Improving the specific antitumor efficacy of ONC by fusion with N-terminal domain of transferrin

Author:

Qi Jianying12,Ye Xianlong1,Li Lingling12,Bai Haijing12,Xu Cunshuan12

Affiliation:

1. College of Life Science, Henan Normal University , Xinxiang, China

2. Key Laboratory for Cell Differentiation Regulation, Henan Normal University , Xinxiang, China

Abstract

Abstract Onconase (ONC) as a novel anti-tumor drug has a significant killing effect on a variety of tumor cells. Drug delivery system mediated by transferrin (TF) and TF receptor (TfR), which can significantly increase the amount of drug uptake in the tumor cells, enhance the initiative target efficiency of drugs and reduce its toxic side effects. It has been widely used in drug delivery and clinical trials. In this study, the rONC-TFn was expressed in Escherichia coli by linking ONC with the N-terminal domain of TF (TFn). ELISA and competitive binding analysis demonstrated that rONC-TFn can bind to TfR. The rONC-TFn protein showed much higher cytotoxicity to the cultured HepG2 and Hela cells than rONC. These results suggested that the N-terminal domain protein of TF promoted the tumor targeting of ONC, and thus the rONC-TFn fusion protein may be further developed as a potential targeted anti-tumor drug.

Funder

Henan Normal University

National Natural Science Foundation of China

Key Scientific Research Programs of Henan Education Department

Publisher

Oxford University Press (OUP)

Subject

Organic Chemistry,Molecular Biology,Applied Microbiology and Biotechnology,General Medicine,Biochemistry,Analytical Chemistry,Biotechnology

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