2018
DOI: 10.1016/j.bmc.2018.02.044
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Xanthone derivatives as phosphoglycerate mutase 1 inhibitors: Design, synthesis, and biological evaluation

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Cited by 24 publications
(26 citation statements)
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“…Since PGAM1 was suggested as a potential therapeutic target for multiple cancer types, several PGAM1 inhibitors have been developed for cancer therapy. 21,22,28,[50][51][52][53] A summary of these inhibitors and their related functions are listed in Table 1. PGAM1 inhibitors are divided into pharmacological inhibitors and genetic inhibitors.…”
Section: Summary Of Pgam1 Inhibitors and Research Directions To Explomentioning
confidence: 99%
See 1 more Smart Citation
“…Since PGAM1 was suggested as a potential therapeutic target for multiple cancer types, several PGAM1 inhibitors have been developed for cancer therapy. 21,22,28,[50][51][52][53] A summary of these inhibitors and their related functions are listed in Table 1. PGAM1 inhibitors are divided into pharmacological inhibitors and genetic inhibitors.…”
Section: Summary Of Pgam1 Inhibitors and Research Directions To Explomentioning
confidence: 99%
“…52 However, because of its multiple targets, its specificity to PGAM1 is poor. 28,54 Wang et al 53 used scaffold hopping and a sulfonamide reversal strategy based on the lead compound PGMI-004A to discover a series of xanthone derivatives (12a-12s) as novel PGAM1 inhibitors. These xanthone derivatives showed stronger efficacy and better specificity than PGMI-004A in the inhibition of PGAM1, as well as an increased anti-proliferative effect in the H1299 cell line.…”
Section: Summary Of Pgam1 Inhibitors and Research Directions To Explomentioning
confidence: 99%
“…Foregoing investigations revealed that PGMI-004A inhibits the PGAM1 activity via directly binding at its catalytic site. 48 Moreover, treatment of PGMI-004A significantly decreased the tumor growth in vivo. Authors declared that PGMI-004A by specifically targeting PGAM1 induced specific toxicity in cancer cells in vivo as well as in primary leukemia cells from cancer patients with no off target effects.…”
Section: Pharmacological Inhibitors Of Pgam1mentioning
confidence: 96%
“…Sulfonamide PGMI‐004A is a structural modification of ARS, by addition of hydrophobic groups through a sulfonamide bond, possibly reduces the cell proliferation in vitro. Foregoing investigations revealed that PGMI‐004A inhibits the PGAM1 activity via directly binding at its catalytic site . Moreover, treatment of PGMI‐004A significantly decreased the tumor growth in vivo.…”
Section: Pharmacological Inhibitors Of Pgam1mentioning
confidence: 99%
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