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Alanine metabolism, transport, and cycling in the brain
Authors:Bröer Stefan  Bröer Angelika  Hansen Jonas T  Bubb William A  Balcar Vladimir J  Nasrallah Fatima A  Garner Brett  Rae Caroline
Institution:School of Biochemistry and Molecular Biology, Australian National University, Acton, Canberra ACT, Australia;
School of Molecular and Microbial Biosciences, The University of Sydney, Sydney, New South Wales, Australia;
Department of Anatomy and Histology, The University of Sydney, Sydney, New South Wales, Australia;
Prince of Wales Medical Research Institute, Randwick, New South Wales, Australia;
School of Chemistry, The University of New South Wales, Sydney, New South Wales, Australia
Abstract:Brain glutamate/glutamine cycling is incomplete without return of ammonia to glial cells. Previous studies suggest that alanine is an important carrier for ammonia transfer. In this study, we investigated alanine transport and metabolism in Guinea pig brain cortical tissue slices and prisms, in primary cultures of neurons and astrocytes, and in synaptosomes. Alanine uptake into astrocytes was largely mediated by system L isoform LAT2, whereas alanine uptake into neurons was mediated by Na+-dependent transporters with properties similar to system B0 isoform B0AT2. To investigate the role of alanine transport in metabolism, its uptake was inhibited in cortical tissue slices under depolarizing conditions using the system L transport inhibitors 2-aminobicyclo2.2.1]heptane-2-carboxylic acid and cycloleucine (1-aminocyclopentanecarboxylic acid; cLeu). The results indicated that alanine cycling occurs subsequent to glutamate/glutamine cycling and that a significant proportion of cycling occurs via amino acid transport system L. Our results show that system L isoform LAT2 is critical for alanine uptake into astrocytes. However, alanine does not provide any significant carbon for energy or neurotransmitter metabolism under the conditions studied.
Keywords:13C NMR spectroscopy  glutamine transport  LAT2  nitrogen metabolism
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