Hydroxyapatite [HA, Ca10(PO4)6(OH)2] is the main constituent of the mineral phase in mammalian bones and teeth enamel. For this reason, HA is widely applied as an orthopaedic and dental biomaterial, both per se and together with other classes of materials, in the form of coating for metal alloys, in composites with polymers and so on. Despite these various applications, fundamental knowledge of the interaction mechanisms of hydroxyapatite with biomolecules is still poorly understood. Many experimental techniques, such as solid state NMR, IR spectroscopy, microscopy and others, have investigated the interaction of HA different samples with macromolecules as biphosphonates, organic acids and amino acids to highlight the inorganic-organic interface reactions. Along the same line, recently, theoretical methods have been devoted to simulate the most relevant HA faces, both bare and in interaction with biomolecules, depending on the theoretical approach. While molecular mechanics and dynamics modelling aims at characterizing the dynamical properties of large quantities of molecules on the surfaces, quantum mechanics can provide more quantitative information at a molecular level. In the present work, B3LYP periodic simulations of the adsorption processes of different molecules on two of the most studied HA surfaces, namely the (001) and the (010), have been carried out by means of the quantum-mechanical CRYSTAL06 code. Gaussian basis set of double-zeta quality in combination with the accurate B3LYP functional have assured the best compromise between cost of the calculation and reliability of the obtained results. Glycine in interaction with HA (001) surface The choice of these peculiar HA faces is due to the fact that HA crystals are elongated in the [0001] direction in both bone matrix and tooth enamel, but some proteins bind preferentially to the (010) crystal faces, as it is found in the literature. These two surface models have been fully optimized as real 2D slabs and characterized with respect to their stability with thickness and to their electronic and vibrational properties, first bare and then in interaction with the following probe molecules, H2O and CO, with the simple organic acid HCOOH, and with some amino acids, i.e. glycine (see Figure), lysine and glutamic acid. In this communication, the reference methodology and the complete characterization of the hydration process as well as the preliminary acid dissolution steps of HA surfaces are addressed. Both energetic and vibrational properties of the models examined will be discussed and, compared to experimental data, deriving form microcalorimetric and IR spectroscopic measurements, when present. As for amino acids adsorption simulations, which are fundamental for the knowledge of HA in vivo behaviour, the stability of different forms of interaction, neutral vs zwitterionic, as well as H2O role in the interaction will be presented.

Periodic B3LYP Modelling of Hydroxyapatite (001) and (010) Surfaces in Interaction with Biomolecules: from H2O to amino acids

CORNO, MARTA;UGLIENGO, Piero
2008-01-01

Abstract

Hydroxyapatite [HA, Ca10(PO4)6(OH)2] is the main constituent of the mineral phase in mammalian bones and teeth enamel. For this reason, HA is widely applied as an orthopaedic and dental biomaterial, both per se and together with other classes of materials, in the form of coating for metal alloys, in composites with polymers and so on. Despite these various applications, fundamental knowledge of the interaction mechanisms of hydroxyapatite with biomolecules is still poorly understood. Many experimental techniques, such as solid state NMR, IR spectroscopy, microscopy and others, have investigated the interaction of HA different samples with macromolecules as biphosphonates, organic acids and amino acids to highlight the inorganic-organic interface reactions. Along the same line, recently, theoretical methods have been devoted to simulate the most relevant HA faces, both bare and in interaction with biomolecules, depending on the theoretical approach. While molecular mechanics and dynamics modelling aims at characterizing the dynamical properties of large quantities of molecules on the surfaces, quantum mechanics can provide more quantitative information at a molecular level. In the present work, B3LYP periodic simulations of the adsorption processes of different molecules on two of the most studied HA surfaces, namely the (001) and the (010), have been carried out by means of the quantum-mechanical CRYSTAL06 code. Gaussian basis set of double-zeta quality in combination with the accurate B3LYP functional have assured the best compromise between cost of the calculation and reliability of the obtained results. Glycine in interaction with HA (001) surface The choice of these peculiar HA faces is due to the fact that HA crystals are elongated in the [0001] direction in both bone matrix and tooth enamel, but some proteins bind preferentially to the (010) crystal faces, as it is found in the literature. These two surface models have been fully optimized as real 2D slabs and characterized with respect to their stability with thickness and to their electronic and vibrational properties, first bare and then in interaction with the following probe molecules, H2O and CO, with the simple organic acid HCOOH, and with some amino acids, i.e. glycine (see Figure), lysine and glutamic acid. In this communication, the reference methodology and the complete characterization of the hydration process as well as the preliminary acid dissolution steps of HA surfaces are addressed. Both energetic and vibrational properties of the models examined will be discussed and, compared to experimental data, deriving form microcalorimetric and IR spectroscopic measurements, when present. As for amino acids adsorption simulations, which are fundamental for the knowledge of HA in vivo behaviour, the stability of different forms of interaction, neutral vs zwitterionic, as well as H2O role in the interaction will be presented.
2008
2nd EuCheMS Chemistry Congress “Chemistry: the global science"
Torino
16-20 settembre 2008
CHEMISTRY: THE GLOBAL SCIENCE
Centro Congressi Internazionale s.r.l
52
52
M. Corno; A. Rimola; C. Busco; V. Bolis; P. Ugliengo
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2318/89806
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