A Suite of "Minimalist" Photo-Crosslinkers for Live-Cell Imaging and Chemical Proteomics: Case Study with BRD4 Inhibitors

Authors
Pan, SijunJang, Se-YoungWang, DanyangLiew, Si SiLi, ZhengqiuLee, Jun-SeokYao, Shao Q.
Issue Date
2017-09-18
Publisher
John Wiley & Sons Ltd.
Citation
Angewandte Chemie International Edition, v.56, no.39, pp.11816 - 11821
Abstract
Affinity-based probes (AfBPs) provide a powerful tool for large-scale chemoproteomic studies of drug-target interactions. The development of high-quality probes capable of recapitulating genuine drug-target engagement, however, could be challenging. Minimalist photo-crosslinkers, which contain an alkyl diazirine group and a chemically tractable tag, could alleviate such challenges, but few are currently available. Herein, we have developed new alkyl diazirine-containing photo-crosslinkers with different bioorthogonal tags. They were subsequently used to create a suite of AfBPs based on GW841819X (a small molecule inhibitor of BRD4). Through invitro and insitu studies under conditions that emulated native drug-target interactions, we have obtained better insights into how a tag might affect the probe's performance. Finally, SILAC-based chemoproteomic studies have led to the discovery of a novel off-target, APEX1. Further studies showed GW841819X binds to APEX1 and caused up-regulation of endogenous DNMT1 expression under normoxia conditions.
Keywords
AFFINITY-BASED PROBES; TARGET IDENTIFICATION; BIOORTHOGONAL LIGATION; KINASE INHIBITORS; ENGAGEMENT; MOLECULES; DISCOVERY; PROTEINS; STRATEGY; AFFINITY-BASED PROBES; TARGET IDENTIFICATION; BIOORTHOGONAL LIGATION; KINASE INHIBITORS; ENGAGEMENT; MOLECULES; DISCOVERY; PROTEINS; STRATEGY; affinity-based probes; bioorthogonal chemistry; epigenetics; live-cell imaging; photo-crosslinkers
ISSN
1433-7851
URI
https://pubs.kist.re.kr/handle/201004/122273
DOI
10.1002/anie.201706076
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KIST Article > 2017
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