Clonal Evaluation of Prostate Cancer Foci in Biopsies with Discontinuous Tumor Involvement by Dual ERG/SPINK1 Immunohistochemistry

The presence of two or more prostate cancer foci separated by intervening benign tissue in a single core is a well-recognized finding on prostate biopsy. Cancer involvement can be measured by including intervening benign tissue or only including the actual cancer involved area. Importantly, this par...

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Autores principales: Fontugne, Jacqueline, Davis, Kristina, Palanisamy, Nallasivam, Udager, Aaron, Mehra, Rohit, McDaniel, Andrew S., Siddiqui, Javed, Rubin, Mark A., Mosquera, Juan Miguel, Tomlins, Scott A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2016
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4732921/
https://www.ncbi.nlm.nih.gov/pubmed/26743468
http://dx.doi.org/10.1038/modpathol.2015.148
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author Fontugne, Jacqueline
Davis, Kristina
Palanisamy, Nallasivam
Udager, Aaron
Mehra, Rohit
McDaniel, Andrew S.
Siddiqui, Javed
Rubin, Mark A.
Mosquera, Juan Miguel
Tomlins, Scott A.
author_facet Fontugne, Jacqueline
Davis, Kristina
Palanisamy, Nallasivam
Udager, Aaron
Mehra, Rohit
McDaniel, Andrew S.
Siddiqui, Javed
Rubin, Mark A.
Mosquera, Juan Miguel
Tomlins, Scott A.
author_sort Fontugne, Jacqueline
collection PubMed
description The presence of two or more prostate cancer foci separated by intervening benign tissue in a single core is a well-recognized finding on prostate biopsy. Cancer involvement can be measured by including intervening benign tissue or only including the actual cancer involved area. Importantly, this parameter is a common enrollment criterion for active surveillance protocols. We hypothesized that spatially distinct prostate cancer foci in biopsies may arise from separate clones, impacting cancer involvement assessment. Hence, we used dual ERG/SPINK1 immunohistochemistry to determine the frequency of separate clones—when separate tumor foci showed discordant ERG and/or SPINK1 status—in discontinuously involved prostate biopsy cores from two academic institutions. In our cohort of 97 prostate biopsy cores with spatially discrete tumor foci (from 80 patients), discontinuous cancer involvement including intervening tissue ranged from 20 to 100% and Gleason scores ranged from 6 to 9. Twenty four (25%) of 97 discontinuously involved cores harbored clonally distinct cancer foci by discordant ERG and/or SPINK1 expression status: 58% (14/24) had one ERG(+) focus, and one ERG(−)/SPINK1(−) focus; 29% (7/24) had one SPINK1(+) focus and one ERG(−)/SPINK1(−) focus; and 13% (3/24) had one ERG(+) focus and one SPINK1(+) focus. ERG and SPINK1 overexpression were mutually exclusive in all tumor foci. In summary, our results demonstrate that ~25% of discontinuously involved prostate biopsy cores showed tumor foci with discordant ERG/SPINK1 status, consistent with multiclonal disease. The relatively frequent presence of multiclonality in discontinuously involved prostate biopsy cores warrants studies on the potential clinical impact of clonality assessment, particularly in cases where tumor volume in a discontinuous core may impact active surveillance eligibility.
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spelling pubmed-47329212016-07-08 Clonal Evaluation of Prostate Cancer Foci in Biopsies with Discontinuous Tumor Involvement by Dual ERG/SPINK1 Immunohistochemistry Fontugne, Jacqueline Davis, Kristina Palanisamy, Nallasivam Udager, Aaron Mehra, Rohit McDaniel, Andrew S. Siddiqui, Javed Rubin, Mark A. Mosquera, Juan Miguel Tomlins, Scott A. Mod Pathol Article The presence of two or more prostate cancer foci separated by intervening benign tissue in a single core is a well-recognized finding on prostate biopsy. Cancer involvement can be measured by including intervening benign tissue or only including the actual cancer involved area. Importantly, this parameter is a common enrollment criterion for active surveillance protocols. We hypothesized that spatially distinct prostate cancer foci in biopsies may arise from separate clones, impacting cancer involvement assessment. Hence, we used dual ERG/SPINK1 immunohistochemistry to determine the frequency of separate clones—when separate tumor foci showed discordant ERG and/or SPINK1 status—in discontinuously involved prostate biopsy cores from two academic institutions. In our cohort of 97 prostate biopsy cores with spatially discrete tumor foci (from 80 patients), discontinuous cancer involvement including intervening tissue ranged from 20 to 100% and Gleason scores ranged from 6 to 9. Twenty four (25%) of 97 discontinuously involved cores harbored clonally distinct cancer foci by discordant ERG and/or SPINK1 expression status: 58% (14/24) had one ERG(+) focus, and one ERG(−)/SPINK1(−) focus; 29% (7/24) had one SPINK1(+) focus and one ERG(−)/SPINK1(−) focus; and 13% (3/24) had one ERG(+) focus and one SPINK1(+) focus. ERG and SPINK1 overexpression were mutually exclusive in all tumor foci. In summary, our results demonstrate that ~25% of discontinuously involved prostate biopsy cores showed tumor foci with discordant ERG/SPINK1 status, consistent with multiclonal disease. The relatively frequent presence of multiclonality in discontinuously involved prostate biopsy cores warrants studies on the potential clinical impact of clonality assessment, particularly in cases where tumor volume in a discontinuous core may impact active surveillance eligibility. 2016-01-08 2016-02 /pmc/articles/PMC4732921/ /pubmed/26743468 http://dx.doi.org/10.1038/modpathol.2015.148 Text en Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Fontugne, Jacqueline
Davis, Kristina
Palanisamy, Nallasivam
Udager, Aaron
Mehra, Rohit
McDaniel, Andrew S.
Siddiqui, Javed
Rubin, Mark A.
Mosquera, Juan Miguel
Tomlins, Scott A.
Clonal Evaluation of Prostate Cancer Foci in Biopsies with Discontinuous Tumor Involvement by Dual ERG/SPINK1 Immunohistochemistry
title Clonal Evaluation of Prostate Cancer Foci in Biopsies with Discontinuous Tumor Involvement by Dual ERG/SPINK1 Immunohistochemistry
title_full Clonal Evaluation of Prostate Cancer Foci in Biopsies with Discontinuous Tumor Involvement by Dual ERG/SPINK1 Immunohistochemistry
title_fullStr Clonal Evaluation of Prostate Cancer Foci in Biopsies with Discontinuous Tumor Involvement by Dual ERG/SPINK1 Immunohistochemistry
title_full_unstemmed Clonal Evaluation of Prostate Cancer Foci in Biopsies with Discontinuous Tumor Involvement by Dual ERG/SPINK1 Immunohistochemistry
title_short Clonal Evaluation of Prostate Cancer Foci in Biopsies with Discontinuous Tumor Involvement by Dual ERG/SPINK1 Immunohistochemistry
title_sort clonal evaluation of prostate cancer foci in biopsies with discontinuous tumor involvement by dual erg/spink1 immunohistochemistry
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4732921/
https://www.ncbi.nlm.nih.gov/pubmed/26743468
http://dx.doi.org/10.1038/modpathol.2015.148
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