Druggability Assessment of Allosteric Proteins by Dynamics Simulations in the Presence of Probe Molecules

Bakan, Ahmet; Nevins, Neysa; Lakdawala, Ami S.; Bahar, İvet

doi:10.1021/ct300117j

Cited by 142 publications

(185 citation statements)

References 83 publications

Supporting

Mentioning

179

Contrasting

Order By: Relevance

“…Currently, the only approaches to cryptic site discovery are exhaustive site-directed small-molecule tethering by experiment (20–22), long time-scale molecular dynamics simulations by computation (6, 8, 23, 24), flexible docking (25, 26), and computational tools for identification of small-molecule binding hot spots (10, 27–30). All of these approaches are time-consuming, expensive, and/or not always successful.…”

Section: Introductionmentioning

confidence: 99%

CryptoSite: Expanding the Druggable Proteome by Characterization and Prediction of Cryptic Binding Sites

Cimermančič

Weinkam

Rettenmaier

et al. 2016

Journal of Molecular Biology

181

293

View full text Add to dashboard Cite

Many proteins have small molecule-binding pockets that are not easily detectable in the ligand-free structures. These cryptic sites require a conformational change to become apparent; a cryptic site can therefore be defined as a site that forms a pocket in a holo structure, but not in the apo structure. Because many proteins appear to lack druggable pockets, understanding and accurately identifying cryptic sites could expand the set of drug targets. Previously, cryptic sites were identified experimentally by fragment-based ligand discovery, and computationally by long molecular dynamics simulations and fragment docking. Here, we begin by constructing a set of structurally defined apo-holo pairs with cryptic sites. Next, we comprehensively characterize the cryptic sites in terms of their sequence, structure, and dynamics attributes. We find that cryptic sites tend to be as conserved in evolution as traditional binding pockets, but are less hydrophobic and more flexible. Relying on this characterization, we use machine learning to predict cryptic sites with relatively high accuracy (for our benchmark, the true positive and false positive rates are 73% and 29%, respectively). We then predict cryptic sites in the entire structurally characterized human proteome (11,201 structures, covering 23% of all residues in the proteome). CryptoSite increases the size of the potentially “druggable” human proteome from ~40% to ~78% of disease-associated proteins. Finally, to demonstrate the utility of our approach in practice, we experimentally validate a cryptic site in protein tyrosine phosphatase 1B using a covalent ligand and NMR spectroscopy. The CryptoSite web server is available at http://salilab.org/cryptosite.

show abstract

Section: Introductionmentioning

confidence: 99%

CryptoSite: Expanding the Druggable Proteome by Characterization and Prediction of Cryptic Binding Sites

Cimermančič

Weinkam

Rettenmaier

et al. 2016

Journal of Molecular Biology

181

293

View full text Add to dashboard Cite

show abstract

“…‘Hot spots’ having all 16 probes bound are identified as druggable [19]. Bakan et al used molecular dynamics simulations for solvent mapping with a different set of small fragment probes and found that the probes bind known allosteric sites during the simulation [20]. Brown and Hajduk earlier showed that molecular dynamics simulations can capture pocket dynamics that result in a more druggable binding pocket in Bcl-xl, while preserving much of the known binding site rigidity of Akt-PH and FKBP [21].…”

Section: Resultsmentioning

confidence: 99%

“…In contrast, it is likely possible to find all known druggable sites using molecular dynamics, including some that are undetectable by our method. However, separating the signal from the noise is challenging [20], [21] since there is a tendency for many pocket openings to be observed. To be clear, our approach does not reveal any new pockets that do not already exist within the rigid structure.…”

Section: Resultsmentioning

confidence: 99%

Structure-Based Druggability Assessment of the Mammalian Structural Proteome with Inclusion of Light Protein Flexibility

2014

View full text Add to dashboard Cite

Advances reported over the last few years and the increasing availability of protein crystal structure data have greatly improved structure-based druggability approaches. However, in practice, nearly all druggability estimation methods are applied to protein crystal structures as rigid proteins, with protein flexibility often not directly addressed. The inclusion of protein flexibility is important in correctly identifying the druggability of pockets that would be missed by methods based solely on the rigid crystal structure. These include cryptic pockets and flexible pockets often found at protein-protein interaction interfaces. Here, we apply an approach that uses protein modeling in concert with druggability estimation to account for light protein backbone movement and protein side-chain flexibility in protein binding sites. We assess the advantages and limitations of this approach on widely-used protein druggability sets. Applying the approach to all mammalian protein crystal structures in the PDB results in identification of 69 proteins with potential druggable cryptic pockets.

show abstract

“…ProDy [147] is a Python toolkit for analyzing proteins and includes facilities for trajectory analysis and druggability predictions using simulations of molecular probes [152]. …”

Section: Ligand Dynamics and Free Energy Calculationsmentioning

confidence: 99%

Open source molecular modeling

Pirhadi

Sunseri

2016

Journal of Molecular Graphics and Modelling

View full text Add to dashboard Cite

The success of molecular modeling and computational chemistry efforts are, by definition, dependent on quality software applications. Open source software development provides many advantages to users of modeling applications, not the least of which is that the software is free and completely extendable. In this review we categorize, enumerate, and describe available open source software packages for molecular modeling and computational chemistry.

show abstract

Druggability Assessment of Allosteric Proteins by Dynamics Simulations in the Presence of Probe Molecules

Cited by 142 publications

References 83 publications

CryptoSite: Expanding the Druggable Proteome by Characterization and Prediction of Cryptic Binding Sites

CryptoSite: Expanding the Druggable Proteome by Characterization and Prediction of Cryptic Binding Sites

Structure-Based Druggability Assessment of the Mammalian Structural Proteome with Inclusion of Light Protein Flexibility

Open source molecular modeling

Contact Info

Product

Resources

About