2010
DOI: 10.4161/cbt.10.10.13371
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Rose Bengal Acetate photodynamic therapy-induced autophagy

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Cited by 26 publications
(23 citation statements)
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“…In particular, mitochondrial- and ER-localized PSs trigger a pro-survival autophagic response to recycle injured organelles [132,133], while, PSs localized and damaging lysosomes block autophagosome formation, thus leading to autophagy inhibition. It has been further demonstrated that also PSs localizing in mitochondria or ER after relocation from their primary damage site, induce autophagic cell death [134,135] in addition to apoptosis [136,137]. The kinetic of apoptosis/autophagy switch strictly depends on cell type, PS type and concentration and light dose.…”
Section: Autophagy-assisted Cancer Therapy: Old and New Insightsmentioning
confidence: 99%
“…In particular, mitochondrial- and ER-localized PSs trigger a pro-survival autophagic response to recycle injured organelles [132,133], while, PSs localized and damaging lysosomes block autophagosome formation, thus leading to autophagy inhibition. It has been further demonstrated that also PSs localizing in mitochondria or ER after relocation from their primary damage site, induce autophagic cell death [134,135] in addition to apoptosis [136,137]. The kinetic of apoptosis/autophagy switch strictly depends on cell type, PS type and concentration and light dose.…”
Section: Autophagy-assisted Cancer Therapy: Old and New Insightsmentioning
confidence: 99%
“…Noteworthy, in Dini’s laboratory it is demonstrated that Rose Bengale Acetate, a PS localizing in ER only after redistribution from its perinuclear primary damage site induces autophagic cell death [107,108] in addition to apoptosis [109,110] in human epitheloid cervix carcinoma HeLa cells. …”
Section: Autophagy In Pdt-photosensitized Cellsmentioning
confidence: 99%
“…Here, we evaluate if oxidative stress elicited by Rose Bengal Acetate-PDT (RBAc-PDT) induces in HeLa cells the in vitro biochemical distinctive properties of ICD such as relocalization, i.e., exposure and/or release, of DAMPs in order to make a prediction about the capacity of RBAc to trigger ICD. In fact, in our previous papers we have demonstrated that RBAc-PDT ensures in HeLa cells the rapid, independent and long-lasting onset of apoptosis and autophagy by several signalling pathways originating from or converging on almost all intracellular organelles (mitochondria, lysosomes, Golgi apparatus and ER), despite RBAc primary perinuclear localization [29][33]. In addition, we showed that 1) apoptotic and autophagic RBAc photokilled HeLa cells efficiently recruit macrophages; 2) macrophages efficiently phagocyte dead HeLa cells; and 3) macrophages following internalization release IL-10, TGF-β and TNF-α [34].…”
Section: Introductionmentioning
confidence: 99%