Magnetization Blocking in Fe2 III Dy2 III Molecular Magnets: Ab Initio Calculations and EPR Spectroscopy.

Abstract

The magnetism and magnetization blocking of a series of [Fe2 Dy2 (OH)2 (teaH)2 (RC6 H4 COO)6 ] complexes was investigated, in which teaH3 =triethanolamine and R=meta-CN (1), para-CN (2), meta-CH3 (3), para-NO2 (4) and para-CH3 (5), by combining ab initio calculations and EPR measurements. The results of broken-symmetry DFT calculations show that in all compounds the Fe-Fe exchange interaction is antiferromagnetic and stronger by far than the Fe-Dy and Dy-Dy interactions. As a result, the lowest two exchange doublets probed by EPR spectroscopy mostly originate from the Ising interaction of the dysprosium ions in all compounds. A correct quantitative description of the splitting of these two doublets requires, however, an explicit account of the Fe-Dy and Fe-Fe interactions. Due to the inversion symmetry of the complexes, the doublets under consideration are described by a collinear Ising exchange interaction. This picture is also supported by the EPR spectra, which could be simulated with parameters close to those extracted from the calculations. The magneto-structural analysis shows an increase of the antiferromagnetic Fe-Fe exchange interaction with increasing Fe-O-Fe angle and Fe-Fe distance. For the Dy-Fe interaction, the opposite tendency is observed, that is, a decrease of antiferromagnetic exchange coupling with increasing Dy-O-Fe angle and Dy-Fe distance. The transversal g factors extracted from the ab initio calculations have values in the range of 0.01-0.2, testifying to the lack of high axiality of the ground state of the dysprosium ions. This explains the lack/poor single-molecule magnetic behavior of this series of compounds at the investigated temperatures of a few Kelvin. Due to a very small gap (fractions of a wavenumber) between the ground and first-excited exchange doublet, relaxation takes place by magnetic moment reversal at individual dysprosium sites in the considered temperature domain.