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The Journal of Immunology, 2005, 174: 3067-3071.
Copyright © 2005 by The American Association of Immunologists

Increased Blood Myeloid Dendritic Cells and Dendritic Cell-Poietins in Langerhans Cell Histiocytosis1

Alexandre Rolland2,*, Lydie Guyon*, Michelle Gill*,{dagger}, Yi-Hong Cai{ddagger}, Jacques Banchereau*, Kenneth McClain3,* and A. Karolina Palucka3,*

* Baylor Institute for Immunology Research, Dallas, TX 75204; {dagger} University of Texas Southwestern Medical Center, Dallas, TX 75390; and {ddagger} Baylor College of Medicine, Texas Children’s Cancer Center, Houston, TX 77030

Langerhans cell histiocytosis (LCH), previously known as histiocytosis X, is a reactive proliferative disease of unknown pathogenesis. Current therapies are based on nonspecific immunosuppression. Because multiple APCs, including Langerhans cells and macrophages, are involved in the lesion formation, we surmised that LCH is a disease of myeloid blood precursors. We found that lin HLA-DR+CD11c-+ precursors of dendritic cells, able to give rise to either Langerhans cells or macrophages, are significantly (p = 0.004) increased in the blood of LCH patients. The analysis of serum cytokines in 24 patients demonstrated significantly elevated levels of hemopoietic cytokines such as fms-like tyrosine kinase ligand (FLT3-L, a dendritic cell-mobilizing factor, ~2-fold) and M-CSF (~4-fold). Higher levels of these cytokines correlated with patients having more extensive disease. Serum levels of FLT3-L and M-CSF were highest in high risk patients with extensive skin and/or multisystem involvement. Finally, patients with bone lesions had relatively higher levels of M-CSF and of stem cell factor. Thus, early hemopoietic cytokines such as FLT3-L, stem cell factor, and M-CSF maybe relevant in LCH pathogenesis and might be considered as novel therapeutic targets.




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