Heterogeneity in SDF-1 expression defines the vasculogenic potential of adult cardiac progenitor cells.
The adult myocardium has been reported to harbor several classes of multipotent progenitor cells (CPCs) with tri-lineage differentiation potential. It is not clear whether c-kit+CPCs represent a uniform precursor population or a more complex mixture of cell types.To characterize and understand vascu...
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doaj-2196d7fc9eaf464391d57f0a6315b77d2020-11-25T02:31:04ZengPublic Library of Science (PLoS)PLoS ONE1932-62032011-01-0168e2401310.1371/journal.pone.0024013Heterogeneity in SDF-1 expression defines the vasculogenic potential of adult cardiac progenitor cells.Claudia O RodriguesLina A ShehadehMichael HoosienValerie OteroInes ChopraNicholas F TsinoremasNanette H BishopricThe adult myocardium has been reported to harbor several classes of multipotent progenitor cells (CPCs) with tri-lineage differentiation potential. It is not clear whether c-kit+CPCs represent a uniform precursor population or a more complex mixture of cell types.To characterize and understand vasculogenic heterogeneity within c-kit+presumptive cardiac progenitor cell populations.c-kit+, sca-1+ CPCs obtained from adult mouse left ventricle expressed stem cell-associated genes, including Oct-4 and Myc, and were self-renewing, pluripotent and clonogenic. Detailed single cell clonal analysis of 17 clones revealed that most (14/17) exhibited trilineage differentiation potential. However, striking morphological differences were observed among clones that were heritable and stable in long-term culture. 3 major groups were identified: round (7/17), flat or spindle-shaped (5/17) and stellate (5/17). Stellate morphology was predictive of vasculogenic differentiation in Matrigel. Genome-wide expression studies and bioinformatic analysis revealed clonally stable, heritable differences in stromal cell-derived factor-1 (SDF-1) expression that correlated strongly with stellate morphology and vasculogenic capacity. Endogenous SDF-1 production contributed directly to vasculogenic differentiation: both shRNA-mediated knockdown of SDF-1 and AMD3100, an antagonist of the SDF-1 receptor CXC chemokine Receptor-4 (CXCR4), reduced tube-forming capacity, while exogenous SDF-1 induced tube formation by 2 non-vasculogenic clones. CPCs producing SDF-1 were able to vascularize Matrigel dermal implants in vivo, while CPCs with low SDF-1 production were not.Clonogenic c-kit+, sca-1+ CPCs are heterogeneous in morphology, gene expression patterns and differentiation potential. Clone-specific levels of SDF-1 expression both predict and promote development of a vasculogenic phenotype via a previously unreported autocrine mechanism.http://europepmc.org/articles/PMC3161114?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Claudia O Rodrigues Lina A Shehadeh Michael Hoosien Valerie Otero Ines Chopra Nicholas F Tsinoremas Nanette H Bishopric |
spellingShingle |
Claudia O Rodrigues Lina A Shehadeh Michael Hoosien Valerie Otero Ines Chopra Nicholas F Tsinoremas Nanette H Bishopric Heterogeneity in SDF-1 expression defines the vasculogenic potential of adult cardiac progenitor cells. PLoS ONE |
author_facet |
Claudia O Rodrigues Lina A Shehadeh Michael Hoosien Valerie Otero Ines Chopra Nicholas F Tsinoremas Nanette H Bishopric |
author_sort |
Claudia O Rodrigues |
title |
Heterogeneity in SDF-1 expression defines the vasculogenic potential of adult cardiac progenitor cells. |
title_short |
Heterogeneity in SDF-1 expression defines the vasculogenic potential of adult cardiac progenitor cells. |
title_full |
Heterogeneity in SDF-1 expression defines the vasculogenic potential of adult cardiac progenitor cells. |
title_fullStr |
Heterogeneity in SDF-1 expression defines the vasculogenic potential of adult cardiac progenitor cells. |
title_full_unstemmed |
Heterogeneity in SDF-1 expression defines the vasculogenic potential of adult cardiac progenitor cells. |
title_sort |
heterogeneity in sdf-1 expression defines the vasculogenic potential of adult cardiac progenitor cells. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2011-01-01 |
description |
The adult myocardium has been reported to harbor several classes of multipotent progenitor cells (CPCs) with tri-lineage differentiation potential. It is not clear whether c-kit+CPCs represent a uniform precursor population or a more complex mixture of cell types.To characterize and understand vasculogenic heterogeneity within c-kit+presumptive cardiac progenitor cell populations.c-kit+, sca-1+ CPCs obtained from adult mouse left ventricle expressed stem cell-associated genes, including Oct-4 and Myc, and were self-renewing, pluripotent and clonogenic. Detailed single cell clonal analysis of 17 clones revealed that most (14/17) exhibited trilineage differentiation potential. However, striking morphological differences were observed among clones that were heritable and stable in long-term culture. 3 major groups were identified: round (7/17), flat or spindle-shaped (5/17) and stellate (5/17). Stellate morphology was predictive of vasculogenic differentiation in Matrigel. Genome-wide expression studies and bioinformatic analysis revealed clonally stable, heritable differences in stromal cell-derived factor-1 (SDF-1) expression that correlated strongly with stellate morphology and vasculogenic capacity. Endogenous SDF-1 production contributed directly to vasculogenic differentiation: both shRNA-mediated knockdown of SDF-1 and AMD3100, an antagonist of the SDF-1 receptor CXC chemokine Receptor-4 (CXCR4), reduced tube-forming capacity, while exogenous SDF-1 induced tube formation by 2 non-vasculogenic clones. CPCs producing SDF-1 were able to vascularize Matrigel dermal implants in vivo, while CPCs with low SDF-1 production were not.Clonogenic c-kit+, sca-1+ CPCs are heterogeneous in morphology, gene expression patterns and differentiation potential. Clone-specific levels of SDF-1 expression both predict and promote development of a vasculogenic phenotype via a previously unreported autocrine mechanism. |
url |
http://europepmc.org/articles/PMC3161114?pdf=render |
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