2018
DOI: 10.1016/j.biochi.2017.11.020
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Multi-targeted effects of G4-aptamers and their antiproliferative activity against cancer cells

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Cited by 23 publications
(31 citation statements)
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“…Multi-targeted effect of G-quadruplex-based aptamers described in [76] enable their interference with integral cellular processes, such as modulation of telomerase activity [56], proliferation of breast adenocarcinoma cells [76], suppression of inflammasome activity in macrophages [77]. In this study, we demonstrated that synthetic ODNs based on G-quadruplex-forming telomere repeats (d(TTAGGG) 4 ) and their modified analogues significantly activate the leukotriene synthesis and other key cellular responses of human neutrophils.…”
Section: Discussionmentioning
confidence: 85%
“…Multi-targeted effect of G-quadruplex-based aptamers described in [76] enable their interference with integral cellular processes, such as modulation of telomerase activity [56], proliferation of breast adenocarcinoma cells [76], suppression of inflammasome activity in macrophages [77]. In this study, we demonstrated that synthetic ODNs based on G-quadruplex-forming telomere repeats (d(TTAGGG) 4 ) and their modified analogues significantly activate the leukotriene synthesis and other key cellular responses of human neutrophils.…”
Section: Discussionmentioning
confidence: 85%
“…Aptamers targeting proteins or other biologically relevant molecules have been selected by screening libraries of DNA or RNA oligos and further studied for the potential therapeutic application. Since it was first discovered that Top1 binds and is inhibited by G4-forming oligos [37,38], other similar results have been reported [39,48,49]. First, using purified Calf Thymus Top1, Shuai et al characterized fourteen different guanine-rich oligos capable of forming either G-quadruplex or quadruplex-duplex hybrid and showed that all of the oligos act as competitive inhibitors of Top1 catalysis [39].…”
Section: G4 Oligos As Top1 Inhibiting Aptamersmentioning
confidence: 83%
“…They were even more effective in inhibiting Top1 when compared to the aptamer first identified as a Top1-specific inhibitor by Shuai et al [39]. The inhibition of Top1 by the G4 oligos was correlated with the inhibition of DNA replication, and this antiproliferative effect was specific to cancer cells [49]. Although the physical interaction between the G4-capable aptamers and Top1 was not determined in these studies, the specific nature of the inhibition strongly suggests that the competitive binding of the aptamers to Top1 underlies the inhibition of the catalytic activity.…”
Section: And D(cactgg-cc-(gggt) 4 -Ta-ccagtg)mentioning
confidence: 96%
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“…G4-aptamers have been extensively documented as therapeutic agents able to activate potent antiproliferative effects in a variety of cancer cell lines [7]. Among G4-aptamers, the anticancer AS1411 is the only one for which Phase II has been completed [41].…”
Section: Discussionmentioning
confidence: 99%