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(Journal of Leukocyte Biology. 2003;73:564-573.)
© 2003 by Society for Leukocyte Biology

Monocyte and macrophage functions in M-CSF-deficient op/op mice during experimental leishmaniasis

Frank Schönlau*, Christian Schlesiger*, Jan Ehrehen*, Stephan Grabbe{dagger}, Clemens Sorg* and Cord Sunderkötter*,{dagger},{ddagger}

* Institute of Experimental Dermatology and
{dagger} Department of Dermatology, University of Münster, Germany; and
{ddagger} Department of Dermatology, University of Ulm, Germany

Correspondence: Cord Sunderkötter, M.D., Department of Dermatology, University of Ulm, Maienweg 12, 89081 Ulm, Germany. E-mail: cord.sunderkoetter{at}medizin.uni-ulm.de

Mice with a naturally occurring Csfmop/Csfmop (op/op) gene mutation lack functional macrophage-colony stimulating factor (M-CSF) and are deficient of M-CSF-derived macrophages. They are severely monocytopenic, and their remaining M-CSF-independent macrophages were shown to differ in differentiation and distinct functions when compared with phenotypically normal mice of the same background. It is not known if osteopetrosis mice (op/op mice) are able to mount a specific immune response against intracellular pathogens, as this would require complex effector functions by macrophages. We therefore investigated the ability of op/op mice and their M-CSF-independent macrophages to combat infection with Leishmania major. op/op mice retained the ability to resist an infection with L. major by mounting a T helper cell type 1 cell response, eliminating parasites and resolving the lesions. Macrophages from op/op mice were able to sufficiently perform effector functions in vitro, such as phagocytosis, production of leishmanicidal nitric oxide (NO), killing of parasites, and release of interleukin (IL)-12. There were quantitative differences, as M-CSF-derived macrophages from hematopoietic organs of control mice showed significantly higher rates of phagocytosis and higher NO release after stimulation with lipopolysaccharides than corresponding macrophages from op/op mice. In contrast, when peritoneally elicited macrophages were used, those from op/op mice revealed a stronger response than those from control mice with regard to release of NO or IL-12. These differences suggest that M-CSF-independent maturation of op/op monocytes subsequent to their release from hematopoietic tissue exerts influence on their effector functions. However, M-CSF or M-CSF-derived macrophages are not necessary for an effective immune response against L. major.

Key Words: Leishmania major • osteopetrosisIL-12




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