RGD4C peptide mediates anti-p21Ras scFv entry into tumor cells and produces an inhibitory effect on the human colon cancer cell line SW480

Chen-Chen Huang; Fang-Rui Liu; Qiang Feng; Xin-Yan Pan; Shu-Ling Song; Ju-Lun Yang

doi:10.1186/s12885-021-08056-4

BMC Cancer (Mar 2021)

RGD4C peptide mediates anti-p21Ras scFv entry into tumor cells and produces an inhibitory effect on the human colon cancer cell line SW480

Chen-Chen Huang,
Fang-Rui Liu,
Qiang Feng,
Xin-Yan Pan,
Shu-Ling Song,
Ju-Lun Yang

Affiliations

Chen-Chen Huang: School of Medicine, Kunming University of Science and Technology
Fang-Rui Liu: School of Medicine, Kunming University of Science and Technology
Qiang Feng: Department of Pathology, 920th Hospital of Joint Logistics Support Force of PLA
Xin-Yan Pan: Department of Pathology, 920th Hospital of Joint Logistics Support Force of PLA
Shu-Ling Song: Department of Pathology, 920th Hospital of Joint Logistics Support Force of PLA
Ju-Lun Yang: School of Medicine, Kunming University of Science and Technology

DOI: https://doi.org/10.1186/s12885-021-08056-4
Journal volume & issue: Vol. 21, no. 1
pp. 1 – 14

Abstract

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Abstract Background We prepared an anti-p21Ras scFv which could specifically bind with mutant and wild-type p21Ras. However, it cannot penetrate the cell membrane, which prevents it from binding to p21Ras in the cytoplasm. Here, the RGD4C peptide was used to mediate the scFv penetration into tumor cells and produce antitumor effects. Methods RGD4C-EGFP and RGD4C-p21Ras-scFv recombinant expression plasmids were constructed to express fusion proteins in E. coli, then the fusion proteins were purified with HisPur Ni-NTA. RGD4C-EGFP was used as reporter to test the factors affecting RGD4C penetration into tumor cell. The immunoreactivity of RGD4C-p21Ras-scFv toward p21Ras was identified by ELISA and western blotting. The ability of RGD4C-p21Ras-scFv to penetrate SW480 cells and colocalization with Ras protein was detected by immunocytochemistry and immunofluorescence. The antitumor activity of the RGD4C-p21Ras-scFv was assessed with the MTT, TUNEL, colony formation and cell migration assays. Chloroquine (CQ) was used an endosomal escape enhancing agent to enhance endosomal escape of RGD4C-scFv. Results RGD4C-p21Ras-scFv fusion protein were successfully expressed and purified. We found that the RGD4C fusion protein could penetrate into tumor cells, but the tumor cell entry of was time and concentration dependent. Endocytosis inhibitors and a low temperature inhibited RGD4C fusion protein endocytosis into cells. The change of the cell membrane potential did not affect penetrability. RGD4C-p21Ras-scFv could penetrate SW480 cells, effectively inhibit the growth, proliferation and migration of SW480 cells and promote this cells apoptosis. In addition, chloroquine (CQ) could increase endosomal escape and improve antitumor activity of RGD4C-scFv in SW480 cells. Conclusion The RGD4C peptide can mediate anti-p21Ras scFv entry into SW480 cells and produce an inhibitory effect, which indicates that RGD4C-p21Ras-scFv may be a potential therapeutic antibody for the treatment of ras-driven cancers.

Published in BMC Cancer

ISSN: 1471-2407 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: http://bmccancer.biomedcentral.com

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