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  • Identification of Covalent ... Identification of Covalent Cyclic Peptide Inhibitors in mRNA Display
    Iskandar, Sabrina E.; Chiou, Lilly F.; Leisner, Tina M. ... Journal of the American Chemical Society, 07/2023, Volume: 145, Issue: 28
    Journal Article
    Peer reviewed

    Peptides have historically been underutilized for covalent inhibitor discovery, despite their unique abilities to interact with protein surfaces and interfaces. This is in part due to a lack of ...
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2.
  • Discovery of a 53BP1 Small ... Discovery of a 53BP1 Small Molecule Antagonist Using a Focused DNA-Encoded Library Screen
    Shell, Devan J.; Foley, Caroline A.; Wang, Qinhong ... Journal of medicinal chemistry, 10/2023, Volume: 66, Issue: 20
    Journal Article
    Peer reviewed
    Open access

    Methyl-lysine reader p53 binding protein 1 (53BP1) is a central mediator of DNA break repair and is associated with various human diseases, including cancer. Thus, high-quality 53BP1 chemical probes ...
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Available for: PNG, UM
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  • SETDB1 Triple Tudor Domain ... SETDB1 Triple Tudor Domain Ligand, (R,R)‑59, Promotes Methylation of Akt1 in Cells
    Uguen, Mélanie; Deng, Yu; Li, Fengling ... ACS chemical biology, 08/2023, Volume: 18, Issue: 8
    Journal Article
    Peer reviewed
    Open access

    Increased expression and hyperactivation of the methyltransferase SET domain bifurcated 1 (SETDB1) are commonly observed in cancer and central nervous system disorders. However, there are currently ...
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4.
  • Discovery of hit compounds ... Discovery of hit compounds for methyl-lysine reader proteins from a target class DNA-encoded library
    Shell, Devan J.; Rectenwald, Justin M.; Buttery, Peter H. ... SLAS discovery, December 2022, 2022-12-00, 20221201, 2022-12-01, Volume: 27, Issue: 8
    Journal Article
    Peer reviewed
    Open access

    •Focused DNA-encoded libraries (DELs) are effective in target class hit discovery.•Reader domains of five methyl-lysine reader proteins screened using a focused DEL.•Hit compounds identified from ...
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