The biodistribution and tissue toxicity of intravenously administered 225-actinium ( 225 Ac) complexed with acetate, ethylene diamine tetraacetic acid (EDTA), 1, 4, 7, 10, 13-pentaazacyclopentadecane-N, N′, N″, N‴, N⁗-pentaacetic acid (PEPA), or the “a” isomer of cyclohexyl diethylenetriamine pentaacetic acid (CHX-DTPA), were examined. The percent of injected dose per organ and per gram of tissue for each chelate complex was determined. 225 Ac-CHX-DTPA was evaluated further for radiotoxic effects. Mice receiving ≥185 kBq 225 Ac-CHX-DTPA suffered 100% morbidity by 5 days and 100% mortality by 8 days postinjection, and all animals evaluated had significant organ damage. The in vivo instability of the 225 Ac-CHX-DTPA complex likely allowed accumulation of free 225 Ac in organs, which resulted in tissue pathology.