Quilamine HQ1-44, an iron chelator vectorized toward tumor cells by the polyamine transport system, inhibits HCT116 tumor growth without adverse effect

Renaud, Stéphanie; Cannie, Isabelle; Ropert, Martine; Lepage, Sylvie; Loréal, Olivier; Deniaud, David; Gaboriau, François

doi:10.1016/j.bcp.2015.06.001

Cited by 3 publications

(1 citation statement)

References 38 publications

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“…Thus the seeking of low-toxic iron chelators or alternative measures, such as exogenous transferrin, exogenous hepcidin, hepcidin analogues, and hepcidin signaling agonists, continues ( Fleming and Ponka, 2012 ). Recent studies reported that novel iron chelators like CN128 ( Sun et al, 2020 ; Chen et al, 2020 ), Quilamine HQ1-44 ( Renaud et al, 2015 ), 1-(N-acetyl-6-aminohexyl)-3-hydroxy-2-methylpyridin-4-one ( Pangjit et al, 2015 ), and some phytochemicals like curcuminoids ( Jiao et al, 2009 ) and quercetin ( Horniblow et al, 2017 ), showed protective functions in many diseases by chelating iron, with no or little side effects. Our study highlighted the use of an iron-deficient diet to induce iron deficiency in restricting ferroptosis and preventing liver injuries, which was harmless than iron chelators because the non-existed side effects and the degree of iron deficiency would not be overwhelmed, for the reason that the iron deficiency induced by iron-deficient diet will increase the iron absorption and the majority of iron source is from the recycle use of iron in aged erythrocytes.…”

Section: Discussionmentioning

confidence: 99%

An iron-deficient diet prevents alcohol- or diethylnitrosamine-induced acute hepatotoxicity in mice by inhibiting ferroptosis

Gao

Wang

Zhang

et al. 2022

Current Research in Food Science

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Section: Discussionmentioning

confidence: 99%

An iron-deficient diet prevents alcohol- or diethylnitrosamine-induced acute hepatotoxicity in mice by inhibiting ferroptosis

Gao

Wang

Zhang

et al. 2022

Current Research in Food Science

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Iron metabolism in colorectal cancer: a balancing act

Estêvão,

da Cruz-Ribeiro,

Cardoso

et al. 2023

Cell Oncol.

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Background Colorectal cancer (CRC) is the third most commonly diagnosed cancer and the second deadliest malignancy worldwide. Current dietary habits are associated with increased levels of iron and heme, both of which increase the risk of developing CRC. The harmful effects of iron overload are related to the induction of iron-mediated pro-tumorigenic pathways, including carcinogenesis and hyperproliferation. On the other hand, iron deficiency may also promote CRC development and progression by contributing to genome instability, therapy resistance, and diminished immune responses. In addition to the relevance of systemic iron levels, iron-regulatory mechanisms in the tumor microenvironment are also believed to play a significant role in CRC and to influence disease outcome. Furthermore, CRC cells are more prone to escape iron-dependent cell death (ferroptosis) than non-malignant cells due to the constitutive activation of antioxidant genes expression. There is wide evidence that inhibition of ferroptosis may contribute to the resistance of CRC to established chemotherapeutic regimens. As such, ferroptosis inducers represent promising therapeutic drugs for CRC. Conclusions and perspectives This review addresses the complex role of iron in CRC, particularly in what concerns the consequences of iron excess or deprivation in tumor development and progression. We also dissect the regulation of cellular iron metabolism in the CRC microenvironment and emphasize the role of hypoxia and of oxidative stress (e.g. ferroptosis) in CRC. Finally, we underline some iron-related players as potential therapeutic targets against CRC malignancy.

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Recent advances in cancer treatment by iron chelators

Corcé

Gouin

Renaud

et al. 2016

Bioorganic & Medicinal Chemistry Letters

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The development of new therapeutic alternatives for cancers is a major public health priority. Among the more promising approaches, the iron depletion strategy based on metal chelation in the tumoral environment has been particularly studied in recent decades. After a short description of the importance of iron for cancer cell proliferation, we will review the different iron chelators developed as potential chemotherapeutics. Finally, the recent efforts to vectorize the chelating agents specifically in the microtumoral environment will be discussed in detail.

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Quilamine HQ1-44, an iron chelator vectorized toward tumor cells by the polyamine transport system, inhibits HCT116 tumor growth without adverse effect

Cited by 3 publications

References 38 publications

An iron-deficient diet prevents alcohol- or diethylnitrosamine-induced acute hepatotoxicity in mice by inhibiting ferroptosis

An iron-deficient diet prevents alcohol- or diethylnitrosamine-induced acute hepatotoxicity in mice by inhibiting ferroptosis

Iron metabolism in colorectal cancer: a balancing act

Recent advances in cancer treatment by iron chelators

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