The central benzodiazepine receptor tracer [N-methyl- 1 1 C]iomazenil (Ro 16-0154) was synthesized by alkylation of the desmethyl precursor noriomazenil with [ 1 1 C]methyl iodide. The [ 1 1 C]CH 3 I (prepared by reduction of [ 1 1 C]CO 2 with LiAlH 4 followed by reaction with HI) was reacted with noriomazenil inN,N -dimethylformamide and Bu 4 N + OH - for 1 min at 80°C and purified by HPLC (C 1 8 , 34% CH 3 CN/H 2 O, 7 mL/min). The product was obtained with synthesis time 35 ± 5 min (mean ± SD, n = 7), radiochemical yield (EOB) 36 ± 16%, radiochemical purity 99 ± 1%, and specific activity 5100 ± 2800 mCi/μmol. Absorbed radiation doses were calculated from previously acquired human biodistribution data. The urinary bladder wall received the highest dose (0.099 mGy/MBq) for 4.8 h voiding interval and the effective dose equivalent was 0.015 mSv/MBq. After i.v. injection of [ 1 1 C]iomazenil in an adult baboon or healthy human volunteer, radioactivity accumulated in the cortex with time-activity curves in agreement with results obtained with [ 1 1 C]flumazenil PET and [ 1 2 3 I]iomazenil SPECT studies. The count rate was sufficient to obtain quantitative images up to 2 h post-injection with a 14 mCi injection. These results suggest that [ 1 1 C]iomazenil will be a useful agent for measuring benzodiazepine receptorsin vivo by positron emission tomography.