Publications by authors named "Youlong Fan"

Covalent probes coupled with chemical proteomics represent a powerful method for investigating small molecule and protein interactions. However, the creation of a reactive warhead within various ligands to form covalent probes has been a major obstacle. Herein, we report a convenient and robust process to assemble a unique electrophile, an α-acyloxyenamide, through a one-step late-stage coupling reaction.

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Because very few targets are currently available for drug development, triple-negative breast cancer (TNBC) has been defined as one of the most difficult diseases for chemotherapy. Herein, we describe a suite of novel electrophilic warheads, which we have used in chemical proteomics studies in a search for potential targets for TNBC. Binding site analysis revealed that these warheads can modify not only highly nucleophilic residues, including cysteine and lysine, but also weakly nucleophilic residues.

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Hepatocellular carcinoma (HCC) is one of the most common malignant tumors. Identification of the underlying mechanism of HCC progression and exploration of new therapeutic drugs are urgently needed. Here, a compound library consisting of 419 FDA-approved drugs was taken to screen potential anticancer drugs.

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Article Synopsis
  • The "inverse drug discovery" strategy explores new cellular targets that aren't typically tapped into by traditional medicinal chemistry.
  • Cyclopropenone, a strong electrophile, has been studied for its ability to react with proteins in live cells, specifically targeting the GSTP1 protein linked to triple-negative breast cancer.
  • The research revealed that cyclopropenones can modify GSTP1 and led to the creation of effective inhibitors that counteract this cancer-driving protein.
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Solution acidification exists under some physiological conditions (e.g. lysosomes in cells) and diseases (e.

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Protein modification by chemical reagents has played an essential role in the treatment of human diseases. However, the reagents currently used are limited to the covalent modification of cysteine and lysine residues. It is thus desirable to develop novel methods that can covalently modify other residues.

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