Expression of Stem Cell Markers in the Human Fetal Kidney

In the human fetal kidney (HFK) self-renewing stem cells residing in the metanephric mesenchyme (MM)/blastema are induced to form all cell types of the nephron till 34(th) week of gestation. Definition of useful markers is crucial for the identification of HFK stem cells. Because wilms' tumor,...

Descripción completa

Detalles Bibliográficos
Autores principales: Metsuyanim, Sally, Harari-Steinberg, Orit, Buzhor, Ella, Omer, Dorit, Pode-Shakked, Naomi, Ben-Hur, Herzl, Halperin, Reuvit, Schneider, David, Dekel, Benjamin
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2009
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2725321/
https://www.ncbi.nlm.nih.gov/pubmed/19696931
http://dx.doi.org/10.1371/journal.pone.0006709
_version_ 1782170509740343296
author Metsuyanim, Sally
Harari-Steinberg, Orit
Buzhor, Ella
Omer, Dorit
Pode-Shakked, Naomi
Ben-Hur, Herzl
Halperin, Reuvit
Schneider, David
Dekel, Benjamin
author_facet Metsuyanim, Sally
Harari-Steinberg, Orit
Buzhor, Ella
Omer, Dorit
Pode-Shakked, Naomi
Ben-Hur, Herzl
Halperin, Reuvit
Schneider, David
Dekel, Benjamin
author_sort Metsuyanim, Sally
collection PubMed
description In the human fetal kidney (HFK) self-renewing stem cells residing in the metanephric mesenchyme (MM)/blastema are induced to form all cell types of the nephron till 34(th) week of gestation. Definition of useful markers is crucial for the identification of HFK stem cells. Because wilms' tumor, a pediatric renal cancer, initiates from retention of renal stem cells, we hypothesized that surface antigens previously up-regulated in microarrays of both HFK and blastema-enriched stem-like wilms' tumor xenografts (NCAM, ACVRIIB, DLK1/PREF, GPR39, FZD7, FZD2, NTRK2) are likely to be relevant markers. Comprehensive profiling of these putative and of additional stem cell markers (CD34, CD133, c-Kit, CD90, CD105, CD24) in mid-gestation HFK was performed using immunostaining and FACS in conjunction with EpCAM, an epithelial surface marker that is absent from the MM and increases along nephron differentiation and hence can be separated into negative, dim or bright fractions. No marker was specifically localized to the MM. Nevertheless, FZD7 and NTRK2 were preferentially localized to the MM and emerging tubules (<10% of HFK cells) and were mostly present within the EpCAM(neg) and EpCAM(dim) fractions, indicating putative stem/progenitor markers. In contrast, single markers such as CD24 and CD133 as well as double-positive CD24(+)CD133(+) cells comprise >50% of HFK cells and predominantly co-express EpCAM(bright), indicating they are mostly markers of differentiation. Furthermore, localization of NCAM exclusively in the MM and in its nephron progenitor derivatives but also in stroma and the expression pattern of significantly elevated renal stem/progenitor genes Six2, Wt1, Cited1, and Sall1 in NCAM(+)EpCAM(-) and to a lesser extent in NCAM(+)EpCAM(+) fractions confirmed regional identity of cells and assisted us in pinpointing the presence of subpopulations that are putative MM-derived progenitor cells (NCAM(+)EpCAM(+)FZD7(+)), MM stem cells (NCAM(+)EpCAM(-)FZD7(+)) or both (NCAM(+)FZD7(+)). These results and concepts provide a framework for developing cell selection strategies for human renal cell-based therapies.
format Text
id pubmed-2725321
institution National Center for Biotechnology Information
language English
publishDate 2009
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-27253212009-08-21 Expression of Stem Cell Markers in the Human Fetal Kidney Metsuyanim, Sally Harari-Steinberg, Orit Buzhor, Ella Omer, Dorit Pode-Shakked, Naomi Ben-Hur, Herzl Halperin, Reuvit Schneider, David Dekel, Benjamin PLoS One Research Article In the human fetal kidney (HFK) self-renewing stem cells residing in the metanephric mesenchyme (MM)/blastema are induced to form all cell types of the nephron till 34(th) week of gestation. Definition of useful markers is crucial for the identification of HFK stem cells. Because wilms' tumor, a pediatric renal cancer, initiates from retention of renal stem cells, we hypothesized that surface antigens previously up-regulated in microarrays of both HFK and blastema-enriched stem-like wilms' tumor xenografts (NCAM, ACVRIIB, DLK1/PREF, GPR39, FZD7, FZD2, NTRK2) are likely to be relevant markers. Comprehensive profiling of these putative and of additional stem cell markers (CD34, CD133, c-Kit, CD90, CD105, CD24) in mid-gestation HFK was performed using immunostaining and FACS in conjunction with EpCAM, an epithelial surface marker that is absent from the MM and increases along nephron differentiation and hence can be separated into negative, dim or bright fractions. No marker was specifically localized to the MM. Nevertheless, FZD7 and NTRK2 were preferentially localized to the MM and emerging tubules (<10% of HFK cells) and were mostly present within the EpCAM(neg) and EpCAM(dim) fractions, indicating putative stem/progenitor markers. In contrast, single markers such as CD24 and CD133 as well as double-positive CD24(+)CD133(+) cells comprise >50% of HFK cells and predominantly co-express EpCAM(bright), indicating they are mostly markers of differentiation. Furthermore, localization of NCAM exclusively in the MM and in its nephron progenitor derivatives but also in stroma and the expression pattern of significantly elevated renal stem/progenitor genes Six2, Wt1, Cited1, and Sall1 in NCAM(+)EpCAM(-) and to a lesser extent in NCAM(+)EpCAM(+) fractions confirmed regional identity of cells and assisted us in pinpointing the presence of subpopulations that are putative MM-derived progenitor cells (NCAM(+)EpCAM(+)FZD7(+)), MM stem cells (NCAM(+)EpCAM(-)FZD7(+)) or both (NCAM(+)FZD7(+)). These results and concepts provide a framework for developing cell selection strategies for human renal cell-based therapies. Public Library of Science 2009-08-21 /pmc/articles/PMC2725321/ /pubmed/19696931 http://dx.doi.org/10.1371/journal.pone.0006709 Text en Metsuyanim 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
Metsuyanim, Sally
Harari-Steinberg, Orit
Buzhor, Ella
Omer, Dorit
Pode-Shakked, Naomi
Ben-Hur, Herzl
Halperin, Reuvit
Schneider, David
Dekel, Benjamin
Expression of Stem Cell Markers in the Human Fetal Kidney
title Expression of Stem Cell Markers in the Human Fetal Kidney
title_full Expression of Stem Cell Markers in the Human Fetal Kidney
title_fullStr Expression of Stem Cell Markers in the Human Fetal Kidney
title_full_unstemmed Expression of Stem Cell Markers in the Human Fetal Kidney
title_short Expression of Stem Cell Markers in the Human Fetal Kidney
title_sort expression of stem cell markers in the human fetal kidney
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2725321/
https://www.ncbi.nlm.nih.gov/pubmed/19696931
http://dx.doi.org/10.1371/journal.pone.0006709
work_keys_str_mv AT metsuyanimsally expressionofstemcellmarkersinthehumanfetalkidney
AT hararisteinbergorit expressionofstemcellmarkersinthehumanfetalkidney
AT buzhorella expressionofstemcellmarkersinthehumanfetalkidney
AT omerdorit expressionofstemcellmarkersinthehumanfetalkidney
AT podeshakkednaomi expressionofstemcellmarkersinthehumanfetalkidney
AT benhurherzl expressionofstemcellmarkersinthehumanfetalkidney
AT halperinreuvit expressionofstemcellmarkersinthehumanfetalkidney
AT schneiderdavid expressionofstemcellmarkersinthehumanfetalkidney
AT dekelbenjamin expressionofstemcellmarkersinthehumanfetalkidney

Ejemplares similares