WEANING OF IMMUNOSUPPRESSION IN LIVER TRANSPLANT RECIPIENTS 1,2

, Abstract Immunosuppression has been sporadically discontinued by noncompliant liver allograft recipients for whom an additional 4 1/2 years of follow-up is provided. These anecdotal observations prompted a previously reported prospective drug withdrawal program in 59 liver recipients. This prospective series has been increased to 95 patients whose weaning was begun between June 1992 and March 1996, 8.4±4.4 (SD) years after liver replacement. A further 4 1/2 years follow-up was obtained of the 5 self-weaned patients. The prospectively weaned recipients (93 livers; 2 liver/ kidney) had undergone transplantation under immunosuppression based on azathioprine (AZA, through 1979), cyclosporine (CsA, 1980–1989), or tacrolimus (TAC, 1989–1994). In patients on CsA or TAC based cocktails, the adjunct drugs were weaned first in the early part of the trial. Since 1994, the T cell–directed drugs were weaned first. Three of the 5 original self-weaned recipients remain well after drug-free intervals of 14 to 17 years. A fourth patient died in a vehicular accident after 11 years off immunosuppression, and the fifth patient underwent retransplantation because of hepatitis C infection after 9 drug-free years; their allografts had no histopathologic evidence of rejection. Eighteen (19%) of the 95 patients in the prospective series have been drug free for from 10 months to 4.8 years. In the total group, 18 (19%) have had biopsy proved acute rejection; 7 (7%) had a presumed acute rejection without biopsy; 37 (39%) are still weaning; and 12 (13%, all well) were withdrawn from the protocol at reduced immunosuppression because of noncompliance (n = 8), recurrent PBC (n = 2), pregnancy (n = 1), and renal failure necessitating kidney transplantation (n = 1). No patients were formally diagnosed with chronic rejection, but 3 (3%) were placed back on preexisting immunosuppression or switched from cyclosporine (CsA) to tacrolimus (TAC) because of histopathologic evidence of duct injury. Two patients with normal liver function died during the trial, both from complications of prior chronic immunosuppression. No grafts suffered permanent functional impairment and only one patient developed temporary jaundice. Long surviving liver transplant recipients are systematically overimmunosuppressed. Consequently, drug weaning, whether incomplete or complete, is an important management strategy providing it is done slowly under careful physician surveillance. Complete weaning from CsA-based regimens has been difficult. Disease recurrence during drug withdrawal was documented in 2 of 13 patients with PBC and could be a risk with other autoimmune disorders.

[1]  D. V. van Thiel,et al.  Evolution of Liver Transplantation , 2007, Hepatology.

[2]  T. Starzl,et al.  The lost chord: microchimerism and allograft survival. , 1996, Immunology today.

[3]  T. Howard,et al.  Evidence that pediatric liver transplant recipients may undergo late rejection episodes in spite of donor-specific microchimerism. , 1996, Transplantation.

[4]  J. Neuberger,et al.  Timing, significance, and prognosis of late acute liver allograft rejection. , 1995, Transplantation.

[5]  C. Delaney,et al.  Variable chimerism, graft-versus-host disease, and tolerance after different kinds of cell and whole organ transplantation from Lewis to brown Norway rats. , 1995, Transplantation.

[6]  T. Starzl,et al.  Weaning of immunosuppression in long-term recipients of living related renal transplants: a preliminary study. , 1995, Transplantation proceedings.

[7]  A. Demetris,et al.  Structural integrity and identification of causes of liver allograft dysfunction occurring more than 5 years after transplantation. , 1995, The American journal of surgical pathology.

[8]  T. Starzl,et al.  Weaning Of Immunosuppression In Long‐Term Liver Transplant Recipients , 1995, Transplantation.

[9]  T. Starzl,et al.  Murine liver allograft transplantation: Tolerance and donor cell chimerism , 1994, Hepatology.

[10]  G. Gores,et al.  Cyclosporine withdrawal for nephrotoxicity in liver transplant recipients does not result in sustained improvement in kidney function and causes cellular and ductopenic rejection , 1994, Hepatology.

[11]  H. Schlitt,et al.  Donor-type microchimerism associated with graft rejection eight years after liver transplantation. , 1994, The New England journal of medicine.

[12]  T. Starzl,et al.  Hematolymphoid cell trafficking, microchimerism, and GVH reactions after liver, bone marrow, and heart transplantation. , 1993, Transplantation proceedings.

[13]  T. Starzl,et al.  Cell migration and chimerism after whole‐organ transplantation: The basis of graft acceptance , 1993, Hepatology.

[14]  T. Starzl,et al.  Cell migration, chimerism, and graft acceptance , 1992, The Lancet.

[15]  D. V. van Thiel,et al.  CONVERSION OF LIVER ALLOGRAFT RECIPIENTS FROM CYCLOSPORINE TO FK506 IMMUNOSUPPRESSIVE THERAPY—A CLINICOPATHOLOGIC STUDY OF 96 PATIENTS , 1992, Transplantation.

[16]  R. Wiesner,et al.  Severe Ductopenic Rejection Following Liver Transplantation: Incidence, Time of Onset, Risk Factors, Treatment, and Outcome , 1992, Seminars in liver disease.

[17]  T. Starzl,et al.  Fifteen years of clinical liver transplantation. , 1979, Gastroenterology.

[18]  T. Starzl,et al.  FK 506 for human liver, kidney, and pancreas transplantation , 1989 .