2016
DOI: 10.1016/j.mrgentox.2016.09.003
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Linking genotoxicity and cytotoxicity with membrane fluidity: A comparative study in ovarian cancer cell lines following exposure to auranofin

Abstract: Auranofin, an organogold compound classified as an anti-rheumatic agent is under phase 2 clinical trials for re-purposing to treat recurrent epithelial ovarian cancer. We have reported earlier that Breast cancer 1, early onset (BRCA1) mutant ovarian cancer cells exhibit increased sensitivity to auranofin. BRCA1 is a DNA repair protein whose functional status is critical in the prognosis of ovarian cancer. Apart from DNA repair capability of cancer cells, membrane fluidity is also implicated in modulating resis… Show more

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Cited by 10 publications
(8 citation statements)
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“…In this light, it is prone not only to the activation of the Nrf2/ARE pathway (Jarolim et al 2017), but also to direct reaction with diverse cell structures (Fleck et al 2012; Jarolim et al 2016). To verify if the effect of the toxin on membrane fluidity was related to oxidation/reaction processes involving the epoxide moiety of the molecule, experiments were performed in the presence of the antioxidant NAC (Oommen et al 2016; Raza et al 2016). NAC significantly reverted the effect of the toxin restoring the membrane fluidity to control levels, as well as restoring cell morphological alteration induced by ATXII (Fig.…”
Section: Discussionmentioning
confidence: 99%
“…In this light, it is prone not only to the activation of the Nrf2/ARE pathway (Jarolim et al 2017), but also to direct reaction with diverse cell structures (Fleck et al 2012; Jarolim et al 2016). To verify if the effect of the toxin on membrane fluidity was related to oxidation/reaction processes involving the epoxide moiety of the molecule, experiments were performed in the presence of the antioxidant NAC (Oommen et al 2016; Raza et al 2016). NAC significantly reverted the effect of the toxin restoring the membrane fluidity to control levels, as well as restoring cell morphological alteration induced by ATXII (Fig.…”
Section: Discussionmentioning
confidence: 99%
“…The toxicity of ROS in these cells was demonstrated by the fact that NAC also prevented auranofin-induced lethality [ 62 ]. Of interest, the DNA damage caused by auranofin-induced ROS seems to be favored by increased membrane fluidity as shown in ovarian cancer cells with higher membrane fluidity (IGROV-1) being more sensitive to auranofin than ovarian cancer cells with lower membrane fluidity (OVCAR-5) [ 63 ]. Altogether, these evidences emphasize that ROS regulation plays a primary role in cancer cell survival and proliferation, and further supports the possible repurposing of auranofin against various cancers due to the pro-oxidative mechanism it triggers.…”
Section: Preclinical Evidence Of Auranofin Monotherapy Eliciting Anti-cancer Effectsmentioning
confidence: 99%
“…Soraphen A has been shown to increase chemosensitivity by modulating membrane fluidity and enhancing drug uptake 46 . Targeting membrane fluidity also enhanced the sensitivity of ovarian cancer cell lines to auranofin, inducing DNA damage and cellular oxidation 101 . Auranofin has successfully entered Phase 2 clinical trials for the treatment of recurrent epithelial ovarian cancer.…”
Section: Exploiting Cancer‐associated Lipid Pool Alterations and Memb...mentioning
confidence: 99%