PLoS ONE (Jan 2021)

A pilot study evaluating GSK1070806 inhibition of interleukin-18 in renal transplant delayed graft function.

  • E Wlodek,
  • R B Kirkpatrick,
  • S Andrews,
  • R Noble,
  • R Schroyer,
  • J Scott,
  • C J E Watson,
  • M Clatworthy,
  • E M Harrison,
  • S J Wigmore,
  • K Stevenson,
  • D Kingsmore,
  • N S Sheerin,
  • O Bestard,
  • H A Stirnadel-Farrant,
  • L Abberley,
  • M Busz,
  • S DeWall,
  • M Birchler,
  • D Krull,
  • K S Thorneloe,
  • A Weber,
  • L Devey

DOI
https://doi.org/10.1371/journal.pone.0247972
Journal volume & issue
Vol. 16, no. 3
p. e0247972

Abstract

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IntroductionDelayed graft function (DGF) following renal transplantation is a manifestation of acute kidney injury (AKI) leading to poor long-term outcome. Current treatments have limited effectiveness in preventing DGF. Interleukin-18 (IL18), a biomarker of AKI, induces interferon-γ expression and immune activation. GSK1070806, an anti-IL18 monoclonal antibody, neutralizes activated (mature) IL18 released from damaged cells following inflammasome activation. This phase IIa, single-arm trial assessed the effect of a single dose of GSK1070806 on DGF occurrence post donation after circulatory death (DCD) kidney transplantation.MethodsThe 3 mg/kg intravenous dose was selected based on prior studies and physiologically based pharmacokinetic (PBPK) modeling, indicating the high likelihood of a rapid and high level of IL18 target engagement when administered prior to kidney allograft reperfusion. Utilization of a Bayesian sequential design with a background standard-of-care DGF rate of 50% based on literature, and confirmed via extensive registry data analyses, enabled a statistical efficacy assessment with a minimal sample size. The primary endpoint was DGF frequency, defined as dialysis requirement ≤7 days post transplantation (except for hyperkalemia). Secondary endpoints included safety, pharmacokinetics and pharmacodynamic biomarkers.ResultsGSK1070806 administration was associated with IL18-GSK1070806 complex detection and increased total serum IL18 levels due to IL18 half-life prolongation induced by GSK1070806 binding. Interferon-γ-induced chemokine levels declined or remained unchanged in most patients. Although the study was concluded prior to the Bayesian-defined stopping point, 4/7 enrolled patients (57%) had DGF, exceeding the 50% standard-of-care rate, and an additional two patients, although not reaching the protocol-defined DGF definition, demonstrated poor graft function. Six of seven patients experienced serious adverse events (SAEs), including two treatment-related SAEs.ConclusionOverall, using a Bayesian design and extensive PBPK dose modeling with only a small sample size, it was deemed unlikely that GSK1070806 would be efficacious in preventing DGF in the enrolled DCD transplant population.Trial registrationNCT02723786.