Signaling through Notch receptors and their transcriptional effector RBP-J is essential for lymphocyte development and function, whereas its role in other immune cell types is unclear. We tested the function of the canonical Notch-RBP pathway in dendritic cell (DC) development and maintenance in vivo. Genetic inactivation of RBP in the bone marrow did not preclude DC lineage commitment but caused the reduction of splenic DC fraction. The inactivation of Ill in DCs using a novel DC-specific deleter strain caused selective loss of the splenic CD8(-)DC subset and reduced the frequency of cytokine-secreting CD8(-)DCs after challenge with Toll-like receptor ligands. In contrast, other splenic DC subsets and M in the lymph nodes and tissues were unaffected. The RBP-J-deficient splenic CD8(-)DCs were depleted at the postprogenitor stage, exhibited increased apoptosis, and lost the expression of the Notch target gene Deltex1. In the spleen, CD8(-)DCs were found adjacent to cells expressing the Notch ligand Delta-like 1 in the marginal zone (MZ) Thus, canonical Notch-l signaling controls the maintenance of CD8(-)DCs in the splenic revealing an unexpected role of the Notch pathway in the innate immune system.

• 出版日期2007-7-9