Negative regulation of TLR9-mediated IFN-α induction by a small-molecule, synthetic TLR7 ligand

JD Marshall, DS Heeke, ML Gesner… - Journal of Leucocyte …, 2007 - academic.oup.com
JD Marshall, DS Heeke, ML Gesner, B Livingston, G Van Nest
Journal of Leucocyte Biology, 2007academic.oup.com
Toll-like receptors (TLRs) are a family of molecules that function as sensors for the detection
of foreign pathogens through the recognition of nonvariable microbial motifs. Although
numerous studies have focused on singular TLRs, less attention has been focused on how
simultaneous signaling of multiple TLRs may result in counter-regulation of the effects of
each. Here, we examine the counter-regulation that occurs during simultaneous stimulation
of TLR7 and TLR9 on human plasmacytoid dendritic cels (PDCs) and B cells. Interestingly …
Abstract
Toll-like receptors (TLRs) are a family of molecules that function as sensors for the detection of foreign pathogens through the recognition of nonvariable microbial motifs. Although numerous studies have focused on singular TLRs, less attention has been focused on how simultaneous signaling of multiple TLRs may result in counter-regulation of the effects of each. Here, we examine the counter-regulation that occurs during simultaneous stimulation of TLR7 and TLR9 on human plasmacytoid dendritic cels (PDCs) and B cells. Interestingly, we observed that the capacity for potent IFN-α-induction by TLR9 ligands like CpG-C and CpG-A is markedly reduced by concurrent small molecule TLR7 stimulation. However, this inhibition is specific to particular CpG motif-containing immunostimulatory sequence (ISS) functions such as IFN-α induction and BDCA-2 down-regulation. Other ISS activities such as PDC expression of CD80/CD86, secretion of IL-6, and B cell proliferation are not altered by the presence of TLR7 ligands (TLR7Ls). In concordance with the ability of TLR7Ls to decrease IFN-α secretion induced by ISS, we also find that the expression of interferon regulatory factor-7 (IRF-7), a transcriptional factor critical for IFN-α expression, is reduced. Furthermore, down-regulation of TLR9 mRNA expression is accelerated after TLR7 stimulation. These data indicate that TLR7 and TLR9 costimulation do not combine synergistically for IFN-α induction and demonstrate that, instead, a negative feedback mechanism has evolved, possibly to prevent levels of IFN-α secretion potentially detrimental to the host.
Oxford University Press