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R406 and its structural analogs reduce SNCA/α-synuclein levels via autophagic degradation

Chao Zhong, Xiaoge Gao, Qi Chen, Bowen Guan, Wanli Wu, Z. Ma, Mengdan Tao, Xihuan Liu, Yu Ding, Yiyan Fei, Yan Liu, Boxun Lu, Zhaoyang Li

2025Autophagy7 citationsDOIOpen Access PDF

Abstract

The presence of neuronal Lewy bodies mainly composed of SNCA/α-synuclein aggregations is a pathological feature of Parkinson disease (PD), whereas reducing SNCA protein levels may slow the progression of this disease. We hypothesized that compounds enhancing SNCA’s interaction with MAP1LC3/LC3 May increase its macroautophagic/autophagic degradation. Here, we conducted small molecule microarray (SMM)-based screening to identify such compounds and revealed that the compound R406 could decrease SNCA protein levels in an autophagy-dependent manner. We further validated the proposed mechanism, in which knockdown of essential gene ATG5 for autophagy formation and using the autophagy inhibitor chloroquine (CQ) blocked the effect of R406. Additionally, R406 also reduced the levels of phosphorylated serine 129 of SNCA (p-S129-SNCA) in SNCA preformed fibrils (PFFs)-induced cellular models and rescued neuron degeneration.

Topics & Concepts

AutophagyBiologyDegradation (telecommunications)Alpha-synucleinNeuroscienceCell biologyParkinson's diseaseGeneticsDiseaseInternal medicineComputer scienceMedicineTelecommunicationsApoptosisParkinson's Disease Mechanisms and TreatmentsNuclear Receptors and SignalingAutophagy in Disease and Therapy