Amino-terminal truncation of CXCR3 agonists impairs receptor signaling and lymphocyte chemotaxis, while preserving antiangiogenic properties

Abstract

Abnormal isoforms of the prion protein (PrP^Sc) that cause prion diseases are propagated and spread within the body by “carrier” cell(s). Cells of the immune system have been strongly implicated in this process. In particular, PrP^Sc is known to accumulate on follicular dendritic cells (FDCs) in individuals affected by variant Creutzfeld-Jakob disease. However, FDCs do not migrate widely and the natural history of prion disorders suggests other cells may be required for the transport of PrP^Sc from the site of ingestion to lymphoid organs and the central nervous system. Substantial evidence suggests that the spread of PrP^Sc requires bone marrow-derived cells that express normal cellular prion protein (PrP^C). This study examined the expression of PrP^C on bone marrow–derived cells that interact with lymphoid follicles. High levels of PrP^C are present on myeloid dendritic cells (DCs) that surround the splenic white pulp. These myeloid DCs are ontologically and functionally distinct from the FDCs. Consistent with these observations, expression of PrP^C was strongly induced during the generation of mature myeloid DCs in vitro. In these cells PrP^Ccolocalized with major histocompatibility complex class II molecules at the level of light microscopy. Furthermore, given the close anatomic and functional connection of myeloid DCs with lymphoid follicles, these results raise the possibility that myeloid DCs may play a role in the propagation of PrP^Sc in humans.