Andrew H. Urbach scite author profile

Between March 3, 1981, and June 1, 1984, 216 children were evaluated for orthotopic liver transplantation. Of the 216 patients, 117 (55%) had received at least one liver transplant by June 1, 1985. Fifty-five (25%) died before transplantation. The 117 patients who received transplants were grouped according to severity of disease and degree of general decompensation at the time of transplantation. The severity of a patient's medical condition with the possible exception of deep hepatic coma, did not predict outcome following orthotopic liver transplantation. Severity variables were assessed at the time of the evaluation. Twenty-three of the 70 variables were found to have prognostic significance with regard to death from progressive liver disease before transplantation. These 23 variables were incorporated into a multivariate model to provide a means of determining the relative risk of death among pediatric patients with end-stage liver disease. This information may allow more informed selection of candidates awaiting liver transplantation.The advent of cyclosporine and advances in surgical technique changed the status of orthotopic liver transplantation from an experimental procedure to accepted care for lethal liver disease. 1 As 1-year survival probabilities approached 66% of OLTx recipients in late 1981 and early 1982, 2 the question of who should receive the next available organ took on critical importance. The improvement in success of OLTx increased the number of children referred for the procedure. More referrals not only sparked an increase in transplantation but drew attention to the shortage of available organs. 3 Twenty-five percent of referred children died of progressive liver disease before transplantation because an appropriate organ could not be located. Donated organs became a precious resource, and their utilization demanded a logical approach to recipient selection.The process of selecting a recipient when a donor liver becomes available is determined primarily by matching the donor and recipient according to size and according to ABO blood group, conforming to blood banking rules of blood transfusions. 4 In situations of great urgency, even ABO incompatibility may be disregarded as a condition for donor recipient matching. 5 No attempt to match minor red cell antigens or Rh factor is made. Extensive tissue typing is not performed because of time constraints, 4 and it appears from retrospective analysis that it may be unnecessary. 4, 5 A number of appropriately matched potential recipients may exist for each donated organ. We attempted to determine whether providing a transplant for the sickest available potential recipient has an adverse effect on transplantation outcome, and second, to develop criteria to distinguish the sickest patient among those with heterogeneous but lethal liver diseases.

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Andrew H. Urbach

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