Quantitative Assessment of Protein Interaction with Methyl-Lysine Analogues by Hybrid Computational and Experimental Approaches

  1. Seeliger, Daniel
  2. Soeroes, Szabolcs
  3. Klingberg, Rebecca
  4. Schwarzer, Dirk ORCID logo
  5. Grubmüller, Helmut
  6. Fischle, Wolfgang

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1000 Titel
  • Quantitative Assessment of Protein Interaction with Methyl-Lysine Analogues by Hybrid Computational and Experimental Approaches
1000 Autor/in
  1. Seeliger, Daniel |
  2. Soeroes, Szabolcs |
  3. Klingberg, Rebecca |
  4. Schwarzer, Dirk |
  5. Grubmüller, Helmut |
  6. Fischle, Wolfgang |
1000 Erscheinungsjahr 2011
1000 LeibnizOpen
1000 Publikationstyp
  1. Artikel |
1000 Online veröffentlicht
  • 2011-10-12
1000 Erschienen in
1000 Quellenangabe
  • 7(1): 150–154
1000 FRL-Sammlung
1000 Copyrightjahr
  • 2011
1000 Lizenz
1000 Verlagsversion
  • http://doi.org/10.1021/cb200363r |
  • https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3265130/ |
1000 Ergänzendes Material
  • http://pubs.acs.org/doi/suppl/10.1021/cb200363r |
1000 Publikationsstatus
1000 Begutachtungsstatus
1000 Sprache der Publikation
1000 Abstract/Summary
  • In cases where binding ligands of proteins are not easily available, structural analogues are often used. For example, in the analysis of proteins recognizing different methyl-lysine residues in histones, methyl-lysine analogues based on methyl-amino-alkylated cysteine residues have been introduced. Whether these are close enough to justify quantitative interpretation of binding experiments is however questionable. To systematically address this issue, we developed, applied, and assessed a hybrid computational/experimental approach that extracts the binding free energy difference between the native ligand (methyl-lysine) and the analogue (methyl-amino-alkylated cysteine) from a thermodynamic cycle. Our results indicate that measured and calculated binding differences are in very good agreement and therefore allow the correction of measured affinities of the analogues. We suggest that quantitative binding parameters for defined ligands in general can be derived by this method with remarkable accuracy.
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1000 Liste der Beteiligten
  1. https://frl.publisso.de/adhoc/creator/U2VlbGlnZXIsIERhbmllbA==|https://frl.publisso.de/adhoc/creator/U29lcm9lcywgU3phYm9sY3M=|https://frl.publisso.de/adhoc/creator/S2xpbmdiZXJnLCBSZWJlY2Nh|http://orcid.org/0000-0002-7477-3319|https://frl.publisso.de/adhoc/creator/R3J1Ym3DvGxsZXIsIEhlbG11dA==|https://frl.publisso.de/adhoc/creator/RmlzY2hsZSwgV29sZmdhbmc=
1000 Label
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  1. Max Planck Society |
  2. Deutsche Forschungsgemeinschaft |
  3. EU |
1000 Fördernummer
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  2. 2079/4-1
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1000 Förderprogramm
  1. -
  2. -
  3. FP6 NoE the Epigenome
1000 Dateien
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    1000 Förderer Max Planck Society |
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  2. 1000 joinedFunding-child
    1000 Förderer Deutsche Forschungsgemeinschaft |
    1000 Förderprogramm -
    1000 Fördernummer 2079/4-1
  3. 1000 joinedFunding-child
    1000 Förderer EU |
    1000 Förderprogramm FP6 NoE the Epigenome
    1000 Fördernummer -
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