BRAF mutations are associated with increased iron regulatory protein‐2 expression in colorectal tumorigenesis

Horniblow, Richard D.; Bedford, Matthew; Hollingworth, Robert M.; Evans, Sarah; Sutton, Emily; Lal, Neeraj; Beggs, Andrew D; Iqbal, Tariq; Tselepis, Chris

doi:10.1111/cas.13234

Cited by 41 publications

(26 citation statements)

References 34 publications

(79 reference statements)

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“…In fact, TfR1 expression increased and FTH1 mRNA expression decreased with no correlation with IRP2 mRNA expression. This is contrary to ndings by Horniblow (2017) in which IRP2 and TfR1 expression both increased in CRC and correlated with each other [30].…”

Section: Discussioncontrasting

confidence: 99%

Intravenous Iron Therapy Replenishes Iron Stores without Enhancing Tumour Responses in Anaemic Patients with Colorectal Cancer: Comparison with Oral Iron Supplementation.

Al-Hassi

Evstatiev

et al. 2020

Preprint

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Background: Oral iron promotes intestinal tumourigenesis in animal models. In humans, expression of iron transport proteins are altered in colorectal cancer. This study examines whether the route of iron therapy alters iron transport and tumour growth. Methods: Colorectal adenocarcinoma patients with pre-operative iron deficiency anaemia received oral ferrous sulphate (n=15), or intravenous ferric carboxymaltose (n=15). Paired (normal and tumour tissues) samples were compared for expression of iron loading, iron transporters, proliferation, apoptosis, Wnt signalling pathway and microsatellite instability using immunohistochemistry and RT-PCR. Results: Iron loading was increased in tumour and distributed to the stroma in intravenous treatment and to the epithelium in oral treatment. The protein and mRNA expression of iron transporters were increased in tumours compared to normal tissues but there were no significant differences between the treatment groups. However, intravenous iron treatment reduced ferritin mRNA levels in tumours (p<0.001) and successfully replenished body iron stores without increasing tumour growth, DNA damage markers, proliferation or apoptosis compared with oral iron treatment. Conclusion: Iron distribution to non-epithelial cells in intravenous iron treatment suggests that iron is less bioavailable to tumour cells. Therefore, intravenous iron supplementation could be a safer option in the treatment of colorectal cancer patients with iron deficiency anaemia due to the differential compartmentalisation of iron within the intestinal mucosa and its efficiency in replenishing body iron levels without increasing the risk of tumour growth.Trial registration: The study was registered with the Medicines and Healthcare Regulatory Agency, clinical trials.gov (NCT01927328) and EudraCT (2013-000209-22).

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Section: Discussioncontrasting

confidence: 99%

Intravenous Iron Therapy Replenishes Iron Stores without Enhancing Tumour Responses in Anaemic Patients with Colorectal Cancer: Comparison with Oral Iron Supplementation.

Al-Hassi

Evstatiev

et al. 2020

Preprint

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“…In prostate cancer cells IRP2 was consistently overexpressed and knockdown inhibited growth in vitro and in vivo, while IRP1 was detected in some cell lines and knockdown only modestly reduced proliferation in vitro (77). IRP2 was overexpressed in colon cancer tissues compared to normal and interestingly, correlated with BRAF mutations and it was confirmed in vitro that IRP2 overexpression was driven by hyperactivation of the MAPK pathway (79). Therefore, the expression and roles of IRPs in cancer differ by tumor type.…”

Section: Iron Regulatory Proteinsmentioning

confidence: 92%

“…correlated with histologic grade and molecular subtype of human breast cancer(76). IRP2 was elevated in colorectal cancers compared to normal colon mucosa(79).…”

mentioning

confidence: 99%

Altered Iron Metabolism and Impact in Cancer Biology, Metastasis, and Immunology

et al. 2020

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Iron is an essential nutrient that plays a complex role in cancer biology. Iron metabolism must be tightly controlled within cells. Whilst fundamental to many cellular processes and required for cell survival, excess labile iron is toxic to cells. Increased iron metabolism is associated with malignant transformation, cancer progression, drug resistance and immune evasion. Depleting intracellular iron stores, either with the use of iron chelating agents or mimicking endogenous regulation mechanisms, such as microRNAs, present attractive therapeutic opportunities, some of which are currently under clinical investigation. Alternatively, iron overload can result in a form of regulated cell death, ferroptosis, which can be activated in cancer cells presenting an alternative anti-cancer strategy. This review focuses on alterations in iron metabolism that enable cancer cells to meet metabolic demands required during different stages of tumorigenesis in relation to metastasis and immune response. The strength of current evidence is considered, gaps in knowledge are highlighted and controversies relating to the role of iron and therapeutic targeting potential are discussed. The key question we address within this review is whether iron modulation represents a useful approach for treating metastatic disease and whether it could be employed in combination with existing targeted drugs and immune-based therapies to enhance their efficacy.

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“…Hypoxia induces the expression of TFR1 and DMT1 in HepG2 cells; however, overexpression of IRP1 could reduce the stability of TfR1 and DMT1 mRNAs under hypoxia condition [ 130 ]. IRP2 is overexpressed in colorectal cancer compared to normal colonic mucosa which is associated with mutations in BRAF, and its expression is positively correlated with TFR1 expression [ 94 ]. IRP2-positive is also a marker of poor prognosis in lung cancer [ 95 ].…”

Section: Alterations Of Iron Homeostasis In Cancer Cellsmentioning

confidence: 99%

Alterations in Cellular Iron Metabolism Provide More Therapeutic Opportunities for Cancer

Zhou

Zhao

Zhang

et al. 2018

IJMS

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Iron is an essential element for the growth and proliferation of cells. Cellular iron uptake, storage, utilization and export are tightly regulated to maintain iron homeostasis. However, cellular iron metabolism pathways are disturbed in most cancer cells. To maintain rapid growth and proliferation, cancer cells acquire large amounts of iron by altering expression of iron metabolism- related proteins. In this paper, normal cellular iron metabolism and the alterations of iron metabolic pathways in cancer cells were summarized. Therapeutic strategies based on targeting the altered iron metabolism were also discussed and disrupting redox homeostasis by intracellular high levels of iron provides new insight for cancer therapy. Altered iron metabolism constitutes a promising therapeutic target for cancer therapy.

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BRAF mutations are associated with increased iron regulatory protein‐2 expression in colorectal tumorigenesis

Cited by 41 publications

References 34 publications

Intravenous Iron Therapy Replenishes Iron Stores without Enhancing Tumour Responses in Anaemic Patients with Colorectal Cancer: Comparison with Oral Iron Supplementation.

Intravenous Iron Therapy Replenishes Iron Stores without Enhancing Tumour Responses in Anaemic Patients with Colorectal Cancer: Comparison with Oral Iron Supplementation.

Altered Iron Metabolism and Impact in Cancer Biology, Metastasis, and Immunology

Alterations in Cellular Iron Metabolism Provide More Therapeutic Opportunities for Cancer

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