A thermosensitive, physically cross-linked
injectable hydrogel
was formulated for the effective and sustained delivery of disulfiram
(DSF) to the cancer cells as there is no hydrogel formulation available
until now for the delivery of DSF. As we know, hydrogels have an advantage
over other drug delivery systems because of their unique properties,
so we proposed to formulate an injectable hydrogel system for the
sustained delivery of an anticancer drug (DSF) to cancer cells. To
investigate the surface morphology, a scanning electron microscope
study was carried out, and for thermal stability of hydrogels, TGA
(thermogravimetric analysis) and DSC (differential scanning calorimetry)
were performed. The rheological behavior of hydrogels was evaluated
with the increasing temperature and time. These developed hydrogels
possessing excellent biocompatibility could be injected at room temperature
following rapid gel formation at body temperature. The swelling index
and in vitro drug release studies were performed at different pH (6.8
and 7.4) and temperatures (25 and 37 °C). The cell viability
of the blank hydrogel, free DSF solution, and Ch/DSF (chitosan/DSF)-loaded
hydrogel was studied by MTT assay on SMMC-7721 cells for 24 and 48
h, which exhibited higher cytotoxicity in a dose-dependent manner
in contrast to the free DSF solution. Moreover, the cellular uptake
of DSF-loaded hydrogels was observed stronger as compared with free
DSF. Hence, chitosan-based hydrogels loaded with DSF possessing exceptional
properties can be used as a novel injectable anticancer drug for the
sustained delivery of DSF for long-term cancer therapy.
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