New diketopiperazines as vectors for peptide protection and brain delivery: Synthesis and biological evaluation

New strategies allowing the transfer of molecules, especially peptides, through the blood-brain barriers are a major pharmacological challenge for the treatment of brain diseases. The present study aims at evaluating in vivo the cerebral bioavailability of carrier systems, based on small and functionalizable 2,5-diketopiperazine (DKP) motifs. We studied 2 different cyclo(Lys-Lys) DKP scaffolds alone and a cyclo(Lys-Gly) DKP carrier bearing as peptide model, the tau protein hexapeptide VQIVYK sequence. The different carrier systems were synthesized and radiolabeled using one of the free domains. The stability, biodistribution, and ability to cross blood-brain barrier were investigated in vivo in mice for Tc-99m-DKP scaffolds, Tc-99m-HVQIVYK peptide alone, and Tc-99m-DKP-VQIVYK. I-125-labelled bovine serum albumin was used as negative control for brain uptake. Both radiolabeled DKPs scaffolds and Tc-99m-DKP-VQIVYK showed a high stability, while peptide Tc-99m-HVQIVYK alone was quickly degraded in vivo. The presence of Tc-99m-DKPs scaffolds and (9)9(mT)c-DKP-VQIVYK was observed in the ventricular and subarachnoid spaces and to a lower extent in the brain parenchyma up to 45 minutes post-injection in mice. This work highlights the potentiality of DKP scaffolds as vectors to transport peptides into the brain by limiting proteolysis and favoring cerebral bioavailability.