Literature DB >> 28355876

Diverse Redoxome Reactivity Profiles of Carbon Nucleophiles.

Vinayak Gupta1, Jing Yang2, Daniel C Liebler3, Kate S Carroll1.   

Abstract

Targeted covalent inhibitors have emerged as a powerful approach in the drug discovery pipeline. Key to this process is the identification of signaling pathways (or receptors) specific to (or overexpressed in) disease cells. In this context, fragment-based ligand discovery (FBLD) has significantly expanded our view of the ligandable proteome and affords tool compounds for biological inquiry. To date, such covalent ligand discovery has almost exclusively employed cysteine-reactive small-molecule fragments. However, functional cysteine residues in proteins are often redox-sensitive and can undergo oxidation in cells. Such reactions are particularly relevant in diseases, like cancer, which are linked to excessive production of reactive oxygen species. Once oxidized, the sulfur atom of cysteine is much less reactive toward electrophilic groups used in the traditional FBLD paradigm. To address this limitation, we recently developed a novel library of diverse carbon-based nucleophile fragments that react selectively with cysteine sulfenic acid formed in proteins via oxidation or hydrolysis reactions. Here, we report analysis of sulfenic acid-reactive C-nucleophile fragments screened against a colon cancer cell proteome. Covalent ligands were identified for >1280 S-sulfenylated cysteines present in "druggable" proteins and orphan targets, revealing disparate reactivity profiles and target preferences. Among the unique ligand-protein interactions identified was that of a pyrrolidinedione nucleophile that reacted preferentially with protein tyrosine phosphatases. Fragment-based covalent ligand discovery with C-nucleophiles affords an expansive snapshot of the ligandable "redoxome" with significant implications for covalent inhibitor pharmacology and also affords new chemical tools to investigate redox-regulation of protein function.

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Year:  2017        PMID: 28355876      PMCID: PMC5898444          DOI: 10.1021/jacs.7b01791

Source DB:  PubMed          Journal:  J Am Chem Soc        ISSN: 0002-7863            Impact factor:   15.419


  52 in total

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2.  Disparate proteome reactivity profiles of carbon electrophiles.

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Journal:  Nat Chem Biol       Date:  2008-05-18       Impact factor: 15.040

3.  Simple synthesis of 1,3-cyclopentanedione derived probes for labeling sulfenic acid proteins.

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Review 4.  Protein arginine methyltransferases and cancer.

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Journal:  Nat Rev Cancer       Date:  2012-12-13       Impact factor: 60.716

5.  Rational design of reversible and irreversible cysteine sulfenic acid-targeted linear C-nucleophiles.

Authors:  Vinayak Gupta; Kate S Carroll
Journal:  Chem Commun (Camb)       Date:  2016-02-25       Impact factor: 6.222

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  31 in total

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2.  Isotopic tagging of oxidized and reduced cysteines (iTORC) for detecting and quantifying sulfenic acids, disulfides, and free thiols in cells.

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3.  Mining for protein S-sulfenylation in Arabidopsis uncovers redox-sensitive sites.

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Review 4.  Proteome-Wide Analysis of Cysteine S-Sulfenylation Using a Benzothiazine-Based Probe.

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6.  Cysteine modifications (oxPTM) and protein sulphenylation-mediated sulfenome expression in plants: evolutionary conserved signaling networks?

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Review 7.  Recent Advances in Selective and Irreversible Covalent Ligand Development and Validation.

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Review 8.  Redox Signaling by Reactive Electrophiles and Oxidants.

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9.  Sulfenylation of Human Liver and Kidney Microsomal Cytochromes P450 and Other Drug-Metabolizing Enzymes as a Response to Redox Alteration.

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10.  A quantitative thiol reactivity profiling platform to analyze redox and electrophile reactive cysteine proteomes.

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