Highly enriched, bipotent, hematopoietic granulocyte macrophage colony-forming cells (GM-CFC) require cytokines for their survival, proliferation, and development. GM-CFC will form neutrophils in the presence of the cytokines stem cell factor and granulocyte colony-stimulating factor, whereas macrophage colony-stimulating factor leads to macrophage formation. Previously, we have shown that the commitment to the macrophage lineage is associated with lipid hydrolysis and translocation of protein kinase C α (PKCα) to the nucleus. Here we have transfected freshly prepared GM-CFC with a constitutively activated form of PKCα, namely PKAC, in which the regulatory domain has been truncated. Greater than 95% of the transfected cells showed over a twofold increase in PKCα expression with the protein being located primarily within the nucleus. The expression of PKAC caused macrophage development even in the presence of stimuli that normally promote only neutrophilic development. Thus, M-CSF–stimulated translocation of PKCα to the nucleus is a signal associated with macrophage development in primary mammalian hematopoietic progenitor cells, and this signal can be mimicked by ectopic PKAC, which is also expressed in the nucleus.
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23 March 1998
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March 23 1998
An Activated Protein Kinase C α Gives a Differentiation Signal for Hematopoietic Progenitor Cells and Mimicks Macrophage Colony-stimulating Factor–stimulated Signaling Events
Andrew Pierce,
Andrew Pierce
*Leukaemia Research Fund Cellular Development Unit, ‡Department of Biomolecular Sciences, University of Manchester Institute of Science and Technology, Manchester, M60 1QD, United Kingdom; §Cancer Research Campaign, Department of Experimental Hematology, Paterson Institute for Cancer Research, Christie Hospital National Health Service Trust, Manchester, M20 9BX, United Kingdom; and ‖Department of Immunology, University of Birmingham, Edgbaston, Birmingham, B15 2TT, United Kingdom
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Clare M. Heyworth,
Clare M. Heyworth
*Leukaemia Research Fund Cellular Development Unit, ‡Department of Biomolecular Sciences, University of Manchester Institute of Science and Technology, Manchester, M60 1QD, United Kingdom; §Cancer Research Campaign, Department of Experimental Hematology, Paterson Institute for Cancer Research, Christie Hospital National Health Service Trust, Manchester, M20 9BX, United Kingdom; and ‖Department of Immunology, University of Birmingham, Edgbaston, Birmingham, B15 2TT, United Kingdom
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Sian E. Nicholls,
Sian E. Nicholls
*Leukaemia Research Fund Cellular Development Unit, ‡Department of Biomolecular Sciences, University of Manchester Institute of Science and Technology, Manchester, M60 1QD, United Kingdom; §Cancer Research Campaign, Department of Experimental Hematology, Paterson Institute for Cancer Research, Christie Hospital National Health Service Trust, Manchester, M20 9BX, United Kingdom; and ‖Department of Immunology, University of Birmingham, Edgbaston, Birmingham, B15 2TT, United Kingdom
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Elaine Spooncer,
Elaine Spooncer
*Leukaemia Research Fund Cellular Development Unit, ‡Department of Biomolecular Sciences, University of Manchester Institute of Science and Technology, Manchester, M60 1QD, United Kingdom; §Cancer Research Campaign, Department of Experimental Hematology, Paterson Institute for Cancer Research, Christie Hospital National Health Service Trust, Manchester, M20 9BX, United Kingdom; and ‖Department of Immunology, University of Birmingham, Edgbaston, Birmingham, B15 2TT, United Kingdom
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T. Michael Dexter,
T. Michael Dexter
*Leukaemia Research Fund Cellular Development Unit, ‡Department of Biomolecular Sciences, University of Manchester Institute of Science and Technology, Manchester, M60 1QD, United Kingdom; §Cancer Research Campaign, Department of Experimental Hematology, Paterson Institute for Cancer Research, Christie Hospital National Health Service Trust, Manchester, M20 9BX, United Kingdom; and ‖Department of Immunology, University of Birmingham, Edgbaston, Birmingham, B15 2TT, United Kingdom
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Janet M. Lord,
Janet M. Lord
*Leukaemia Research Fund Cellular Development Unit, ‡Department of Biomolecular Sciences, University of Manchester Institute of Science and Technology, Manchester, M60 1QD, United Kingdom; §Cancer Research Campaign, Department of Experimental Hematology, Paterson Institute for Cancer Research, Christie Hospital National Health Service Trust, Manchester, M20 9BX, United Kingdom; and ‖Department of Immunology, University of Birmingham, Edgbaston, Birmingham, B15 2TT, United Kingdom
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P. Jane Owen-Lynch,
P. Jane Owen-Lynch
*Leukaemia Research Fund Cellular Development Unit, ‡Department of Biomolecular Sciences, University of Manchester Institute of Science and Technology, Manchester, M60 1QD, United Kingdom; §Cancer Research Campaign, Department of Experimental Hematology, Paterson Institute for Cancer Research, Christie Hospital National Health Service Trust, Manchester, M20 9BX, United Kingdom; and ‖Department of Immunology, University of Birmingham, Edgbaston, Birmingham, B15 2TT, United Kingdom
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Gwen Wark,
Gwen Wark
*Leukaemia Research Fund Cellular Development Unit, ‡Department of Biomolecular Sciences, University of Manchester Institute of Science and Technology, Manchester, M60 1QD, United Kingdom; §Cancer Research Campaign, Department of Experimental Hematology, Paterson Institute for Cancer Research, Christie Hospital National Health Service Trust, Manchester, M20 9BX, United Kingdom; and ‖Department of Immunology, University of Birmingham, Edgbaston, Birmingham, B15 2TT, United Kingdom
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Anthony D. Whetton
Anthony D. Whetton
*Leukaemia Research Fund Cellular Development Unit, ‡Department of Biomolecular Sciences, University of Manchester Institute of Science and Technology, Manchester, M60 1QD, United Kingdom; §Cancer Research Campaign, Department of Experimental Hematology, Paterson Institute for Cancer Research, Christie Hospital National Health Service Trust, Manchester, M20 9BX, United Kingdom; and ‖Department of Immunology, University of Birmingham, Edgbaston, Birmingham, B15 2TT, United Kingdom
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Andrew Pierce
,
Clare M. Heyworth
,
Sian E. Nicholls
,
Elaine Spooncer
,
T. Michael Dexter
,
Janet M. Lord
,
P. Jane Owen-Lynch
,
Gwen Wark
,
Anthony D. Whetton
*Leukaemia Research Fund Cellular Development Unit, ‡Department of Biomolecular Sciences, University of Manchester Institute of Science and Technology, Manchester, M60 1QD, United Kingdom; §Cancer Research Campaign, Department of Experimental Hematology, Paterson Institute for Cancer Research, Christie Hospital National Health Service Trust, Manchester, M20 9BX, United Kingdom; and ‖Department of Immunology, University of Birmingham, Edgbaston, Birmingham, B15 2TT, United Kingdom
Address all correspondence to Anthony D. Whetton, Leukaemia Research Fund Cellular Development Unit, UMIST, Sackville St., Manchester M60 1QD, United Kingdom. Tel.: 44 161 200 4184. Fax: 44 161 236 0409. E-mail: [email protected]
Received:
June 04 1997
Revision Received:
December 23 1997
Online ISSN: 1540-8140
Print ISSN: 0021-9525
1998
J Cell Biol (1998) 140 (6): 1511–1518.
Article history
Received:
June 04 1997
Revision Received:
December 23 1997
Citation
Andrew Pierce, Clare M. Heyworth, Sian E. Nicholls, Elaine Spooncer, T. Michael Dexter, Janet M. Lord, P. Jane Owen-Lynch, Gwen Wark, Anthony D. Whetton; An Activated Protein Kinase C α Gives a Differentiation Signal for Hematopoietic Progenitor Cells and Mimicks Macrophage Colony-stimulating Factor–stimulated Signaling Events . J Cell Biol 23 March 1998; 140 (6): 1511–1518. doi: https://doi.org/10.1083/jcb.140.6.1511
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