Effects of acute dietary iron overload in pigs (sus scrofa) with induced type 2 diabetes mellitus
Author
dc.contributor.author
Espinoza, A.
Author
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Morales, S.
es_CL
Author
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Arredondo Olguín, Miguel
es_CL
Admission date
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2014-12-23T11:51:40Z
Available date
dc.date.available
2014-12-23T11:51:40Z
Publication date
dc.date.issued
2014
Cita de ítem
dc.identifier.citation
Biol Trace Elem Res (2014) 158:342–352
en_US
Identifier
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DOI: 10.1007/s12011-014-9944-4
Identifier
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https://repositorio.uchile.cl/handle/2250/124139
General note
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Articulo de publicación ISI
en_US
Abstract
dc.description.abstract
Epidemiological studies have reported an association
between high iron (Fe) levels and elevated risk of developing
type 2 diabetes mellitus (T2D). It is believed that the
formation of Fe-catalyzed hydroxyl radicals may contribute to
the development of diabetes. Our goal was to determine the
effect of a diet with a high Fe content on type 2 diabetic pigs.
Four groups of piglets were studied: (1) control group, basal
diet; (2) Fe group, basal diet with 3,000 ppm ferrous sulfate;
(3) diabetic group (streptozotocin-induced type 2 diabetes)
with basal diet; (4) diabetic/Fe group, diabetic animals/
3,000 ppm ferrous sulfate. For 2 months, biochemical and
hematological parameters were evaluated. Tissue samples of
liver and duodenum were obtained to determine mRNA relative
abundance of DMT1, ferroportin (Fpn), ferritin (Fn),
hepcidin (Hpc), and transferrin receptor by qRT-PCR. Fe
group presented increased levels of hematological (erythrocytes,
hematocrit, and hemoglobin) and iron parameters.
Diabetic/Fe group showed similar behavior as Fe group but
in lesser extent. The relative abundance of different genes in
the four study groups yielded a different expression pattern.
DMT1 showed a lower expression in the two iron groups
compared with control and diabetic animals, and Hpc showed
an increased on its expression in Fe and diabetic/Fe groups.
Diabetic/Fe group presents greater expression of Fn and Fpn.
These results suggest that there is an interaction between Fe
nutrition, inflammation, and oxidative stress in the diabetes
development.
en_US
Patrocinador
dc.description.sponsorship
This project was funded in part by (1)
Comisión Nacional de Investigación Científica y Tecnológica
(CONICYT)—Scholarship for Doctoral Thesis 2010; (2) Programa de
Investigación Domeyko en Salud, Universidad de Chile—Scholarship
Doctoral Thesis 2010; and (3) FONDECYT Grant 1110080 to MA