In Situ Nanofiber Formation Blocks AXL and GAS6 Binding to Suppress Ovarian Cancer Development

Author:

Yin Han1,Hua Yue1,Feng Songwei1,Xu Yi1,Ding Yue1,Liu Sicong1,Chen Dongsheng2,Du Furong2,Liang Gaolin3ORCID,Zhan Wenjun3,Shen Yang1

Affiliation:

1. Department of Obstetrics and Gynecology Zhongda Hospital School of Medicine Southeast University 87 Dingjiaqiao Nanjing Jiangsu 210009 China

2. State Key Laboratory of Translational Medicine and Innovative Drug Development Jiangsu Simcere Diagnostics Co., Ltd. 699‐18 Xuanwu Avenue Nanjing Jiangsu 210042 China

3. State Key Laboratory of Digital Medical Engineering School of Biological Science and Medical Engineering Southeast University 2 Sipailou Nanjing Jiangsu 210096 China

Abstract

AbstractAnexelekto (AXL) is an attractive molecular target for ovarian cancer therapy because of its important role in ovarian cancer initiation and progression. To date, several AXL inhibitors have entered clinical trials for the treatment of ovarian cancer. However, the disadvantages of low AXL affinity and severe off‐target toxicity of these inhibitors limit their further clinical applications. Herein, by rational design of a nonapeptide derivative Nap‐Phe‐Phe‐Glu‐Ile‐Arg‐Leu‐Arg‐Phe‐Lys (Nap‐IR), a strategy of in situ nanofiber formation is proposed to suppress ovarian cancer growth. After administration, Nap‐IR specifically targets overexpressed AXL on ovarian cancer cell membranes and undergoes a receptor‐instructed nanoparticle‐to‐nanofiber transition. In vivo and in vitro experiments demonstrate that in situ formed Nap‐IR nanofibers efficiently induce apoptosis of ovarian cancer cells by blocking AXL activation and disrupting subsequent downstream signaling events. Remarkably, Nap‐IR can synergistically enhance the anticancer effect of cisplatin against HO8910 ovarian tumors. It is anticipated that the Nap‐IR can be applied in clinical ovarian cancer therapy in the near future.

Funder

National Natural Science Foundation of China

Natural Science Foundation of Jiangsu Province

Publisher

Wiley

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