Issue 13, 2018

Folding mechanisms steer the amyloid fibril formation propensity of highly homologous proteins

Abstract

Significant advances in the understanding of the molecular determinants of fibrillogenesis can be expected from comparative studies of the aggregation propensities of proteins with highly homologous structures but different folding pathways. Here, we fully characterize, by means of stopped-flow, T-jump, CD and DSC experiments, the unfolding mechanisms of three highly homologous proteins, zinc binding Ros87 and Ml153–149 and zinc-lacking Ml452–151. The results indicate that the three proteins significantly differ in terms of stability and (un)folding mechanisms. Particularly, Ros87 and Ml153–149 appear to be much more stable to guanidine denaturation and are characterized by folding mechanisms including the presence of an intermediate. On the other hand, metal lacking Ml452–151 folds according to a classic two-state model. Successively, we have monitored the capabilities of Ros87, Ml452–151 and Ml153–149 to form amyloid fibrils under native conditions. Particularly, we show, by CD, fluorescence, DLS, TEM and SEM experiments, that after 168 hours, amyloid formation of Ros87 has started, while Ml153–149 has formed only amorphous aggregates and Ml452–151 is still monomeric in solution. This study shows how metal binding can influence protein folding pathways and thereby control conformational accessibility to aggregation-prone states, which in turn changes aggregation kinetics, shedding light on the role of metal ions in the development of protein deposition diseases.

Graphical abstract: Folding mechanisms steer the amyloid fibril formation propensity of highly homologous proteins

Supplementary files

Article information

Article type
Edge Article
Submitted
11 Phe 2018
Accepted
28 Kol 2018
First published
01 Ube 2018
This article is Open Access

All publication charges for this article have been paid for by the Royal Society of Chemistry
Creative Commons BY license

Chem. Sci., 2018,9, 3290-3298

Folding mechanisms steer the amyloid fibril formation propensity of highly homologous proteins

G. Malgieri, G. D'Abrosca, L. Pirone, A. Toto, M. Palmieri, L. Russo, M. F. M. Sciacca, R. Tatè, V. Sivo, I. Baglivo, R. Majewska, M. Coletta, P. V. Pedone, C. Isernia, M. De Stefano, S. Gianni, E. M. Pedone, D. Milardi and R. Fattorusso, Chem. Sci., 2018, 9, 3290 DOI: 10.1039/C8SC00166A

This article is licensed under a Creative Commons Attribution 3.0 Unported Licence. You can use material from this article in other publications without requesting further permissions from the RSC, provided that the correct acknowledgement is given.

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