Iron overload, measured as serum ferritin, increases brain damage induced by focal ischemia and early reperfusion
► Iron worsens ischemic damage induced by transient ischemia and early reperfusion. ► Iron plays an important role in evolution of penumbra to infarct. ► Ferritin is not an acute phase protein after ischemia. ► Ferritin is a good indicator of body iron levels after ischemia. High levels of iron, mea...
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Veröffentlicht in: | Neurochemistry international 2012-12, Vol.61 (8), p.1364-1369 |
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Sprache: | eng |
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Zusammenfassung: | ► Iron worsens ischemic damage induced by transient ischemia and early reperfusion. ► Iron plays an important role in evolution of penumbra to infarct. ► Ferritin is not an acute phase protein after ischemia. ► Ferritin is a good indicator of body iron levels after ischemia.
High levels of iron, measured as serum ferritin, are associated to a worse outcome after stroke. However, it is not known whether ischemic damage might increase ferritin levels as an acute phase protein or whether iron overload affects stroke outcome. The objectives are to study the effect of stroke on serum ferritin and the contribution of iron overload to ischemic damage.
Swiss mice were fed with a standard diet or with a diet supplemented with 2.5% carbonyl iron to produce iron overload. Mice were submitted to permanent (by ligature and by in situ thromboembolic models) or transient focal ischemia (by ligature for 1 or 3h).
Treatment with iron diet produced an increase in the basal levels of ferritin in all the groups. However, serum ferritin did not change after ischemia. Animals submitted to permanent ischemia had the same infarct volume in the groups studied. However, in mice submitted to transient ischemia followed by early (1h) but not late reperfusion (3h), iron overload increased ischemic damage and haemorrhagic transformation.
Iron worsens ischemic damage induced by transient ischemia and early reperfusion. In addition, ferritin is a good indicator of body iron levels but not an acute phase protein after ischemia. |
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ISSN: | 0197-0186 1872-9754 |
DOI: | 10.1016/j.neuint.2012.09.014 |