4.5 Article

α-Haemoglobin regulates sympathoadrenal cell metabolism to maintain a catecholaminergic phenotype

Journal

BIOCHEMICAL JOURNAL
Volume 441, Issue -, Pages 843-850

Publisher

PORTLAND PRESS LTD
DOI: 10.1042/BJ20111640

Keywords

dopamine; haemoglobin; oxidative stress; sympathadrenal lineage; tyrosine hydroxylase

Funding

  1. Gene Expression Nervous System Atlas (GENSAT) Project [NINDS] [N01NS02331, HHSN271200723701C]
  2. Marcelino Botin Foundation
  3. Spanish Ministry of Science and Education
  4. Andalusian Government
  5. Instituto de Salud Carlos III

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Discovery of haemoglobin A expression outside of the erythroid cell lineage suggests that oxygen transport is the main, but not the unique, function of adult haemoglobin chains in mammals. The contribution of haemoglobin A to antioxidant defences has been proposed in the territories where it is expressed. Catecholaminergic cells rely on an active oxidative metabolism to accomplish their biological function, but are exposed to strong oxidative stress due to metabolism of catecholaminergic transmitters. We show in the present study that peripheral catecholaminegic cells express the alpha- and not the beta-haemoglobin A chains, and that alpha-haemoglobin expression could modulate the antioxidant capabilities of these cells. We also show that alpha-haemoglobin overexpression in PC12 cells leads to a selective increase of tyrosine hydroxylase synthesis and activity. This is achieved by means of a reorganization of antioxidant defences, decreasing cytoplasmic glutathione peroxidase and superoxide dismutase, and increasing mitochondrial peroxidase. Moreover, alpha-haemoglobin induces a decrease in lipogenesis and increase in lipid degradation, situations that help save NAD(P)H and favour supply of acetyl-CoA to the tricarboxylic acid cycle and production of reducing equivalents in the cell. All of these results point to a role for alpha-haemoglobin as a regulator of catecholaminergic cell metabolism required for phenotype acquisition and maintenance.

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