RT Journal Article SR Electronic T1 Extracellular Cation Binding Pocket Is Essential For Ion Conduction Of OsHKT2;2 JF bioRxiv FD Cold Spring Harbor Laboratory SP 471003 DO 10.1101/471003 A1 Janin Riedelsberger A1 Ariela Vergara-Jaque A1 Miguel Piñeros A1 Ingo Dreyer A1 Wendy González YR 2018 UL http://biorxiv.org/content/early/2018/11/16/471003.abstract AB HKT channels mediate sodium uniport or sodium and potassium symport in plants. Monocotyledons express a higher number of HKT proteins than dicotyledons, and it is only within this clade of HKT channels that cation symport mechanisms are found. The prevailing ion composition in the extracellular medium affects the transport abilities of various HKT channels by changing their selectivity or ion transport rates. How this mutual effect is achieved at the molecular level is still unknown. Here, we built a homology model of the monocotyledonous OsHKT2;2, which shows sodium and potassium symport activity, and performed molecular dynamics simulations in the presence of sodium and potassium ions. By analyzing ion-protein interactions, we identified a cation binding pocket on the extracellular protein surface, which is formed by residues P71, D75, D501 and K504. Proline and the two aspartate residues coordinate cations, while K504 forms salt bridges with D75 and D501 and may be involved in the forwarding of cations towards the pore entrance. Functional validation via electrophysiological experiments confirmed the biological relevance of the predicted ion binding pocket and identified K504 as a central key residue. Mutation of the cation coordinating residues affected the functionality of HKT only slightly. Additional in silico mutants and simulations of K504 supported experimental results.