The aim of the study was to develop
and evaluate the efficacy of
a functionalized layer-by-layer (LbL) assembled film entrapped with
oxaliplatin (OX) and signal transducer and activator of transcription
3 (STAT3) siRNA in the localized treatment of colon cancer. The LbL
film was prepared by the sequential layering of chitosan (CS) and
alginate to attain desired physical and mechanical properties. The
film was functionalized by coating folic acid-conjugated CS on one
side. On the other side, polycaprolactone was coated as a backing
layer to provide directional drug release. OX was entrapped within
the layers of the film, while STAT3 siRNA was complexed with CS to
form nanoparticles before entrapment in the LbL film. The CS–siRNA
nanoparticles were taken up by the colon carcinoma, Caco-2 cells within
3 h and provided concentration-dependent reduction in STAT3 protein
expression. The functionalized LbL film (F-LbL film) selectively adhered
to the colon cancer tissue in the mice model, whereas the nonfunctionalized
film adhered to the normal colon tissue. The combination of OX and
STAT3 siRNA provided significantly greater tumor regression, survival
rate, and STAT3 protein suppression after localized delivery through
oral administration compared with intravenous administration. Taken
together, the F-LbL film can selectively bind to colon tumors for
localized delivery of drugs to treat colon cancer.
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