Cortical metabolism in pyruvate dehydrogenase deficiency revealed by ex vivo multiplet (13)C NMR of the adult mouse brain.

[pyruvate dehydrogenase deficiency]

The pyruvate dehydrogenase complex (PDC ), required for complete glucose oxidation , is essential for brain development . Although PDC deficiency is associated with a severe clinical syndrome , little is known about its effects on either substrate oxidation or synthesis of key metabolites such as glutamate and glutamine . Computational simulations of brain metabolism indicated that a 25 % reduction in flux through PDC and a corresponding increase in flux from an alternative source of acetyl-CoA would substantially alter the (13 )C NMR spectrum obtained from brain tissue . Therefore , we evaluated metabolism of [1 ,6 -(13 )C (2 )]glucose (oxidized by both neurons and glia ) and [1 ,2 -(13 )C (2 )]acetate (an energy source that bypasses PDC ) in the cerebral cortex of adult mice mildly and selectively deficient in brain PDC activity , a viable model that recapitulates the human disorder . Intravenous infusions were performed in conscious mice and extracts of brain tissue were studied by (13 )C NMR . We hypothesized that mice deficient in PDC must increase the proportion of energy derived from acetate metabolism in the brain . Unexpectedly , the distribution of (13 )C in glutamate and glutamine , a measure of the relative flux of acetate and glucose into the citric acid cycle , was not altered . The (13 )C labeling pattern in glutamate differed significantly from glutamine , indicating preferential oxidation of [1 ,2 -(13 )C ]acetate relative to [1 ,6 -(13 )C ]glucose by a readily discernible metabolic domain of the brain of both normal and mutant mice , presumably glia . These findings illustrate that metabolic compartmentation is preserved in the PDC -deficient cerebral cortex , probably reflecting intact neuron-glia metabolic interactions , and that a reduction in brain PDC activity sufficient to induce cerebral dysgenesis during development does not appreciably disrupt energy metabolism in the mature brain .