Background

Inhibition of T-cell activation is the most effective to prevent acute cellular rejection. Protein kinase C (PKC) theta is a crucial signaling enzyme in the activation of T lymphocytes. The research for the PKC theta inhibitor led to the development of AS2521780. We investigated the PKC isozyme selectivity of AS2521780 and the effects of this compound on acute rejection both in a rat cardiac transplant model and a non-human primate (NHP) renal transplant model.

Methods

PKC isozyme selectivity of AS2521780 was examined using human PKC isozymes (Α, Β, Γ, Δ, Ε, Ζ, ð, and Θ). Heterotopic cardiac transplantation from ACI to Lewis rats were performed and cardiac allograft survival was evaluated by daily monitoring palpation. Life-supporting renal transplantations were performed between ABO-compatible, MLR-mismatched NHPs and renal allograft survival was evaluated by the determination of the level of plasma creatinine and the general symptoms of recipients.

Results

AS2521780 inhibited PKC theta more potently than other PKC isozymes. AS2521780 prolonged cardiac allograft survival in rats dose dependently both by monotherapy and combination therapy with FK506 or MMF. AS2521780 also prolonged renal allograft survival in NHPs by combination therapy with FK506. AS2521780 was well tolerated in both rats and NHPs transplant recipients.

Conclusions

These studies are the first to demonstrate that AS2521780, a PKC theta selective inhibitor, could prolong allograft survival not only in rats but also in NHPs. Thus, AS2521780 may have the potential to offer an alternative to the therapies in the transplantation fields.

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