In vivo 31 P MR spectral patterns and reproducibility in cancer patients studied in a multi-institutional trial

F. Arias-Mendoza; G. S. Payne; K. L. Zakian; A. J. Schwarz; M. Stubbs; R. Stoyanova; D. Ballon; F. A. Howe; J. A. Koutcher; M. O. Leach; J. R. Griffiths; A. Heerschap; J. D. Glickson; S. J. Nelson; J. L. Evelhoch; H. C. Charles; T. R. Brown; J. Cruz-Lobo; J. Murphy-Boesch; W. G. Negendank; A. Shukla-Dave; A. Oregioni; D. J. Collins; N. R. Maisey; Sabrina Ronen; Victoria L. Doyle; Mark Rijpkema; H. Poptani; R. E. Lenkinski; D. B. Vigneron; Jiani Hu

doi:10.1002/nbm.1057

In vivo ³¹ P MR spectral patterns and reproducibility in cancer patients studied in a multi-institutional trial

F. Arias-Mendoza, G. S. Payne, K. L. Zakian, A. J. Schwarz, M. Stubbs, R. Stoyanova, D. Ballon, F. A. Howe, J. A. Koutcher, M. O. Leach, J. R. Griffiths, A. Heerschap, J. D. Glickson, S. J. Nelson, J. L. Evelhoch, H. C. Charles, T. R. Brown, J. Cruz-Lobo, J. Murphy-Boesch, W. G. NegendankA. Shukla-Dave, A. Oregioni, D. J. Collins, N. R. Maisey, Sabrina Ronen, Victoria L. Doyle, Mark Rijpkema, H. Poptani, R. E. Lenkinski, D. B. Vigneron, Jiani Hu

Research output: Contribution to journal › Article › peer-review

48 Scopus citations

Abstract

The standardization and reproducibility of techniques required to acquire anatomically localized ³¹p MR spectra non-invasively while studying tumors in cancer patients in a multi-institutional group at 1.5 Tare reported. This initial group of patients was studied from 1995 to 2000 to test the feasibility of acquiring in vivo localized ³¹P MRS in clinical MR spectrometers. The cancers tested were non-Hodgkin's lymphomas, sarcomas of soft tissue and bone, breast carcinomas and head and neck carcinomas. The best accrual and spectral quality were achieved with the non-Hodgkin's lymphomas. The initial analysis of the spectral values of the sum of phosphoethanolamine plus phosphocholine normalized by the content of nucleotide triphosphates in a homogeneous sample of 32 NHL patients studied by in vivo ³¹P MRS showed good reproducibility among different institutions. No statistical differences were found between the institution with the largest number of cases accrued and the rest of the multi-institutional NHL data (2.2 ± 0.64, mean ± standard error; n = 17, vs 2.08 ± 0.14, n = 15). The preliminary data reported demonstrate that the institutions involved in this trial are obtaining reproducible ³¹P MR spectroscopic data non-invasively from human tumors. This is a fundamental prerequisite for the international cooperative group to be able to demonstrate the clinical value of the normalized determination of phosphoethanolamine plus phosphocholine by ³¹P MRS as predictor for treatment response in cancer patients.

Original language	English (US)
Pages (from-to)	504-512
Number of pages	9
Journal	NMR in biomedicine
Volume	19
Issue number	4
DOIs	https://doi.org/10.1002/nbm.1057
State	Published - Jun 2006

Keywords

Breast carcinomas
Cancer
Head and neck carcinomas
Localized P MR spectroscopy
Multi-institutional group
Non-Hodgkin's lymphomas
Non-invasive
Phosphocholine
Phosphoethanolamine
Reproducibility
Sarcomas of soft tissue and bone

ASJC Scopus subject areas

Molecular Medicine
Radiology Nuclear Medicine and imaging
Spectroscopy

Access to Document

10.1002/nbm.1057

Cite this

Arias-Mendoza, F., Payne, G. S., Zakian, K. L., Schwarz, A. J., Stubbs, M., Stoyanova, R., Ballon, D., Howe, F. A., Koutcher, J. A., Leach, M. O., Griffiths, J. R., Heerschap, A., Glickson, J. D., Nelson, S. J., Evelhoch, J. L., Charles, H. C., Brown, T. R., Cruz-Lobo, J., Murphy-Boesch, J., ... Hu, J. (2006). In vivo ³¹ P MR spectral patterns and reproducibility in cancer patients studied in a multi-institutional trial. NMR in biomedicine, 19(4), 504-512. https://doi.org/10.1002/nbm.1057

Arias-Mendoza, F, Payne, GS, Zakian, KL, Schwarz, AJ, Stubbs, M, Stoyanova, R, Ballon, D, Howe, FA, Koutcher, JA, Leach, MO, Griffiths, JR, Heerschap, A, Glickson, JD, Nelson, SJ, Evelhoch, JL, Charles, HC, Brown, TR, Cruz-Lobo, J, Murphy-Boesch, J, Negendank, WG, Shukla-Dave, A, Oregioni, A, Collins, DJ, Maisey, NR, Ronen, S, Doyle, VL, Rijpkema, M, Poptani, H, Lenkinski, RE, Vigneron, DB & Hu, J 2006, 'In vivo ³¹ P MR spectral patterns and reproducibility in cancer patients studied in a multi-institutional trial', NMR in biomedicine, vol. 19, no. 4, pp. 504-512. https://doi.org/10.1002/nbm.1057

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title = "In vivo 31 P MR spectral patterns and reproducibility in cancer patients studied in a multi-institutional trial",

abstract = "The standardization and reproducibility of techniques required to acquire anatomically localized 31p MR spectra non-invasively while studying tumors in cancer patients in a multi-institutional group at 1.5 Tare reported. This initial group of patients was studied from 1995 to 2000 to test the feasibility of acquiring in vivo localized 31P MRS in clinical MR spectrometers. The cancers tested were non-Hodgkin's lymphomas, sarcomas of soft tissue and bone, breast carcinomas and head and neck carcinomas. The best accrual and spectral quality were achieved with the non-Hodgkin's lymphomas. The initial analysis of the spectral values of the sum of phosphoethanolamine plus phosphocholine normalized by the content of nucleotide triphosphates in a homogeneous sample of 32 NHL patients studied by in vivo 31P MRS showed good reproducibility among different institutions. No statistical differences were found between the institution with the largest number of cases accrued and the rest of the multi-institutional NHL data (2.2 ± 0.64, mean ± standard error; n = 17, vs 2.08 ± 0.14, n = 15). The preliminary data reported demonstrate that the institutions involved in this trial are obtaining reproducible 31P MR spectroscopic data non-invasively from human tumors. This is a fundamental prerequisite for the international cooperative group to be able to demonstrate the clinical value of the normalized determination of phosphoethanolamine plus phosphocholine by 31P MRS as predictor for treatment response in cancer patients.",

keywords = "Breast carcinomas, Cancer, Head and neck carcinomas, Localized P MR spectroscopy, Multi-institutional group, Non-Hodgkin's lymphomas, Non-invasive, Phosphocholine, Phosphoethanolamine, Reproducibility, Sarcomas of soft tissue and bone",

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AU - Arias-Mendoza, F.

AU - Payne, G. S.

AU - Zakian, K. L.

AU - Schwarz, A. J.

AU - Stubbs, M.

AU - Stoyanova, R.

AU - Ballon, D.

AU - Howe, F. A.

AU - Koutcher, J. A.

AU - Leach, M. O.

AU - Griffiths, J. R.

AU - Heerschap, A.

AU - Glickson, J. D.

AU - Nelson, S. J.

AU - Evelhoch, J. L.

AU - Charles, H. C.

AU - Brown, T. R.

AU - Cruz-Lobo, J.

AU - Murphy-Boesch, J.

AU - Negendank, W. G.

AU - Shukla-Dave, A.

AU - Oregioni, A.

AU - Collins, D. J.

AU - Maisey, N. R.

AU - Ronen, Sabrina

AU - Doyle, Victoria L.

AU - Rijpkema, Mark

AU - Poptani, H.

AU - Lenkinski, R. E.

AU - Vigneron, D. B.

AU - Hu, Jiani

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AB - The standardization and reproducibility of techniques required to acquire anatomically localized 31p MR spectra non-invasively while studying tumors in cancer patients in a multi-institutional group at 1.5 Tare reported. This initial group of patients was studied from 1995 to 2000 to test the feasibility of acquiring in vivo localized 31P MRS in clinical MR spectrometers. The cancers tested were non-Hodgkin's lymphomas, sarcomas of soft tissue and bone, breast carcinomas and head and neck carcinomas. The best accrual and spectral quality were achieved with the non-Hodgkin's lymphomas. The initial analysis of the spectral values of the sum of phosphoethanolamine plus phosphocholine normalized by the content of nucleotide triphosphates in a homogeneous sample of 32 NHL patients studied by in vivo 31P MRS showed good reproducibility among different institutions. No statistical differences were found between the institution with the largest number of cases accrued and the rest of the multi-institutional NHL data (2.2 ± 0.64, mean ± standard error; n = 17, vs 2.08 ± 0.14, n = 15). The preliminary data reported demonstrate that the institutions involved in this trial are obtaining reproducible 31P MR spectroscopic data non-invasively from human tumors. This is a fundamental prerequisite for the international cooperative group to be able to demonstrate the clinical value of the normalized determination of phosphoethanolamine plus phosphocholine by 31P MRS as predictor for treatment response in cancer patients.

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KW - Non-Hodgkin's lymphomas

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KW - Phosphocholine

KW - Phosphoethanolamine

KW - Reproducibility

KW - Sarcomas of soft tissue and bone

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