The trend in affinity of two 1,2-hydroxypyridinonate
lanthanide(III)
receptorsLnIII-2,2-Li-HOPO and LnIII-3,3-Gly-HOPO (LnIII = LaIII, PrIII, NdIII, SmIII, EuIII, GdIII, TbIII, DyIII, HoIII, ErIII, TmIII, YbIII, and LuIII)for
phosphate across the series was investigated by luminescence spectroscopy
via competition against the central europium(III) analog. Regardless
of the ligand, the rare earth receptors display a steep and continuous
increase in affinity for their phosphate guest across the series,
with the later lanthanides displaying the highest affinity for the
oxyanion. This trend mirrors that of the stability of the lanthanide
receptors, which also increases significantly and continuously from
LaIII to LuIII. For these two ligands, the ionic
radius of a rare earth, a parameter directly linked to its Lewis acidity,
correlates strongly with its affinity for anions, regardless of whether
that anion is the one coordinating it (in this case the 1,2-hydroxypyridinonate
ligand) or the guest targeted by the lanthanide receptor (in this
case phosphate). These observations are indicative of a lack of steric
hindrance for coordination of phosphate. Advantageously, increased
efficacy of the lanthanide receptor comes with increased stability.
The remarkably high stability of LuIII-2,2-Li-HOPO, combined
with its high affinity for phosphate, makes it a particularly promising
candidate for translational application to medical or environmental
sequestration of phosphate since the higher stability will further
reduce the risk of the rare earth leaching during anion separation.
The unusually large difference in stability between lanthanide complexes
(the LuIII complex of 2,2-Li-HOPO is at least 7 orders
of magnitude more stable than the LaIII one) bodes well
for potential applications in rare earth separation.
