Gallardo, R; Ramakers, M; De Smet, F; Claes, F; Khodaparast, L; Khodaparast, L; Couceiro, JR; ... Rousseau, F; + view all Gallardo, R; Ramakers, M; De Smet, F; Claes, F; Khodaparast, L; Khodaparast, L; Couceiro, JR; Langenberg, T; Siemons, M; Nyström, S; Young, LJ; Laine, RF; Young, L; Radaelli, E; Benilova, I; Kumar, M; Staes, A; Desager, M; Beerens, M; Vandervoort, P; Luttun, A; Gevaert, K; Bormans, G; Dewerchin, M; Van Eldere, J; Carmeliet, P; Vande Velde, G; Verfaillie, C; Kaminski, CF; De Strooper, B; Hammarström, P; Nilsson, KPR; Serpell, L; Schymkowitz, J; Rousseau, F; - view fewer (2016) De novo design of a biologically active amyloid. Science , 354 (6313) , Article aah4949. 10.1126/science.aah4949.

Preview

Text De Strooper_Gallardo et al_Science 2016_author's copy.pdf - Accepted Version Download (14MB) | Preview

Abstract

Most human proteins possess amyloidogenic segments, but only about 30 are associated with amyloid-associated pathologies, and it remains unclear what determines amyloid toxicity. We designed vascin, a synthetic amyloid peptide, based on an amyloidogenic fragment of vascular endothelial growth factor receptor 2 (VEGFR2), a protein that is not associated to amyloidosis. Vascin recapitulates key biophysical and biochemical characteristics of natural amyloids, penetrates cells, and seeds the aggregation of VEGFR2 through direct interaction. We found that amyloid toxicity is observed only in cells that both express VEGFR2 and are dependent on VEGFR2 activity for survival. Thus, amyloid toxicity here appears to be both protein-specific and conditional-determined by VEGFR2 loss of function in a biological context in which target protein function is essential.

Download activity - last month

Export as CSVXMLJSON

Download activity - last 12 months

Export as JSONCSVXML

Downloads by country - last 12 months

Export as XMLCSVJSON

Archive Staff Only

View Item