Lipophilic Guanidine with Enhanced Stability for Use in Cesium Separation from Legacy High-Level Nuclear Waste

Abstract

Guanidine functional groups are found in a variety of biologically active molecules and specialized molecules used in industrial applications but often suffer from instability because of their tendency to hydrolyze. Here, guanidines with differently structured alkyl groups were synthesized and their stabilities tested to determine if there is a relationship between the locus of branching in the alkyl groups attached to a guanidine and its hydrolytic stability under the hypothesis that increased steric hindrance to hydrolytic attack will increase stability. The guanidines examined in this work are pertinent to the next-generation caustic-side solvent extraction (NG-CSSX) process, which was developed for the removal of radioactive cesium from highly radioactive and complex alkaline solutions. In the NG-CSSX process, a lipophilic alkylguanidine solvent component is highly important to maintain the effectiveness of the Cs+ stripping of the loaded organic solvent putatively by sequestering extractable anions. Currently used for this purpose, N,N′,N″-tri(3,7-dimethyloctyl)guanidine (TiDG) succumbs to slow hydrolysis under process conditions. Guided by quantum chemical calculations, two new guanidines with large, sterically bulky alkyl substituents have been designed, synthesized, and tested. More sterically hindering alkyl groups were found to increase the stability of guanidines, particularly for the guanidine with branching closest to the guanidine N atom: N,N′-dicyclohexyl-N″-(10-nonadecyl)guanidine (DCNDG). DCNDG was found to have a stability toward hydrolysis 8 to 44 times greater than that of TiDG under different simulated NG-CSSX process conditions, making it one of the most hydrolysis-resistant guanidine molecules reported to date.