Although C-labelled sulfur-containing amino acids (SAAs) including L-methyl-[C]methionine and -[C]-methyl-L-cysteine, are attractive tracers for glioma positron emission tomography (PET) imaging, their applications are limited by the short half-life of the radionuclide C ( = 20.4 min). However, development of F-labelled SAAs (F, = 109.8 min) without significant structural changes or relying on prosthetic groups remains to be a great challenge due to the absence of adequate space for chemical modification. : We herein present F-trifluoromethylated D- and L-cysteines which were designed by replacing the methyl group with F-trifluoromethyl group using a structure-based bioisosterism strategy. These two enantiomers were synthesized stereoselectively from serine-derived cyclic sulfamidates a nucleophilic F-trifluoromethylthiolation reaction followed by a deprotection reaction. Furthermore, we conducted preliminary and studies to investigate the feasibility of using F-trifluoromethylated cysteines as PET tracers for glioma imaging. : The two-step radiosynthesis provided the desired products in excellent enantiopurity ( > 99%) with 14% ± 3% of radiochemical yield. cell study demonstrated that both enantiomers were taken up efficiently by C6 tumor cells and were mainly transported by systems L and ASC. Among them, the D-enantiomer exhibited relatively good stability and high tumor-specific accumulation in the animal studies. : Our findings indicate that F-trifluoromethylated D-cysteine, a new SAA tracer, may be a potential candidate for glioma imaging. Taken together, our study represents a first step toward developing F-trifluoromethylated cysteines as structure-mimetic tracers for PET tumor imaging.