Hot-spot identification on a broad class of proteins and RNA suggest unifying principles of molecular recognition.

Hot-spot identification on a broad class of proteins and RNA suggest unifying principles of molecular recognition.

Chemically diverse fragments tend to collectively bind at localized sites on proteins, which is a cornerstone of fragment-based techniques. A central question is how general are these strategies for predicting a wide variety of molecular interactions such as small molecule-protein, protein-protein a...

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Main Authors: John L Kulp, Ian S Cloudsdale, Frank Guarnieri
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2017-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC5570288?pdf=render
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spelling doaj-bbbf70291bbd4f1390481321a4d7946f2020-11-24T21:34:06ZengPublic Library of Science (PLoS)PLoS ONE1932-62032017-01-01128e018332710.1371/journal.pone.0183327Hot-spot identification on a broad class of proteins and RNA suggest unifying principles of molecular recognition.John L KulpIan S CloudsdaleJohn L KulpFrank GuarnieriChemically diverse fragments tend to collectively bind at localized sites on proteins, which is a cornerstone of fragment-based techniques. A central question is how general are these strategies for predicting a wide variety of molecular interactions such as small molecule-protein, protein-protein and protein-nucleic acid for both experimental and computational methods. To address this issue, we recently proposed three governing principles, (1) accurate prediction of fragment-macromolecule binding free energy, (2) accurate prediction of water-macromolecule binding free energy, and (3) locating sites on a macromolecule that have high affinity for a diversity of fragments and low affinity for water. To test the generality of these concepts we used the computational technique of Simulated Annealing of Chemical Potential to design one small fragment to break the RecA-RecA protein-protein interaction and three fragments that inhibit peptide-deformylase via water-mediated multi-body interactions. Experiments confirm the predictions that 6-hydroxydopamine potently inhibits RecA and that PDF inhibition quantitatively tracks the water-mediated binding predictions. Additionally, the principles correctly predict the essential bound waters in HIV Protease, the surprisingly extensive binding site of elastase, the pinpoint location of electron transfer in dihydrofolate reductase, the HIV TAT-TAR protein-RNA interactions, and the MDM2-MDM4 differential binding to p53. The experimental confirmations of highly non-obvious predictions combined with the precise characterization of a broad range of known phenomena lend strong support to the generality of fragment-based methods for characterizing molecular recognition.http://europepmc.org/articles/PMC5570288?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author John L Kulp
Ian S Cloudsdale
John L Kulp
Frank Guarnieri
spellingShingle John L Kulp
Ian S Cloudsdale
John L Kulp
Frank Guarnieri
Hot-spot identification on a broad class of proteins and RNA suggest unifying principles of molecular recognition.
PLoS ONE
author_facet John L Kulp
Ian S Cloudsdale
John L Kulp
Frank Guarnieri
author_sort John L Kulp
title Hot-spot identification on a broad class of proteins and RNA suggest unifying principles of molecular recognition.
title_short Hot-spot identification on a broad class of proteins and RNA suggest unifying principles of molecular recognition.
title_full Hot-spot identification on a broad class of proteins and RNA suggest unifying principles of molecular recognition.
title_fullStr Hot-spot identification on a broad class of proteins and RNA suggest unifying principles of molecular recognition.
title_full_unstemmed Hot-spot identification on a broad class of proteins and RNA suggest unifying principles of molecular recognition.
title_sort hot-spot identification on a broad class of proteins and rna suggest unifying principles of molecular recognition.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2017-01-01
description Chemically diverse fragments tend to collectively bind at localized sites on proteins, which is a cornerstone of fragment-based techniques. A central question is how general are these strategies for predicting a wide variety of molecular interactions such as small molecule-protein, protein-protein and protein-nucleic acid for both experimental and computational methods. To address this issue, we recently proposed three governing principles, (1) accurate prediction of fragment-macromolecule binding free energy, (2) accurate prediction of water-macromolecule binding free energy, and (3) locating sites on a macromolecule that have high affinity for a diversity of fragments and low affinity for water. To test the generality of these concepts we used the computational technique of Simulated Annealing of Chemical Potential to design one small fragment to break the RecA-RecA protein-protein interaction and three fragments that inhibit peptide-deformylase via water-mediated multi-body interactions. Experiments confirm the predictions that 6-hydroxydopamine potently inhibits RecA and that PDF inhibition quantitatively tracks the water-mediated binding predictions. Additionally, the principles correctly predict the essential bound waters in HIV Protease, the surprisingly extensive binding site of elastase, the pinpoint location of electron transfer in dihydrofolate reductase, the HIV TAT-TAR protein-RNA interactions, and the MDM2-MDM4 differential binding to p53. The experimental confirmations of highly non-obvious predictions combined with the precise characterization of a broad range of known phenomena lend strong support to the generality of fragment-based methods for characterizing molecular recognition.
url http://europepmc.org/articles/PMC5570288?pdf=render
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