X-ray and Nuclear Spectroscopies to Reveal the Element-Specific Oxidation States and Electronic Spin States for Nanoparticulated Manganese Cyanidoferrates and Analogs

Author:

Wang Hongxin1ORCID,Huang Songping D.2,Young Anthony T.3,Cramer Stephen P.1ORCID,Yoda Yoshitaka4,Li Lei5

Affiliation:

1. SETI Institute, Mountain View, CA 94043, USA

2. Department of Chemistry and Biochemistry, Kent State University, Kent, OH 44242, USA

3. Lawrence Berkeley National Laboratory, Berkeley, CA 94720, USA

4. Precision Spectroscopy Division, SPring-8 Facility, Japan Synchrotron Radiation Research Institute (JASRI), Sayo 679-5198, Japan

5. Synchrotron Radiation Research Center, Hyogo Science and Technology Association, Kouto 679-5165, Japan

Abstract

In this publication, the potential non-gadolinium magnetic resonant imaging agent—nanoparticulate K2Mn[Fe(CN)6]—its comparison sample KFe[Co(CN)6], as well as their reference samples were measured and analyzed using Mn, Co and Fe L-edge X-ray absorption spectroscopy (L XAS). From the information obtained, we conclude that K2Mn[Fe (CN)6] has a high spin (hs)-Mn(II) and a low spin (ls)-Fe(II), while KFe[Co(CN)6] has an hs-Fe(II) and an ls-Co(III). In these Prussian blue (PB) analog structures, the L XAS analysis also led to the conclusion that the hs-Mn(II) in K2Mn[Fe(CN)6] or the hs-Fe(II) in KFe[Co(CN)6] bonds to the N in the [M(CN)6]4−/3− ions (where M = Fe(II) or Co(III)), while the ls-Fe(II) in K2Mn[Fe(CN)6] or the ls-Co(III) in KFe[Co(CN)6] bonds to the C in the [M(CN)6]4−/3− ion, suggesting the complexed metalloligand [Mn(II) or Fe(II)] occupies the N-bound site in PB. Then, nuclear resonant vibrational spectroscopy (NRVS) was used to confirm the results from the L XAS measurements: the Mn(II), Eu(III), Gd(III), Fe(II) cations complexed by [M(CN)6]n−-metalloligand all take the N-bound site in PB-like structures. Our NRVS studies also prove that iron in the K2Mn[Fe(CN)6] compound has a 2+ oxidation state and is surrounded by the C donor atoms in the [M(CN)6]n− ions.

Funder

NIH

Publisher

MDPI AG

Subject

General Medicine

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