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YAP maintains the dynamics of TDP-43 condensates and antagonizes TDP-43 pathological aggregates

NATURE CELL BIOLOGY. 2025-06; 
Jiaqi Zhang, Jiaojiao Hu, Ruogu Liu, Tian Zhou, Xuewei Luo, Peigang Liang, Zaichao Xie, Qinyue Zhao, Yan Chen, Dan Du, Cong Liu, Yiming Zheng, Dan Li, Bo Wang
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Proteins, Expression, Isolation and Analysis Cell lysates were prepared using lysis buffer and then incubated with anti-DYKDDDDK G1 affinity resin (GenScript, L00432-10) for 2 h at 4 °C. Following this, the beads were washed five times with lysis buffer. Subsequently, the immunopurified proteins were eluted using 3×Flag peptide (GenScript, RP10586CN) in elution buffer (500 mM Tris pH 8.0, 150 mM NaCl and 0.5 mg ml−1). For immunoprecipitation, the supernatants were incubated with anti-DYKDDDDK G1 Affinity beads (Genscript, L00432-10) for 3 h at 4 °C. Get A Quote

摘要

Recent studies exploring the underlying pathomechanisms of amyotrophic lateral sclerosis (ALS), a fatal motor neuron disorder, have focused on biomolecular condensates. Here we reveal an unexpected function for YAP, a central component of the Hippo pathway, in regulating the dynamic behaviour of stress granules and TDP-43 condensates, a role that is independent of its transcriptional activity in the Hippo pathway. YAP directly binds to TDP-43. This interaction directly promotes the homotypic multimerization and phase separation of TDP-43 while inhibiting its hyperphosphorylation and solidification under stress conditions. Remarkably, YAP, whose messenger RNA levels are reduced in patients with ALS, is found to ... More

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