The program REFMAC5 from CCP4 was modified to allow the simultaneous use of X-ray crystallographic data and paramagnetic NMR data (pseudocontact shifts and self-orientation residual dipolar couplings) and/or diamagnetic residual dipolar couplings. Incorporation of these long-range NMR restraints in REFMAC5 can reveal differences between solid-state and solution conformations of molecules or, in their absence, can be used together with X-ray crystallographic data for structural refinement. Since NMR and X-ray data are complementary, when a single structure is consistent with both sets of data and still maintains reasonably 'ideal' geometries, the reliability of the derived atomic model is expected to increase. The program was tested on five different proteins: the catalytic domain of matrix metalloproteinase 1, GB3, ubiquitin, free calmodulin and calmodulin complexed with a peptide. In some cases the joint refinement produced a single model consistent with both sets of observations, while in other cases it indicated, outside the experimental uncertainty, the presence of different protein conformations in solution and in the solid state.

Simultaneous use of solution NMR and X-ray data in REFMAC5 for joint refinement/detection of structural differences / Mauro Rinaldelli;Enrico Ravera;Vito Calderone;Giacomo Parigi;Garib N. Murshudov;Claudio Luchinat. - In: ACTA CRYSTALLOGRAPHICA. SECTION D. - ISSN 1399-0047. - STAMPA. - 70:(2014), pp. 958-967. [10.1107/S1399004713034160]

Simultaneous use of solution NMR and X-ray data in REFMAC5 for joint refinement/detection of structural differences

RINALDELLI, MAURO;RAVERA, ENRICO;CALDERONE, VITO;PARIGI, GIACOMO;LUCHINAT, CLAUDIO
2014

Abstract

The program REFMAC5 from CCP4 was modified to allow the simultaneous use of X-ray crystallographic data and paramagnetic NMR data (pseudocontact shifts and self-orientation residual dipolar couplings) and/or diamagnetic residual dipolar couplings. Incorporation of these long-range NMR restraints in REFMAC5 can reveal differences between solid-state and solution conformations of molecules or, in their absence, can be used together with X-ray crystallographic data for structural refinement. Since NMR and X-ray data are complementary, when a single structure is consistent with both sets of data and still maintains reasonably 'ideal' geometries, the reliability of the derived atomic model is expected to increase. The program was tested on five different proteins: the catalytic domain of matrix metalloproteinase 1, GB3, ubiquitin, free calmodulin and calmodulin complexed with a peptide. In some cases the joint refinement produced a single model consistent with both sets of observations, while in other cases it indicated, outside the experimental uncertainty, the presence of different protein conformations in solution and in the solid state.
2014
70
958
967
Mauro Rinaldelli;Enrico Ravera;Vito Calderone;Giacomo Parigi;Garib N. Murshudov;Claudio Luchinat
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Utilizza questo identificatore per citare o creare un link a questa risorsa: https://hdl.handle.net/2158/891727
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