Utility of azathioprine metabolite measurements in post‐transplant recurrent autoimmune and immune‐mediated hepatitis

  Patients with post‐transplant immune‐mediated hepatitis (IMH) and recurrent autoimmune hepatitis (RAIH) have a poor outcome and a higher need for retransplantation. Azathioprine (AZA) is used as adjunctive immunosuppression after transplantation; optimizing its dose may be a key point in preserving graft function. Complications of high AZA dosing make dose escalation potentially problematic. Our aim was to correlate AZA metabolite levels with therapeutic effects, toxicity, and adherence to medication in children with IMH and RAIH. Charts of 14 patients were retrospectively reviewed. The post‐transplant diagnosis was based on liver biopsy and autoimmune markers. AZA was prescribed after establishing the post‐transplant diagnosis. AZA was started at 1.1 (1.0–1.8) mg/kg/day. Routine biochemical studies, tacrolimus levels, 6‐thioguanine (6‐TG) and 6‐methylmercaptopurine levels were assessed every 8 wk. AZA dose was routinely adjusted to achieve 6‐TG levels between 235 and 450 pmol per 8 × 10 8 RBC. A total of 92 samples from 14 patients were reviewed. Four patients were excluded because of non‐adherence. AZA dose was increased by 245% resulting in eight of 10 patients in the target range; no hepatic or bone marrow toxicity was observed. ALT levels and steroid requirements were significantly reduced (p < 0.05). The AZA dose required to achieve target 6‐TG levels was significantly greater in children <10 yr. AZA metabolite testing in children post‐liver transplant is useful in assessing adherence to medication and it is potentially helpful in optimizing medication dosing. In younger children the AZA dose requirements were two to four times higher than previously reported standard doses.