Title of article
Determining the oxidation states of manganese in NT2 cells and cultured astrocytes
Author/Authors
Karlene K. Gunter، نويسنده , , Michael Aschner، نويسنده , , Lisa M. Miller، نويسنده , , Roman Eliseev، نويسنده , , Jason Salter، نويسنده , , Katie Anderson، نويسنده , , Thomas E. Gunter، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2006
Pages
11
From page
1816
To page
1826
Abstract
Excessive brain manganese (Mn) can produce a syndrome called “manganism”, which correlates with loss of striatal dopamine and cell death in the striatum and globus pallidus. The prevalent hypothesis for the cause of this syndrome has been oxidation of cell components by the strong oxidizing agent, Mn3+, either formed by oxidation of intracellular Mn2+ or transported into the cell as Mn3+. We have recently used X-ray absorption near edge structure spectroscopy (XANES) to determine the oxidation states of manganese complexes in brain and liver mitochondria and in nerve growth factor (NGF)-induced and non-induced PC12 cells. No evidence was found for stabilization or accumulation of Mn3+ complexes because of oxidation of Mn2+ by reactive oxygen species in these tissues. Here we extend these studies of manganese oxidation state to cells of brain origin, human neuroteratocarcinoma (NT2) cells and primary cultures of rat astrocytes. Again we find no evidence for stabilization or accumulation of any Mn3+ complex derived from oxidation of Mn2+ under a range of conditions.
Keywords
Mn oxidation states , XANES spectroscopy , NT2 cells , Astrocytes , Mn toxicity
Journal title
Neurobiology of Aging
Serial Year
2006
Journal title
Neurobiology of Aging
Record number
820899
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