2018
DOI: 10.1021/jacs.8b06011
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Visible-Light-Activated Quinolone Carbon-Monoxide-Releasing Molecule: Prodrug and Albumin-Assisted Delivery Enables Anticancer and Potent Anti-Inflammatory Effects

Abstract: The delivery of controlled amounts of carbon monoxide (CO) to biological targets is of significant current interest. Very few CO-releasing compounds are currently known that can be rigorously controlled in terms of the location and amount of CO released. To address this deficiency, we report herein a new metal-free, visible-light-induced CO-releasing molecule (photoCORM) and its prodrug oxidized form, which offer new approaches to controlled, localized CO delivery. The new photoCORM, based on a 3-hydroxybenzo[… Show more

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Cited by 111 publications
(124 citation statements)
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References 66 publications
(156 reference statements)
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“…In a carrageenan‐induced rat paw edema model, CORM‐2‐loaded lipid nanoparticles with extended CO release half‐life and improved water solubility displayed higher anti‐inflammatory effects compared to both indomethacin and CORM‐2 solution (Figure a) . Recently, a metal‐free 3‐hydroxybenzo[g]quinolone photoCORM has been used in combination with BSA to exert anticancer and potent anti‐inflammatory activities (Figure d) . The anti‐inflammatory feature of this complex is noteworthy as the complex can attenuate LPS‐induced murine macrophage cells inflammation at unprecedented nanomolar concentrations.…”
Section: Carbon Monoxide Releasing Nanomaterialsmentioning
confidence: 99%
“…In a carrageenan‐induced rat paw edema model, CORM‐2‐loaded lipid nanoparticles with extended CO release half‐life and improved water solubility displayed higher anti‐inflammatory effects compared to both indomethacin and CORM‐2 solution (Figure a) . Recently, a metal‐free 3‐hydroxybenzo[g]quinolone photoCORM has been used in combination with BSA to exert anticancer and potent anti‐inflammatory activities (Figure d) . The anti‐inflammatory feature of this complex is noteworthy as the complex can attenuate LPS‐induced murine macrophage cells inflammation at unprecedented nanomolar concentrations.…”
Section: Carbon Monoxide Releasing Nanomaterialsmentioning
confidence: 99%
“…This difference may result from variances in protein binding and/or cellular uptake. It is worth noting that 20 is the first photoCORM to show nanomolar anti‐inflammatory effects . The CO release byproduct 21 is non‐toxic up to 100 μM.…”
Section: Fluorescence Trackable Metal‐free Co‐releasing Molecules or mentioning
confidence: 97%
“…Notably, 20 is best delivered to cells using bovine serum albumin (BSA) as a carrier protein. The binding constant for 20 to BSA is more than >900‐fold stronger than that of 19 , with both binding to the protein in a 1 : 1 stoichiometry ,. In the absence of visible light and in the presence of a physiologically relevant amount of BSA (0.6 mM) 20 exhibits no toxicity up to 100 μM in A549 cells whereas 19 is mildly toxic (IC 50 =82 μM).…”
Section: Fluorescence Trackable Metal‐free Co‐releasing Molecules or mentioning
confidence: 99%
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