Author:
Al-Hassi Hafid O.,Ng Oliver,Evstatiev Rayko,Mangalika Manel,Worton Natalie,Jambrich Manuela,Khare Vineeta,Phipps Oliver,Keeler Barrie,Gasche Christoph,Acheson Austin G.,Brookes Matthew J.
Abstract
AbstractOral iron promotes intestinal tumourigenesis in animal models. In humans, expression of iron transport proteins are altered in colorectal cancer. This study examined whether the route of iron therapy alters iron transport and tumour growth. 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 and Wnt signalling using immunohistochemistry and RT-PCR. Iron loading was increased in tumour and distributed to the stroma in intravenous treatment and to the epithelium in oral treatment. Protein and mRNA expression of proliferation and 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 and replenished body iron stores. Iron distribution to non-epithelial cells in intravenous iron suggests that iron is less bioavailable to tumour cells. Therefore, intravenous iron may be a better option in the treatment of colorectal cancer patients with iron deficiency anaemia due to its efficiency in replenishing iron levels while its effect on proliferation and iron metabolism is similar to that of oral iron treatment.
Funder
The Rotha Abraham Bequest, the Royal Wolverhampton NHS Trust, Wolverhampton, UK.
National Institute for Health Research
The Medical Scientific Fund of the Mayor of the City of Vienna, Vienna, Austria.
Publisher
Springer Science and Business Media LLC
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