Development of a microarray platform for FFPET profiling: application to the classification of human tumors

BACKGROUND: mRNA profiling has become an important tool for developing and validating prognostic assays predictive of disease treatment response and outcome. Archives of annotated formalin-fixed paraffin-embedded tissues (FFPET) are available as a potential source for retrospective studies. Methods...

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Autores principales: Duenwald, Sven, Zhou, Mingjie, Wang, Yanqun, Lejnine, Serguei, Kulkarni, Amit, Graves, Jaime, Smith, Ryan, Castle, John, Tokiwa, George, Fine, Bernard, Dai, Hongyue, Fare, Thomas, Marton, Matthew
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2009
Materias:
Methodology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2732596/
https://www.ncbi.nlm.nih.gov/pubmed/19638234
http://dx.doi.org/10.1186/1479-5876-7-65
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author Duenwald, Sven
Zhou, Mingjie
Wang, Yanqun
Lejnine, Serguei
Kulkarni, Amit
Graves, Jaime
Smith, Ryan
Castle, John
Tokiwa, George
Fine, Bernard
Dai, Hongyue
Fare, Thomas
Marton, Matthew
author_facet Duenwald, Sven
Zhou, Mingjie
Wang, Yanqun
Lejnine, Serguei
Kulkarni, Amit
Graves, Jaime
Smith, Ryan
Castle, John
Tokiwa, George
Fine, Bernard
Dai, Hongyue
Fare, Thomas
Marton, Matthew
author_sort Duenwald, Sven
collection PubMed
description BACKGROUND: mRNA profiling has become an important tool for developing and validating prognostic assays predictive of disease treatment response and outcome. Archives of annotated formalin-fixed paraffin-embedded tissues (FFPET) are available as a potential source for retrospective studies. Methods are needed to profile these FFPET samples that are linked to clinical outcomes to generate hypotheses that could lead to classifiers for clinical applications. METHODS: We developed a two-color microarray-based profiling platform by optimizing target amplification, experimental design, quality control, and microarray content and applied it to the profiling of FFPET samples. We profiled a set of 50 fresh frozen (FF) breast cancer samples and assigned class labels according to the signature and method by van 't Veer et al [1] and then profiled 50 matched FFPET samples to test how well the FFPET data predicted the class labels. We also compared the sorting power of classifiers derived from FFPET sample data with classifiers derived from data from matched FF samples. RESULTS: When a classifier developed with matched FF samples was applied to FFPET data to assign samples to either "good" or "poor" outcome class labels, the classifier was able to assign the FFPET samples to the correct class label with an average error rate = 12% to 16%, respectively, with an Odds Ratio = 36.4 to 60.4, respectively. A classifier derived from FFPET data was able to predict the class label in FFPET samples (leave-one-out cross validation) with an error rate of ~14% (p-value = 3.7 × 10(-7)). When applied to the matched FF samples, the FFPET-derived classifier was able to assign FF samples to the correct class labels with 96% accuracy. The single misclassification was attributed to poor sample quality, as measured by qPCR on total RNA, which emphasizes the need for sample quality control before profiling. CONCLUSION: We have optimized a platform for expression analyses and have shown that our profiling platform is able to accurately sort FFPET samples into class labels derived from FF classifiers. Furthermore, using this platform, a classifier derived from FFPET samples can reliably provide the same sorting power as a classifier derived from matched FF samples. We anticipate that these techniques could be used to generate hypotheses from archives of FFPET samples, and thus may lead to prognostic and predictive classifiers that could be used, for example, to segregate patients for clinical trial enrollment or to guide patient treatment.
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spelling pubmed-27325962009-08-27 Development of a microarray platform for FFPET profiling: application to the classification of human tumors Duenwald, Sven Zhou, Mingjie Wang, Yanqun Lejnine, Serguei Kulkarni, Amit Graves, Jaime Smith, Ryan Castle, John Tokiwa, George Fine, Bernard Dai, Hongyue Fare, Thomas Marton, Matthew J Transl Med Methodology BACKGROUND: mRNA profiling has become an important tool for developing and validating prognostic assays predictive of disease treatment response and outcome. Archives of annotated formalin-fixed paraffin-embedded tissues (FFPET) are available as a potential source for retrospective studies. Methods are needed to profile these FFPET samples that are linked to clinical outcomes to generate hypotheses that could lead to classifiers for clinical applications. METHODS: We developed a two-color microarray-based profiling platform by optimizing target amplification, experimental design, quality control, and microarray content and applied it to the profiling of FFPET samples. We profiled a set of 50 fresh frozen (FF) breast cancer samples and assigned class labels according to the signature and method by van 't Veer et al [1] and then profiled 50 matched FFPET samples to test how well the FFPET data predicted the class labels. We also compared the sorting power of classifiers derived from FFPET sample data with classifiers derived from data from matched FF samples. RESULTS: When a classifier developed with matched FF samples was applied to FFPET data to assign samples to either "good" or "poor" outcome class labels, the classifier was able to assign the FFPET samples to the correct class label with an average error rate = 12% to 16%, respectively, with an Odds Ratio = 36.4 to 60.4, respectively. A classifier derived from FFPET data was able to predict the class label in FFPET samples (leave-one-out cross validation) with an error rate of ~14% (p-value = 3.7 × 10(-7)). When applied to the matched FF samples, the FFPET-derived classifier was able to assign FF samples to the correct class labels with 96% accuracy. The single misclassification was attributed to poor sample quality, as measured by qPCR on total RNA, which emphasizes the need for sample quality control before profiling. CONCLUSION: We have optimized a platform for expression analyses and have shown that our profiling platform is able to accurately sort FFPET samples into class labels derived from FF classifiers. Furthermore, using this platform, a classifier derived from FFPET samples can reliably provide the same sorting power as a classifier derived from matched FF samples. We anticipate that these techniques could be used to generate hypotheses from archives of FFPET samples, and thus may lead to prognostic and predictive classifiers that could be used, for example, to segregate patients for clinical trial enrollment or to guide patient treatment. BioMed Central 2009-07-28 /pmc/articles/PMC2732596/ /pubmed/19638234 http://dx.doi.org/10.1186/1479-5876-7-65 Text en Copyright © 2009 Duenwald et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Methodology
Duenwald, Sven
Zhou, Mingjie
Wang, Yanqun
Lejnine, Serguei
Kulkarni, Amit
Graves, Jaime
Smith, Ryan
Castle, John
Tokiwa, George
Fine, Bernard
Dai, Hongyue
Fare, Thomas
Marton, Matthew
Development of a microarray platform for FFPET profiling: application to the classification of human tumors
title Development of a microarray platform for FFPET profiling: application to the classification of human tumors
title_full Development of a microarray platform for FFPET profiling: application to the classification of human tumors
title_fullStr Development of a microarray platform for FFPET profiling: application to the classification of human tumors
title_full_unstemmed Development of a microarray platform for FFPET profiling: application to the classification of human tumors
title_short Development of a microarray platform for FFPET profiling: application to the classification of human tumors
title_sort development of a microarray platform for ffpet profiling: application to the classification of human tumors
topic Methodology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2732596/
https://www.ncbi.nlm.nih.gov/pubmed/19638234
http://dx.doi.org/10.1186/1479-5876-7-65
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