Abstract

The main objective of this application is to use multinuclear NMR spectroscopy to provide detailed knowledge of the dynamic response of tumor biology to hyperthermia and hyperglycemia. This information will be used to: 1) elucidate the mechanism by which hyperglycemia enhances the sensitivity of tumors to hyperthermia; 2) determine the physiological parameters which affect tumor metabolism under conditions of hyperthermia and hyperglycemia; and 3) evaluate the efficacy of NMR spectroscopy as a monitor and predictor of tumor response to hyperthermia and hyperglycemia. Implicit in the pursuit of these goals is the requirement to better understand how tumor physiology is reflected in NMR spectra in vivo. The mechanism by which hyperglycemia reduces tumor pH and blood flow and the effect of these two factors on thermal sensitivity will be examined by assessing the importance of a) glycolysis (determined by measuring rates of glucose consumption and lactic acid production using 13C labelled substrates and 13C NMR and observing the effect of mannitol, a non-metabolizable carbohydrate, on tumor pH, blood flow, and thermal sensitivity) and b) reduced blood flow (determined by observing the effect of hyperglycemia on the same factors when a perfluorocarbon blood substitute is used). The contributions of cells, in different environments in a tumor, to the in vivo 31p NMR spectrum will be examined by observing the effects of pH, pO2, nutrient concentration, flow rate and temperature on the spectrum of a homogeneous population of cells in vitro. Physiological parameters which affect tumor metabolism under conditions of mild (40 degrees-42 degrees C) or severe (greater than 45 degrees C) hyperthermia (+- hyperglycemia) will be determined by correlating the changes observed by NMR with measured values of tumor blood flow (determined by 15-0 activation and 19F NMR techniques) and well-perfused fraction (determined by 15-0 activation technique), and tumor response to treatment (determined by tumor growth delay and the fraction of clonogenic cells surviving treatment). The clinical efficacy of NMR as a monitor and predictor of tumor response to hyperthermia and hyperglycemia will be assessed by evaluating the ability of the NMR markers, determined from the above studies, to monitor and predict tumor response to treatment in individual mice using two tumors of different thermal sensitivities (i.e., RIF-1 in C3H mice and EMT6 in BALB/c mice) and a tumor with a substrain-dependent response to hyperglycemia (i.e., RIF-1 in C3H/Anf and C3H/Hej mice).

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA040411-01
Application #
3180290
Study Section
Diagnostic Radiology Study Section (RNM)
Project Start
1985-09-30
Project End
1988-06-30
Budget Start
1985-09-30
Budget End
1988-06-30
Support Year
1
Fiscal Year
1985
Total Cost
Indirect Cost

  Institution

Name
Wayne State University
Department
Type
Schools of Medicine
DUNS #
City
Detroit
State
MI
Country
United States
Zip Code
48202

  Publications

Spees, William M; Evelhoch, Jeffrey L; Thompson, Paul A et al. (2005) Defining the pHi-hyperthermia sensitivity relationship for the RIF-1 tumor in vivo: a 31P MR spectroscopy study. Radiat Res 164:86-99
Bezabeh, T; Evelhoch, J L; Sloop, D J et al. (2004) Methodology for applied 4 MHz RF hyperthermia concomitant with 31P NMR spectroscopic monitoring of murine tumours. Int J Hyperthermia 20:637-45
Bezabeh, T; Evelhoch, J L; Thompson, P et al. (2004) Therapeutic efficacy as predicted by quantitative assessment of murine RIF-1 tumour pH and phosphorous metabolite response during hyperthermia: an in vivo 31P NMR study. Int J Hyperthermia 20:335-57
Soto, G E; Zhu, Z; Evelhoch, J L et al. (1996) Tumor 31P NMR pH measurements in vivo: a comparison of inorganic phosphate and intracellular 2-deoxyglucose-6-phosphate as pHnmr indicators in murine radiation-induced fibrosarcoma-1. Magn Reson Med 36:698-704
Ackerman, J J; Soto, G E; Spees, W M et al. (1996) The NMR chemical shift pH measurement revisited: analysis of error and modeling of a pH dependent reference. Magn Reson Med 36:674-83
Evelhoch, J L (1992) Measurement of tumor blood flow by deuterium NMR and the effects of modifiers. NMR Biomed 5:290-5
Hwang, Y Y; Kim, S G; Evelhoch, J L et al. (1992) Nonglycolytic acidification of murine radiation-induced fibrosarcoma 1 tumor via 3-O-methyl-D-glucose monitored by 1H, 2H, 13C, and 31P nuclear magnetic resonance spectroscopy. Cancer Res 52:1259-66
Neil, J J; Song, S K; Ackerman, J J (1992) Concurrent quantification of tissue metabolism and blood flow via 2H/31P NMR in vivo. II. Validation of the deuterium NMR washout method for measuring organ perfusion. Magn Reson Med 25:56-66
Bezabeh, T; Ackerman, J J (1992) Chemical exchange in tissue extracts revisited: bicarbonate and deuterium isotope effects on 31P resonances of phosphoethanolamine and phosphocreatine. NMR Biomed 5:364-7
Mattiello, J; Evelhoch, J L (1991) Relative volume-average murine tumor blood flow measurement via deuterium nuclear magnetic resonance spectroscopy. Magn Reson Med 18:320-34

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