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PAC-FragmentDEL – photoactivated covalent capture of DNA-encoded fragments for hit discovery

We describe a novel approach for screening fragments against a protein that combines the sensitivity of DNA-encoded library technology with the ability of fragments to explore what will bind. Each of the members of the library consists of a fragment which is linked to a photoactivatable diazirine mo...

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Autores principales: Ma, Huiyong, Murray, James B., Luo, Huadong, Cheng, Xuemin, Chen, Qiuxia, Song, Chao, Duan, Cong, Tan, Ping, Zhang, Lifang, Liu, Jian, Morgan, Barry A., Li, Jin, Wan, Jinqiao, Baker, Lisa M., Finnie, William, Guetzoyan, Lucie, Harris, Richard, Hendrickson, Nicole, Matassova, Natalia, Simmonite, Heather, Smith, Julia, Hubbard, Roderick E., Liu, Guansai
Formato: Online Artículo Texto
Lenguaje:English
Publicado: RSC 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9667776/
https://www.ncbi.nlm.nih.gov/pubmed/36426238
http://dx.doi.org/10.1039/d2md00197g
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author Ma, Huiyong
Murray, James B.
Luo, Huadong
Cheng, Xuemin
Chen, Qiuxia
Song, Chao
Duan, Cong
Tan, Ping
Zhang, Lifang
Liu, Jian
Morgan, Barry A.
Li, Jin
Wan, Jinqiao
Baker, Lisa M.
Finnie, William
Guetzoyan, Lucie
Harris, Richard
Hendrickson, Nicole
Matassova, Natalia
Simmonite, Heather
Smith, Julia
Hubbard, Roderick E.
Liu, Guansai
author_facet Ma, Huiyong
Murray, James B.
Luo, Huadong
Cheng, Xuemin
Chen, Qiuxia
Song, Chao
Duan, Cong
Tan, Ping
Zhang, Lifang
Liu, Jian
Morgan, Barry A.
Li, Jin
Wan, Jinqiao
Baker, Lisa M.
Finnie, William
Guetzoyan, Lucie
Harris, Richard
Hendrickson, Nicole
Matassova, Natalia
Simmonite, Heather
Smith, Julia
Hubbard, Roderick E.
Liu, Guansai
author_sort Ma, Huiyong
collection PubMed
description We describe a novel approach for screening fragments against a protein that combines the sensitivity of DNA-encoded library technology with the ability of fragments to explore what will bind. Each of the members of the library consists of a fragment which is linked to a photoactivatable diazirine moiety. Split and pool synthesis combines each fragment with a set of linkers with the version of the library reported here containing some 70k different compounds, each with an individual DNA code. Incubation of the library with a protein sample is followed by photoactivation, washing and subsequent PCR and sequencing which allows the individual fragment hits to be identified. We illustrate how the approach allows successful hit fragment identification using only microgram quantities of material for two targets. PAK4 is a kinase for which conventional fragment screening has generated many advance leads. The as yet undrugged target, 2-epimerase, presents a more challenging active site for identification of hit compounds. In both cases, PAC-FragmentDEL identified fragments validated as hits by ligand-observed NMR measurements and crystal structure determination of off-DNA sample binding to the proteins.
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spelling pubmed-96677762022-11-23 PAC-FragmentDEL – photoactivated covalent capture of DNA-encoded fragments for hit discovery Ma, Huiyong Murray, James B. Luo, Huadong Cheng, Xuemin Chen, Qiuxia Song, Chao Duan, Cong Tan, Ping Zhang, Lifang Liu, Jian Morgan, Barry A. Li, Jin Wan, Jinqiao Baker, Lisa M. Finnie, William Guetzoyan, Lucie Harris, Richard Hendrickson, Nicole Matassova, Natalia Simmonite, Heather Smith, Julia Hubbard, Roderick E. Liu, Guansai RSC Med Chem Chemistry We describe a novel approach for screening fragments against a protein that combines the sensitivity of DNA-encoded library technology with the ability of fragments to explore what will bind. Each of the members of the library consists of a fragment which is linked to a photoactivatable diazirine moiety. Split and pool synthesis combines each fragment with a set of linkers with the version of the library reported here containing some 70k different compounds, each with an individual DNA code. Incubation of the library with a protein sample is followed by photoactivation, washing and subsequent PCR and sequencing which allows the individual fragment hits to be identified. We illustrate how the approach allows successful hit fragment identification using only microgram quantities of material for two targets. PAK4 is a kinase for which conventional fragment screening has generated many advance leads. The as yet undrugged target, 2-epimerase, presents a more challenging active site for identification of hit compounds. In both cases, PAC-FragmentDEL identified fragments validated as hits by ligand-observed NMR measurements and crystal structure determination of off-DNA sample binding to the proteins. RSC 2022-08-26 /pmc/articles/PMC9667776/ /pubmed/36426238 http://dx.doi.org/10.1039/d2md00197g Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by-nc/3.0/
spellingShingle Chemistry
Ma, Huiyong
Murray, James B.
Luo, Huadong
Cheng, Xuemin
Chen, Qiuxia
Song, Chao
Duan, Cong
Tan, Ping
Zhang, Lifang
Liu, Jian
Morgan, Barry A.
Li, Jin
Wan, Jinqiao
Baker, Lisa M.
Finnie, William
Guetzoyan, Lucie
Harris, Richard
Hendrickson, Nicole
Matassova, Natalia
Simmonite, Heather
Smith, Julia
Hubbard, Roderick E.
Liu, Guansai
PAC-FragmentDEL – photoactivated covalent capture of DNA-encoded fragments for hit discovery
title PAC-FragmentDEL – photoactivated covalent capture of DNA-encoded fragments for hit discovery
title_full PAC-FragmentDEL – photoactivated covalent capture of DNA-encoded fragments for hit discovery
title_fullStr PAC-FragmentDEL – photoactivated covalent capture of DNA-encoded fragments for hit discovery
title_full_unstemmed PAC-FragmentDEL – photoactivated covalent capture of DNA-encoded fragments for hit discovery
title_short PAC-FragmentDEL – photoactivated covalent capture of DNA-encoded fragments for hit discovery
title_sort pac-fragmentdel – photoactivated covalent capture of dna-encoded fragments for hit discovery
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9667776/
https://www.ncbi.nlm.nih.gov/pubmed/36426238
http://dx.doi.org/10.1039/d2md00197g
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