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Potential pharmacological chaperones targeting cancer-associated MCL-1 and Parkinson disease-associated alpha-synuclein SCIE SCOPUS

Title
Potential pharmacological chaperones targeting cancer-associated MCL-1 and Parkinson disease-associated alpha-synuclein
Authors
Oh, MLee, JHWang, WLee, HSLee, WSBurlak, CIm, WHoang, QQLim, HS
Date Issued
2014-07-29
Publisher
NATL ACAD SCIENCES
Abstract
Pharmacological chaperones are small molecules that bind to proteins and stabilize them against thermal denaturation or proteolytic degradation, as well as assist or prevent certain protein-protein assemblies. These activities are being exploited for the development of treatments for diseases caused by protein instability and/or aberrant protein-protein interactions, such as those found in certain forms of cancers and neurodegenerative diseases. However, designing or discovering pharmacological chaperones for specific targets is challenging because of the relatively featureless protein target surfaces, the lack of suitable chemical libraries, and the shortage of efficient high-throughput screening methods. In this study, we attempted to address all these challenges by synthesizing a diverse library of small molecules that mimic protein a-helical secondary structures commonly found in protein-protein interaction surfaces. This was accompanied by establishing a facile "on-bead" high-throughput screening method that allows for rapid and efficient discovery of potential pharmacological chaperones and for identifying novel chaperones/inhibitors against a cancer-associated protein, myeloid cell leukemia 1 (MCL-1), and a Parkinson disease-associated protein, a-synuclein. Our data suggest that the compounds and methods described here will be useful tools for the development of pharmaceuticals for complex-disease targets that are traditionally deemed "undruggable.
Keywords
hemical biology; drug discovery; helical mimetic; PROTEIN-PROTEIN INTERACTIONS; SOLID-PHASE SYNTHESIS; SMALL-MOLECULE; HELIX MIMETICS; COMBINATORIAL LIBRARIES; PEPTIDE LIBRARY; DRUG DISCOVERY; HOT-SPOTS; PEPTOIDS; INHIBITION
URI
https://oasis.postech.ac.kr/handle/2014.oak/13040
DOI
10.1073/PNAS.1320556111
ISSN
0027-8424
Article Type
Article
Citation
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, vol. 111, no. 30, page. 11007 - 11012, 2014-07-29
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임현석LIM, HYUN SUK
Dept of Chemistry
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