Proton-coupled electron transfer modulates the metal release of blood serum iron transferrin

Abstract

Serum transferrin (sTf) is a key iron-transport protein in vertebrates, exhibiting an extraordinary affinity for Fe(III). Typically, only ∼30% of sTf is saturated with Fe(III), leaving a significant fraction of its binding sites available for other metal ions, including heavy metals and radionuclides. While iron release under endosomal pH is well-understood to proceed via protonation mechanisms, the release pathways at physiological pH remain less clear and are subject to multiple competing mechanisms. To address this, we employed extensive multi-scale modelling—combining molecular dynamics, metadynamics, and electronic structure calculations—to probe Fe(III) release under physiological conditions. Our investigations focused on three key pathways: direct protonation, one-electron reduction, and proton-coupled electron transfer (PCET). Calculated reduction potentials of approximately 1.3 V for both synthetic and protein models indicate that direct reduction is thermodynamically unfavourable, consistent with experimental observations.

Graphical abstract: Proton-coupled electron transfer modulates the metal release of blood serum iron transferrin

Supplementary files

Article information

Article type
Paper
Submitted
30 Jul 2025
Accepted
31 Aug 2025
First published
17 Sep 2025

Dalton Trans., 2025, Advance Article

Proton-coupled electron transfer modulates the metal release of blood serum iron transferrin

M. Sundararajan, L. Mishra, N. K. Bharti and S. P. Mantry, Dalton Trans., 2025, Advance Article , DOI: 10.1039/D5DT01803J

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