Abstract

A clinical magnetic resonance examination incorporating localized lH spectroscopy, localized 31P spectroscopy, and proton imaging, will be developed. This will be used to observe the physiologic and metabolic state of adult supratentorial gliomas in vivo. These tumors are rarely successfully excised completely, due to their location and/or size. A group of patients, with unresectable or minimally resected tumors, will be examined prior to radiation (or radiation plus chemotherapy), during its course and at its conclusion, and at the normal follow-up visit (1-6 months after the conclusion of radiation therapy). The spectral information will be mapped to the anatomical magnetic resonance images, in order to correlate variations in metabolism with regions of tumor and normal tissue. A smaller group of patients with completely resected tumors will be examined at 6-month intervals; spectral data from the excision region will be correlated with recurrence or continued freedom from tumor. The in vivo 31P observations will be made using chemical shift imaging (CSI). This technique will allow simultaneous observation of both the affected and normal hemispheres, with maximal resolution of 3-3.5 cm for 31P spectra. IH spectra will be collected by a stimulated-echo localization technique, possibly combined with 1-dimensional CSI. IH spectra will also be collected from both normal and pathological regions, with a spatial resolution of 2-3 cm. The data will be analyzed using an automatic software program developed at Fox Chase which allows for peak identification and quantification with automatic baseline estimation (PIQABLE). An automatic data analysis of this type is necessary to deal with the large number of spectra produced in these clinical observations. Spectroscopic data will be displayed as overlays on the proton image so that the full range of metabolic information provided by the spectral observations can be fully utilized in determining the differences between tumor and normal tissue, and the changes in gliomas in response to therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA049516-01
Application #
3193663
Study Section
Diagnostic Radiology Study Section (RNM)
Project Start
1989-03-10
Project End
1993-02-28
Budget Start
1989-03-10
Budget End
1990-02-28
Support Year
1
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
Fox Chase Cancer Center
Department
Type
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19111

  Publications

Broniscer, A; Gajjar, A; Bhargava, R et al. (1997) Brain stem involvement in children with neurofibromatosis type 1: role of magnetic resonance imaging and spectroscopy in the distinction from diffuse pontine glioma. Neurosurgery 40:331-7; discussion 337-8
Taylor, J S; Langston, J W; Reddick, W E et al. (1996) Clinical value of proton magnetic resonance spectroscopy for differentiating recurrent or residual brain tumor from delayed cerebral necrosis. Int J Radiat Oncol Biol Phys 36:1251-61
Reddick, W E; Langston, J W; Meyer, W H et al. (1994) Discrete signal processing of dynamic contrast-enhanced MR imaging: statistical validation and preliminary clinical application. J Magn Reson Imaging 4:397-404
Murphy-Boesch, J; Srinivasan, R; Carvajal, L et al. (1994) Two configurations of the four-ring birdcage coil for 1H imaging and 1H-decoupled 31P spectroscopy of the human head. J Magn Reson B 103:103-14
Ogg, R J; Kingsley, P B; Taylor, J S (1994) WET, a T1- and B1-insensitive water-suppression method for in vivo localized 1H NMR spectroscopy. J Magn Reson B 104:1-10
Kingsley, P B (1994) Scalar coupling and zero-quantum coherence relaxation in STEAM: implications for spectral editing of lactate. Magn Reson Med 31:315-9
Murphy-Boesch, J; Stoyanova, R; Srinivasan, R et al. (1993) Proton-decoupled 31P chemical shift imaging of the human brain in normal volunteers. NMR Biomed 6:173-80
Hanna, S L; Reddick, W E; Parham, D M et al. (1993) Automated pixel-by-pixel mapping of dynamic contrast-enhanced MR images for evaluation of osteosarcoma response to chemotherapy: preliminary results. J Magn Reson Imaging 3:849-53
Jeneson, J A; Nelson, S J; Vigneron, D B et al. (1992) Two-dimensional 31P-chemical shift imaging of intramuscular heterogeneity in exercising human forearm muscle. Am J Physiol 263:C357-64
Vigneron, D B; Nelson, S J; Murphy-Boesch, J et al. (1990) Chemical shift imaging of human brain: axial, sagittal, and coronal P-31 metabolite images. Radiology 177:643-9

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