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A Fluorogenic ONOO - -Triggered Carbon Monoxide Donor for Mitigating Brain Ischemic Damage.

Linfeng XingBin WangJin LiXinjian GuoXicun LuXiaohua ChenHaitao SunZhenrong SunXiao LuoSuhua QiXuhong QianYoujun Yang
Published in: Journal of the American Chemical Society (2022)
Ischemia-reperfusion (I/R) injuries are from the secondary radicals of ONOO - . Direct radical scavenging is difficult because of their high reactivity. ONOO - is longer-lived than the radicals in the biological milieu. Scavenging ONOO - suppresses radical generation preventively. CO is neuroprotective during ischemia. With the scaffold of carbon-caged xanthene, we designed an OONO - -triggered CO donor ( PCOD585 ). Notably, PCOD585 exhibited a concomitant fluorescence turn-on upon ONOO - detection, facilitating microscopic monitoring. PCOD585 was cytoprotective in oxygen-glucose deprivation (OGD)-insulted PC-12 cells. It was permeable to the blood-brain barrier and further exhibited neuroprotective effects to MCAO rats by reducing infarction volume, cell apoptosis, and brain edema.
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