Rapid Discovery of Functional Small Molecule Ligands against Proteomic Targets through Library-Against-Library Screening

[Image: see text] Identifying “druggable” targets and their corresponding therapeutic agents are two fundamental challenges in drug discovery research. The one-bead-one-compound (OBOC) combinatorial library method has been developed to discover peptides or small molecules that bind to a specific tar...

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Autores principales: Wu, Chun-Yi, Wang, Don-Hong, Wang, Xiaobing, Dixon, Seth M., Meng, Liping, Ahadi, Sara, Enter, Daniel H., Chen, Chao-Yu, Kato, Jason, Leon, Leonardo J., Ramirez, Laura M., Maeda, Yoshiko, Reis, Carolina F., Ribeiro, Brianna, Weems, Brittany, Kung, Hsing-Jien, Lam, Kit S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2016
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4908505/
https://www.ncbi.nlm.nih.gov/pubmed/27053324
http://dx.doi.org/10.1021/acscombsci.5b00194
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author Wu, Chun-Yi
Wang, Don-Hong
Wang, Xiaobing
Dixon, Seth M.
Meng, Liping
Ahadi, Sara
Enter, Daniel H.
Chen, Chao-Yu
Kato, Jason
Leon, Leonardo J.
Ramirez, Laura M.
Maeda, Yoshiko
Reis, Carolina F.
Ribeiro, Brianna
Weems, Brittany
Kung, Hsing-Jien
Lam, Kit S.
author_facet Wu, Chun-Yi
Wang, Don-Hong
Wang, Xiaobing
Dixon, Seth M.
Meng, Liping
Ahadi, Sara
Enter, Daniel H.
Chen, Chao-Yu
Kato, Jason
Leon, Leonardo J.
Ramirez, Laura M.
Maeda, Yoshiko
Reis, Carolina F.
Ribeiro, Brianna
Weems, Brittany
Kung, Hsing-Jien
Lam, Kit S.
author_sort Wu, Chun-Yi
collection PubMed
description [Image: see text] Identifying “druggable” targets and their corresponding therapeutic agents are two fundamental challenges in drug discovery research. The one-bead-one-compound (OBOC) combinatorial library method has been developed to discover peptides or small molecules that bind to a specific target protein or elicit a specific cellular response. The phage display cDNA expression proteome library method has been employed to identify target proteins that interact with specific compounds. Here, we combined these two high-throughput approaches, efficiently interrogated approximately 10(13) possible molecular interactions, and identified 91 small molecule compound beads that interacted strongly with the phage library. Of 19 compounds resynthesized, 4 were cytotoxic against cancer cells; one of these compounds was found to interact with EIF5B and inhibit protein translation. As more binding pairs are confirmed and evaluated, the “library-against-library” screening approach and the resulting small molecule–protein domain interaction database may serve as a valuable tool for basic research and drug development.
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spelling pubmed-49085052016-06-16 Rapid Discovery of Functional Small Molecule Ligands against Proteomic Targets through Library-Against-Library Screening Wu, Chun-Yi Wang, Don-Hong Wang, Xiaobing Dixon, Seth M. Meng, Liping Ahadi, Sara Enter, Daniel H. Chen, Chao-Yu Kato, Jason Leon, Leonardo J. Ramirez, Laura M. Maeda, Yoshiko Reis, Carolina F. Ribeiro, Brianna Weems, Brittany Kung, Hsing-Jien Lam, Kit S. ACS Comb Sci [Image: see text] Identifying “druggable” targets and their corresponding therapeutic agents are two fundamental challenges in drug discovery research. The one-bead-one-compound (OBOC) combinatorial library method has been developed to discover peptides or small molecules that bind to a specific target protein or elicit a specific cellular response. The phage display cDNA expression proteome library method has been employed to identify target proteins that interact with specific compounds. Here, we combined these two high-throughput approaches, efficiently interrogated approximately 10(13) possible molecular interactions, and identified 91 small molecule compound beads that interacted strongly with the phage library. Of 19 compounds resynthesized, 4 were cytotoxic against cancer cells; one of these compounds was found to interact with EIF5B and inhibit protein translation. As more binding pairs are confirmed and evaluated, the “library-against-library” screening approach and the resulting small molecule–protein domain interaction database may serve as a valuable tool for basic research and drug development. American Chemical Society 2016-04-06 2016-06-13 /pmc/articles/PMC4908505/ /pubmed/27053324 http://dx.doi.org/10.1021/acscombsci.5b00194 Text en Copyright © 2016 American Chemical Society This is an open access article published under an ACS AuthorChoice License (http://pubs.acs.org/page/policy/authorchoice_termsofuse.html) , which permits copying and redistribution of the article or any adaptations for non-commercial purposes.
spellingShingle Wu, Chun-Yi
Wang, Don-Hong
Wang, Xiaobing
Dixon, Seth M.
Meng, Liping
Ahadi, Sara
Enter, Daniel H.
Chen, Chao-Yu
Kato, Jason
Leon, Leonardo J.
Ramirez, Laura M.
Maeda, Yoshiko
Reis, Carolina F.
Ribeiro, Brianna
Weems, Brittany
Kung, Hsing-Jien
Lam, Kit S.
Rapid Discovery of Functional Small Molecule Ligands against Proteomic Targets through Library-Against-Library Screening
title Rapid Discovery of Functional Small Molecule Ligands against Proteomic Targets through Library-Against-Library Screening
title_full Rapid Discovery of Functional Small Molecule Ligands against Proteomic Targets through Library-Against-Library Screening
title_fullStr Rapid Discovery of Functional Small Molecule Ligands against Proteomic Targets through Library-Against-Library Screening
title_full_unstemmed Rapid Discovery of Functional Small Molecule Ligands against Proteomic Targets through Library-Against-Library Screening
title_short Rapid Discovery of Functional Small Molecule Ligands against Proteomic Targets through Library-Against-Library Screening
title_sort rapid discovery of functional small molecule ligands against proteomic targets through library-against-library screening
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4908505/
https://www.ncbi.nlm.nih.gov/pubmed/27053324
http://dx.doi.org/10.1021/acscombsci.5b00194
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