Abstract
Atorvastatin was radioiodinated and formulated using chloramine-Tviaan electrophilic substitution reaction for the development of a potential radiopharmaceutical for targeting liver. The impact of different reaction parameters and conditions that affected the labeling yield such as pH of the reaction, concentration of atorvastatin and reaction time were optimized in order to increase the radioiodination efficiency. The labeling yield was 94.3 +/- 1.41 %.In vitroanalysis demonstrated that the compound was steady for up to 24 h. The liver uptake was 40.35% and the clearance pathways proceedviathe hepatobiliary and renal clearance.