Strong interactions with polyethylenimine-coated human serum albumin nanoparticles (PEI-HSA NPs) alter alpha-synuclein conformation and aggregation kinetics

摘要

The interaction between nanoparticles (NPs) and the small intrinsically disordered protein alpha-synuclein (alpha SN), whose aggregation is central in the development of Parkinson's disease, is of great relevance in biomedical applications of NPs as drug carriers. Here we showed using a combination of different techniques that alpha SN interacts strongly with positively charged polyethylenimine-coated human serum albumin (PEI-HSA) NPs, leading to a significant alteration in the alpha SN secondary structure. In contrast, the weak interactions of alpha SN with HSA NPs allowed alpha SN to remain unfolded. These different levels of interactions had different effects on alpha SN aggregation. While the weakly interacting HSA NPs did not alter the aggregation kinetic parameters of alpha SN, the rate of primary nucleation increased in the presence of PEI-HSA NPs. The aggregation rate changed in a PEI-HSA NP-concentration dependent and size independent manner and led to fibrils which were covered with small aggregates. Furthermore, PEI-HSA NPs reduced the level of membrane-perturbing oligomers and reduced oligomer toxicity in cell assays, highlighting a potential role for NPs in reducing alpha SN pathogenicity in vivo. Collectively, our results highlight the fact that a simple modification of NPs can strongly modulate interactions with target proteins, which may have important and positive implications in NP safety.