Metformin
(MET) is a common treatment for type II diabetes. Here,
we demonstrate the anticancer activity of a polymeric metformin derivative.
We successfully synthesized the polypeptide (poly-l-lysine
[PLL]) derivative of metformin (LysMET) and demonstrated its capacity
as an anticancer therapeutic and gene carrier. miRNA-320a was loaded
into the cationic LysMET and enveloped in a lipid bilayer, and a MUC1-specific
aptamer was conjugated to the surface (A-Lipo@mLysMET). The LysMET-containing
guanidine moiety was more tolerable than the secondary amine-containing
PLL. LysMET showed similar efficacy to MET in the induction of HT-29
tumor suppression, indicating the importance of the biguanide moiety.
The synergistic effect of miRNA-320a and LysMET treatment significantly
decreased cell viability compared with LysMET treatment alone, which
was attributed to the role of miRNA in the β-catenin pathway.
A-Lipo@mLysMET showed excellent antitumor efficacy and significantly
reduced the tumor burden in all groups. AMPKα phosphorylation
was markedly increased by LysMET compared with the control, with significant
inhibition of the mTOR pathway. The TUNEL assay showed that apoptosis
was the main mechanism responsible for cancer cell death and that
A-Lipo@mLysMET resulted in the highest proportion of TUNEL-positive
cells (∼36%). No noticeable organ damage was observed after
treatment with either LysMET or A-Lipo@mLysMET, confirming the excellent
safety profile of guanide-modified polymers. Overall, we demonstrated
the feasibility of LysMET for the effective control of tumor progression
as well as its dual role, as both a drug and a gene carrier.
Various dipyrazolylmethanes were synthesized and nitro-substituted compound displayed an excellent turn-off fluorescence sensing property for the detection of Cu2+ ions.
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