Title | A comparative study of the relationship between protein structure and beta-aggregation in globular and intrinsically disordered proteins. |
Publication Type | Journal Article |
Year of Publication | 2004 |
Authors | Linding R, Schymkowitz J, Rousseau F, Diella F, Serrano L |
Journal | J Mol Biol |
Volume | 342 |
Issue | 1 |
Pagination | 345-53 |
Date Published | 2004 Sep 03 |
ISSN | 0022-2836 |
Keywords | Algorithms, Humans, Hydrophobic and Hydrophilic Interactions, Protein Conformation, Proteins |
Abstract | A growing number of proteins are being identified that are biologically active though intrinsically disordered, in sharp contrast with the classic notion that proteins require a well-defined globular structure in order to be functional. At the same time recent work showed that aggregation and amyloidosis are initiated in amino acid sequences that have specific physico-chemical properties in terms of secondary structure propensities, hydrophobicity and charge. In intrinsically disordered proteins (IDPs) such sequences would be almost exclusively solvent-exposed and therefore cause serious solubility problems. Further, some IDPs such as the human prion protein, synuclein and Tau protein are related to major protein conformational diseases. However, this scenario contrasts with the large number of unstructured proteins identified, especially in higher eukaryotes, and the fact that the solubility of these proteins is often particularly good. We have used the algorithm TANGO to compare the beta aggregation tendency of a set of globular proteins derived from SCOP and a set of 296 experimentally verified, non-redundant IDPs but also with a set of IDPs predicted by the algorithms DisEMBL and GlobPlot. Our analysis shows that the beta-aggregation propensity of all-alpha, all-beta and mixed alpha/beta globular proteins as well as membrane-associated proteins is fairly similar. This illustrates firstly that globular structures possess an appreciable amount of structural frustration and secondly that beta-aggregation is not determined by hydrophobicity and beta-sheet propensity alone. We also show that globular proteins contain almost three times as much aggregation nucleating regions as IDPs and that the formation of highly structured globular proteins comes at the cost of a higher beta-aggregation propensity because both structure and aggregation obey very similar physico-chemical constraints. Finally, we discuss the fact that although IDPs have a much lower aggregation propensity than globular proteins, this does not necessarily mean that they have a lower potential for amyloidosis. |
DOI | 10.1016/j.jmb.2004.06.088 |
Alternate Journal | J Mol Biol |
PubMed ID | 15313629 |