The osteogenic growth peptide (OGP) was characterized recently in regenerating bone marrow (BM) and normal serum. In vitro, the OGP regulates stromal-cell proliferation and differentiated functions. In vivo, an increase in serum OGP accompanies the osteogenic phase of postablation BM regeneration. The present results in normal mice show that OGP induces a balanced increase in WBC counts and overall BM cellularity. In mice receiving myeloablative irradiation and syngeneic or semiallogeneic BM transplants, OGP stimulates hematopoietic reconstruction and doubles the survival rate; these effects are dependent on initiating the OGP administration before irradiation. Chimerism measurements in semiallogeneic graft recipients suggest no preferential effect of OGP on residual host cells. The data implicate OGP in the acceleration of hematopoiesis secondary to expansion of the stromal microenvironment and/or enhancement of stroma-derived signals to stem cells. The low-dose effectiveness of OGP is explained by the demonstration of an autocrine positive feedback loop that together with the OGP-binding protein sustains high serum levels of the peptide. A potential OGP-based treatment in combination with chemoradiotherapy is attractive because of the OGP-induced balanced multi-lineage enhancement of hematopoiesis and possible replacement of expensive recombinant cytokines by a readily synthesized peptide.
ARTICLES|
December 15, 1996
Osteogenic growth peptide increases blood and bone marrow cellularity and enhances engraftment of bone marrow transplants in mice
O Gurevitch,
O Gurevitch
Department of Bone Marrow Transplantation and Cancer/Immunobiology Research Laboratory, Hadassah-Hebrew University Hospital, Jerusalem, Israel.
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S Slavin,
S Slavin
Department of Bone Marrow Transplantation and Cancer/Immunobiology Research Laboratory, Hadassah-Hebrew University Hospital, Jerusalem, Israel.
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A Muhlrad,
A Muhlrad
Department of Bone Marrow Transplantation and Cancer/Immunobiology Research Laboratory, Hadassah-Hebrew University Hospital, Jerusalem, Israel.
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A Shteyer,
A Shteyer
Department of Bone Marrow Transplantation and Cancer/Immunobiology Research Laboratory, Hadassah-Hebrew University Hospital, Jerusalem, Israel.
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D Gazit,
D Gazit
Department of Bone Marrow Transplantation and Cancer/Immunobiology Research Laboratory, Hadassah-Hebrew University Hospital, Jerusalem, Israel.
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M Chorev,
M Chorev
Department of Bone Marrow Transplantation and Cancer/Immunobiology Research Laboratory, Hadassah-Hebrew University Hospital, Jerusalem, Israel.
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M Vidson,
M Vidson
Department of Bone Marrow Transplantation and Cancer/Immunobiology Research Laboratory, Hadassah-Hebrew University Hospital, Jerusalem, Israel.
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M Namdar-Attar,
M Namdar-Attar
Department of Bone Marrow Transplantation and Cancer/Immunobiology Research Laboratory, Hadassah-Hebrew University Hospital, Jerusalem, Israel.
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E Berger,
E Berger
Department of Bone Marrow Transplantation and Cancer/Immunobiology Research Laboratory, Hadassah-Hebrew University Hospital, Jerusalem, Israel.
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I Bleiberg,
I Bleiberg
Department of Bone Marrow Transplantation and Cancer/Immunobiology Research Laboratory, Hadassah-Hebrew University Hospital, Jerusalem, Israel.
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I Bab
I Bab
Department of Bone Marrow Transplantation and Cancer/Immunobiology Research Laboratory, Hadassah-Hebrew University Hospital, Jerusalem, Israel.
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Blood (1996) 88 (12): 4719–4724.
Citation
O Gurevitch, S Slavin, A Muhlrad, A Shteyer, D Gazit, M Chorev, M Vidson, M Namdar-Attar, E Berger, I Bleiberg, I Bab; Osteogenic growth peptide increases blood and bone marrow cellularity and enhances engraftment of bone marrow transplants in mice. Blood 1996; 88 (12): 4719–4724. doi: https://doi.org/10.1182/blood.V88.12.4719.bloodjournal88124719
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