Publication: Synaptic proteins and phospholipids are increased in gerbil brain by administering uridine plus docosahexaenoic acid orally
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Date
2006-05-09
Authors
Ulus, İsmail Hakkı
Cansev, Mehmet
Authors
Wurtman, Richard J.
Watkins, Carol J.
Wang, Lei
Marzloff, George
Journal Title
Journal ISSN
Volume Title
Publisher
Elsevier Science
Abstract
The synthesis of brain phosphatidy1choline may utilize three circulating precursors: choline; a pyrimidine (e.g., uridine, converted via UTP to brain CTP); and a PUFA (e.g., docosahexaenoic acid); phosphatidylethanolamine may utilize two of these, a pyrimidine and a PUFA. We observe that consuming these precursors can substantially increase membrane phosphatide and synaptic protein levels in gerbil brains. (Pyrimidine metabolism in gerbils, but not rats, resembles that in humans.) Animals received, daily for 4 weeks, a diet containing choline chloride and UMP (a uridine source) and/or DHA by gavage. Brain phosphatidy1choline rose by 13-22% with uridine and choline alone, or DHA alone, or by 45% with the combination, phosphatidylethanolamine and the other phosphatides increasing by 39-74%. Smaller elevations occurred after 1-3 weeks. The combination also increased the vesicular protein Synapsin-1 by 41%, the postsynaptic protein PSD-95 by 38% and the neurite neurofibrillar proteins NF-70 and NF-M by up to 102% and 48%, respectively. However, it had no effect on the cytoskeletal protein beta-tubulin. Hence, the quantity of synaptic membrane probably increased. The precursors act by enhancing the substrate saturation of enzymes that initiate their incorporation into phosphatidylcholine and phosphatidylethanolamine and by UTP-mediated activation of P2Y receptors. Alzheimer's disease brains contain fewer and smaller synapses and reduced levels of synaptic proteins, membrane phosphatides, choline and DHA. The three phosphatide precursors might thus be useful in treating this disease..
Description
Keywords
Neurosciences & neurology, Alzheimer's disease, Synaptic protein, Neuronal membrane, Phosphatidylcholine, Uridine, Docosahexaenoic acid, Neurite outgrowth, Alzheimers-disease, Nerve growth-factor, Polyunsaturated fatty-acid, Release, Impairment, Rats, Supplementation, Cytidine, Cdp-choline, Animalia, Gerbillinae
Citation
Wurtman, R. J. vd. (2006). ''Synaptic proteins and phospholipids are increased in gerbil brain by administering uridine plus docosahexaenoic acid orally''. Brain Research, 1088, 83-92.