Synapsin and α-synuclein represent a growing list of condensate-forming proteins where the material states of condensates are directly linked to cellular functions (e.g., neurotransmission) and pathology (e.g., neurodegeneration). However, quantifying condensate material properties in living systems has been a substantial challenge. Here, we develop micropipette aspiration and whole-cell patch-clamp (MAPAC), a platform that allows direct material quantification of condensates in live cells. We find 10,000-fold variations in the viscoelasticity of synapsin condensates, regulated by the partitioning of α-synuclein, a marker for synucleinopathies. Through in vitro reconstitutions, we identify multiple molecular factors that distinctly regulate the viscosity, interfacial tension, and maturation of synapsin condensates, confirming the cellular roles of α-synuclein. Overall, our study provides unprecedented quantitative insights into the material properties of neuronal condensates and reveals a crucial role of α-synuclein in regulating condensate viscoelasticity. Furthermore, we envision MAPAC applicable to study a broad range of condensates in vivo.
Live-cell quantification reveals viscoelastic regulation of synapsin condensates by α-synuclein.
活细胞定量分析揭示了α-突触核蛋白对突触蛋白凝聚体的粘弹性调节
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作者:Wang Huan, Hoffmann Christian, Tromm Johannes V, Su Xiao, Elliott Jordan, Wang Han, Deng Mengying, McClenaghan Conor, Baum Jean, Pang Zhiping P, Milovanovic Dragomir, Shi Zheng
| 期刊: | Science Advances | 影响因子: | 12.500 |
| 时间: | 2025 | 起止号: | 2025 Apr 18; 11(16):eads7627 |
| doi: | 10.1126/sciadv.ads7627 | 研究方向: | 细胞生物学 |
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