Fragmenting the S100B-p53 interaction: Combined virtual/biophysical screening approaches to identify ligands

Mariangela Agamennone; Lucia Cesari; Daniela Lalli; Elisa Turlizzi; Rebecca Del Conte; Paola Turano; Stefano Mangani; Alessandro Padova

doi:10.1002/cmdc.200900393

Fragmenting the S100B-p53 interaction: Combined virtual/biophysical screening approaches to identify ligands

Mariangela Agamennone, Lucia Cesari, Daniela Lalli, Elisa Turlizzi, Rebecca Del Conte, Paola Turano, Stefano Mangani, Alessandro Padova

Risultato della ricerca: Contributo su rivista › Articolo in rivista › peer review

Abstract

S100B contributes to cell proliferation by binding the C terminus of p53 and inhibiting its tumor suppressor function. The use of multiple computational approaches to screen fragment libraries targeting the human S100B-p53 interaction site is reported. This in silico screening led to the identification of 280 novel prospective ligands. NMR spectroscopic experiments revealed specific binding at the p53 interaction site for a set of these compounds and confirmed their potential for further rational optimization. The X-ray crystal structure determined for one of the binders revealed key intermolecular interactions, thus paving the way for structure-based ligand optimization.

Lingua originale	Inglese
pagine (da-a)	428-435
Numero di pagine	8
Rivista	ChemMedChem
Volume	5
Numero di pubblicazione	3
DOI	https://doi.org/10.1002/cmdc.200900393
Stato di pubblicazione	Pubblicato - 1 mar 2010
Pubblicato esternamente	Sì

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abstract = "S100B contributes to cell proliferation by binding the C terminus of p53 and inhibiting its tumor suppressor function. The use of multiple computational approaches to screen fragment libraries targeting the human S100B-p53 interaction site is reported. This in silico screening led to the identification of 280 novel prospective ligands. NMR spectroscopic experiments revealed specific binding at the p53 interaction site for a set of these compounds and confirmed their potential for further rational optimization. The X-ray crystal structure determined for one of the binders revealed key intermolecular interactions, thus paving the way for structure-based ligand optimization.",

keywords = "Fragment-based drug design, NMR spectroscopy, Protein-protein interactions, X-ray diffraction",

author = "Mariangela Agamennone and Lucia Cesari and Daniela Lalli and Elisa Turlizzi and {Del Conte}, Rebecca and Paola Turano and Stefano Mangani and Alessandro Padova",

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AU - Turlizzi, Elisa

AU - Del Conte, Rebecca

AU - Turano, Paola

AU - Mangani, Stefano

AU - Padova, Alessandro

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AB - S100B contributes to cell proliferation by binding the C terminus of p53 and inhibiting its tumor suppressor function. The use of multiple computational approaches to screen fragment libraries targeting the human S100B-p53 interaction site is reported. This in silico screening led to the identification of 280 novel prospective ligands. NMR spectroscopic experiments revealed specific binding at the p53 interaction site for a set of these compounds and confirmed their potential for further rational optimization. The X-ray crystal structure determined for one of the binders revealed key intermolecular interactions, thus paving the way for structure-based ligand optimization.

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Fragmenting the S100B-p53 interaction: Combined virtual/biophysical screening approaches to identify ligands

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