Detecting Validated Intracellular ROS Generation with 18F-dihydroethidine-Based PET

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Abstract

Purpose: To determine the sensitivity of the 18F-radiolabelled dihydroethidine analogue ([18F]DHE) to ROS in a validated ex vivo model of tissue oxidative stress. Procedures: The sensitivity of [18F]DHE to various ROS-generating systems was first established in vitro. Then, isolated rat hearts were perfused under constant flow, with contractile function monitored by intraventricular balloon. Cardiac uptake of infused [18F]DHE (50–150 kBq.min−1) was monitored by γ-detection, while ROS generation was invoked by menadione infusion (0, 10, or 50 μm), validated by parallel measures of cardiac oxidative stress. Results: [18F]DHE was most sensitive to oxidation by superoxide and hydroxyl radicals. Normalised [18F]DHE uptake was significantly greater in menadione-treated hearts (1.44 ± 0.27) versus control (0.81 ± 0.07) (p < 0.05, n = 4/group), associated with concomitant cardiac contractile dysfunction, glutathione depletion, and PKG1α dimerisation. Conclusion: [18F]DHE reports on ROS in a validated model of oxidative stress where perfusion (and tracer delivery) is unlikely to impact its pharmacokinetics.

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Waters, E. C. T., Baark, F., Yu, Z., Mota, F., Eykyn, T. R., Yan, R., & Southworth, R. (2022). Detecting Validated Intracellular ROS Generation with 18F-dihydroethidine-Based PET. Molecular Imaging and Biology, 24(3), 377–383. https://doi.org/10.1007/s11307-021-01683-0

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