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Chemical Chaperones to Inhibit Endoplasmic Reticulum Stress: Implications in Diseasesopen access

Authors
Jeon, Jae-HoIm, SomyoungKim, Hyo ShinLee, DongyunJeong, KwiwanKu, Jin-MoNam, Tae-Gyu
Issue Date
Dec-2022
Publisher
Dove Medical Press Ltd
Keywords
endoplasmic reticulum stress; unfolded protein response; chemical chaperone; drug discovery; diabetes; cardiovascular disease; neurodegeneration; lysosomal storage disease
Citation
Drug Design, Development and Therapy, v.16, pp 4385 - 4397
Pages
13
Indexed
SCIE
SCOPUS
Journal Title
Drug Design, Development and Therapy
Volume
16
Start Page
4385
End Page
4397
URI
https://scholarworks.bwise.kr/erica/handle/2021.sw.erica/112972
DOI
10.2147/DDDT.S393816
ISSN
1177-8881
Abstract
The endoplasmic reticulum (ER) is responsible for structural transformation or folding of de novo proteins for transport to the Golgi. When the folding capacity of the ER is exceeded or excessive accumulation of misfolded proteins occurs, the ER enters a stressed condition (ER stress) and unfolded protein responses (UPR) are triggered in order to rescue cells from the stress. Recovery of ER proceeds toward either survival or cell apoptosis. ER stress is implicated in many pathologies, such as diabetes, cardiovascular diseases, inflammatory diseases, neurodegeneration, and lysosomal storage diseases. As a survival or adaptation mechanism, chaperone molecules are upregulated to manage ER stress. Chemical versions of chaperone have been developed in search of drug candidates for ER stress-related diseases. In this review, synthetic or semi-synthetic chemical chaperones are categorized according to potential therapeutic area and listed along with their chemical structure and activity. Although only a few chemical chaperones have been approved as pharmaceutical drugs, a dramatic increase in literatures over the recent decades indicates enormous amount of efforts paid by many researchers. The efforts warrant clearer understanding of ER stress and the related diseases and consequently will offer a promising drug discovery platform with chaperone activity.
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