Mice lacking granulocyte colony-stimulating factor have chronic neutropenia, granulocyte and macrophage progenitor cell deficiency, and impaired neutrophil …

GJ Lieschke, D Grail, G Hodgson, D Metcalf, E Stanley… - 1994 - ashpublications.org
GJ Lieschke, D Grail, G Hodgson, D Metcalf, E Stanley, C Cheers, KJ Fowler, S Basu…
1994ashpublications.org
Mice lacking granulocyte colony-stimulating factor (G-CSF) were generated by targeted
disruption of the G-CSF gene in embryonal stem cells. G-CSF-deficient mice (genotype G-
CSF-/-) are viable, fertile, and superficially healthy, but have a chronic neutropenia.
Peripheral blood neutrophil levels were 20% to 30% of wild-type mice (genotype G-CSF+/+)
and mice heterozygous for the null mutation had intermediate neutrophil levels, suggesting
a gene-dosage effect. In the marrow of G-CSF-/-mice, granulopoietic precursor cells were …
Abstract
Mice lacking granulocyte colony-stimulating factor (G-CSF) were generated by targeted disruption of the G-CSF gene in embryonal stem cells. G-CSF-deficient mice (genotype G-CSF-/-) are viable, fertile, and superficially healthy, but have a chronic neutropenia. Peripheral blood neutrophil levels were 20% to 30% of wild-type mice (genotype G- CSF+/+) and mice heterozygous for the null mutation had intermediate neutrophil levels, suggesting a gene-dosage effect. In the marrow of G- CSF-/- mice, granulopoietic precursor cells were reduced by 50% and there were reduced levels of granulocyte, macrophage, and blast progenitor cells. Despite G-CSF deficiency, mature neutrophils were still present in the blood and marrow, indicating that other factors can support neutrophil production in vivo. G-CSF-/- mice had reduced numbers of neutrophils available for rapid mobilization into the circulation by a single dose of G-CSF. G-CSF administration reversed the granulopoietic defect of G-CSF-/- mice. One day of G-CSF administration to G-CSF-/- mice elevated circulating neutrophil levels to normal, and after 4 days of G-CSF administration, G-CSF+/+ and G-CSF- /- marrows were morphologically indistinguishable. G-CSF-/- mice had a markedly impaired ability to control infection with Listeria monocytogenes, with diminished neutrophil and delayed monocyte increases in the blood and reduced infection-driven granulopoiesis. Collectively, these observations indicate that G-CSF is indispensible for maintaining the normal quantitative balance of neutrophil production during “steady-state” granulopoiesis in vivo and also implicate G-CSF in “emergency” granulopoiesis during infections.
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