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Halogen-enriched fragment libraries as leads for drug rescue of mutant p53.


ABSTRACT: The destabilizing p53 cancer mutation Y220C creates a druggable surface crevice. We developed a strategy exploiting halogen bonding for lead discovery to stabilize the mutant with small molecules. We designed halogen-enriched fragment libraries (HEFLibs) as starting points to complement classical approaches. From screening of HEFLibs and subsequent structure-guided design, we developed substituted 2-(aminomethyl)-4-ethynyl-6-iodophenols as p53-Y220C stabilizers. Crystal structures of their complexes highlight two key features: (i) a central scaffold with a robust binding mode anchored by halogen bonding of an iodine with a main-chain carbonyl and (ii) an acetylene linker, enabling the targeting of an additional subsite in the crevice. The best binders showed induction of apoptosis in a human cancer cell line with homozygous Y220C mutation. Our structural and biophysical data suggest a more widespread applicability of HEFLibs in drug discovery.

SUBMITTER: Wilcken R 

PROVIDER: S-EPMC3789257 | biostudies-literature | 2012 Apr

REPOSITORIES: biostudies-literature

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Halogen-enriched fragment libraries as leads for drug rescue of mutant p53.

Wilcken Rainer R   Liu Xiangrui X   Zimmermann Markus O MO   Rutherford Trevor J TJ   Fersht Alan R AR   Joerger Andreas C AC   Boeckler Frank M FM  

Journal of the American Chemical Society 20120405 15


The destabilizing p53 cancer mutation Y220C creates a druggable surface crevice. We developed a strategy exploiting halogen bonding for lead discovery to stabilize the mutant with small molecules. We designed halogen-enriched fragment libraries (HEFLibs) as starting points to complement classical approaches. From screening of HEFLibs and subsequent structure-guided design, we developed substituted 2-(aminomethyl)-4-ethynyl-6-iodophenols as p53-Y220C stabilizers. Crystal structures of their compl  ...[more]

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