2012
DOI: 10.1002/ijch.201200016
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Photoimmunotherapy and Irradiance Modulation Reduce Chemotherapy Cycles and Toxicity in a Murine Model for Ovarian Carcinomatosis: Perspective and Results

Abstract: Significant toxicities from multiple cycles of chemotherapy often cause delays or early termination of treatment, leading to poor outcomes in ovarian cancer patients. Complementary modalities that potentiate the efficacy of traditional agents with fewer cycles and less toxicity are needed. Photodynamic therapy is a mechanistically-distinct modality that synergizes with chemo and biologic agents. A combination regimen with a clinically relevant chemotherapy cocktail (cisplatin + paclitaxel) and anti-EGFR target… Show more

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Cited by 32 publications
(46 citation statements)
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References 112 publications
(194 reference statements)
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“…Furthermore, taPIT enables a ∼17-fold increase in the maximum tolerated photodynamic dose compared with targeted, always-on immunoconjugates for PIT [0.5-1 mg·kg −1 photodynamic agent with 3-6 J·cm −1 per quadrant (21,23,40)]. Thus, taPIT enables unprecedented photodynamic doses for treating disseminated metastatic disease by overcoming nonspecific toxicities associated with-both targeted and nontargeted-alwayson agents.…”
Section: Resultsmentioning
confidence: 99%
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“…Furthermore, taPIT enables a ∼17-fold increase in the maximum tolerated photodynamic dose compared with targeted, always-on immunoconjugates for PIT [0.5-1 mg·kg −1 photodynamic agent with 3-6 J·cm −1 per quadrant (21,23,40)]. Thus, taPIT enables unprecedented photodynamic doses for treating disseminated metastatic disease by overcoming nonspecific toxicities associated with-both targeted and nontargeted-alwayson agents.…”
Section: Resultsmentioning
confidence: 99%
“…5A; a second cycle added no significant benefit). As a further comparative benchmark, prior work indicates 10% and 50% tumor burden reduction for one and two cycles, respectively, of combination cisplatin plus paclitaxel chemotherapy-at the same doses used here (Materials and Methods)-in this mouse model of metastatic ovarian cancer (23). The relatively poor response to chemotherapy alone may be due to intrinsic resistance-the OVCAR5 cells used in this model have sevenfold resistance to cisplatin relative to a platinum-sensitive cell line (31) and contain a subpopulation of stem-like cells that are stimulated by chemotherapy (8).…”
Section: Resultsmentioning
confidence: 99%
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