Effects of interferon alpha on human osteoprogenitor cell growth and differentiation in vitro
Effects of interferon alpha on human osteoprogenitor cell growth and differentiation in vitro
The specific effects of interferon alpha (IFNalpha), on the differentiation pathways of human osteogenic cells are not known. The aim of this study was to investigate possible effects of IFNalpha on osteogenic development by investigating cell differentiation, colony formation (colony forming unit-fibroblastic, CFU-F), cell proliferation, and gene expression, in particular bone morphogenetic protein (BMP) expression, of human bone marrow osteoprogenitor cells. Human bone marrow fibroblasts were cultured with or without the addition of IFNalpha (5-1,000 IU/ml) in the presence and absence of dexamethasone (10 nM) and ascorbate (100 microM), which are agents known to affect osteogenic differentiation. IFNalpha produced a significant dose-dependent inhibition of cell proliferation and alkaline phosphatase specific activity at concentrations as low as 50 IU/ml. IFNalpha (50-1,000 IU/ml) inhibited the stimulation of alkaline phosphatase specific activity induced by ascorbate and dexamethasone. Examination of CFU-F showed dose- and time-dependent inhibitions of colony formation and reductions in both colony size and alkaline phosphatase-positive CFU-F colonies particularly at earlier times. Reactivity with an antibody specific for osteoprogenitors (HOP-26), was reduced in IFNalpha-treated cultures. Northern blot analysis showed a significant dose-dependent up-regulation of BMP-2 mRNA, estrogen receptor alpha mRNA and osteocalcin mRNA expression in ascorbate/dexamethasone cultures. In contrast, IFNalpha significantly inhibited BMP-2 mRNA expression in the absence of ascorbate and dexamethasone. In conclusion, IFNalpha inhibits human osteoprogenitor cell proliferation, CFU- F formation, HOP-26 expression, and alkaline phosphatase specific activity and modulates BMP-2 gene expression. These results suggest a role for IFNalpha in local bone turnover through the specific and direct modulation of osteoprogenitor proliferation and differentiation.
372-385
Oreffo, R.O.
ff9fff72-6855-4d0f-bfb2-311d0e8f3778
Romberg, S.
e9887c6f-7c77-4e34-b051-d78b6b214ed8
Virdi, A.S.
71654d0a-5481-4ff8-86d8-1c3d9c0aafd7
Joyner, C.J.
394f90ea-2c90-476f-a1af-73a2fad4168b
Berven, S.
2ba952fe-d544-4987-bdaa-e21b71dae850
Triffitt, J.T.
06d3019a-06e6-4abd-9e73-f073d621e1f9
1 September 1999
Oreffo, R.O.
ff9fff72-6855-4d0f-bfb2-311d0e8f3778
Romberg, S.
e9887c6f-7c77-4e34-b051-d78b6b214ed8
Virdi, A.S.
71654d0a-5481-4ff8-86d8-1c3d9c0aafd7
Joyner, C.J.
394f90ea-2c90-476f-a1af-73a2fad4168b
Berven, S.
2ba952fe-d544-4987-bdaa-e21b71dae850
Triffitt, J.T.
06d3019a-06e6-4abd-9e73-f073d621e1f9
Oreffo, R.O., Romberg, S., Virdi, A.S., Joyner, C.J., Berven, S. and Triffitt, J.T.
(1999)
Effects of interferon alpha on human osteoprogenitor cell growth and differentiation in vitro.
Journal of Cellular Biochemistry, 74 (3), .
(doi:10.1002/(SICI)1097-4644(19990901)74:3<372::AID-JCB6>3.0.CO;2-H).
(PMID:10412039)
Abstract
The specific effects of interferon alpha (IFNalpha), on the differentiation pathways of human osteogenic cells are not known. The aim of this study was to investigate possible effects of IFNalpha on osteogenic development by investigating cell differentiation, colony formation (colony forming unit-fibroblastic, CFU-F), cell proliferation, and gene expression, in particular bone morphogenetic protein (BMP) expression, of human bone marrow osteoprogenitor cells. Human bone marrow fibroblasts were cultured with or without the addition of IFNalpha (5-1,000 IU/ml) in the presence and absence of dexamethasone (10 nM) and ascorbate (100 microM), which are agents known to affect osteogenic differentiation. IFNalpha produced a significant dose-dependent inhibition of cell proliferation and alkaline phosphatase specific activity at concentrations as low as 50 IU/ml. IFNalpha (50-1,000 IU/ml) inhibited the stimulation of alkaline phosphatase specific activity induced by ascorbate and dexamethasone. Examination of CFU-F showed dose- and time-dependent inhibitions of colony formation and reductions in both colony size and alkaline phosphatase-positive CFU-F colonies particularly at earlier times. Reactivity with an antibody specific for osteoprogenitors (HOP-26), was reduced in IFNalpha-treated cultures. Northern blot analysis showed a significant dose-dependent up-regulation of BMP-2 mRNA, estrogen receptor alpha mRNA and osteocalcin mRNA expression in ascorbate/dexamethasone cultures. In contrast, IFNalpha significantly inhibited BMP-2 mRNA expression in the absence of ascorbate and dexamethasone. In conclusion, IFNalpha inhibits human osteoprogenitor cell proliferation, CFU- F formation, HOP-26 expression, and alkaline phosphatase specific activity and modulates BMP-2 gene expression. These results suggest a role for IFNalpha in local bone turnover through the specific and direct modulation of osteoprogenitor proliferation and differentiation.
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e-pub ahead of print date: 19 July 1999
Published date: 1 September 1999
Organisations:
Human Development & Health
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Local EPrints ID: 360870
URI: http://eprints.soton.ac.uk/id/eprint/360870
ISSN: 0730-2312
PURE UUID: 73d71bb0-fd9a-4ba5-9520-f313302f4930
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Date deposited: 09 Jan 2014 11:36
Last modified: 15 Mar 2024 03:04
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Author:
S. Romberg
Author:
A.S. Virdi
Author:
C.J. Joyner
Author:
S. Berven
Author:
J.T. Triffitt
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