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Amyloid-like Aggregates Sequester Numerous Metastable Proteins with Essential Cellular Functions

Overview
Journal Cell
Publisher Cell Press
Specialty Cell Biology
Date 2011 Jan 11
PMID 21215370
Citations 341
Authors
Heidi Olzscha
Sonya M Schermann
Andreas C Woerner
Stefan Pinkert
Michael H Hecht
Gian G Tartaglia
Michele Vendruscolo
Manajit Hayer-Hartl
F Ulrich Hartl
R Martin Vabulas
Affiliations
Soon will be listed here.
Abstract

Protein aggregation is linked with neurodegeneration and numerous other diseases by mechanisms that are not well understood. Here, we have analyzed the gain-of-function toxicity of artificial β sheet proteins that were designed to form amyloid-like fibrils. Using quantitative proteomics, we found that the toxicity of these proteins in human cells correlates with the capacity of their aggregates to promote aberrant protein interactions and to deregulate the cytosolic stress response. The endogenous proteins that are sequestered by the aggregates share distinct physicochemical properties: They are relatively large in size and significantly enriched in predicted unstructured regions, features that are strongly linked with multifunctionality. Many of the interacting proteins occupy essential hub positions in cellular protein networks, with key roles in chromatin organization, transcription, translation, maintenance of cell architecture and protein quality control. We suggest that amyloidogenic aggregation targets a metastable subproteome, thereby causing multifactorial toxicity and, eventually, the collapse of essential cellular functions.

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