Literature DB >> 18364257

Ranking the selectivity of PubChem screening hits by activity-based protein profiling: MMP13 as a case study.

Ryuichiro Nakai1, Cleo M Salisbury, Hugh Rosen, Benjamin F Cravatt.   

Abstract

High-throughput screening (HTS) has become an integral part of academic and industrial efforts aimed at developing new chemical probes and drugs. These screens typically generate several 'hits', or lead active compounds, that must be prioritized for follow-up medicinal chemistry studies. Among primary considerations for ranking lead compounds is selectivity for the intended target, especially among mechanistically related proteins. Here, we show how the chemical proteomic technology activity-based protein profiling (ABPP) can serve as a universal assay to rank HTS hits based on their selectivity across many members of an enzyme superfamily. As a case study, four metalloproteinase-13 (MMP13) inhibitors of similar potency originating from a publically supported HTS and reported in PubChem were tested by ABPP for selectivity against a panel of 27 diverse metalloproteases. The inhibitors could be readily separated into two groups: (1) those that were active against several metalloproteases and (2) those that showed high selectivity for MMP13. The latter set of inhibitors was thereby designated as more suitable for future medicinal chemistry optimization. We anticipate that ABPP will find general utility as a platform to rank the selectivity of lead compounds emerging from HTS assays for a wide variety of enzymes.

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Year:  2008        PMID: 18364257      PMCID: PMC2661618          DOI: 10.1016/j.bmc.2008.03.018

Source DB:  PubMed          Journal:  Bioorg Med Chem        ISSN: 0968-0896            Impact factor:   3.641


  26 in total

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3.  Reversible inhibitors of fatty acid amide hydrolase that promote analgesia: evidence for an unprecedented combination of potency and selectivity.

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4.  S1P1-selective in vivo-active agonists from high-throughput screening: off-the-shelf chemical probes of receptor interactions, signaling, and fate.

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5.  Proteomic profiling of metalloprotease activities with cocktails of active-site probes.

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8.  ADAM 12, a disintegrin metalloprotease, interacts with insulin-like growth factor-binding protein-3.

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9.  Identification of peptide substrates for human MMP-11 (stromelysin-3) using phage display.

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Authors:  Reid G Hendry; Leanne M Bilawchuk; David J Marchant
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Review 3.  Inhibition of MMPs and ADAM/ADAMTS.

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Journal:  Biochem Pharmacol       Date:  2019-02-28       Impact factor: 5.858

4.  A novel method for mining highly imbalanced high-throughput screening data in PubChem.

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Journal:  J Med Chem       Date:  2014-11-11       Impact factor: 7.446

6.  Tofacitinib Inhibits STAT Phosphorylation and Matrix Metalloproteinase-3, -9 and -13 Production by C28/I2 Human Juvenile Chondrocytes.

Authors:  Jessica R Thorpe; Rachel A Wilson; Sam Mesiano; Charles J Malemud
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7.  Substrate-driven mapping of the degradome by comparison of sequence logos.

Authors:  Julian E Fuchs; Susanne von Grafenstein; Roland G Huber; Christian Kramer; Klaus R Liedl
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  7 in total

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