Identification of CD68+ lin− peripheral blood cells with dendritic precursor characteristics

H Strobl, C Scheinecker, E Riedl… - The Journal of …, 1998 - journals.aai.org
H Strobl, C Scheinecker, E Riedl, B Csmarits, C Bello-Fernandez, WF Pickl, O Majdic…
The Journal of Immunology, 1998journals.aai.org
Expression of CD68 (macrosialin) in the absence of surface and lysosomal lineage marker
molecules is a characteristic feature of T zone-associated plasmacytoid monocytes, which
were recently shown to represent precursors of dendritic cells (DC). We demonstrate here a
minor population of strongly CD68-positive (CD68 bright) blood cells that lack all analyzed
myeloid surface (CD14−, CD33−, CD13−, CD11b−, CD11c−) and lysosomal
(myeloperoxidase, MPO− and lysozyme, LZ−) marker molecules (0.4±2% of the total …
Abstract
Expression of CD68 (macrosialin) in the absence of surface and lysosomal lineage marker molecules is a characteristic feature of T zone-associated plasmacytoid monocytes, which were recently shown to represent precursors of dendritic cells (DC). We demonstrate here a minor population of strongly CD68-positive (CD68 bright) blood cells that lack all analyzed myeloid surface (CD14−, CD33−, CD13−, CD11b−, CD11c−) and lysosomal (myeloperoxidase, MPO− and lysozyme, LZ−) marker molecules (0.4±2% of the total mononuclear cells). These CD68 bright, lineage marker-negative (lin−) cells can be induced to proliferate in the presence of IL-3. They do not acquire myeloid features even upon stimulation with granulocyte-macrophage CSF plus IL-1, IL-3, and IL-6. Instead, these cells develop typical DC characteristics upon culture. Furthermore, these CD68 bright lin− DC precursors acquire mature DC characteristics (CD86+, CD83+, CD54 bright) upon stimulation with CD40 ligand plus IL-3. A second subset of DC precursor-like blood cells was found to weakly express CD68 (0.3±0.2% of the total mononuclear cells) and to coexpress several myeloid lineage associated molecules (LZ+, CD11c+, CD33+, CD13+). Cells of this second subset resemble both previously described myeloid-related peripheral blood DC and germinal center DC. Analysis of peripheral blood leukocytes for CD68 thus revealed the existence of two cell subsets that phenotypically resemble lymphoid tissue-associated DC. The unique phenotype CD68 bright lin− is highly reminiscent of T zone-associated plasmacytoid monocytes. CD68 bright lin− blood leukocytes also functionally resemble plasmacytoid monocytes. The lack of all analyzed myeloid features by CD68 bright lin− blood leukocytes suggests that these cells arise from a novel nonmyeloid human DC differentiation pathway.
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