作者
Joseph E Ippolito, Matthew E Merritt, Fredrik Bäckhed, Krista L Moulder, Steven Mennerick, Jill K Manchester, Seth T Gammon, David Piwnica-Worms, Jeffrey I Gordon
发表日期
2006/8/15
期刊
Proceedings of the National Academy of Sciences
卷号
103
期号
33
页码范围
12505-12510
出版商
National Academy of Sciences
简介
To identify metabolic features that support the aggressive behavior of human neuroendocrine (NE) cancers, we examined metastatic prostate NE tumors and derived prostate NE cancer (PNEC) cell lines from a transgenic mouse model using a combination of magic angle spinning NMR spectroscopy, in silico predictions of biotransformations that observed metabolites may undergo, biochemical tests of these predictions, and electrophysiological/calcium imaging studies. Malignant NE cells undergo excitation and increased proliferation when their GABAA, glutamate, and/or glycine receptors are stimulated, use glutamate and GABA as substrates for NADH biosynthesis, and produce propylene glycol, a precursor of pyruvate derived from glycine that increases levels of circulating free fatty acids through extra-NE cell effects. Treatment of nude mice containing PNEC tumor xenografts with (i) amiloride, a diuretic that …
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