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- W2890477831 endingPage "2161" @default.
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- W2890477831 abstract "The molecular chaperones are central mediators of protein homeostasis. In that role, they engage in widespread protein-protein interactions (PPIs) with each other and with their client proteins. Together, these PPIs form the backbone of a network that ensures proper vigilance over the processes of protein folding, trafficking, quality control, and degradation. The core chaperones, such as the heat shock proteins Hsp60, Hsp70, and Hsp90, are widely expressed in most tissues, yet there is growing evidence that the PPIs among them may be re-wired in disease conditions. This possibility suggests that these PPIs, and perhaps not the individual chaperones themselves, could be compelling drug targets. Indeed, recent efforts have yielded small molecules that inhibit (or promote) a subset of inter-chaperone PPIs. These chemical probes are being used to study chaperone networks in a range of models, and the successes with these approaches have inspired a community-wide objective to produce inhibitors for a broader set of targets. In this Review, we discuss progress toward that goal and point out some of the challenges ahead." @default.
- W2890477831 created "2018-09-27" @default.
- W2890477831 creator A5040066574 @default.
- W2890477831 creator A5067529915 @default.
- W2890477831 date "2019-02-01" @default.
- W2890477831 modified "2023-10-17" @default.
- W2890477831 title "Inhibitors and chemical probes for molecular chaperone networks" @default.
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