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Characterization and multipotentiality of human fetal femur-derived cells: implications for skeletal tissue regeneration

Characterization and multipotentiality of human fetal femur-derived cells: implications for skeletal tissue regeneration
Characterization and multipotentiality of human fetal femur-derived cells: implications for skeletal tissue regeneration
To date, the plasticity, multipotentiality and characteristics of progenitor cells from fetal skeletal tissue remain poorly defined. This study has examined cell populations from human fetal femurs in comparison to adultderived mesenchymal cell populations. Real-time quantitative polymerase chain reaction demonstrated expression of mesenchymal progenitor cell markers by fetal-derived cells in comparison to unselected adult-derived and immunoselected STRO-1 enriched adult populations. Multipotentiality was examined using cells derived from femurs and single-cell clones, cultureexpanded from explants, and maintained in basal medium prior to exposure to adipogenic, osteogenic and chondrogenic conditions. Adipocyte formation was confirmed by Oil Red O lipid staining and aP2 immunocytochemistry, with expression of peroxisome proliferation-activated receptor-Y detected only in adipogenic conditions. In chondrogenic pellets, chondrocytes lodged within lacunae and embedded within dense proteoglycan matrix were observed using Alcian blue/Sirius red staining and type II collagen immunocytochemistry. Osteogenic differentiation was confirmed by alkaline phosphatase staining and type I collagen immunocytochemistry as well as gene expression of osteopontin and osteocalcin. Single cell clonal analysis was used to demonstrate multipotentiality of the fetal-derived populations with the formation of adipogenic, chondrogenic and osteogenic populations. Mineralization and osteoid formation was observed following culture on biomimetic scaffolds with extensive matrix accumulation both in vitro and in vivo after subcutaneous implantation in severely compromised immunodeficient mice. These studies demonstrate the proliferative and multipotential properties of fetal femur-derived cells in comparison to adult-derived cells. Selective differentiation and immunophenotyping will determine the potential of these fetal cells as a unique alternative model and cell source in the restoration of damaged tissue.
fetal, mesenchymal stem cell, osteoprogenitor, differentiation, tissue regeneration, immunophenotyping, female, fetus, polymerase chain reaction, stem cell transplantation, health, osteocalcin, cell survival, cells, human, transplantation, heterologous, base sequence, nude, cytology
1066-5099
1042-1053
Mirmalek-Sani, Sayed-Hadi
af9188b9-3124-40c0-8cd4-203a0fb490f9
Tare, Rahul S.
587c9db4-e409-4e7c-a02a-677547ab724a
Morgan, Suzanne M.
e8af487a-f03a-43a5-a0f4-7093b508434b
Roach, Helmtrud I.
ca2ff1f4-1ada-4c56-9097-cd27ca4d199e
Wilson, David I.
1500fca1-7082-4271-95f4-691f1d1252a2
Hanley, Neil A.
bf03f7bb-f377-44fb-8344-0bb1ca8b2ef9
Oreffo, Richard O.C.
ff9fff72-6855-4d0f-bfb2-311d0e8f3778
Mirmalek-Sani, Sayed-Hadi
af9188b9-3124-40c0-8cd4-203a0fb490f9
Tare, Rahul S.
587c9db4-e409-4e7c-a02a-677547ab724a
Morgan, Suzanne M.
e8af487a-f03a-43a5-a0f4-7093b508434b
Roach, Helmtrud I.
ca2ff1f4-1ada-4c56-9097-cd27ca4d199e
Wilson, David I.
1500fca1-7082-4271-95f4-691f1d1252a2
Hanley, Neil A.
bf03f7bb-f377-44fb-8344-0bb1ca8b2ef9
Oreffo, Richard O.C.
ff9fff72-6855-4d0f-bfb2-311d0e8f3778

Mirmalek-Sani, Sayed-Hadi, Tare, Rahul S., Morgan, Suzanne M., Roach, Helmtrud I., Wilson, David I., Hanley, Neil A. and Oreffo, Richard O.C. (2005) Characterization and multipotentiality of human fetal femur-derived cells: implications for skeletal tissue regeneration. Stem Cells, 24 (4), 1042-1053. (doi:10.1634/stemcells.2005-0368).

Record type: Article

Abstract

To date, the plasticity, multipotentiality and characteristics of progenitor cells from fetal skeletal tissue remain poorly defined. This study has examined cell populations from human fetal femurs in comparison to adultderived mesenchymal cell populations. Real-time quantitative polymerase chain reaction demonstrated expression of mesenchymal progenitor cell markers by fetal-derived cells in comparison to unselected adult-derived and immunoselected STRO-1 enriched adult populations. Multipotentiality was examined using cells derived from femurs and single-cell clones, cultureexpanded from explants, and maintained in basal medium prior to exposure to adipogenic, osteogenic and chondrogenic conditions. Adipocyte formation was confirmed by Oil Red O lipid staining and aP2 immunocytochemistry, with expression of peroxisome proliferation-activated receptor-Y detected only in adipogenic conditions. In chondrogenic pellets, chondrocytes lodged within lacunae and embedded within dense proteoglycan matrix were observed using Alcian blue/Sirius red staining and type II collagen immunocytochemistry. Osteogenic differentiation was confirmed by alkaline phosphatase staining and type I collagen immunocytochemistry as well as gene expression of osteopontin and osteocalcin. Single cell clonal analysis was used to demonstrate multipotentiality of the fetal-derived populations with the formation of adipogenic, chondrogenic and osteogenic populations. Mineralization and osteoid formation was observed following culture on biomimetic scaffolds with extensive matrix accumulation both in vitro and in vivo after subcutaneous implantation in severely compromised immunodeficient mice. These studies demonstrate the proliferative and multipotential properties of fetal femur-derived cells in comparison to adult-derived cells. Selective differentiation and immunophenotyping will determine the potential of these fetal cells as a unique alternative model and cell source in the restoration of damaged tissue.

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More information

Published date: April 2005
Additional Information: Tissue-specific stem cells
Keywords: fetal, mesenchymal stem cell, osteoprogenitor, differentiation, tissue regeneration, immunophenotyping, female, fetus, polymerase chain reaction, stem cell transplantation, health, osteocalcin, cell survival, cells, human, transplantation, heterologous, base sequence, nude, cytology

Identifiers

Local EPrints ID: 25820
URI: http://eprints.soton.ac.uk/id/eprint/25820
ISSN: 1066-5099
PURE UUID: 7869e54e-af5b-45f6-aa2e-58a01e485a96
ORCID for Rahul S. Tare: ORCID iD orcid.org/0000-0001-8274-8837
ORCID for Richard O.C. Oreffo: ORCID iD orcid.org/0000-0001-5995-6726

Catalogue record

Date deposited: 12 Apr 2006
Last modified: 16 Mar 2024 03:39

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Contributors

Author: Sayed-Hadi Mirmalek-Sani
Author: Rahul S. Tare ORCID iD
Author: Suzanne M. Morgan
Author: Helmtrud I. Roach
Author: David I. Wilson
Author: Neil A. Hanley

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