Structural Basis for Chaperone-Independent Ubiquitination of Tau Protein by Its E3 Ligase CHIP.
Francesca MunariLuca MollicaCarlo ValenteFrancesca ParoliniElham Ataie KachoieGiorgio ArrigoniMariapina D'OnofrioStefano CapaldiMichael AssfalgPublished in: Angewandte Chemie (International ed. in English) (2022)
The multi-site ubiquitination of Tau protein found in Alzheimer's disease filaments hints at the failed attempt of neurons to remove early toxic species. The ubiquitin-dependent degradation of Tau is regulated in vivo by the E3 ligase CHIP, a quality controller of the cell proteome dedicated to target misfolded proteins for degradation. In our study, by using site-resolved NMR, biochemical and computational methods, we elucidate the structural determinants underlying the molecular recognition between the ligase and its intrinsically disordered substrate. We reveal a multi-domain dynamic interaction that explains how CHIP can direct ubiquitination of Tau at multiple sites even in the absence of chaperones, including its typical partner Hsp70/Hsc70. Our findings thus provide mechanistic insight into the chaperone-independent engagement of a disordered protein by its E3 ligase.
Keyphrases
- structural basis
- cerebrospinal fluid
- heat shock protein
- heat shock
- high throughput
- protein protein
- amino acid
- circulating tumor cells
- single cell
- magnetic resonance
- social media
- small molecule
- spinal cord
- transcription factor
- genome wide
- gene expression
- dna methylation
- spinal cord injury
- hepatitis c virus
- stem cells
- oxidative stress