Development of attenuated Orf virus as a safe oncolytic viral vector for nasopharyngeal carcinoma treatment.

IF 4 3区医学 Q2 VIROLOGY

Virology Journal Pub Date : 2025-02-25 DOI:10.1186/s12985-025-02672-3

Yumiko Yamada, Yu-Chih Wang, Hao-Ping Liu, Greg Ryan Gerongano, Ching-Yu Tseng, Shu-Chen Liu, Guan-Ru Liao, Chao-Chin Chang, Jiunn-Wang Liao, Mei-Lin Wang, Yuan-Yen Chang, Fong-Yuan Lin, Wei-Li Hsu

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引用次数: 0

Abstract

Background: Orf virus (ORFV) is gaining attention as a promising viral vector for cancer therapy because of its unique properties. Recent studies have shown that ORFV could be effective against various cancers, particularly nasopharyngeal carcinoma. This research explores the ability of wild-type ORFV and recombinant ORFVs, which lack specific virulence factors, to kill NPC cells and modulate the immune response.

Methods: Two NPC cell lines, HK1 (from Hong Kong) and TW02 (from Taiwan), were infected with wild-type ORFV and two recombinant ORFVs lacking either vascular endothelial growth factor (VEGF) or chemokine binding protein (CBP) virulence factors. The oncolytic effects were evaluated by assessing cell death pathways, particularly pyroptosis, which was monitored through the cleavage of gasdermin E (GSDME). The activation of survival pathways, such as focal adhesion kinase (FAK) and AKT, was also analyzed. In addition, the influence of ORFV infection on natural killer (NK) cell recruitment and cytotoxicity was investigated. In vivo experiments were conducted in a xenograft mouse model in which HK1 tumors were used to evaluate the antitumor activity of wild-type ORFV and two deletion-mutant ORFVs.

Results: Wild-type ORFV effectively killed NPC cells, especially HK1 cells. The recombinant ORFVs, despite being attenuated by the loss of VEGF or CBP, retained the ability to infect and cause NPC cell death, with the CBP-deleted virus showing notable effectiveness in HK1 cells. Early ORFV infection led to pyroptosis via GSDME cleavage, causing cell detachment and a reduction in FAK and AKT activation. ORFV also enhanced NK cell recruitment and boosted NK cell-mediated cytotoxicity in infected NPC cells. In the HK1 xenograft model, CBP-deleted ORFV significantly inhibited tumor growth.

Conclusion: ORFV, particularly the wild-type and CBP-deleted variants, has significant potential as an oncolytic viral vector for NPC therapy. It induces cell death via pyroptosis and enhances immune-mediated tumor cell destruction through NK cells. The attenuated CBP-deleted ORFV offers a safer and effective option for cancer treatment, making it a promising candidate for future therapeutic applications.

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作为鼻咽癌治疗安全溶瘤病毒载体的减毒Orf病毒的研制。

背景：Orf病毒（ORFV）由于其独特的性质，作为一种有前景的癌症治疗病毒载体而受到关注。最近的研究表明，ORFV可能对各种癌症，特别是鼻咽癌有效。本研究探讨了缺乏特异性毒力因子的野生型ORFV和重组型ORFV杀伤鼻咽癌细胞和调节免疫应答的能力。方法：用野生型ORFV和重组型ORFV分别感染2株鼻咽癌细胞株HK1（香港）和TW02（台湾），ORFV分别缺乏血管内皮生长因子（VEGF）和趋化因子结合蛋白（CBP）毒力因子。通过评估细胞死亡途径来评估溶瘤作用，特别是通过气皮蛋白E （GSDME）的裂解来监测焦亡。我们还分析了存活通路的激活情况，如局灶黏附激酶（FAK）和AKT。此外，研究了ORFV感染对自然杀伤细胞（NK）募集和细胞毒性的影响。采用HK1肿瘤异种移植小鼠模型进行体内实验，评价野生型ORFV和两种缺失突变型ORFV的抗肿瘤活性。结果：野生型ORFV能有效杀伤鼻咽癌细胞，尤其是HK1细胞。重组ORFVs，尽管由于VEGF或CBP的缺失而减弱，但保留了感染和导致鼻咽癌细胞死亡的能力，CBP缺失的病毒在HK1细胞中显示出显著的有效性。早期ORFV感染通过GSDME切割导致细胞凋亡，导致细胞脱离，FAK和AKT活性降低。ORFV还能增强NK细胞募集，增强NK细胞介导的鼻咽癌细胞毒性。在HK1异种移植模型中，cbp缺失的ORFV显著抑制肿瘤生长。结论：ORFV，特别是野生型和cbp缺失的变体，具有作为鼻咽癌治疗溶瘤病毒载体的巨大潜力。它通过焦亡诱导细胞死亡，并通过NK细胞增强免疫介导的肿瘤细胞破坏。减毒的cbp缺失ORFV为癌症治疗提供了一种更安全有效的选择，使其成为未来治疗应用的有希望的候选者。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Virology Journal 医学-病毒学

CiteScore

7.40

自引率

2.10%

发文量

186

审稿时长

1 months

期刊介绍： Virology Journal is an open access, peer reviewed journal that considers articles on all aspects of virology, including research on the viruses of animals, plants and microbes. The journal welcomes basic research as well as pre-clinical and clinical studies of novel diagnostic tools, vaccines and anti-viral therapies. The Editorial policy of Virology Journal is to publish all research which is assessed by peer reviewers to be a coherent and sound addition to the scientific literature, and puts less emphasis on interest levels or perceived impact.