Interactions of iron, dopamine and neuromelanin pathways in brain aging and Parkinson's disease
Author
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Zucca, Fabio A.
Author
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Segura Aguilar, Juan
Author
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Ferrari, Emanuele
Author
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Muñoz, Patricia
Author
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Paris Pizarro, Irmgard
Author
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Sulzer, David
Author
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Sarna, Tadeusz
Author
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Casella, Luigi
Author
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Zecca, Luigi
Admission date
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2019-03-18T11:53:42Z
Available date
dc.date.available
2019-03-18T11:53:42Z
Publication date
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2017
Cita de ítem
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Prog Neurobiol. 2017 August ; 155: 96–119
Identifier
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18735118
Identifier
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03010082
Identifier
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10.1016/j.pneurobio.2015.09.012
Identifier
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https://repositorio.uchile.cl/handle/2250/166708
Abstract
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There are several interrelated mechanisms involving iron, dopamine, and neuromelanin in neurons.
Neuromelanin accumulates during aging and is the catecholamine-derived pigment of the
dopamine neurons of the substantia nigra and norepinephrine neurons of the locus coeruleus, the
two neuronal populations most targeted in Parkinson’s disease. Many cellular redox reactions rely
on iron, however an altered distribution of reactive iron is cytotoxic. In fact, increased levels of
iron in the brain of Parkinson’s disease patients are present. Dopamine accumulation can induce
neuronal death; however, excess dopamine can be removed by converting it into a stable
compound like neuromelanin, and this process rescues the cell. Interestingly, the main iron
compound in dopamine and norepinephrine neurons is the neuromelanin-iron complex, since
neuromelanin is an effective metal chelator. Neuromelanin serves to trap iron and provide neuronal
protection from oxidative stress. This equilibrium between iron, dopamine, and neuromelanin is
crucial for cell homeostasis and in some cellular circumstances can be disrupted. Indeed, when
neuromelanin-containing organelles accumulate high load of toxins and iron during aging a
neurodegenerative process can be triggered. In addition, neuromelanin released by degenerating
neurons activates microglia and the latter cause neurons death with further release of
neuromelanin, then starting a self-propelling mechanism of neuroinflammation and
neurodegeneration. Considering the above issues, age-related accumulation of neuromelanin in
dopamine neurons shows an interesting link between aging and neurodegeneration.
Patrocinador
dc.description.sponsorship
Italian Ministry of Education, University, and Research (MIUR) - National Research Programme (PNR) - CNR Flagship "InterOmics'' Project PB.P05 PNR - CNR Aging program Lombardy Region - CNR MbMM Project 18089/RCC MIUR-Research Projects of National Interest (PRIN) 2010M2JARJ FONDECYT 1100165 Parkinson's Disease Foundation JPB Foundation NIH DA07418 DA10154