Publications by authors named "Kristine Senkane"

Article Synopsis
  • Creatine kinases (CKs) help make energy during times when our bodies need lots of it, like when we're growing or exercising a lot.
  • In some fast-growing cancers, problems with CKs can cause issues, but we don’t have effective medicines to target them yet.
  • Researchers created a new drug called CKi which specifically targets CKs, making it harmful to certain cancer cells, and found it also helps understand how CKs affect inflammation in immune cells.
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The emerging use of covalent ligands as chemical probes and drugs would benefit from an expanded repertoire of cysteine-reactive electrophiles for efficient and diverse targeting of the proteome. Here we use the endogenous electrophile sensor of mammalian cells, the KEAP1-NRF2 pathway, to discover cysteine-reactive electrophilic fragments from a reporter-based screen for NRF2 activation. This strategy identified a series of 2-sulfonylpyridines that selectively react with biological thiols via nucleophilic aromatic substitution (SAr).

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Reversible covalency, achieved with, for instance, highly electron-deficient olefins, offers a compelling strategy to design chemical probes and drugs that benefit from the sustained target engagement afforded by irreversible compounds, while avoiding permanent protein modification. Reversible covalency has mainly been evaluated for cysteine residues in individual kinases and the broader potential for this strategy to engage cysteines across the proteome remains unexplored. Herein, we describe a mass-spectrometry-based platform that integrates gel filtration with activity-based protein profiling to assess cysteine residues across the human proteome for both irreversible and reversible interactions with small-molecule electrophiles.

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