Limits of [(18)F]-FLT PET as a Biomarker of Proliferation in Oncology

BACKGROUND: Non-invasive imaging biomarkers of cellular proliferation hold great promise for quantifying response to personalized medicine in oncology. An emerging approach to assess tumor proliferation utilizes the positron emission tomography (PET) tracer 3’-deoxy-3’[(18)F]-fluorothymidine, [(18)F...

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Autores principales: McKinley, Eliot T., Ayers, Gregory D., Smith, R. Adam, Saleh, Samir A., Zhao, Ping, Washington, Mary Kay, Coffey, Robert J., Manning, H. Charles
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3598948/
https://www.ncbi.nlm.nih.gov/pubmed/23554961
http://dx.doi.org/10.1371/journal.pone.0058938
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author McKinley, Eliot T.
Ayers, Gregory D.
Smith, R. Adam
Saleh, Samir A.
Zhao, Ping
Washington, Mary Kay
Coffey, Robert J.
Manning, H. Charles
author_facet McKinley, Eliot T.
Ayers, Gregory D.
Smith, R. Adam
Saleh, Samir A.
Zhao, Ping
Washington, Mary Kay
Coffey, Robert J.
Manning, H. Charles
author_sort McKinley, Eliot T.
collection PubMed
description BACKGROUND: Non-invasive imaging biomarkers of cellular proliferation hold great promise for quantifying response to personalized medicine in oncology. An emerging approach to assess tumor proliferation utilizes the positron emission tomography (PET) tracer 3’-deoxy-3’[(18)F]-fluorothymidine, [(18)F]-FLT. Though several studies have associated serial changes in [(18)F]-FLT-PET with elements of therapeutic response, the degree to which [(18)F]-FLT-PET quantitatively reflects proliferative index has been continuously debated for more that a decade. The goal of this study was to elucidate quantitative relationships between [(18)F]-FLT-PET and cellular metrics of proliferation in treatment naïve human cell line xenografts commonly employed in cancer research. METHODS AND FINDINGS: [(18)F]-FLT-PET was conducted in human cancer xenograft-bearing mice. Quantitative relationships between PET, thymidine kinase 1 (TK1) protein levels and immunostaining for proliferation markers (Ki67, TK1, PCNA) were evaluated using imaging-matched tumor specimens. Overall, we determined that [(18)F]-FLT-PET reflects TK1 protein levels, yet the cell cycle specificity of TK1 expression and the extent to which tumors utilize thymidine salvage for DNA synthesis decouple [(18)F]-FLT-PET data from standard estimates of proliferative index. CONCLUSIONS: Our findings illustrate that [(18)F]-FLT-PET reflects tumor proliferation as a function of thymidine salvage pathway utilization. Unlike more general proliferation markers, such as Ki67, [(18)F]-FLT PET reflects proliferative indices to variable and potentially unreliable extents. [(18)F]-FLT-PET cannot discriminate moderately proliferative, thymidine salvage-driven tumors from those of high proliferative index that rely primarily upon de novo thymidine synthesis. Accordingly, the magnitude of [(18)F]-FLT uptake should not be considered a surrogate of proliferative index. These data rationalize the diversity of [(18)F]-FLT-PET correlative results previously reported and suggest future best-practices when [(18)F]-FLT-PET is employed in oncology.
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spelling pubmed-35989482013-04-02 Limits of [(18)F]-FLT PET as a Biomarker of Proliferation in Oncology McKinley, Eliot T. Ayers, Gregory D. Smith, R. Adam Saleh, Samir A. Zhao, Ping Washington, Mary Kay Coffey, Robert J. Manning, H. Charles PLoS One Research Article BACKGROUND: Non-invasive imaging biomarkers of cellular proliferation hold great promise for quantifying response to personalized medicine in oncology. An emerging approach to assess tumor proliferation utilizes the positron emission tomography (PET) tracer 3’-deoxy-3’[(18)F]-fluorothymidine, [(18)F]-FLT. Though several studies have associated serial changes in [(18)F]-FLT-PET with elements of therapeutic response, the degree to which [(18)F]-FLT-PET quantitatively reflects proliferative index has been continuously debated for more that a decade. The goal of this study was to elucidate quantitative relationships between [(18)F]-FLT-PET and cellular metrics of proliferation in treatment naïve human cell line xenografts commonly employed in cancer research. METHODS AND FINDINGS: [(18)F]-FLT-PET was conducted in human cancer xenograft-bearing mice. Quantitative relationships between PET, thymidine kinase 1 (TK1) protein levels and immunostaining for proliferation markers (Ki67, TK1, PCNA) were evaluated using imaging-matched tumor specimens. Overall, we determined that [(18)F]-FLT-PET reflects TK1 protein levels, yet the cell cycle specificity of TK1 expression and the extent to which tumors utilize thymidine salvage for DNA synthesis decouple [(18)F]-FLT-PET data from standard estimates of proliferative index. CONCLUSIONS: Our findings illustrate that [(18)F]-FLT-PET reflects tumor proliferation as a function of thymidine salvage pathway utilization. Unlike more general proliferation markers, such as Ki67, [(18)F]-FLT PET reflects proliferative indices to variable and potentially unreliable extents. [(18)F]-FLT-PET cannot discriminate moderately proliferative, thymidine salvage-driven tumors from those of high proliferative index that rely primarily upon de novo thymidine synthesis. Accordingly, the magnitude of [(18)F]-FLT uptake should not be considered a surrogate of proliferative index. These data rationalize the diversity of [(18)F]-FLT-PET correlative results previously reported and suggest future best-practices when [(18)F]-FLT-PET is employed in oncology. Public Library of Science 2013-03-15 /pmc/articles/PMC3598948/ /pubmed/23554961 http://dx.doi.org/10.1371/journal.pone.0058938 Text en © 2013 McKinley et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
McKinley, Eliot T.
Ayers, Gregory D.
Smith, R. Adam
Saleh, Samir A.
Zhao, Ping
Washington, Mary Kay
Coffey, Robert J.
Manning, H. Charles
Limits of [(18)F]-FLT PET as a Biomarker of Proliferation in Oncology
title Limits of [(18)F]-FLT PET as a Biomarker of Proliferation in Oncology
title_full Limits of [(18)F]-FLT PET as a Biomarker of Proliferation in Oncology
title_fullStr Limits of [(18)F]-FLT PET as a Biomarker of Proliferation in Oncology
title_full_unstemmed Limits of [(18)F]-FLT PET as a Biomarker of Proliferation in Oncology
title_short Limits of [(18)F]-FLT PET as a Biomarker of Proliferation in Oncology
title_sort limits of [(18)f]-flt pet as a biomarker of proliferation in oncology
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3598948/
https://www.ncbi.nlm.nih.gov/pubmed/23554961
http://dx.doi.org/10.1371/journal.pone.0058938
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