Management of Tumor Necrosis Factor α Inhibitor Therapy After Renal Transplantation: A Comparative Analysis and Associated Outcomes

Caroline S Quinn; Margaret R Jorgenson; Jillian L Descourouez; Brenda L Muth; Brad C Astor; Didier A Mandelbrot

doi:10.1177/1060028018802814

Management of Tumor Necrosis Factor α Inhibitor Therapy After Renal Transplantation: A Comparative Analysis and Associated Outcomes

Ann Pharmacother. 2019 Mar;53(3):268-275. doi: 10.1177/1060028018802814. Epub 2018 Sep 20.

Authors

Caroline S Quinn¹, Margaret R Jorgenson¹, Jillian L Descourouez¹, Brenda L Muth², Brad C Astor², Didier A Mandelbrot²

Affiliations

¹ 1 University of Wisconsin Hospital and Clinics, Madison WI, USA.
² 2 University of Wisconsin School of Medicine and Public Health, Madison, WI, USA.

PMID: 30234366
DOI: 10.1177/1060028018802814

Abstract

Background: Biologic agents inhibiting the tumor necrosis factor α pathway (TNFα-Is) are used to treat systemic inflammatory diseases. The best management of these agents after renal transplantation is unknown.

Objective: Evaluate peritransplant use of TNFα-Is and associated outcomes.

Methods: Retrospective, single-center study of adult renal-transplant-recipients (RTRs) transplanted between 1/1/1998-12/31/2017, who received TNFα-Is for inflammatory disease prior to transplant. Qualifying patients were divided into 2 cohorts: patients who resumed TNFα-Is after transplant and those who did not. Outcomes were evaluated.

Results: A total of 5256 renal transplants occurred in the study window; 14 patients met inclusion criteria. Primary indication for TNFα-I was Crohn's-disease (CD; 57.1%). Infliximab was utilized most frequently (50%). Seven RTRs resumed TNFα-I posttransplant; mean time to resumption of 10.6±4.35 months (median=6 months), 85.7% for CD. Immunosuppression was modified in 2 patients (28.6%) in response to restarting TNFα-I therapy. Seven RTRs did not resume TNFα-Is following transplant; the majority of these had rheumatic diseases. There was no significant difference in time to first bacterial or fungal infection, rejection, or patient survival between the 2 groups. Last measured estimated glomerular-filtration-rate was similar between groups (TNFα-I: 41 ± 14.2 vs 48.6 ± 8.6, P = 0.25). No patient had cytomegalovirus infection; however, 42.8% of each cohort had documented BK virus infection. Malignancy occurred more frequently in the cohort that resumed TNFα-Is (42.8% vs 14.3%, P = 0.24); however, this was not statistically significant. Conclusion and Relevance: TNFα-I therapy prior to renal-transplant is relatively uncommon. The decision to continue therapy after transplant must balance risks of infection and malignancy against inflammatory disease recurrence. A multidisciplinary treatment approach is necessary as use of TNFα-I affects immunosuppressive management and appears to affect transplant outcomes. Future studies are needed to further clarify the role of TNFα-I therapy use in RTRs with inflammatory disorders focusing on its correlation with both BK and malignancy.

Keywords: cancer; infectious disease; inflammatory bowel disease; renal transplant; rheumatology.

Publication types

Comparative Study

MeSH terms

Adult
Crohn Disease / drug therapy*
Crohn Disease / immunology
Cytomegalovirus Infections / epidemiology*
Cytomegalovirus Infections / immunology
Electronic Health Records
Female
Graft Rejection / prevention & control
Humans
Immunosuppressive Agents / administration & dosage
Immunosuppressive Agents / adverse effects
Immunosuppressive Agents / therapeutic use*
Kidney Transplantation*
Male
Middle Aged
Polyomavirus Infections / epidemiology*
Polyomavirus Infections / immunology
Retrospective Studies
Tumor Necrosis Factor-alpha / antagonists & inhibitors*

Substances

Immunosuppressive Agents
Tumor Necrosis Factor-alpha