Non‐viral Gene Therapy for Melanoma Using Lysenin from Eisenia Foetida

Author:

Ren Min1,Yang Ling1,He Liming1,Wang Jie1,Zhao Wei1,Yang Chunli1,Yang Shuai1,Cheng Hao2,Huang Meijuan3,Gou Maling1ORCID

Affiliation:

1. Department of Biotherapy Cancer Center and State Key Laboratory of Biotherapy West China Hospital Sichuan University Chengdu Sichuan 610041 China

2. Huahang Microcreate Technology Co., Ltd Chengdu Sichuan 610041 China

3. Division of Thoracic Tumor Multimodality Treatment and Department of Medical Oncology Cancer Center West China Hospital Sichuan University Chengdu Sichuan 610041 China

Abstract

AbstractEarthworms, long utilized in traditional medicine, serve as a source of inspiration for modern therapeutics. Lysenin, a defensive factor in the coelom fluid of the earthworm Eisenia fetida, has multiple bioactivities. However, the inherent toxicity of Lysenin as a pore‐forming protein (PFP) restricts its application in therapy. Here, a gene therapy strategy based on Lysenin for cancer treatment is presented. The formulation consists of polymeric nanoparticles complexed with the plasmid encoding Lysenin. After transfection in vitro, melanoma cells can express Lysenin, resulting in necrosis, autophagy, and immunogenic cell death. The secretory signal peptide alters the intracellular distribution of the expressed product of Lysenin, thereby potentiating its anticancer efficacy. The intratumor injection of Lysenin gene formulation can efficiently kill the transfected melanoma cells and activate the antitumor immune response. Notably, no obvious systemic toxicity is observed during the treatment. Non‐viral gene therapy based on Lysenin derived from Eisenia foetida exhibits potential in cancer therapy, which can inspire future cancer therapeutics.

Funder

Natural Science Foundation of Sichuan Province

Publisher

Wiley

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