Abstract
Protein destabilization by mutations or external stresses may lead to misfolding and aggregation in the cell. Often, damage is not limited to a simple loss of function, but the hydrophobic exposure of aggregate surfaces may impair membrane functions and promote the aggregation of other proteins. Such a “proteinacious infectious” behavior is not limited to prion diseases. It is associated to most protein-misfolding neurodegenerative diseases and to aging in general. With the molecular chaperones and proteases, cells have evolved powerful tools that can specifically recognize and act upon misfolded and aggregated proteins. Whereas some chaperones passively prevent aggregate formation and propagation, others actively unfold and solubilize stable aggregates. In particular, ATPase chaperones and proteases serve as an intracellular defense network that can specifically identify and actively remove by refolding or degradation potentially infectious cytotoxic aggregates.
| Original language | English |
|---|---|
| Title of host publication | Protein Misfolding, Aggregation and Conformational Diseases |
| Subtitle of host publication | Part A: Protein Aggregation and Conformational Diseases |
| Editors | Vladimir N. Uversky, Anthony L. Fink |
| Publisher | Springer New York |
| Pages | 165-174 |
| Number of pages | 10 |
| ISBN (Electronic) | 9780387259192 |
| ISBN (Print) | 9780387259185 |
| DOIs | |
| State | Published - Jun 2006 |
| Externally published | Yes |