Prostate cancer cell phenotypes based on AGR2 and CD10 expression

The combination of expression patterns of AGR2 and CD10 by prostate cancer provided four phenotypes that correlated with clinical outcome. Based on immunophenotyping, CD10(low)AGR2(high), CD10(high)AGR2(high), CD10(low)AGR2(low), and CD10(high)AGR2(low) were distinguished. AGR2(+) tumors were associ...

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Autores principales: Ho, Melissa E., Quek, Sue-Ing, True, Lawrence D., Morrissey, Colm, Corey, Eva, Vessella, Robert L., Dumpit, Ruth, Nelson, Peter S., Maresh, Erin L., Mah, Vei, Alavi, Mohammed, Kim, Sara R., Bagryanova, Lora, Horvath, Steve, Chia, David, Goodglick, Lee, Liu, Alvin Y.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2013
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3638070/
https://www.ncbi.nlm.nih.gov/pubmed/23348903
http://dx.doi.org/10.1038/modpathol.2012.238
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author Ho, Melissa E.
Quek, Sue-Ing
True, Lawrence D.
Morrissey, Colm
Corey, Eva
Vessella, Robert L.
Dumpit, Ruth
Nelson, Peter S.
Maresh, Erin L.
Mah, Vei
Alavi, Mohammed
Kim, Sara R.
Bagryanova, Lora
Horvath, Steve
Chia, David
Goodglick, Lee
Liu, Alvin Y.
author_facet Ho, Melissa E.
Quek, Sue-Ing
True, Lawrence D.
Morrissey, Colm
Corey, Eva
Vessella, Robert L.
Dumpit, Ruth
Nelson, Peter S.
Maresh, Erin L.
Mah, Vei
Alavi, Mohammed
Kim, Sara R.
Bagryanova, Lora
Horvath, Steve
Chia, David
Goodglick, Lee
Liu, Alvin Y.
author_sort Ho, Melissa E.
collection PubMed
description The combination of expression patterns of AGR2 and CD10 by prostate cancer provided four phenotypes that correlated with clinical outcome. Based on immunophenotyping, CD10(low)AGR2(high), CD10(high)AGR2(high), CD10(low)AGR2(low), and CD10(high)AGR2(low) were distinguished. AGR2(+) tumors were associated with longer recurrence-free survival and CD10(+) tumors with shorter recurrence-free survival. In high-stage cases, the CD10(low)AGR2(high) phenotype was associated with a 9-fold higher recurrence-free survival than the CD10(high)AGR2(low) phenotype. The CD10(high)AGR2(high) and CD10(low)AGR2(low) phenotypes were intermediate. The CD10(high)AGR2(low) phenotype was most frequent in high-grade primary tumors. Conversely, bone and other soft tissue metastases, and derivative xenografts, expressed more AGR2 and less CD10. AGR2 protein was readily detected in tumor metastases. The CD10(high)AGR2(low) phenotype in primary tumors is predictive of poor outcome; however, the CD10(low)AGR2(high) phenotype is more common in metastases. It appears that AGR2 has a protective function in primary tumors but may have a role in the distal spread of tumor cells.
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spelling pubmed-36380702013-12-01 Prostate cancer cell phenotypes based on AGR2 and CD10 expression Ho, Melissa E. Quek, Sue-Ing True, Lawrence D. Morrissey, Colm Corey, Eva Vessella, Robert L. Dumpit, Ruth Nelson, Peter S. Maresh, Erin L. Mah, Vei Alavi, Mohammed Kim, Sara R. Bagryanova, Lora Horvath, Steve Chia, David Goodglick, Lee Liu, Alvin Y. Mod Pathol Article The combination of expression patterns of AGR2 and CD10 by prostate cancer provided four phenotypes that correlated with clinical outcome. Based on immunophenotyping, CD10(low)AGR2(high), CD10(high)AGR2(high), CD10(low)AGR2(low), and CD10(high)AGR2(low) were distinguished. AGR2(+) tumors were associated with longer recurrence-free survival and CD10(+) tumors with shorter recurrence-free survival. In high-stage cases, the CD10(low)AGR2(high) phenotype was associated with a 9-fold higher recurrence-free survival than the CD10(high)AGR2(low) phenotype. The CD10(high)AGR2(high) and CD10(low)AGR2(low) phenotypes were intermediate. The CD10(high)AGR2(low) phenotype was most frequent in high-grade primary tumors. Conversely, bone and other soft tissue metastases, and derivative xenografts, expressed more AGR2 and less CD10. AGR2 protein was readily detected in tumor metastases. The CD10(high)AGR2(low) phenotype in primary tumors is predictive of poor outcome; however, the CD10(low)AGR2(high) phenotype is more common in metastases. It appears that AGR2 has a protective function in primary tumors but may have a role in the distal spread of tumor cells. 2013-01-25 2013-06 /pmc/articles/PMC3638070/ /pubmed/23348903 http://dx.doi.org/10.1038/modpathol.2012.238 Text en http://www.nature.com/authors/editorial_policies/license.html#terms 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
Ho, Melissa E.
Quek, Sue-Ing
True, Lawrence D.
Morrissey, Colm
Corey, Eva
Vessella, Robert L.
Dumpit, Ruth
Nelson, Peter S.
Maresh, Erin L.
Mah, Vei
Alavi, Mohammed
Kim, Sara R.
Bagryanova, Lora
Horvath, Steve
Chia, David
Goodglick, Lee
Liu, Alvin Y.
Prostate cancer cell phenotypes based on AGR2 and CD10 expression
title Prostate cancer cell phenotypes based on AGR2 and CD10 expression
title_full Prostate cancer cell phenotypes based on AGR2 and CD10 expression
title_fullStr Prostate cancer cell phenotypes based on AGR2 and CD10 expression
title_full_unstemmed Prostate cancer cell phenotypes based on AGR2 and CD10 expression
title_short Prostate cancer cell phenotypes based on AGR2 and CD10 expression
title_sort prostate cancer cell phenotypes based on agr2 and cd10 expression
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3638070/
https://www.ncbi.nlm.nih.gov/pubmed/23348903
http://dx.doi.org/10.1038/modpathol.2012.238
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