SHORT-TERM OUTCOMES WITH NO TAPERING TACROLIMUS TO BELATACEPT CONVERSION IN RENAL TRANSPLANT RECIPIENTS (RTRs)

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https://storage.unitedwebnetwork.com/files/1099/2b5990f5296464cdfc8495029735673e.pdf

Abstract Title

First Name *

Adela

Last Name *

Mattiazzi

Co-author 1

Katherine Balloveras katherine.balloveras@jhsmiami.org Jackson Memorial Hospital Pharmacy Miami

Co-author 2

Pierina Cabrera pierina.cabrerarios@jhsmiami.org Jackson Memorial Hospital Pharmacy Miami

Co-author 3

Tiffany Uhlyar tiffany.uhlyar@jhsmiami.org Jackson Memorial Hospital Pharmacy MIami

Co-author 4

Naomi Pierre naomi.pierre@jhsmiami.org Jackson Memorial Hospital Pharmacy Miami

Co-author 5

Alejandra Centeno alexandra.centeno@jhsmiami.org Jackson Memorial Hospital Pharmacy Miami

Co-author 6

Co-author 7

Co-author 8

Co-author 9

Co-author 10

Co-author 11

Co-author 12

Co-author 13

Co-author 14

Co-author 15

Introduction

Several tacrolimus to belatacept conversion protocols have been described in the literature using various forms of tapering tacrolimus over days to weeks. Biopsy proven acute rejection (BPAR) post conversion ranged from 3-33%. The purpose of this study was to assess short-term efficacy of stopping tacrolimus at belatacept initiation while using a more reduced initial phase regimen than described previously in patients within 6 months of transplant.

Methods

A single-center retrospective chart review was conducted in RTRs converted to belatacept from tacrolimus between January 1, 2021 to March 31, 2022. Kidney transplant only patients were included if 18 years or older and converted to belatacept without tacrolimus tapering. Patients were excluded if started on de novo regimen or if patient continued on tacrolimus while on belatacept. Belatacept was dosed at 5 mg/kg IV every two weeks for three doses if patients were within 6 months of transplant, or times five doses if transplanted 6 months or more from conversion prior to starting the maintenance phase. Standard induction protocol included anti-thymocyte globulin and methylprednisolone. Primary outcomes include BPAR, graft loss and patient survival within 6 months of conversion. Secondary outcomes included the incidence of antibody-mediated rejection (AMR), T-cell mediated rejection, CMV viremia, BK viremia, COVID-19 infection, and changes in serum creatinine and eGFR from the time of conversion and at 6 month post-conversion.

Results

Twenty-eight RTRs met criteria, with the majority converted within 6 months of transplant (92.9%). Three patients (10.7%) had BPAR, 2 had graft loss (7.1%), with 92.8% patient survival at 6 months. Of those with BPAR, all had cellular rejection and no AMR. The two patients with graft loss were due to infections ( aspergillosis and COVID-19) Five patients developed CMV viremia, none had BK viremia and 6 (21.4%) had COVID-19. Mean serum creatinine 6 months after conversion was 3.2 mg/dL [1.39-10.71]. Change in serum creatinine at 6 months after conversion was – 1.0 mg/dL. Mean eGFR 6 months after conversion was 29.2 mL/min/1.73m2 [6-61].

Conclusions

Herein we describe a novel approach to converting kidney transplant patients from tacrolimus to belatacept without tapering tacrolimus and using fewer initial phase doses than standard in off-labeling regimens described previously with comparable outcomes.

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