Autocatalytic strategy for tuning drug release from peptide-drug supramolecular hydrogel

被引:0
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作者
Yuqin Wu [1 ]
Tian Xia [1 ]
Xiaohui Ma [1 ]
Lei Lei [1 ]
Lulu Du [1 ]
Xiaoning Xu [1 ]
Xiangyi Liu [1 ]
Yueting Shi [1 ]
Xingyi Li [1 ]
Deqing Lin [1 ]
机构
[1] Institute of Biomedical Engineering, School of Ophthalmology & Optometry and Eye Hospital, Wenzhou Medical University
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TQ460.1 [基础理论]; TQ427.26 [];
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摘要
Peptide-drug conjugates(PDCs) composed of peptide, spacer and drug have gained extensive attention in the field of drug delivery owing to its precise control over the drug payload and architecture. However,the achievement of controllable and rapid drug release at targeted site by PDCs is still a great challenge for pharmaceutist. Herein, we introduced the histidine residue into PDCs to generate a supramolecular hydrogel via a p H-trigger strategy, which exhibited an autocatalytic effect to precisely tune drug release from PDCs hydrogel. Using indomethacin(Idm) as model drug, various PDCs(Y(Idm)EEH, Y(Idm)EEK and Y(Idm)EER) were synthesized and their self-assembling properties were investigated in terms of critical aggregation concentration(CAC), transmission electron microscopy(TEM) and rheometer. Introduction of histidine residue into PDCs presented a robust catalytic activity on the ester hydrolysis of p-nitrophenyl acetate in aqueous solution, as well conferred the autocatalytic capacity to hydrolyze the PDCs into active parent drug(Idm). Overall, we reported an autocatalytic activity of histidine residue to precisely tune drug release from PDCs hydrogels.
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页码:220 / 224
页数:5
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