Molecular design and anti-melanoma activity of a novel bullfrog antibacterial peptide RGD-chimera

Mengyue Liu; Xuan Jiang; Chao Fu; Ruili Zhao; Tianming Jin; Jifei Ma; Shunyi Qin; Liu An Li; Ye Hu; Xin Zhang

doi:10.3892/ol.2020.12376

Molecular design and anti-melanoma activity of a novel bullfrog antibacterial peptide RGD-chimera

Oncol Lett. 2021 Feb;21(2):115. doi: 10.3892/ol.2020.12376. Epub 2020 Dec 15.

Authors

Mengyue Liu¹, Xuan Jiang¹, Chao Fu¹, Ruili Zhao¹, Tianming Jin¹, Jifei Ma¹, Shunyi Qin¹, Liu An Li¹, Ye Hu¹, Xin Zhang¹

Affiliation

¹ Tianjin Key Laboratory of Agricultural Animal Breeding and Healthy Husbandry, College of Animal Science and Veterinary Medicine, Tianjin Agricultural University, Tianjin 300384, P.R. China.

Abstract

Melanoma is a common malignant skin tumor, which is the only fatal skin tumor at present. Melanoma has a high degree of malignancy and metastasis. The activity of modified Temporin-La (T-La) peptides from bullfrog skin were evaluated for antitumor activity and improved targeting in melanoma cells. The amino acid sequence of T-La was modified, resulting in the antitumor peptide, T-La (FS). T-La and T-La (FS) were coupled to the RGD small molecule polypeptide to form the chimeric peptides RGD-T-La and RGD-T-La (FS), respectively. The secondary structures for the peptides, evaluated using circular dichroism, were found to be α-helical. The structure of T-La was evaluated using bioinformatics. In addition, the antitumor effects of the modified peptide and the targeting of RGD chimeric peptide to the tumor in vivo and in vitro were analyzed. Antitumor activity was measured in vitro using the MTT assay. Tumor cells with high integrin αvβ3 expression were detected using flow cytometry, and tumor cells were screened for sensitivity to RGD-T-La (FS) to establish a tumor model in nude mice. The effects of the peptides on tumor cells were measured using laser confocal microscopy in real-time. The mechanism of the peptide antitumor activity in tumor cells was evaluated with scanning electron microscopy. B16 melanoma cells were the most sensitive to the peptides, for which the cell survival rate was 24.65% for 10 µg/ml RGD-T-La (FS). RGD-La (FS) had a rapid effect on tumor cells. RGD chimeric polypeptides exhibited site-targeting cytotoxic effects in tumor cells. In the B16 melanoma mouse model, the peptides exhibited antitumor effects against early melanoma development and induced tumor apoptosis, possibly by inhibiting VEGF and promoting caspase-3 expression. Overall, the present study provides a scientific basis for the application of small molecule antimicrobial peptides as targeted antitumor agents and lays the foundation for the clinical application of these peptides as antitumor drugs.

Keywords: RGD-chimera; antitumor effect; antitumor peptide; melanoma cells; targeting.