Beneficial effect of amrinone on murine cardiac allograft survival

Abstract

SUMMARY: Amrinone is a non-glycoside positive inotropic agent with an inhibitory effect on a cyclic adenosine monophosphate (AMP) phosphodiesterase isoenzyme. In the present study, we examined the immunosuppressive action of amrinone, since several other cyclic AM P-elevating agents have been shown to suppress T lymphocyte activation. First, the in vivo. effects of amrinone were investigated. Oral amrinone treatment, at 40mg/kg per day, significantly prolonged median cardiac allograft survival compared with non-treated controls (220 days versus 10-5 days, P<0.01) when DBA/2 mouse hearts (H-2d) were heterotopically transplanted into C57B1/6 mice (H-2d). Histopathological examination showed that there was less prominent cellular infiltration in the amrinone-treated than in the non-treated allografts. Plasma amrinone concentrations of mice after a single oral dose of 40mg/kg were within the range of clinical relevance. To clarify the mechanism of action, in vitro. studies were done. The generation of specific cytotoxic T lymphocytes after mixed lymphocyte culture was significantly suppressed by addition of amrinone to the culture medium at 5μg/ml. The production of IL-2 and the interferon-gamma during mixed lymphocyte culture was also suppressed by amrinone at 5 μg/ml. However, the level of intracellular cyclic AMP in mouse splenic lymphocytes was not affected significantly by the same dose of amrinone. In conclusion, amrinone has immunosuppressive actions at the therapeutic doses, and it may be a beneficial agent for therapy against acute cardiac allograft rejection.