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Oncolytic virus OVV-03 enhances CAR-T cell therapy against glioblastoma via immune modulation and specific HER2 upregulation.

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Oncoimmunology 📖 저널 OA 100% 2025: 71/71 OA 2026: 27/27 OA 2025~2026 2026 Vol.15(1) p. 2612377 cited 1 OA Virus-based gene therapy research
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PubMed DOI PMC OpenAlex 마지막 보강 2026-04-28
OpenAlex 토픽 · Virus-based gene therapy research CAR-T cell therapy research Viral Infectious Diseases and Gene Expression in Insects

Tang Y, E Q, Ma L, Li X, Zhang Y, Wang W

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Glioblastoma (GBM) remains therapeutically challenging due to treatment resistance and immunosuppression.

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APA Yi Tang, E Qinzhi, et al. (2026). Oncolytic virus OVV-03 enhances CAR-T cell therapy against glioblastoma via immune modulation and specific HER2 upregulation.. Oncoimmunology, 15(1), 2612377. https://doi.org/10.1080/2162402X.2025.2612377
MLA Yi Tang, et al.. "Oncolytic virus OVV-03 enhances CAR-T cell therapy against glioblastoma via immune modulation and specific HER2 upregulation.." Oncoimmunology, vol. 15, no. 1, 2026, pp. 2612377.
PMID 41496551 ↗

Abstract

Glioblastoma (GBM) remains therapeutically challenging due to treatment resistance and immunosuppression. Oncolytic virotherapy offers a promising strategy. This study engineered OVV-03, a novel HER2-armed oncolytic vesicular stomatitis virus (VSV), and evaluated its efficacy against GBM. OVV-03 demonstrated potent infectivity and cytotoxicity in GBM cell lines and patient-derived cells, inducing caspase-dependent apoptosis and suppressing proliferation/clonogenicity. In murine GBM models, OVV-03 significantly suppressed tumor growth, improved survival, and enhanced CD8⁺ T cell infiltration. Single-cell RNA sequencing revealed OVV-03 remodels the tumor immune microenvironment by boosting cytotoxic T cell activity and inhibiting immunosuppressive pathways, notably PD-L1/PD-1 signaling. Mechanistically, OVV-03 downregulated PD-L1 by inhibiting the JNK-c-Fos/c-Jun axis, reversible by TNF- stimulation. Critically, OVV-03 synergized with B7H3- or HER2-targeted CAR-T cells, inducing superior tumor regression and prolonged survival in orthotopic models. These findings demonstrate that OVV-03 exerts potent antitumor effects through direct oncolysis and immune activation, including PD-L1 modulation. Its synergistic combination with CAR-T cells highlights OVV-03 as a highly promising oncolytic immunovirotherapy platform for GBM.

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