Abstract

Describing risk factors and outcomes in kidney transplant recipients with oxalate nephropathy (ON) may help elucidate the pathogenesis and guide treatment strategies. We used a large single-center database to identify patients with ON and categorized them into delayed graft function with ON (DGF-ON) and late ON. Incidence density sampling was used to select controls. A total of 37 ON cases were diagnosed between 1/2011 and 1/2021. DGF-ON (n=13) was diagnosed in 1.05% of the DGF population. Pancreatic atrophy on imaging (36.4% vs. 2.9%, p=0.002) and gastric bypass history (7.7% vs. 0%; p=0.06) were more common in DGF-ON than with controls with DGF requiring biopsy but without evidence of ON. DGF-ON was not associated with worse graft survival (p=0.98) or death-censored graft survival (p=0.48). Late ON (n=24) was diagnosed after a mean of 78.2 months. Late ON patients were older (mean age 55.1 vs. 48.4 years; p=0.02), more likely to be women (61.7% vs. 37.5%; p=0.03), have gastric bypass history (8.3% vs. 0.8%; p=0.02) and pancreatic atrophy on imaging (38.9% vs. 13.3%; p=0.02). Late ON was associated with an increased risk of graft failure (HR 2.0; p=0.07) and death-censored graft loss (HR 2.5; p=0.10). We describe two phenotypes of ON after kidney transplantation: DGF-ON and late ON. Our study is the first to our knowledge to evaluate DGF-ON with DGF controls without ON. Although limited by small sample size, DGF-ON was not associated with adverse outcomes when compared with controls. Late ON predicted worse allograft outcomes.

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