Belatacept in kidney transplant patients with systemic lupus erythematosus

Anca Askanase; Irene Carrión-Barberà; Melissa Fajardo; Demetra Tsapepas; Hilda Fernandez

doi:10.1136/lupus-2019-000355

Lupus Science and Medicine (Dec 2019)

Belatacept in kidney transplant patients with systemic lupus erythematosus

Anca Askanase,
Irene Carrión-Barberà,
Melissa Fajardo,
Demetra Tsapepas,
Hilda Fernandez

Affiliations

Anca Askanase: 1Queen Elizabeth II Health Sciences Center and Dalhousie University, Rheumatology/Medicine, Halifax, Nova Scotia, Canada
Irene Carrión-Barberà: Department of Rheumatology, Hospital del Mar, Barcelona, Spain
Melissa Fajardo: 2Columbia University Medical Center, Nephrology, New York, United States of America
Demetra Tsapepas: 2Columbia University Medical Center, Nephrology, New York, United States of America
Hilda Fernandez: 2Columbia University Medical Center, Nephrology, New York, United States of America

DOI: https://doi.org/10.1136/lupus-2019-000355
Journal volume & issue: Vol. 6, no. 1

Abstract

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Objectives Lupus nephritis (LN) requires renal replacement therapy in 10%–30% of patients. About 30% of these patients receive a kidney transplant. Belatacept is a second-generation, selective, T-cell co-stimulator blocker (inhibits cytotoxic, T-lymphocyte antigen 4, CTLA-4) used as an alternative to calcineurin inhibitors (CNI) for maintenance regimens after kidney transplantation. The pathogenic relevance of CTLA-4 inhibition and the favourable cardiovascular profile of belatacept make it an attractive therapeutic option in systemic lupus erythematosus (SLE). Intravenous administration of belatacept ensures therapeutic adherence.Methods This retrospective, single-centre study evaluates the outcomes of LN kidney transplant recipients treated with belatacept for reasons not related to SLE at the Columbia University Lupus and Renal Transplant Cohort.Results Belatacept was started in six patients on CNI regimens at 15.5±17.1 months following transplantation for LN. In five patients, creatinine levels stabilised 6 months after belatacept, one returned to haemodialysis due to CNI toxicity and pyelonephritis and one relisted for a kidney transplant following acute cellular rejection and cortical necrosis. Five patients are followed for extrarenal lupus; no extrarenal manifestations were documented in the other two patients. Data on SLE disease activity pre-belatacept and post-belatacept were available and scored in three patients using the SLE Disease Activity Index Glucocorticosteroid Index (SLEDAI-2KG), which accounts for clinical and laboratory manifestations, as well as steroid dose. Mean SLEDAI-2KG decreased from 13 to 7.6.Conclusion Belatacept in LN kidney transplant recipients may decrease extrarenal manifestations, attenuate CNI toxicity and stabilise allograft function, providing a better alternative to CNI regimens. Furthermore, these data suggest that belatacept, although initiated for reasons not related to SLE, might have a beneficial effect in SLE.

Published in Lupus Science and Medicine

ISSN: 2053-8790 (Online)
Publisher: BMJ Publishing Group
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Immunologic diseases. Allergy
Website: https://lupus.bmj.com

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