Treatment with hCDR1 down-regulated the expression of the latter molecule.51 Our present results, as well as previous data, indicate that treatment with hCDR1 affects a number of cell types and pathways. Figure 8 summarizes schematically our updated knowledge on the effects of treatment of SLE-affected mice with hCDR1 on T and B cells. As illustrated in the Fig. 8, the expression of CD74/CD44 complex in B cells of the treated mice is down-regulated along with down-regulation of the ligand of this complex, MIF, which results in suppressed expression of survival molecules, (e.g. Bcl-xL). Previous studies suggested
that suppression of NF-κB signalling mediated the latter,17,19 in agreement with our findings following down-regulation of selleck screening library BAFF in the hCDR1-treated mice.16 In addition to the inhibitory effect of hCDR1 on the state of activation of B cells,8 the resultant enhancement of B-cell apoptosis may lead to the reduced production of dsDNA specific autoantibodies. In the T-cell compartment, however, hCDR1 induced CD4 and CD8 regulatory T cells,6,7 up-regulated the expression of Bcl-xL, and led to decreased rates of T-cell apoptosis and inhibition of T-cell activation.8,9 As a result, the production of pathogenic cytokines was significantly down-regulated. The reduced production of autoantibodies and pathogenic cytokines
is associated Epigenetics Compound Library in vitro with clinical amelioration of SLE manifestations. In conclusion, the present work has shown the involvement of the CD74/MIF pathway in the development of pathogenic B cells and in SLE-afflicted target organs. Moreover, treatment with the tolerogenic peptide, hCDR1, ameliorates disease manifestations, at least in part, by affecting this pathway. The authors have no financial conflicts of interest. “
“Antigen-presenting cell-associated four-domain MHC class II (MHC-II) molecules play a central role in activating
autoreactive CD4+ T cells involved in multiple sclerosis (MS) and type 1 diabetes (T1D). In contrast, two-domain MHC-II structures with the same Thymidylate synthase covalently attached self-peptide (recombinant T-cell receptor ligands (RTLs)) can regulate pathogenic CD4+ T cells and reverse clinical signs of experimental autoimmune diseases. RTL1000, which is composed of the β1α1 domains of human leukocyte antigen (HLA)-DR2 linked to the encephalitogenic human myelin oligodendrocyte glycoprotein (MOG)-35-55 peptide, was recently shown to be safe and well tolerated in a phase I clinical trial in MS. To evaluate the opposing biological effects of four- versus two-domain MHC-II structures, we screened phage Fab antibodies (Abs) for the neutralizing activity of RTL1000. Five different TCR-like Abs were identified that could distinguish between the two- versus four-domain MHC–peptide complexes while the cognate TCR was unable to make such a distinction.