Abstract
BackgroundChronic Renal Allograft Dysfunction (CRAD) is responsible for a large number of graft failures. We have abrogated acute T-cell rejections using Ahmedabad Tolerance Induction Protocol (ATIP) with hematopoietic stem cell transplantation (HSCT) under non-myeloablative conditioning pre-transplant. However B-cell mediated rejections and CRAD continue to haunt us. We carried out retrospective analysis of renal allograft biopsies performed in the last 4 years to evaluate the effect of ATIP on CRAD.Materials and methodsBiopsies diagnosed as per modified Banff criteria belonged to 2 groups: ATIP under low dose immunosuppression of cyclosporine/Azathioprine/Mycofenolate mofetil+ Prednisolone, subjected to donor leucocyte transfusion, anti-T/B cell antibodies, low dose target specific irradiation, cyclophosphamide, cyclosporin followed by HSCT pre-transplant; controls who opted out of ATIP were transplanted under standard triple drug immunosuppression. Demographics of both groups were comparable.ResultsIncidence of chronic changes was higher in controls (17.5%) vs. 10.98% in ATIP over a mean follow up of 151.9 months in the former and 130.9 months in the latter. Proteinuria and hypertension were higher in controls (48.4%) vs. ATIP (32.7%) with chronic transplant glomerulopathy, focal global sclerosis in 67.7% in controls vs. 46.7% in ATIP, acute on chronic T/B cell rejection in 51.6% controls vs. 28.1% ATIP, with peritubular capillary C4d deposits in 19.4% controls vs. 1.9% ATIP biopsies. Acute on chronic calcineurin inhibitor toxicity was higher in ATIP (71.9%) vs. 48.4% in controls.ConclusionChronic immune injury was less with ATIP vs controls as compared to a higher incidence of chronic calcineurin inhibitor toxicity in the former.
Highlights
Chronic Renal Allograft Dysfunction (CRAD) is responsible for a large number of graft failures
Acute on chronic calcineurin inhibitor toxicity was higher in Ahmedabad Tolerance Induction Protocol (ATIP) (71.9%) vs. 48.4% in controls
Chronic immune injury was less with ATIP vs controls as compared to a higher incidence of chronic calcineurin inhibitor toxicity in the former
Summary
Chronic Renal Allograft Dysfunction (CRAD) is responsible for a large number of graft failures. We carried out retrospective analysis of renal allograft biopsies performed in the last 4 years to evaluate the effect of ATIP on CRAD. Significant improvement in 1 year renal allograft and patient survival rates have been achieved over the last 10 years as a result of newer immunosuppressive regimes and the increasing use of living donors for transplantation. Up to 50% grafts are lost to chronic renal allograft dysfunction (CRAD). [1] We have been modifying Ahmedabad Tolerance Induction Protocol (ATIP) to achieve transplantation tolerance in our renal allograft recipients since 1998. The present study aims to evaluate the effect of ATIP on CRAD in our living-related renal allograft recipients
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