Whilst a coincidental flare of the patient’s underlying RA seems implausible in the setting of high-dose immunosuppression, an alternative hypothesis is that immune system dysregulation induced by use of immunosuppressant medication caused a paradoxical response and subsequent flare of the patient’s RA. The pathogenesis of different autoimmune diseases is heterogeneous – as demonstrated by the variation in response to different immunosuppressants
and recurrence rates of autoimmune primary diseases after transplantation. Disruption of immune Cobimetinib ic50 system homeostasis with potentially undesirable or paradoxical responses has also been demonstrated by administration of
different immunosuppressants and immunomodulators. A INCB024360 concentration specific example includes medications from the interferon family being associated with promotion of renal allograft rejection, exacerbation of pre-existing autoimmune disease and development of de novo autoimmune disease in certain populations.[3] The pathogenesis of RA is complex, and recent studies suggest disease activity in RA is mediated by an imbalance between Th17 and T-regulatory (T-reg) cells.[4] T-regs are thought to suppress pathologic immune responses in autoimmune disease. In RA, reduced number of T-regs and dysfunctional T-regs have been observed, and depletion of T-regs in a mouse model of RA increases disease activity which can then be reversed with adoptive transfer of T-regs.[4] Medications used in renal transplantation
which specifically target IL-2 may be implicated in disrupting this Th17/T-reg balance. Li et al. reported that tacrolimus (blocker of IL-2 transcription) at serum concentrations above 6 ng/mL, compared with lower tacrolimus level, cyclosporine A and sirolimus in renal transplant recipients, was associated with Florfenicol greater imbalance between Th17/T-reg cell numbers in peripheral blood, specifically higher Th17 levels and lower T-reg levels.[5] Basiliximab, a monoclonal antibody directed against IL-2 receptors, may therefore also be implicated in this hypothesis. Bluestone et al. compared the effect of basiliximab in addition to standard immunosuppression (cyclosporine A, mycophenolate mofetil and steroid taper) with belatacept (a CTLA-4Ig) and standard immunosuppression on T-regs in peripheral blood after renal transplantation.[6] A profound but transient reduction in CD4+CD25+FOXP3 T-regs was observed in the basiliximab but not the belatacept arm within 7 days of treatment. Our case describes acute onset polyarthritis immediately after transplantation.
Related posts:
- In the late referral group, 15 patients required commencement of
- No serum miRNA was regulated exclusively in aUC compared with iUC
- Renal transplantation for APS patients with ESKD is associated wi
- DS had three pregnancies with high complication rates, the first
- In addition, the cytokine imbalance of psoriasis is clearly illus