Binding patterns of vanadium to transferrin in healthy human serum studied with HPLC/high resolution ICP-MS

Literature Information

Publication Date 2003-11-27
DOI 10.1039/B311013N
Impact Factor 4.616
Authors

Megumi Hamano Nagaoka, Hiroshi Akiyama, Tamio Maitani


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Abstract

Vanadium (V) is an essential metal for mammals. It has different valence states. In blood, V is bound to transferrin (Tf), a glycoprotein that has two metal-binding sites (C-lobe site and N-lobe site). In the present study, the binding patterns of V to serum Tf were analyzed by combined on-line HPLC and high-resolution ICP-MS (HPLC/HR-ICP-MS). The levels of 51V, 56Fe and 32S, which are interfered with polyatomic ions such as 35Cl16O+, 38Ar13C+ and 37Cl14N+, 40Ar16O+ and 40Ca16O+, and 16O2+, respectively, when using quadrupole ICP-MS, could be monitored simultaneously by HR-ICP-MS at a resolution of m/Δm = 4000. Sample (a 1 ml portion of serum from a healthy person or 2 mg of human serum Tf (hTf)) was directly subjected to HPLC equipped with an anion-exchange column. V in human serum without any in vitro V spike was detected as VC–Tf (V bound to C-lobe site of Tf) and metal2–Tf. Since V(III) was most favorable in terms of the binding to hTf in the presence of bicarbonate and V bound to the C-lobe site of hTf was detected only in the case of V(III) among the three valence states of V, it was suggested that a part, at least, of V in the VC–Tf in healthy human serum may be present as V(III), in addition to the generally accepted V(IV).

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