In Vitro and in Vivo13C and 31P NMR analyses of phosphocholine metabolism in rat glioma cells

Gillies, Robert J.; Barry, Judith; Ross, Brian D.

doi:10.1002/mrm.1910320306

Cited by 75 publications

(71 citation statements)

References 33 publications

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“…In general, the consensus is that tissues with high proliferative potential or tissues that are oncogenically transformed are also highly cellular in the absence of compensating apoptotic mechanisms or limitations of vascular supply. Consistent with this, many studies strongly have suggested that the Cho peak detected by in vivo MRS may be elevated because the volume of interest is highly cellular (Chang et al, 1995;Miller et al, 1996b;Cheng et al, 2000b) or includes cells with high PCho which may be due to increased proliferative potential (Daly et al, 1987;Daly and Cohen, 1989;Gillies et al, 1994a;Mahmood et al, 1994;Aiken and Gillies, 1996;Aiken et al, 1996) or includes cells which are oncogenically transformed (Bhakoo et al, 1996;Aboagye and Bhujwalla, 1999;Ackerstaff et al, 2001). It was recently reported that in ex vivo high resolution MR spectra (which show much higher than the spectra obtained in vivo) of a biopsy from a cerebellar primitive neuroectodermal tumor, myo-inositol, taurine and phosphorylethanolamine contribute to the in vivo signal at 3.2 ppm, usually attributed to Cho-containing compounds (Tugnoli et al, 2001).…”

Section: Biological Aspects Of Selected Metabolites Detected By Protomentioning

confidence: 78%

“…The Cho peak consists of water-soluble Cho-containing compounds, such as phosphocholine (PCho) and glycerophosphocholine (GPC), and free choline (Barker et al, 1994), versus membrane-bound phospatidylcholine (Miller et al, 1996a). In vivo MRS reveals that phosphomonoesters (PME), such as phosphocholine (PCho) and phosphoethanolamine (PEth), are elevated in tumors and rapidly proliferating tissues (Daly et al, 1987;Daly and Cohen, 1989;Gillies et al, 1994a). Furthermore, elevations in PCho and PEth correlate with increased cell growth or increased cell degradation, and have been shown to occur in human tumors, as well as in animal tumor models and cell lines.…”

Section: Biological Aspects Of Selected Metabolites Detected By Protomentioning

confidence: 99%

“…For instance, actively proliferating cultures show dramatically lower PCho/PEth as compared to stationary cultures (Aiken and Gillies, 1996). Gillies et al, found that PCho levels are lowest, and PEth levels are highest in non-proliferating cells and concluded there is a decrease in the biosynthesis of PCho concomitant with a reduction in culture growth (Gillies et al, 1994b). Mahmood et al, found a strong radiation dose-dependent response in the relative PCho/PEth ratio, suggesting that changes in the PCho levels may be related to cell proliferation and/or radiation-induced membrane damage (Mahmood et al, 1994).…”

Section: Biological Aspects Of Selected Metabolites Detected By Protomentioning

confidence: 99%

See 2 more Smart Citations

Pediatric Brain Tumors: Magnetic Resonance Spectroscopic Imaging

Tzika¹,

Astrakas²,

Zarifi³

2011

Diagnostic Techniques and Surgical Management of Brain Tumors

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Section: Biological Aspects Of Selected Metabolites Detected By Protomentioning

confidence: 78%

Section: Biological Aspects Of Selected Metabolites Detected By Protomentioning

confidence: 99%

Section: Biological Aspects Of Selected Metabolites Detected By Protomentioning

confidence: 99%

See 1 more Smart Citation

Pediatric Brain Tumors: Magnetic Resonance Spectroscopic Imaging

Tzika¹,

Astrakas²,

Zarifi³

2011

Diagnostic Techniques and Surgical Management of Brain Tumors

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“…In most cases, enhanced phospholipid biosynthesis and reduced phospholipid breakdown were observed in long-term chronic situations such as tumors and high phosphomonoester (PME) levels have been hypothesized to be the best biochemical marker to distinguish some cancerous from normal tissues (16,17,43,52,55,62,65) and to monitor tumor treatment outcome (69,75). Some but not all of these observations might be due to the fact that under certain conditions PC strongly correlates with cell proliferation (4,6,21,26,62,68,72,82). Ting et al (80) compared the metabolism of different human breast cancer cells and normal mammary epithelial cells with a similar proliferative activity.…”

Section: Discussionmentioning

confidence: 99%

“…Among other things, measurement of tumor energetics by 31 P-NMR spectroscopy provides useful information about tumor oxygenation/ hypoxia and potential therapeutic resistance. However, there is some controversy about the relevance of the additional parameters that can be monitored in tumors via phosphorous NMR, e.g., phospholipid metabolism (15,16,26,43,44,62,68,79). It was previously reported that most human tumors contain high concentrations of phosphomonoesters, with the major compounds being identified as phosphorylethanolamine (PE) and phosphorylcholine (PC) (15,54,72).…”

mentioning

confidence: 99%

Phosphorous metabolites and steady-state energetics of transformed fibroblasts during three-dimensional growth

Kunz-Schughart

Freyer

2002

American Journal of Physiology-Cell Physiology

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and MR1 spheroids represent separate transformed phenotypes originated from the same rat fibroblasts that differ in three-dimensional (3D) growth kinetics, histological structure, and oxygenation status. In the present study, 31 P-NMR spectroscopy of perfused spheroid suspensions was used to investigate cellular energetics relative to 3D growth, development of necrosis, and cell cycle distribution. Both spheroid types were characterized by a remarkably low amount of free (inorganic) phosphate (Pi) and a low phosphocreatine peak. The ratio of nucleoside triphosphate (NTP) to Pi ranged between 1.5 and 2.0. Intracellular pH, NTP-to-Pi ratio, and NTP/cell remained constant throughout spheroid growth, being unaffected by the emergence of oxygen deficiency, cell quiescence, and necrosis. However, a 50% decrease in the ratio of the lipid precursors phosphorylcholine and phosphorylethanolamine (PC/PE) was observed with increasing spheroid size and was correlated with an increased G1/G0 phase cell fraction. In addition, the ratio of the phospholipid degradation products glycerophosphorylcholine and glycerophosphorylethanolamine (GPC/ GPE) increased with spheroid diameter in Rat1-T1 aggregates. We conclude that changes in phospholipid metabolism, rather than alterations in energy-rich phosphates, reflect cell quiescence in spheroid cultures, because cells in the inner oxygen-deficient zones seem to adapt their energy metabolism to the environmental conditions before necrotic cell destruction. energy metabolism; tumor biology; nuclear magnetic resonance spectroscopy; phospholipids; quiescence MAGNETIC RESONANCE SPECTROSCOPY (MRS) is increasingly utilized as an in vivo method to monitor cell metabolism and tissue oxygenation in various organs and diseases (17,27,41,49). New approaches include its application in neuropsychiatric and toxicology research (5, 10, 46, 61), and it is widely applied in pharmacokinetic and comparative physiological studies (47,50,56,67,84). MRS has also become a powerful technological tool providing noninvasive access to tumor bioenergetic state because of its most attractive feature of nondestructively measuring chemical compounds in intact, living tissues (17, 27). Combinations of advanced MRS techniques with labeled compounds and genetic manipulation are now allowing in situ measurements of specific metabolic pathways in tumors (8,58,67,71,87).Experimental, preclinical, and clinical spectroscopy results indicate that cancers have typical metabolic characteristics that might be of diagnostic and/or prognostic relevance and could be used to some extent as predictors of cancer treatment outcome (17,24, 31,42,45,51,54,57,64,70). Among other things, measurement of tumor energetics by 31 P-NMR spectroscopy provides useful information about tumor oxygenation/ hypoxia and potential therapeutic resistance. However, there is some controversy about the relevance of the additional parameters that can be monitored in tumors via phosphorous NMR, e.g., phospholipid metabolism (15,16,26,43,44,62,68,79). It was ...

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