Kooperatív Doktori Program(KDP-2020) Támogató: NKFIH
Chemotherapy is still one of the main therapeutic approaches in cancer therapy. Nevertheless,
its poor selectivity causes severe toxic side effects that, together with the development
of drug resistance in tumor cells, results in a limitation for its application. Tumor-targeted
drug delivery is a possible choice to overcome these drawbacks. As well as monoclonal
antibodies, peptides are promising targeting moieties for drug delivery. However,
the development of peptide-drug conjugates (PDCs) is still a big challenge. The main
reason is that the conjugates have to be stable in circulation, but the drug or its
active metabolite should be released efficiently in the tumor cells. For this purpose,
suitable linker systems are needed that connect the drug molecule with the homing
peptide. The applied linker systems are commonly categorized as cleavable and non-cleavable
linkers. Both the groups possess advantages and disadvantages that are summarized
briefly in this manuscript. Moreover, in this review paper, we highlight the benefit
of oxime-linked anthracycline-peptide conjugates in the development of PDCs. For instance,
straightforward synthesis as well as a conjugation reaction proceed in excellent yields,
and the autofluorescence of anthracyclines provides a good tool to select the appropriate
homing peptides. Furthermore, we demonstrate that these conjugates can be used properly
in in vivo studies. The results indicate that the oxime-linked PDCs are potential
candidates for targeted tumor therapy.
