Osteosarcoma
is a common malignant bone tumor that tends to occur
in adolescents, with surgical resection of the tumor tissue as its
standard treatment. After surgery, long-term chemotherapy should be
performed to prevent patients from recrudescence. However, conventional
chemotherapy drugs impose many serious side effects on patients. It
is significant to optimize a chemotherapy drug delivery system. Herein,
we present an injectable self-healing hydrogel carrying curcumin with
pH-responsive drug release and selective toxicity for osteosarcoma
therapy. Amino-gelatin and oxidized starch were synthesized and used
as substrates to prepare hydrogels based on imine linkages. Polymerized
β-CD was synthesized to encapsulate curcumin and incorporate
it into hydrogels. As a dynamic covalent bond, imine linkages endowed
the hydrogel with injectability and self-healing properties. Under
acidic conditions, the hydrogel presented a pH-responsive curcumin
release property due to instable imine linkages, showing a higher
cumulative release of curcumin at pH 6.5 than at pH 7.4. Moreover,
hydrogels could continuously release curcumin for more than 28 days,
featuring a sudden early release and a slow late release. Interestingly,
differentiated from healthy osteoblasts, the hydrogel showed selective
cytotoxicity to osteosarcoma cells and could even accelerate the differentiation
of osteoblasts owing to the incorporation of curcumin. Briefly speaking,
as a drug delivery system, the composite hydrogel can be widely applied
for osteosarcoma treatment.
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