Electron transfer-based combination therapy of cisplatin with tetramethyl-
            <i>p</i>
            -phenylenediamine for ovarian, cervical, and lung cancers

Luo, Ting; Yu, Jianqing; Nguyen, Jenny; Wang, Chun Rong; Bristow, Robert G.; Jaffray, David A.; Zhou, Xiao Zhen; Lu, Kun Ping; Lü, Qing

doi:10.1073/pnas.1203451109

Cited by 30 publications

(53 citation statements)

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“…Chemotherapy is among the pilot methods of treatment for cancer patients (Florea and Büsselberg 2011;Luo et al 2012;Raschi and De Ponti 2012). Several investigators have reported that anticancer agents have been utilized for the chemotherapy of various cancers such as sarcoma small cell lung cancer, ovarian cancer, lymphomas, germ cell tumors, and CNS disability (Iwata et al 2012;Lee et al 2012a, b;Rinne et al 2012), but they have also been implicated in causing various kinds of toxicity after treatment in cancer patients measured as adverse effects (Dharap et al 2005;Erkurt et al 2008).…”

Section: Introductionmentioning

confidence: 96%

Neuroprotective activities of curcumin and quercetin with potential relevance to mitochondrial dysfunction induced by oxaliplatin

Waseem

Parvez

2015

Protoplasma

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Peripheral neurotoxicity is one of the serious dose-limiting side effects of oxaliplatin (Oxa) when used in the treatment of malignant conditions. It is documented that it elicits major side effects specifically neurotoxicity due to oxidative stress forcing the patients to limit its clinical use in long-term treatment. Oxidative stress has been proven to be involved in Oxa-induced toxicity including neurotoxicity. The mitochondria have recently emerged as targets for anticancer drugs in various kinds of toxicity including neurotoxicity that can lead to neoplastic disease. However, there is paucity of literature involving the role of the mitochondria in mediating Oxa-induced neurotoxicity and its underlying mechanism is still debatable. The purpose of this study was to investigate the dose-dependent damage caused by Oxa on isolated brain mitochondria under in vitro conditions. The study was also designed to investigate the neuroprotective effects of nutraceuticals, curcumin (CMN), and quercetin (QR) on Oxa-induced mitochondrial oxidative stress and respiratory chain complexes in the brain of rats. Oxidative stress biomarkers, levels of nonenzymatic antioxidants, activities of enzymatic antioxidants, and mitochondrial complexes were evaluated against the neurotoxicity induced by Oxa. Pretreatment with CMN and QR significantly replenished the mitochondrial lipid peroxidation levels and protein carbonyl content induced by Oxa. CMN and QR ameliorated altered nonenzymatic and enzymatic antioxidants and complex enzymes of mitochondria. We conclude that CMN and QR, by attenuating oxidative stress as evident by mitochondrial dysfunction, hold promise as agents that can potentially reduce Oxa-induced adverse effects in the brain.

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Section: Introductionmentioning

confidence: 96%

Neuroprotective activities of curcumin and quercetin with potential relevance to mitochondrial dysfunction induced by oxaliplatin

Waseem

Parvez

2015

Protoplasma

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“…2 and Supplementary Fig. S1, we further measured DNA DSBs in cancer cells treated by FMD-2Br-DAB in combination with IR (225 kV X-rays), using the HCS DNA Damage (gH2AX) Kit (24)(25)(26). Figure 3 shows the fluorescence images of cervical cancer (ME-180) cells with/without the treatment of 25/200 mmol/L FMD and the yield of DNA DSBs detected by gH2AX foci with various X-ray doses, respectively.…”

Section: In Vitro Dna Dsb Measurements In Cancer Cellsmentioning

confidence: 99%

“…At 12 hours after X-ray irradiation, the cells were fixed and stained. Following the detailed protocol provided by the manufacturer, we performed the HCS DNA Damage Assay of the treated cells, as described previously (24)(25)(26). The images of cells were acquired with a Nikon Eclipse TS100 fluorescence microscope; quantitative analyses of activated gH2AX (DNA DBS yield) in the cells were performed using an Image J software.…”

Section: In Vitro Dna Dsb Assaymentioning

confidence: 99%

“…The details have been given previously (24)(25)(26). Briefly, cells were plated at a density of 7 Â 10 3 cells/well in 96-well plates.…”

Section: In Vitro Cell Viability and Clonogenic Assaysmentioning

confidence: 99%

“…Our mechanistic studies in FMD (12)(13)(14)(15)(16)(17)(18)(19)22) provide remarkable opportunities to improve the therapies of existing drugs and to develop new effective drugs. Indeed, our studies have led to the development of novel cisplatin-based combination therapies that could significantly improve the therapeutic efficacy of cisplatin against human ovarian, cervical, and lung cancers (25). On the basis of our new understanding of differential intracellular environments between normal and cancerous cells, we have also discovered a new family of non-platinum-based molecules (called FMD molecules) that selectively kill cancer cells and protect normal cells, effective for targeted chemotherapy of multiple cancers (26).…”

Section: Introductionmentioning

confidence: 99%

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In Vitro and In Vivo Studies of a New Class of Anticancer Molecules for Targeted Radiotherapy of Cancer

Wang

Mahmood

Zhang

et al. 2016

Molecular Cancer Therapeutics

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There is a compelling need to develop anticancer therapies that target cancer cells and tissues. Arising from innovative femtomedicine studies, a new class of non-platinum-based halogenated molecules (called FMD molecules) that selectively kill cancer cells and protect normal cells in treatments of multiple cancers has been discovered. This article reports the first observation of the radiosensitizing effects of such compounds in combination with ionizing radiation for targeted radiotherapy of a variety of cancers. We present in vitro and in vivo studies focused on combination with radiotherapy of cervical, ovarian, head and neck, and lung cancers. Our results demonstrate that treatments of various cancer

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Mitochondria‐mediated mitigatory role of curcumin in cisplatin‐induced nephrotoxicity

Waseem

Kaushik

Parvez

2013

Cell Biochemistry & Function

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Cisplatin (CP) is one of the most potent chemotherapeutic anti-tumour drugs, and it has been implicated in renal toxicity. Oxidative stress has been proven to be involved in CP-induced toxicity including nephrotoxicity. However, there is paucity of literature involving role of mitochondria in mediating CP-induced renal toxicity, and its underlying mechanism remains unclear. Therefore, the present study was undertaken to examine the antioxidant potential of curcumin (CMN; a natural polyphenolic compound) against the mitochondrial toxicity of CP in kidneys of male rats. Acute toxicity was induced by a single intra-peritoneal injection of CP (6 mg kg(-1) ). We studied the ameliorative effect of CMN pre-treatment (200 mg kg(-1) ) on the toxicity of CP in rat kidney mitochondria. CP caused a significant elevation in the mitochondrial lipid peroxidation (LPO) levels and protein carbonyl (PC) content. Pre-treatment of rat with CMN significantly replenished the mitochondrial LPO levels and PC content. It also restored the CP-induced modulatory effects on altered enzymatic and non-enzymatic antioxidants in kidney mitochondria. We hypothesize that the reno-protective effects of CMN may be related to its predisposition to scavenge free radicals, and upregulate antioxidant machinery in kidney mitochondria.

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Electron transfer-based combination therapy of cisplatin with tetramethyl- p -phenylenediamine for ovarian, cervical, and lung cancers

Cited by 30 publications

References 50 publications

Neuroprotective activities of curcumin and quercetin with potential relevance to mitochondrial dysfunction induced by oxaliplatin

Neuroprotective activities of curcumin and quercetin with potential relevance to mitochondrial dysfunction induced by oxaliplatin

In Vitro and In Vivo Studies of a New Class of Anticancer Molecules for Targeted Radiotherapy of Cancer

Mitochondria‐mediated mitigatory role of curcumin in cisplatin‐induced nephrotoxicity

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