Hyperacute rejection-engineered oncolytic virus for interventional clinical trial in refractory cancer patients

Liping Zhong, Lu Gan(Theranostics (New Zealand)), Bing Wang(Second Xiangya Hospital of Central South University), Liang Cao(The First People's Hospital of Changde), Fei Yao(The First Affiliated Hospital of Guangxi University of Traditional Chinese Medicine), Wenlin Gong(Theranostics (New Zealand)), Hongmei Peng(The First People's Hospital of Changde), Zhiming Deng(The First People's Hospital of Changde), Guoyou Xiao(Tumor Hospital of Guangxi Medical University), Xiyu Liu(Theranostics (New Zealand)), Jintong Na(Theranostics (New Zealand)), Desong Xia(Theranostics (New Zealand)), Xianjun Yu(Fudan University Shanghai Cancer Center), Zhikun Zhang(Theranostics (New Zealand)), Xiang Bangde(Tumor Hospital of Guangxi Medical University), Yu Huo(Theranostics (New Zealand)), Dan Yan(The First Affiliated Hospital of Guangxi University of Traditional Chinese Medicine), Zhixin Dong(The First Affiliated Hospital of Guangxi University of Traditional Chinese Medicine), Fang Fang(The First Affiliated Hospital of Guangxi University of Traditional Chinese Medicine), Yun Ma(Tumor Hospital of Guangxi Medical University), Guanqiao Jin(Tumor Hospital of Guangxi Medical University), Danke Su(Tumor Hospital of Guangxi Medical University), Xiuli Liu(Theranostics (New Zealand)), Rui Li(Tumor Hospital of Guangxi Medical University), H Liao(Tumor Hospital of Guangxi Medical University), Chao Tang(Theranostics (New Zealand)), Jian He(Theranostics (New Zealand)), Zhiping Tang(First Affiliated Hospital of GuangXi Medical University), Shilai Zhang(Tumor Hospital of Guangxi Medical University), Bingqing Qiu(Tumor Hospital of Guangxi Medical University), Zhi Yang(Tumor Hospital of Guangxi Medical University), Lihui Yang(Guangxi Medical University), Ziqin Chen(The First People's Hospital of Changde), Mengsi Zeng(The First People's Hospital of Changde), Ronghua Feng(The First People's Hospital of Changde), Jie-ge Jiao(Tropical Bioscience and Biotechnology Research Institute), Yuan Liao(Theranostics (New Zealand)), Tinghua Wang(Theranostics (New Zealand)), Liangliang Wu(Theranostics (New Zealand)), Zhengcheng Mi(Theranostics (New Zealand)), Ziqun Liu(Central South University), Si Shi(Fudan University Shanghai Cancer Center), Kun Zhang, Wei Shi, Yongxiang Zhao
Cell
January 17, 2025
Cited by 82Open Access
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Abstract

Recently, oncolytic virus (OV) therapy has shown great promise in treating malignancies. However, intravenous safety and inherent lack of immunity are two significant limitations in clinical practice. Herein, we successfully developed a recombinant Newcastle disease virus with porcine α1,3GT gene (NDV-GT) triggering hyperacute rejection. We demonstrated its feasibility in preclinical studies. The intravenous NDV-GT showed superior ability to eradicate tumor cells in our innovative CRISPR-mediated primary hepatocellular carcinoma monkeys. Importantly, the interventional clinical trial treating 20 patients with relapsed/refractory metastatic cancer (Chinese Clinical Trial Registry of WHO, ChiCTR2000031980) showed a high rate (90.00%) of disease control and durable responses, without serious adverse events and clinically functional neutralizing antibodies, further suggesting that immunogenicity is minimal under these conditions and demonstrating the feasibility of NDV-GT for immunovirotherapy. Collectively, our results demonstrate the high safety and efficacy of intravenous NDV-GT, thus providing an innovative technology for OV therapy in oncological therapeutics and beyond.


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