factors have been identified, such as mutations and/or duplication events in the α-synuclein (SNCA) gene [177]. Of all the neurodegenerative diseases discussed, how dysregulation of PcG and TrxG proteins might contribute to PD pathology is the least studied and understood.…”

Section: Parkinson's Diseasementioning

confidence: 99%

The Dynamic Partnership of Polycomb and Trithorax in Brain Development and Diseases

Kuehner

Yao

2019

Epigenomes

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Epigenetic mechanisms, including DNA and histone modifications, are pivotal for normal brain development and functions by modulating spatial and temporal gene expression. Dysregulation of the epigenetic machinery can serve as a causal role in numerous brain disorders. Proper mammalian brain development and functions depend on the precise expression of neuronal-specific genes, transcription factors and epigenetic modifications. Antagonistic polycomb and trithorax proteins form multimeric complexes and play important roles in these processes by epigenetically controlling gene repression or activation through various molecular mechanisms. Aberrant expression or disruption of either protein group can contribute to neurodegenerative diseases. This review focus on the current progress of Polycomb and Trithorax complexes in brain development and disease, and provides a future outlook of the field.

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Section: Parkinson's Diseasementioning

confidence: 99%

The Dynamic Partnership of Polycomb and Trithorax in Brain Development and Diseases

Kuehner

Yao

2019

Epigenomes

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“…Es existieren zahlreiche Hinweise darauf, dass der neurodegenerative Prozess an den Axonterminalen beginnt, an denen sich auch physiologisch ungefaltetes, monomeres Synuklein befindet, das an der Exozytose präsynaptischer Vesikel beteiligt ist [40]. Beim IPS kommt es, ausgehend von den Axonterminalen, zu einer retrograden Degeneration, und es wird diskutiert, ob die Lewy-Pathologie im Rahmen eines Detoxifizierungsprozess ein Epiphänomen und somit nur einen indirekten Marker der Degeneration darstellt [41,42]. Damit korrelierend gehen neuere Arbeiten davon aus, das bereits 50-60% der nigrostriatalen Axonterminalen, aber nur etwa 30% der dopaminergen Neurone der SN degeneriert sind, wenn erste motorische Symptome in Erscheinung treten [43].…”

Section: Efferente Projektionen Der Snunclassified

Struktur und Efferenzen der Substantia nigra pars compacta beim idiopathischen Parkinson-Syndrom

Falkenburger

Jost

Ransmayr

et al. 2020

Fortschr Neurol Psychiatr

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ZusammenfassungEs besteht Konsens, dass das neuropathologische Merkmal des idiopathischen Parkinson-Syndroms (IPS) der neuronale Zellverlust der Substantia nigra pars compacta (SNc) in Verbindung mit einer Lewy-Pathologie ist. Die transsynaptische Ausbreitung der Lewy-Pathologie wird als wesentlich in der Parkinson-Pathogenese angesehen. Daher ist die Kenntnis präexistenter neuroanatomischer Verbindungen der SNc wesentlich. Wir beschreiben hier neuere tierexperimentelle Befunde zu den afferenten und efferenten Projektionen der SNc und diskutieren die Evidenz für und gegen die sequentielle transsynaptische Ausbreitung der Lewy-Pathologie in der Pathogenese des IPS.

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“…The discoveries of the causative genes of various fPDs (PARKs) have greatly contributed to investigation into the molecular mechanism of sPD. Based on the information obtained from postmortem brains from fPD patients and fPD-derived iPS cells, DA oxidation, oxidative/endoplasmic reticulum (ER) stress, aggregation of toxic misfolded α-synuclein oligomers, mitochondrial dysfunction, alterations in the ubiquitin-proteasome and autophagy-lysosome systems, and neuroinflammation are assumed to be a central mechanism resulting in neurodegeneration, as described below in more detail (Burbulla et al 2017;Chen et al 2015;Sánchez-Danés et al 2012;Woodard et al 2014;Riederer et al 2019). DA and α-synuclein protein oligomers (causative protein of autosomal dominant fPD type 1/4; PARK1/4; Polymeropoulos et al 1997) are assumed to be key molecules for neurodegeneration in PD.…”

Section: Mechanism Of Spd Hypothesized From Causative Proteins Of Fpdmentioning

confidence: 99%

Monoamine Oxidase Inhibitor (MAO-I)-Mediated Neuroprotection for Treating Parkinson’s Disease

Nagatsu¹,

Nakashima²

2020

NeuroPsychopharmacotherapy

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α-Synuclein in Parkinson’s disease: causal or bystander?

Cited by 100 publications

References 260 publications

The Dynamic Partnership of Polycomb and Trithorax in Brain Development and Diseases

The Dynamic Partnership of Polycomb and Trithorax in Brain Development and Diseases

Struktur und Efferenzen der Substantia nigra pars compacta beim idiopathischen Parkinson-Syndrom

Monoamine Oxidase Inhibitor (MAO-I)-Mediated Neuroprotection for Treating Parkinson’s Disease

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