Polymeric prodrug combination to exploit the therapeutic potential of antimicrobial peptides against cancer cells

被引:32
|
作者
Kelly, G. J. [1 ]
Kia, A. Foltyn-Arfa [2 ]
Hassan, F. [3 ]
O'Grady, S. [3 ]
Morgan, M. P. [3 ]
Creaven, B. S. [2 ]
McClean, S. [4 ]
Harmey, J. H. [3 ]
Devocelle, M. [1 ]
机构
[1] Royal Coll Surgeons Ireland, Dept Pharmaceut & Med Chem, Ctr Synth & Chem Biol, 123 St Stephens Green, Dublin 2, Ireland
[2] Inst Technol Tallaght, Dept Sci, Dublin 24, Ireland
[3] Royal Coll Surgeons Ireland, Mol & Cellular Therapeut, 123 St Stephens Green, Dublin 2, Ireland
[4] Inst Technol Tallaght, Ctr Microbial Host Interact, Dublin 24, Ireland
基金
爱尔兰科学基金会;
关键词
HOST-DEFENSE PEPTIDES; ANTICANCER ACTIVITY; CATHEPSIN-B; DOXORUBICIN; STRATEGIES; LIGATION; RELEASE; AGENTS; MODEL; OXIME;
D O I
10.1039/c6ob01815g
中图分类号
O62 [有机化学];
学科分类号
070303 ; 081704 ;
摘要
Antimicrobial Peptides (AMPs) have unique anticancer properties, but their clinical application is currently limited by an inadequate margin of safety. A prodrug strategy associated with a combination therapy approach could address this limitation by increasing their therapeutic index and their efficacy. Accordingly, the first targeted anticancer polymeric prodrug candidates of AMPs, intended for combination therapy with another polymeric prodrug of an approved antineoplastic agent (doxorubicin), were synthesized as either a PEG-based dual-release prodrug or two individual pegylated prodrugs. The latter are based on a cathepsin B-labile peptide linker and an acid-sensitive acyl hydrazone bond for the AMP and doxorubicin prodrugs, respectively. Anticancer activities and toxicity differentials achieved with the free peptide and its polymer conjugates against ovarian, cancer and non-malignant, cells, indicate that protease-dependent reversible pegylation could be implemented to increase the therapeutic indices of AMPs in cancer therapy. The results obtained also show that this approach can be developed if the releasable PEG linker can be optimised to conciliate the attributes and restrictions of pegylation against proteases. In addition, combination of the polymeric prodrugs of the AMP and of doxorubicin provides additive antitumor effects which could be exploited to enhance the efficacy of the AMP candidate.
引用
收藏
页码:9278 / 9286
页数:9
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