A hypoxia-activated near infrared fluorescent probe for cyclooxygenase-2 and in vivo imaging for tumor and inflammation

摘要

Tumor is one of the most serious diseases, and its early diagnosis is of great significance for improving the prognosis and patient survival rate. Herein, aiming at the detection of cyclooxygenase-2 (COX-2), which plays an important role in tumorigenesis, we synthesized a NIR fluorescent probeYZP1, by using near infrared fluorescent dye Cy5.5 as the fluorophore and indomethacin (IMC) as the targeting group. Due to the quenching effect of azo group, the fluorescence ofYZP1was quenched. Under hypoxia condition and the reduction of Cytochrome P450 reductase, the azo bond ofYZP1was broken, and the fluorescence quantum yield increased from 0.0028 to 0.125. Furthermore, when HeLa cells were co-incubated withYZP1under hypoxia condition, remarkable red fluorescence were observed, and the ratio of fluorescence intensity between hypoxic and normoxic cells could reach 9 folds. After treated with the celecoxib, an inhibitor of COX-2, of different concentrations, the fluorescence will be weakened gradually, which verify the binding ofYZP1and COX-2. Finally, by using mouse inflammation model and tumor xenograft model, the in vivo imaging ability ofYZP1was also demonstrated.