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Review
. 2019 Jul;126(7):815-840.
doi: 10.1007/s00702-019-02025-9. Epub 2019 Jun 25.

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

Peter Riederer  1   2 Daniela Berg  3 Nicolas Casadei  4 Fubo Cheng  4 Joseph Classen  5 Christian Dresel  6 Wolfgang Jost  7 Rejko Krüger  8   9 Thomas Müller  10 Heinz Reichmann  11 Olaf Rieß  12 Alexander Storch  13   14 Sabrina Strobel  15 Thilo van Eimeren  16 Hans-Ullrich Völker  17 Jürgen Winkler  18 Konstanze F Winklhofer  19 Ullrich Wüllner  20 Friederike Zunke  21 Camelia-Maria Monoranu  15
Affiliations
Review

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

Peter Riederer et al. J Neural Transm (Vienna). 2019 Jul.

Abstract

Parkinson's disease (PD) comprises a spectrum of disorders with differing subtypes, the vast majority of which share Lewy bodies (LB) as a characteristic pathological hallmark. The process(es) underlying LB generation and its causal trigger molecules are not yet fully understood. α-Synuclein (α-syn) is a major component of LB and SNCA gene missense mutations or duplications/triplications are causal for rare hereditary forms of PD. As typical sporadic PD is associated with LB pathology, a factor of major importance is the study of the α-syn protein and its pathology. α-Syn pathology is, however, also evident in multiple system atrophy (MSA) and Lewy body disease (LBD), making it non-specific for PD. In addition, there is an overlap of these α-synucleinopathies with other protein-misfolding diseases. It has been proven that α-syn, phosphorylated tau protein (pτ), amyloid beta (Aβ) and other proteins show synergistic effects in the underlying pathogenic mechanisms. Multiple cell death mechanisms can induce pathological protein-cascades, but this can also be a reverse process. This holds true for the early phases of the disease process and especially for the progression of PD. In conclusion, while rare SNCA gene mutations are causal for a minority of familial PD patients, in sporadic PD (where common SNCA polymorphisms are the most consistent genetic risk factor across populations worldwide, accounting for 95% of PD patients) α-syn pathology is an important feature. Conversely, with regard to the etiopathogenesis of α-synucleinopathies PD, MSA and LBD, α-syn is rather a bystander contributing to multiple neurodegenerative processes, which overlap in their composition and individual strength. Therapeutic developments aiming to impact on α-syn pathology should take this fact into consideration.

Keywords: Autophagy; Gene expression; Lysosome; Neuroinflammation; Neuromelanin; Parkinson’s disease; Proteasome; Protein interactions; SNCA gene; Synucleinopathy; Therapy; α-Synuclein.

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