The aim of the project is to obtain an understanding of the atomic mechanisms and interactions which determine whether an amyloidogenic peptide forms a fibril or aggregates into an amorphous or oligomeric structure. In particular, we will study the conformation of Aβ aggregates in presence of αB-crystallin, and characterise the confor¬mational changes in comparison to Aβ fibril structure. In addition, we investigate cross-amyloid interaction surface mimic (ISM) inhibitors that efficiently prevent fibril formation and rescue cells from the cytotoxicity induced by Aβ. Furthermore, we will study the influence of other cellular components on the structure and the dynamics of the aggregates, which are commonly found co aggregated in vivo, such as glycosaminoglycans (GAGs) and serum amyloid P (SAP). The final goal is to understand how structural changes correlate with cellular toxicity.

DFG Programme Collaborative Research Centres

Subproject of SFB 1035:  Control of Protein Function by Conformational Switching

Applicant Institution Technische Universität München (TUM)

Project Head Professor Dr. Bernd Reif