The Iron Chelator, Deferasirox, as a Novel Strategy for Cancer Treatment: Oral Activity Against Human Lung Tumor Xenografts and Molecular Mechanism of Action

Lui, Goldie Y.L.; Obeidy, Peyman; Ford, Samuel J.; Tselepis, Chris; Sharp, Danae M.; Jansson, Patric J.; Kalinowski, Danuta S.; Kovačević, Žaklina; Lovejoy, David B.; Richardson, Des R.

doi:10.1124/mol.112.081893

Cited by 114 publications

(109 citation statements)

References 56 publications

(79 reference statements)

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“…We observed a dose-dependent antiproliferative activity of DFX in pancreatic cancer cell lines, consistent with the results of previous studies in esophageal cancer cell lines [22] or lung cancer cell lines [23]. Although a number of studies have attempted to elucidate the anti-cancer mechanisms of iron chelators, their mechanisms are not well known [12].…”

Section: Discussionsupporting

confidence: 90%

“…As DFX is given to patients orally, we administered DFX as a saline suspension given orally in accordance with previous studies [22, 23]. DFX administered orally at 160 and 200 mg/kg (every second day, three treatments per week for 21 days) resulted in marked inhibition of tumor growth as determined by measurements of tumor volume and tumor weight (Fig.…”

Section: Resultsmentioning

confidence: 93%

“…On the other hand, DFX, a recently identified iron chelator, can be administered orally once daily because it is orally active and has a long half-life of 7–18 h. DFX is currently used for the treatment of iron-overload disease and is considered an alternative to DFO [16]. The antiproliferative activity of DFX has been investigated in various cancers [22, 23, 29, 30]. However, there have previously been no studies of the effects of DFX in pancreatic cancer; this study is the first to elucidate the antiproliferative activity of DFX against pancreatic cancer cells.…”

Section: Discussionmentioning

confidence: 99%

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Deferasirox, a novel oral iron chelator, shows antiproliferative activity against pancreatic cancer in vitro and in vivo

et al. 2016

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BackgroundIron is essential for cell replication, metabolism and growth. Because neoplastic cells have high iron requirements due to their rapid proliferation, iron depletion may be a novel therapeutic strategy for cancer. Deferasirox (DFX), a novel oral iron chelator, has been successful in clinical trials in iron-overload patients and has been expected to become an anticancer agent. However, no studies have investigated the effects of DFX on pancreatic cancer. This study aimed to elucidate the effects of DFX against pancreatic cancer.MethodsThe effects of DFX on cell cycle, proliferation, and apoptosis were examined in three human pancreatic cancer cell lines: BxPC-3, HPAF-II, and Panc 10.05. The effect of orally administered DFX on the growth of BxPC-3 pancreatic cancer xenografts was also examined in nude mice. Additionally, microarray analysis was performed using tumors excised from xenografts.ResultsDFX inhibited pancreatic cancer cell proliferation in a dose-dependent manner. A concentration of 10 μM DFX arrested the cell cycle in S phase, whereas 50 and 100 μM DFX induced apoptosis. In nude mice, orally administered DFX at 160 and 200 mg/kg suppressed xenograft tumor growth with no serious side effects (n = 5; average tumor volumes of 674 mm3 for controls vs. 327 mm3 for 160 mg/kg DFX, p <0.05; average tumor volumes of 674 mm3 for controls vs. 274 mm3 for 200 mg/kg DFX, p <0.05). Importantly, serum biochemistry analysis indicated that serum levels of ferritin were significantly decreased by the oral administration of 160 or 200 mg/kg DFX (n = 5; average serum ferritin of 18 ng/ml for controls vs. 9 ng/ml for 160 mg/kg DFX, p <0.05; average serum ferritin of 18 ng/ml for controls vs. 10 ng/ml for 200 mg/kg DFX, p <0.05). Gene expression analysis revealed that most genes in pancreatic adenocarcinoma signaling, especially transforming growth factor-ß1 (TGF-ß1), were downregulated by DFX.ConclusionsDFX has potential as a therapeutic agent for pancreatic cancer. Iron depletion was essential for the antiproliferative effect of DFX in a preclinical model, and DFX acted through the suppression of TGF-ß signaling.

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Section: Discussionsupporting

confidence: 90%

Section: Resultsmentioning

confidence: 93%

Section: Discussionmentioning

confidence: 99%

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Deferasirox, a novel oral iron chelator, shows antiproliferative activity against pancreatic cancer in vitro and in vivo

et al. 2016

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“…Deferasirox (Dfx), a tridentate chelator that allows iron redox cycling, is an orally available iron chelator that has promise as an antineoplastic. Dfx has been shown to inhibit the growth of various types of malignant cells in cell culture [66,67] and in xenograft models [68,69]. There is also a case report of Dfx contributing to complete remission in a patient with recurrent acute myelogenous leukemia [70].…”

Section: Dysregulated Iron Metabolism Supports Cancer Growth and Survmentioning

confidence: 99%

Regulators of Iron Homeostasis: New Players in Metabolism, Cell Death, and Disease

Bogdan

Miyazawa

Hashimoto

et al. 2016

Trends in Biochemical Sciences

701

518

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Iron is necessary for life, but can also cause cell death. Accordingly, cells evolved a robust, tightly regulated suite of genes for maintaining iron homeostasis. Previous mechanistic studies on iron homeostasis have granted insight into the role of iron in human health and disease. We highlight new regulators of iron metabolism, including iron-trafficking proteins [solute carrier family 39, SLC39, also known as ZRT/IRT-like protein, ZIP; and poly-(rC)-binding protein, PCBP] and a cargo receptor (NCOA4) that is crucial for release of ferritin-bound iron. We also discuss emerging roles of iron in apoptosis and a novel iron-dependent cell death pathway termed ‘ferroptosis’, the dysregulation of iron metabolism in human pathologies, and the use of iron chelators in cancer therapy.

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“…Aberrant tumor cell iron handling is central to its toxicity (43,44). Studies underway should clarify effects of iron in experimental (45)(46)(47) and human (48)(49)(50) malignancy. Little information is available on effects of iron reduction on blood coagulation.…”

Section: Current Status Of Anticoagulant Effects On Cancer Outcomesmentioning

confidence: 99%

Anticoagulation, ferrotoxicity and the future of translational lung cancer research

Zacharski¹

2016

Transl. Lung Cancer Res.

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Numerous studies have shown that elements of coagulation reactions mediate tumor cell proliferation, motility (invasiveness), tissue remodeling and metastasis. Coagulation activation is virtually a universal feature of human malignancy that differs from the clotting response to injury in that it is selfperpetuating rather than self-attenuating. Coagulation activation participates in tumor matrix deposition and

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The Iron Chelator, Deferasirox, as a Novel Strategy for Cancer Treatment: Oral Activity Against Human Lung Tumor Xenografts and Molecular Mechanism of Action

Cited by 114 publications

References 56 publications

Deferasirox, a novel oral iron chelator, shows antiproliferative activity against pancreatic cancer in vitro and in vivo

Deferasirox, a novel oral iron chelator, shows antiproliferative activity against pancreatic cancer in vitro and in vivo

Regulators of Iron Homeostasis: New Players in Metabolism, Cell Death, and Disease

Anticoagulation, ferrotoxicity and the future of translational lung cancer research

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