Blood-derived iron mediates free radical production and neuronal death in the hippocampal CA1 area following transient forebrain ischemia in rat

Ui Jin Park; Young Ae Lee; Sun Mi Won; Jin Hwan Lee; Seung Hee Kang; Joe E. Springer; Yong Beom Lee; Byoung Joo Gwag

doi:10.1007/s00401-010-0785-8

Blood-derived iron mediates free radical production and neuronal death in the hippocampal CA1 area following transient forebrain ischemia in rat

Ui Jin Park, Young Ae Lee, Sun Mi Won, Jin Hwan Lee, Seung Hee Kang, Joe E. Springer, Yong Beom Lee, Byoung Joo Gwag

Research output: Contribution to journal › Article › peer-review

90 Scopus citations

Abstract

Abnormal brain iron homeostasis has been proposed as a pathological event leading to oxidative stress and neuronal injury under pathological conditions. We examined the possibility that neuronal iron overload would mediate free radical production and delayed neuronal death (DND) in hippocampal CA1 area after transient forebrain ischemia (TFI). Mitochondrial free radicals (MFR) were biphasically generated in CA1 neurons 0.5-8 and 48-60 h after TFI. Treatment with Neu2000, a potent spin trapping molecule, as well as trolox, a vitamin E analogue, blocked the biphasic MFR production and attenuated DND in the CA1, regardless of whether it was administered immediately or even 24 h after reperfusion. The late increase in MFR was accompanied by iron accumulation and blocked by the administration of deferoxamine-an iron chelator. Iron accumulation was attributable to prolonged upregulation of the transferrin receptor and to increased uptake of peripheral iron through a leaky blood-brain barrier. Infiltration of iron-containing cells and iron accumulation were attenuated by depletion of circulating blood cells through X-ray irradiation of the whole body except the head. The present findings suggest that excessive iron transported from blood mediates slowly evolving oxidative stress and neuronal death in CA1 after TFI, and that targeting iron-mediated oxidative stress holds extended therapeutic time window against an ischemic event.

Original language	English
Pages (from-to)	459-473
Number of pages	15
Journal	Acta Neuropathologica
Volume	121
Issue number	4
DOIs	https://doi.org/10.1007/s00401-010-0785-8
State	Published - Apr 2011

Bibliographical note

Funding Information:
Acknowledgments This work was supported by grants from the Brain Korea 21 Project for Medical Science, Ajou University, the 21C Frontier R&D Program in Neuroscience from Ministry of Education, Science and Technology, and Neurotech Pharmaceuticals.

Funding

Acknowledgments This work was supported by grants from the Brain Korea 21 Project for Medical Science, Ajou University, the 21C Frontier R&D Program in Neuroscience from Ministry of Education, Science and Technology, and Neurotech Pharmaceuticals.

Funders	Funder number
Neurotech Pharmaceuticals Co.
Ministry of Education, Culture, Sports, Science and Technology

Keywords

Blood-brain barrier
CA1 pyramidal neurons
Free radicals
Iron
Transferrin receptor
Transient forebrain ischemia

ASJC Scopus subject areas

Pathology and Forensic Medicine
Clinical Neurology
Cellular and Molecular Neuroscience

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10.1007/s00401-010-0785-8

Cite this

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title = "Blood-derived iron mediates free radical production and neuronal death in the hippocampal CA1 area following transient forebrain ischemia in rat",

abstract = "Abnormal brain iron homeostasis has been proposed as a pathological event leading to oxidative stress and neuronal injury under pathological conditions. We examined the possibility that neuronal iron overload would mediate free radical production and delayed neuronal death (DND) in hippocampal CA1 area after transient forebrain ischemia (TFI). Mitochondrial free radicals (MFR) were biphasically generated in CA1 neurons 0.5-8 and 48-60 h after TFI. Treatment with Neu2000, a potent spin trapping molecule, as well as trolox, a vitamin E analogue, blocked the biphasic MFR production and attenuated DND in the CA1, regardless of whether it was administered immediately or even 24 h after reperfusion. The late increase in MFR was accompanied by iron accumulation and blocked by the administration of deferoxamine-an iron chelator. Iron accumulation was attributable to prolonged upregulation of the transferrin receptor and to increased uptake of peripheral iron through a leaky blood-brain barrier. Infiltration of iron-containing cells and iron accumulation were attenuated by depletion of circulating blood cells through X-ray irradiation of the whole body except the head. The present findings suggest that excessive iron transported from blood mediates slowly evolving oxidative stress and neuronal death in CA1 after TFI, and that targeting iron-mediated oxidative stress holds extended therapeutic time window against an ischemic event.",

keywords = "Blood-brain barrier, CA1 pyramidal neurons, Free radicals, Iron, Transferrin receptor, Transient forebrain ischemia",

author = "Park, \{Ui Jin\} and Lee, \{Young Ae\} and Won, \{Sun Mi\} and Lee, \{Jin Hwan\} and Kang, \{Seung Hee\} and Springer, \{Joe E.\} and Lee, \{Yong Beom\} and Gwag, \{Byoung Joo\}",

note = "Funding Information: Acknowledgments This work was supported by grants from the Brain Korea 21 Project for Medical Science, Ajou University, the 21C Frontier R\&D Program in Neuroscience from Ministry of Education, Science and Technology, and Neurotech Pharmaceuticals.",

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AU - Park, Ui Jin

AU - Lee, Young Ae

AU - Won, Sun Mi

AU - Lee, Jin Hwan

AU - Kang, Seung Hee

AU - Springer, Joe E.

AU - Lee, Yong Beom

AU - Gwag, Byoung Joo

N1 - Funding Information: Acknowledgments This work was supported by grants from the Brain Korea 21 Project for Medical Science, Ajou University, the 21C Frontier R&D Program in Neuroscience from Ministry of Education, Science and Technology, and Neurotech Pharmaceuticals.

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N2 - Abnormal brain iron homeostasis has been proposed as a pathological event leading to oxidative stress and neuronal injury under pathological conditions. We examined the possibility that neuronal iron overload would mediate free radical production and delayed neuronal death (DND) in hippocampal CA1 area after transient forebrain ischemia (TFI). Mitochondrial free radicals (MFR) were biphasically generated in CA1 neurons 0.5-8 and 48-60 h after TFI. Treatment with Neu2000, a potent spin trapping molecule, as well as trolox, a vitamin E analogue, blocked the biphasic MFR production and attenuated DND in the CA1, regardless of whether it was administered immediately or even 24 h after reperfusion. The late increase in MFR was accompanied by iron accumulation and blocked by the administration of deferoxamine-an iron chelator. Iron accumulation was attributable to prolonged upregulation of the transferrin receptor and to increased uptake of peripheral iron through a leaky blood-brain barrier. Infiltration of iron-containing cells and iron accumulation were attenuated by depletion of circulating blood cells through X-ray irradiation of the whole body except the head. The present findings suggest that excessive iron transported from blood mediates slowly evolving oxidative stress and neuronal death in CA1 after TFI, and that targeting iron-mediated oxidative stress holds extended therapeutic time window against an ischemic event.

AB - Abnormal brain iron homeostasis has been proposed as a pathological event leading to oxidative stress and neuronal injury under pathological conditions. We examined the possibility that neuronal iron overload would mediate free radical production and delayed neuronal death (DND) in hippocampal CA1 area after transient forebrain ischemia (TFI). Mitochondrial free radicals (MFR) were biphasically generated in CA1 neurons 0.5-8 and 48-60 h after TFI. Treatment with Neu2000, a potent spin trapping molecule, as well as trolox, a vitamin E analogue, blocked the biphasic MFR production and attenuated DND in the CA1, regardless of whether it was administered immediately or even 24 h after reperfusion. The late increase in MFR was accompanied by iron accumulation and blocked by the administration of deferoxamine-an iron chelator. Iron accumulation was attributable to prolonged upregulation of the transferrin receptor and to increased uptake of peripheral iron through a leaky blood-brain barrier. Infiltration of iron-containing cells and iron accumulation were attenuated by depletion of circulating blood cells through X-ray irradiation of the whole body except the head. The present findings suggest that excessive iron transported from blood mediates slowly evolving oxidative stress and neuronal death in CA1 after TFI, and that targeting iron-mediated oxidative stress holds extended therapeutic time window against an ischemic event.

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KW - CA1 pyramidal neurons

KW - Free radicals

KW - Iron

KW - Transferrin receptor

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Blood-derived iron mediates free radical production and neuronal death in the hippocampal CA1 area following transient forebrain ischemia in rat

Abstract

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Keywords

ASJC Scopus subject areas

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