Stapled peptides in the p53 pathway: Computer simulations reveal novel interactions of the staples with the target protein

Stapled peptides in the p53 pathway: Computer simulations reveal novel interactions of the staples with the target protein

Atomistic simulations of a set of stapled peptides derived from the transactivation domain of p53 (designed by Verdine & colleagues, JACS 2007 129:2456) and complexed to MDM2 reveal that the good binders are uniquely characterized by higher helicity and by extensive interactions between the hydr...

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Veröffentlicht in:Cell cycle (Georgetown, Tex.) Tex.), 2010-11, Vol.9 (22), p.4560-4568
Hauptverfasser: Joseph, Thomas Leonard, Lane, David, Verma, Chandra S.
Format: Artikel
Sprache:eng
Schlagworte:
Amino Acid Sequence
Binding
Biology
Bioscience
Calcium
Cancer
Cell
Cycle
Humans
Landes
Molecular Dynamics Simulation
Molecular Sequence Data
Nuclear Proteins - antagonists & inhibitors
Nuclear Proteins - metabolism
Organogenesis
Peptides - chemistry
Protein Binding
Protein Structure, Tertiary
Proteins
Proto-Oncogene Proteins - antagonists & inhibitors
Proto-Oncogene Proteins - metabolism
Proto-Oncogene Proteins c-mdm2 - chemistry
Proto-Oncogene Proteins c-mdm2 - metabolism
Tumor Suppressor Protein p53 - chemistry
Tumor Suppressor Protein p53 - metabolism
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Zusammenfassung:Atomistic simulations of a set of stapled peptides derived from the transactivation domain of p53 (designed by Verdine & colleagues, JACS 2007 129:2456) and complexed to MDM2 reveal that the good binders are uniquely characterized by higher helicity and by extensive interactions between the hydrocarbon staples and the MDM2 surface; in contrast the poor binders have reduced helicity and their staples are mostly solvent exposed. Our studies also find that the best binders can also potentially inhibit MDMX with similar affinities, suggesting that such stapled peptides can be evolved for dual inhibition with therapeutic potential.
ISSN:1538-4101
1551-4005
DOI:10.4161/cc.9.22.13816