Aberrant folding, condensation and aggregation of the Huntingtin protein (HTT) is driven by an expansion of the polyQ tract in HTT exon-1. Different protein species of HTT exon-1, including aberrantly folded monomers, oligomers, fibrils and condensates have been identified in vitro and in vivo. However, our understanding of the formation and interconversion of these protein species as well as their toxicity is limited. Moreover, how cellular factors such as molecular chaperones influence these protein species is largely unclear, preventing the development of novel therapeutic interventions in polyQ expansion diseases. In this proposal we will focus on condensates as intermediate states on the pathway to pathological aggregates. We will investigate the aberrant folding and association of the HTT exon-1 monomers and how these molecular events promote condensation and fibrilization. With the obtained insights, we will next dissect how chaperones influence aberrant folding and association of the HTT exon-1 and how they interact with HTT exon-1 condensates. We will bring specific expertise and techniques (such as Fast Relaxation Imaging) to the FOR that will allow us to analyze the underlying kinetics of these molecular processes in living cells. Collaborative work in the context of the FOR will encompass complementary in vitro, in vivo and in silico studies, providing a much deeper mechanistic understanding of the role of chaperones and condensates in protein misfolding diseases.

DFG Programme Research Units

Subproject of FOR 5872:  Chaperone-mediated regulation of the emergence of disease-causing amyloids inside biomolecular condensates