The combination of molecular dynamics with crystallography for elucidating protein-ligand interactions: A case study involving peanut lectin complexes with T-antigen and lactose

J. V. Pratap; G. M. Bradbrook; G. B. Reddy; A. Surolia; J. Raftery; J. R. Helliwell; M. Vijayan

doi:10.1107/S0907444901011957

The combination of molecular dynamics with crystallography for elucidating protein-ligand interactions: A case study involving peanut lectin complexes with T-antigen and lactose

J. V. Pratap, G. M. Bradbrook, G. B. Reddy, A. Surolia, J. Raftery, J. R. Helliwell, M. Vijayan

Research output: Contribution to journal › Article › peer-review

Abstract

Peanut lectin binds T-antigen [Galβ(1-3)GalNAc] with an order of magnitude higher affinity than it binds the disaccharide lactose. The crystal structures of the two complexes indicate that the higher affinity for T-antigen is generated by two water bridges involving the acetamido group. Fresh calorimetric measurements on the two complexes have been carried out in the temperature range 280-313 K. Four sets of nanosecond molecular-dynamics (MD) simulations, two at 293 K and the other two at 313 K, were performed on each of the two complexes. At each temperature, two somewhat different protocols were used to hydrate the complex in the two runs. Two MD runs under slightly different conditions for each complex served to assess the reliability of the approach for exploring protein-ligand interactions. Enthalpies based on static calculations and on MD simulations favour complexation involving T-antigen. The simulations also brought to light ensembles of direct and water-mediated protein-sugar interactions in both the cases. These ensembles provide a qualitative explanation for the temperature dependence of the thermodynamic parameters of peanut lectin-T-antigen interaction and for the results of one of the two mutational studies on the lectin. They also support the earlier conclusion that the increased affinity of peanut lectin for T-antigen compared with that for lactose is primarily caused by additional water bridges involving the acetamido group. The calculations provide a rationale for the observed sugar-binding affinity of one of the two available mutants. Detailed examination of the calculations point to the need for exercising caution in interpreting results of MD simulations: while long simulations are not possible owing to computational reasons, it is desirable to carry out several short simulations with somewhat different initial conditions.

Original language	English
Pages (from-to)	1584-1594
Number of pages	10
Journal	Acta Crystallographica Section D: Biological Crystallography
Volume	57
Issue number	11
DOIs	https://doi.org/10.1107/S0907444901011957
Publication status	Published - 2001

Keywords

Association enthalpy; Association entropy; Formation constant; Free energy of binding (combination of mol. dynamics with crystallog. for elucidating protein-ligand interactions); Molecular association (direct and water-mediated protein-sugar interactions in peanut lectin-disaccharide complexes); Simulation and Modeling (mol. dynamics; combination of mol. dynamics with crystallog. for elucidating protein-ligand interactions); Agglutinins and Lectins Role: BSU (Biological study, unclassified), PRP (Properties), BIOL (Biological study) (peanut lectin, complexes with T-antigen and lactose; comparative anal. of peanut lectin complexes with T-antigen and lactose); Conformation (protein; comparative anal. of peanut lectin complexes with T-antigen and lactose); Hydration (role of water bridges in interaction of T-antigen with peanut lectin)

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10.1107/S0907444901011957

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Pratap, J. V., Bradbrook, G. M., Reddy, G. B., Surolia, A., Raftery, J., Helliwell, J. R., & Vijayan, M. (2001). The combination of molecular dynamics with crystallography for elucidating protein-ligand interactions: A case study involving peanut lectin complexes with T-antigen and lactose. Acta Crystallographica Section D: Biological Crystallography, 57(11), 1584-1594. https://doi.org/10.1107/S0907444901011957

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title = "The combination of molecular dynamics with crystallography for elucidating protein-ligand interactions: A case study involving peanut lectin complexes with T-antigen and lactose",

abstract = "Peanut lectin binds T-antigen [Galβ(1-3)GalNAc] with an order of magnitude higher affinity than it binds the disaccharide lactose. The crystal structures of the two complexes indicate that the higher affinity for T-antigen is generated by two water bridges involving the acetamido group. Fresh calorimetric measurements on the two complexes have been carried out in the temperature range 280-313 K. Four sets of nanosecond molecular-dynamics (MD) simulations, two at 293 K and the other two at 313 K, were performed on each of the two complexes. At each temperature, two somewhat different protocols were used to hydrate the complex in the two runs. Two MD runs under slightly different conditions for each complex served to assess the reliability of the approach for exploring protein-ligand interactions. Enthalpies based on static calculations and on MD simulations favour complexation involving T-antigen. The simulations also brought to light ensembles of direct and water-mediated protein-sugar interactions in both the cases. These ensembles provide a qualitative explanation for the temperature dependence of the thermodynamic parameters of peanut lectin-T-antigen interaction and for the results of one of the two mutational studies on the lectin. They also support the earlier conclusion that the increased affinity of peanut lectin for T-antigen compared with that for lactose is primarily caused by additional water bridges involving the acetamido group. The calculations provide a rationale for the observed sugar-binding affinity of one of the two available mutants. Detailed examination of the calculations point to the need for exercising caution in interpreting results of MD simulations: while long simulations are not possible owing to computational reasons, it is desirable to carry out several short simulations with somewhat different initial conditions.",

keywords = "Association enthalpy; Association entropy; Formation constant; Free energy of binding (combination of mol. dynamics with crystallog. for elucidating protein-ligand interactions); Molecular association (direct and water-mediated protein-sugar interactions in peanut lectin-disaccharide complexes); Simulation and Modeling (mol. dynamics; combination of mol. dynamics with crystallog. for elucidating protein-ligand interactions); Agglutinins and Lectins Role: BSU (Biological study, unclassified), PRP (Properties), BIOL (Biological study) (peanut lectin, complexes with T-antigen and lactose; comparative anal. of peanut lectin complexes with T-antigen and lactose); Conformation (protein; comparative anal. of peanut lectin complexes with T-antigen and lactose); Hydration (role of water bridges in interaction of T-antigen with peanut lectin)",

author = "Pratap, {J. V.} and Bradbrook, {G. M.} and Reddy, {G. B.} and A. Surolia and J. Raftery and Helliwell, {J. R.} and M. Vijayan",

year = "2001",

doi = "10.1107/S0907444901011957",

language = "English",

volume = "57",

pages = "1584--1594",

journal = "Acta Crystallographica Section D: Biological Crystallography",

issn = "0907-4449",

publisher = "International Union of Crystallography",

number = "11",

}

Pratap, JV, Bradbrook, GM, Reddy, GB, Surolia, A, Raftery, J, Helliwell, JR & Vijayan, M 2001, 'The combination of molecular dynamics with crystallography for elucidating protein-ligand interactions: A case study involving peanut lectin complexes with T-antigen and lactose', Acta Crystallographica Section D: Biological Crystallography, vol. 57, no. 11, pp. 1584-1594. https://doi.org/10.1107/S0907444901011957

The combination of molecular dynamics with crystallography for elucidating protein-ligand interactions: A case study involving peanut lectin complexes with T-antigen and lactose. / Pratap, J. V.; Bradbrook, G. M.; Reddy, G. B. et al.
In: Acta Crystallographica Section D: Biological Crystallography, Vol. 57, No. 11, 2001, p. 1584-1594.

Research output: Contribution to journal › Article › peer-review

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T1 - The combination of molecular dynamics with crystallography for elucidating protein-ligand interactions: A case study involving peanut lectin complexes with T-antigen and lactose

AU - Pratap, J. V.

AU - Bradbrook, G. M.

AU - Reddy, G. B.

AU - Surolia, A.

AU - Raftery, J.

AU - Helliwell, J. R.

AU - Vijayan, M.

PY - 2001

Y1 - 2001

N2 - Peanut lectin binds T-antigen [Galβ(1-3)GalNAc] with an order of magnitude higher affinity than it binds the disaccharide lactose. The crystal structures of the two complexes indicate that the higher affinity for T-antigen is generated by two water bridges involving the acetamido group. Fresh calorimetric measurements on the two complexes have been carried out in the temperature range 280-313 K. Four sets of nanosecond molecular-dynamics (MD) simulations, two at 293 K and the other two at 313 K, were performed on each of the two complexes. At each temperature, two somewhat different protocols were used to hydrate the complex in the two runs. Two MD runs under slightly different conditions for each complex served to assess the reliability of the approach for exploring protein-ligand interactions. Enthalpies based on static calculations and on MD simulations favour complexation involving T-antigen. The simulations also brought to light ensembles of direct and water-mediated protein-sugar interactions in both the cases. These ensembles provide a qualitative explanation for the temperature dependence of the thermodynamic parameters of peanut lectin-T-antigen interaction and for the results of one of the two mutational studies on the lectin. They also support the earlier conclusion that the increased affinity of peanut lectin for T-antigen compared with that for lactose is primarily caused by additional water bridges involving the acetamido group. The calculations provide a rationale for the observed sugar-binding affinity of one of the two available mutants. Detailed examination of the calculations point to the need for exercising caution in interpreting results of MD simulations: while long simulations are not possible owing to computational reasons, it is desirable to carry out several short simulations with somewhat different initial conditions.

AB - Peanut lectin binds T-antigen [Galβ(1-3)GalNAc] with an order of magnitude higher affinity than it binds the disaccharide lactose. The crystal structures of the two complexes indicate that the higher affinity for T-antigen is generated by two water bridges involving the acetamido group. Fresh calorimetric measurements on the two complexes have been carried out in the temperature range 280-313 K. Four sets of nanosecond molecular-dynamics (MD) simulations, two at 293 K and the other two at 313 K, were performed on each of the two complexes. At each temperature, two somewhat different protocols were used to hydrate the complex in the two runs. Two MD runs under slightly different conditions for each complex served to assess the reliability of the approach for exploring protein-ligand interactions. Enthalpies based on static calculations and on MD simulations favour complexation involving T-antigen. The simulations also brought to light ensembles of direct and water-mediated protein-sugar interactions in both the cases. These ensembles provide a qualitative explanation for the temperature dependence of the thermodynamic parameters of peanut lectin-T-antigen interaction and for the results of one of the two mutational studies on the lectin. They also support the earlier conclusion that the increased affinity of peanut lectin for T-antigen compared with that for lactose is primarily caused by additional water bridges involving the acetamido group. The calculations provide a rationale for the observed sugar-binding affinity of one of the two available mutants. Detailed examination of the calculations point to the need for exercising caution in interpreting results of MD simulations: while long simulations are not possible owing to computational reasons, it is desirable to carry out several short simulations with somewhat different initial conditions.

KW - Association enthalpy; Association entropy; Formation constant; Free energy of binding (combination of mol. dynamics with crystallog. for elucidating protein-ligand interactions); Molecular association (direct and water-mediated protein-sugar interactions

U2 - 10.1107/S0907444901011957

DO - 10.1107/S0907444901011957

M3 - Article

SN - 0907-4449

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JO - Acta Crystallographica Section D: Biological Crystallography

JF - Acta Crystallographica Section D: Biological Crystallography

IS - 11

ER -

Pratap JV, Bradbrook GM, Reddy GB, Surolia A, Raftery J, Helliwell JR et al. The combination of molecular dynamics with crystallography for elucidating protein-ligand interactions: A case study involving peanut lectin complexes with T-antigen and lactose. Acta Crystallographica Section D: Biological Crystallography. 2001;57(11):1584-1594. doi: 10.1107/S0907444901011957

The combination of molecular dynamics with crystallography for elucidating protein-ligand interactions: A case study involving peanut lectin complexes with T-antigen and lactose

Abstract

Keywords

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