Increased CMV disease and "severe" BK viremia with belatacept vs. sirolimus three-drug maintenance immunosuppression

Gregory Petrossian; Jorge Ortiz; Alejandro Chiodo Ortiz; Kathryn Addonizio; Alexander Hsiao; Rosy James; Naoru Koizumi; Sunil Patel; Robert Plews

doi:10.1016/j.trim.2023.101857

Increased CMV disease and "severe" BK viremia with belatacept vs. sirolimus three-drug maintenance immunosuppression

Transpl Immunol. 2023 Aug:79:101857. doi: 10.1016/j.trim.2023.101857. Epub 2023 May 16.

Authors

Gregory Petrossian¹, Jorge Ortiz², Alejandro Chiodo Ortiz³, Kathryn Addonizio³, Alexander Hsiao³, Rosy James⁴, Naoru Koizumi⁴, Sunil Patel⁵, Robert Plews⁶

Affiliations

¹ Albany Medical Center, Albany, NY, United States of America. Electronic address: petrosg@amc.edu.
² Eerie County Medical Center, Buffalo, NY, United States of America.
³ Albany Medical Center, Albany, NY, United States of America.
⁴ George Mason University, Fairfax, VA, United States of America.
⁵ University Medical Center of Southern Nevada, Las Vegas, NV, United States of America.
⁶ University of Cincinnati, Cincinnati, OH, United States of America.

PMID: 37201797
DOI: 10.1016/j.trim.2023.101857

Abstract

Objectives: Belatacept may provide benefit in delayed graft function, but its association with infectious complications is understudied. We aim to assess the incidence of CMV and BK viremia in patients treated with sirolimus or belatacept as part of a three-drug immunosuppression regimen after kidney transplantation.

Materials and methods: Kidney transplant recipients from 01/01/2015 to 10/01/2021 were retrospectively reviewed. Maintenance immunosuppression was either tacrolimus, mycophenolate and sirolimus (B⁰) or tacrolimus, mycophenolate, and belatacept (5.0 mg/kg monthly) (B¹). Primary outcomes of interest were BK and CMV viremia which were followed until the end of the study period. Secondary outcomes included graft function (serum creatinine, eGFR) and acute rejection through 12 months.

Results: Belatacept was initiated in patients with a higher mean kidney donor profile index (B⁰:0.36 vs. B¹:0.44, p = .02) with more delayed graft function (B⁰:6.1% vs. B¹:26.1%, p < .001). Belatacept therapy was associated with more "severe" CMV viremia >25,000 copies/mL (B⁰:1.2% vs. B¹:5.9%, p = .016) and CMV disease (B⁰:0.41% vs. B¹:4.2%, p = .015). However, there was no difference in the overall incidence of CMV viremia >200 IU/mL (B⁰:9.4% vs. B¹:13.5%, p = .28). There was no difference in the incidence of BK viremia >200 IU/mL (B⁰:29.7% vs. B¹:31.1%, p = .78) or BK-associated nephropathy (B⁰:2.4% vs. B¹:1.7%, p = .58), but belatacept was associated with "severe" BK viremia, defined as >10,000 IU/mL (B⁰:13.0% vs. B¹:21.8%, p = .03). The mean serum Cr was significantly higher with belatacept therapy at 1-year follow up (B⁰:1.24 mg/dL vs. B¹:1.43 mg/dL, p = .003). Biopsy-proven acute rejection (B⁰:1.2% vs. B¹:2.6%, p = .35) and graft loss (B⁰:1.2% vs. B¹:0.84%, p = .81) were comparable at 12 months.

Conclusions: Belatacept therapy was associated with an increased risk of CMV disease and "severe" CMV and BK viremia. However, this regimen did not increase the overall incidence of infection and facilitated comparable acute rejection and graft loss at 12-month follow up.

Keywords: BK polyomavirus; Belatacept; Cytomegalovirus; Kidney transplantation; Sirolimus.

MeSH terms

Abatacept / therapeutic use
BK Virus*
Cytomegalovirus Infections* / drug therapy
Cytomegalovirus Infections* / epidemiology
Delayed Graft Function / drug therapy
Graft Rejection / epidemiology
Humans
Immunosuppression Therapy
Immunosuppressive Agents / adverse effects
Immunosuppressive Agents / therapeutic use
Polyomavirus Infections* / drug therapy
Polyomavirus Infections* / epidemiology
Retrospective Studies
Sirolimus / therapeutic use
Tacrolimus / therapeutic use
Viremia / drug therapy
Viremia / epidemiology

Substances

Sirolimus
Abatacept
Tacrolimus
Immunosuppressive Agents