Aberrant protein aggregation causes numerous neurological diseases including Creutzfeldt Jakob disease (CJD), but the aggregation mechanisms remain poorly understood. Here, we report AFM results on the formation pathways of beta-oligomers and nonfibrillar aggregates from wild-type full-length recombinant human prion protein (WT) and an insertion mutant (10OR) with five additional octapeptide repeats linked to familial CJD. Upon partial denaturing, seeds consisting of 3-4 monomers quickly appeared. Oligomers of similar to 11-22 monomers then formed through direct interaction of seeds, rather than by subsequent monomer attachment All larger aggregates formed through association of these beta-oligomers. Although both WT and 10OR exhibited identical aggregation mechanisms, the latter oligomerized faster due to lower solubility and, hence, thermodynamic stability. This novel aggregation pathway has implications for pion diseases as well as others caused by protein aggregation.

• 出版日期2011-6-8