Human papillomavirus associated head and neck cancer (HPVâ+âHNC) is rising globally, emphasizing the need for improved therapeutic and screening strategies. To test novel therapies and study HPV-related disease progression, it is vital to develop relevant preclinical models. However, many fail to address critical concerns, including generating a representative immune microenvironment and adequately modeling HPV-driven malignant transformation. Recent multi-omics studies reveal the significance of HPV integration location in HPV-related carcinogenesis and highlight the necessity of targeted treatment methods. Thus, we have developed a murine model of HPV16â+âHNC modifying the published CRISPR-based Somatic Oncogene kNock-In for Cancer Modeling (CRISPR-SONIC) system for precise integration of HPV oncogenes. We showed that CRISPR-SONIC knock-in of Kras(G12D), HPV16 E6 and E7, and a luciferase reporter at the murine β-actin 3'-UTR locus could induce spontaneous buccal tumors with sarcomatous morphology under transient or selective immunosuppression. Both preventative and therapeutic pNGVL4a-CRT/E7(detox) DNA vaccination could induce HPV16 E7-specific immune response and reduce tumor growth. Furthermore, CRISPR-SONIC knock-in of HPV16 E6 and E7 with co-delivery of HNC-relevant oncogenes AKT and c-Myc produced tumors in NSG mice capturing the characteristic carcinomic morphology of HPVâ+âHNC. Overall, our model offers a robust platform for evaluating new therapies and exploring HPV-related carcinogenesis.
Generation of a spontaneous murine HPVâ+âoral cancer model with site-specific oncogene insertion using CRISPR-SONIC.
利用 CRISPR-SONIC 技术,通过位点特异性癌基因插入,构建自发性小鼠 HPV+ 口腔癌模型
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作者:Tao Julia, Murray Jason, Tu Hsin-Fang, Fan Darrell, Tsai Ya-Chea, Hu Ming-Hung, Wu Annie A, Xing Deyin, Hung Chien-Fu, Wu T-C
| 期刊: | Cell and Bioscience | 影响因子: | 6.200 |
| 时间: | 2025 | 起止号: | 2025 Jun 18; 15(1):84 |
| doi: | 10.1186/s13578-025-01427-5 | 研究方向: | 肿瘤 |
| 疾病类型: | 口腔癌 | ||
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