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Title: Chlor(am)ination of iopamidol: Kinetics, pathways and disinfection by-products formation.
Author: Tian FX, Xu B, Lin YL, Hu CY, Zhang TY, Xia SJ, Chu WH, Gao NY.
Journal: Chemosphere; 2017 Oct; 184():489-497. PubMed ID: 28618281.
Abstract:
The degradation kinetics, pathways and disinfection by-products (DBPs) formation of iopamidol by chlorine and chloramines were investigated in this paper. The chlorination kinetics can be well described by a second-order model. The apparent second-order rate constants of iopamidol chlorination significantly increased with solution pH. The rate constants of iopamidol with HOCl and OCl^- were calculated as (1.66 ± 0.09) × 10^-3 M^-1 s^-1 and (0.45± 0.02) M^-1 s^-1, respectively. However, the chloramination of iopamidol fitted well with third-order kinetics and the maximum of the apparent rate constant occurred at pH 7. It was inferred that the free chlorine (i.e., HOCl and OCl^-) can react with iopamidol while the combined chlorine species (i.e., NH₂Cl and NHCl₂) were not reactive with iopamidol. The main intermediates during chlorination or chloramination of iopamidol were identified using ultra performance liquid chromatography - electrospray ionization-mass spectrometry (UPLC-ESI-MS), and the destruction pathways including stepwise deiodination, hydroxylation as well as chlorination were then proposed. The regular and iodinated DBPs formed during chlorination and chloramination of iopamidol were measured. It was found that iodine conversion from iopamidol to toxic iodinated DBPs distinctly increased during chloramination. The results also indicated that although chloramines were much less reactive than chlorine toward iopamidol, they led to the formation of much more toxic iodinated DBPs, especially CHI₃.

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