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Hitting on the move: Targeting intrinsically disordered protein states of the MDM2-p53 interaction.


ABSTRACT: Intrinsically disordered proteins are an emerging class of proteins without a folded structure and currently disorder-based drug targeting remains a challenge. p53 is the principal regulator of cell division and growth whereas MDM2 consists its main negative regulator. The MDM2-p53 recognition is a dynamic and multistage process that amongst other, employs the dissociation of a transient ?-helical N-terminal ''lid'' segment of MDM2 from the proximity of the p53-complementary interface. Several small molecule inhibitors have been reported to inhibit the formation of the p53-MDM2 complex with the vast majority mimicking the p53 residues Phe19, Trp23 and Leu26. Recently, we have described the transit from the 3-point to 4-point pharmacophore model stabilizing this intrinsically disordered N-terminus by increasing the binding affinity by a factor of 3. Therefore, we performed a thorough SAR analysis, including chiral separation of key compound which was evaluated by FP and 2D NMR. Finally, p53-specific anti-cancer activity towards p53-wild-type cancer cells was observed for several representative compounds.

SUBMITTER: Neochoritis CG 

PROVIDER: S-EPMC7008132 | biostudies-literature | 2019 Nov

REPOSITORIES: biostudies-literature

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Hitting on the move: Targeting intrinsically disordered protein states of the MDM2-p53 interaction.

Neochoritis Constantinos G CG   Atmaj Jack J   Twarda-Clapa Aleksandra A   Surmiak Ewa E   Skalniak Lukasz L   Köhler Lisa-Maria LM   Muszak Damian D   Kurpiewska Katarzyna K   Kalinowska-Tłuścik Justyna J   Beck Barbara B   Holak Tad A TA   Dömling Alexander A  

European journal of medicinal chemistry 20190806


Intrinsically disordered proteins are an emerging class of proteins without a folded structure and currently disorder-based drug targeting remains a challenge. p53 is the principal regulator of cell division and growth whereas MDM2 consists its main negative regulator. The MDM2-p53 recognition is a dynamic and multistage process that amongst other, employs the dissociation of a transient α-helical N-terminal ''lid'' segment of MDM2 from the proximity of the p53-complementary interface. Several s  ...[more]

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