RESUMO
Up-regulation of Hsp20 protein levels in response to amyloid fibril formation is considered a key protective response against the onset of Alzheimer's disease (AD). Indeed, the physical interaction between Hsp20 and Aß is known to prevent Aß oligomerisation and protects neuronal cells from Aß mediated toxicity, however, details of the molecular mechanism and regulatory cell signalling events behind this process have remained elusive. Using both conventional MTT end-point assays and novel real time measurement of cell impedance, we show that Hsp20 protects human neuroblastoma SH-SY5Y cells from the neurotoxic effects of Aß. In an attempt to provide a mechanism for the neuroprotection afforded by Hsp20, we used peptide array, co-immunoprecipitation analysis and NMR techniques to map the interaction between Hsp20 and Aß and report a binding mode where Hsp20 binds adjacent to the oligomerisation domain of Aß, preventing aggregation. The Hsp20/Aß interaction is enhanced by Hsp20 phosphorylation, which serves to increase association with low molecular weight Aß species and decrease the effective concentration of Hsp20 required to disrupt the formation of amyloid oligomers. Finally, using a novel fluorescent assay for the real time evaluation of morphology-specific Aß aggregation, we show that phospho-dependency of this effect is more pronounced for fibrils than for globular Aß forms and that 25mers corresponding to the Hsp20 N-terminal can be used as Aß aggregate inhibitors. Our report is the first to provide a molecular model for the Hsp20/Aß complex and the first to suggest that modulation of the cAMP/cGMP pathways could be a novel route to enhance Hsp20-mediated attenuation of Aß fibril neurotoxicity.