Polyclonal rabbit gamma globulins against a human cytotoxic CD4 T cell clone: II. Use in prevention of rejection in kidney transplantation: A pilot study

M Hourmant, F Babinet, D Cantarovich, M Latour… - …, 1989 - journals.lww.com
M Hourmant, F Babinet, D Cantarovich, M Latour, J Carcagne, H Vie, M Bonneville…
Transplantation, 1989journals.lww.com
Antiblast globulins (GAB) were prepared by immunization of rabbits with activated T
lymphocytes (AT) derived from a rejected kidney allograft. AT consisted of a CD4+(CD3+,
CD2+ TCR alpha+ beta+) clone cytotoxic for HLA DR8-positive targets. The immunizing
cells were adapted to industrial growth conditions by repetitive stimulations with an EBV-
transformed line from the kidney donor and recombinant IL-2. In the pilot study, GAB (1.0–
1.5 mg/kg/day) was given in 12-hr infusions, in association with prednisone (Pred) 1 …
Abstract
Antiblast globulins (GAB) were prepared by immunization of rabbits with activated T lymphocytes (AT) derived from a rejected kidney allograft. AT consisted of a CD4+(CD3+, CD2+ TCR alpha+ beta+) clone cytotoxic for HLA DR8-positive targets. The immunizing cells were adapted to industrial growth conditions by repetitive stimulations with an EBV-transformed line from the kidney donor and recombinant IL-2. In the pilot study, GAB (1.0–1.5 mg/kg/day) was given in 12-hr infusions, in association with prednisone (Pred) 1 mg/kg/day and azathioprine (Aza) 2 mg/kg/day, as prophylactic treatment of rejection in 12 kidney-transplanted patients during the first 2 weeks postgrafting. GAB dosage was further adapted according to the level of circulating E-rosette-forming T cells (ERFT). Cyclosporine A (8 mg/kg/day) was given at day 14 as a monotherapy after Pred and Aza were progressively tapered. No patient died, but one kidney was lost from surgical complication. No rejection occurred under GAB treatment; 41% of patients had at least one episode in the first 3 months and 16% from 3 to 9 months. GAB side effects were minor (skin rash: 2, low grade fever: 4) except for one acute serum sickness. Platelet and white blood cell counts were unchanged, but there was a significant decrease in hemoglobin during the 2 weeks of GAB infusions. Few infectious episodes occurred (3 bacterial, 2 viral). GAB monitoring showed a dramatic drop in T11+, T3+, T4+, and T8+ circulating T cells (< 10% of normal values between days 3 and 14), whereas EFRT cells had a delayed and somewhat lower decrease (< 10% after day 6 only). Consequently, mean GAB doses had to be raised to 1.3 mg/kg/day at day 4 and 1.6 at days 8 and 14. This pilot study suggests that this new bioreagent should be of major interest in the prophylaxis and treatment of rejection in allograft recipients. A controlled study is in progress.
Lippincott Williams & Wilkins