<P>Background: Despite new agent development and short-term benefits in patients with
Colorectal Cancer (CRC), metastatic CRC cure rates have not improved due to high rates of
oxaliplatin resistance and toxicity. There is an urgent need for effective tools to prevent and treat
CRC and reduce morbidity and mortality of CRC patients. Exploring the effects of bioactive
peptides on the antitumor to CRC was of vital importance to the clinical application.
</P><P>
Objective: This study aimed to investigate the therapeutic impact of Anticancer Bioactive Peptides
(ACBP) on anticancer effect of oxaliplatin (LOHP) in human colorectal cancer xenografts models
in nude mice.
</P><P>
Methods: HCT-116 cells were cultured in vitro via CCK-8 assays and the absorbance was
measured at 450 nm. Apoptosis and cell cycle were assessed by Flow Cytometry (FCM) in vitro.
HCT-116 human colorectal cancer cells inoculated subcutaneously in nude mice of treatment with
PBS (GG), ACBP, LOHP, ACBP+LOHP (A+L) in vivo. The quality of life was assessed by dietary
amount of nude mice, the weight of nude mice, inhibition rates, tumor weight and tumor volume.
Immunohistochemistry and RT-qPCR method was conducted to determine the levels of apoptosisregulating
proteins/genes in transplanted tumors.
</P><P>
Results: ACBP induced substantial reductions in viable cell numbers and apoptosis of HCT116
cells in combined with LOHP in vitro. Compared with the control GG group, ACBP combined low
dose oxaliplatin (U) group demonstrated significantly different tumor volume, the rate of apoptosis,
the expression levels of Cyt-C, caspase-3,8,9 proteins and corresponding RNAs (P<0.05). The
expression of pro-apoptotic proteins in the cytoplasm around the nucleus was significantly
enhanced by ACBP. Short term intermittent use of ACBP alone indicted a certain inhibitory effect
on tumor growth, and improve the quality of life of tumor bearing nude mice.
</P><P>
Conclusion: ACBP significantly increased the anti-cancer responses of low dose oxaliplatin
(L-LOHP), thus, significantly improving the quality of life of tumor-bearing nude mice.</P>
Development of an orthotopic transplantation model in nude mice that simulates the clinical features of human lung cancer
