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dc.contributor.authorShimizu, Kazuhide
dc.contributor.authorKahramanian, Andranik
dc.contributor.authorJabbar, Muzammil Arif Din Abdul
dc.contributor.authorTurna Demir, Fatma
dc.contributor.authorGokyer, Dilan
dc.contributor.authorUthamacumaran, Abicumaran
dc.contributor.authorRajan, Anant
dc.contributor.authorSaad, Mohammad Ahsan
dc.contributor.authorGorham, Joshua
dc.contributor.authorWakimoto, Hiroko
dc.contributor.authorMartuza, Robert L.
dc.contributor.authorRabkin, Samuel D.
dc.contributor.authorHasan, Tayyaba
dc.contributor.authorWakimoto, Hiroaki
dc.date.accessioned2023-09-07T06:33:35Z
dc.date.available2023-09-07T06:33:35Z
dc.date.issued2023
dc.identifier.citationShimizu, K., Kahramanian, A., Jabbar, M. A. D. A., Turna Demir, F., Gokyer, D., Uthamacumaran, A., Rajan, A., Saad, M. A., Gorham, J., Wakimoto, H., Martuza, R., Rabkin, S. D., Hasan, T. & Wakimoto, H. (2023). Photodynamic augmentation of oncolytic virus therapy for central nervous system malignancies. Cancer Letters, 572.en_US
dc.identifier.issn1872-7980
dc.identifier.urihttp://hdl.handle.net/20.500.12566/1753
dc.description.abstractOncolytic viruses (OVs) have emerged as a clinical therapeutic modality potentially effective for cancers that evade conventional therapies, including central nervous system malignancies. Rationally designed combinatorial strategies can augment the efficacy of OVs by boosting tumor-selective cytotoxicity and modulating the tumor microenvironment (TME). Photodynamic therapy (PDT) of cancer not only mediates direct neoplastic cell death but also primes the TME to sensitize the tumor to secondary therapies, allowing for the combination of two potentially synergistic therapies with broader targets. Here, we created G47Δ-KR, clinical oncolytic herpes simplex virus G47Δ that expresses photosensitizer protein KillerRed (KR). Optical properties and cytotoxic effects of G47Δ-KR infection followed by amber LED illumination (peak wavelength: 585–595 nm) were examined in human glioblastoma (GBM) and malignant meningioma (MM) models in vitro. G47Δ-KR infection of tumor cells mediated KR expression that was activated by LED and produced reactive oxygen species, leading to cell death that was more robust than G47Δ-KR without light. In vivo, we tested photodynamic-oncolytic virus (PD-OV) therapy employing intratumoral injection of G47Δ-KR followed by laser light tumor irradiation (wavelength: 585 nm) in GBM and MM xenografts. PD-OV therapy was feasible in these models and resulted in potent anti-tumor effects that were superior to G47Δ-KR alone (without laser light) or laser light alone. RNA sequencing analysis of post-treatment tumor samples revealed PD-OV therapy-induced increases in TME infiltration of variable immune cell types. This study thus demonstrated the proof-of-concept that G47Δ-KR enables PD-OV therapy for neuro-oncological malignancies and warrants further research to advance potential clinical translation.en_US
dc.description.sponsorshipThis work was supported by Meningioma Mommas (to Hiroaki W.) and National Institutes of Health (R01NS032677 to R.L.M. and R01CA160762 to S.D.R.). F.T.D was supported by 2219-International Postdoctoral Research Fellowship Program from the Scientific and Technological Research Council of Turkey (TÜBITAK), ˙ Ankara, Turkey. The authors thank Drs. Bill Farinelli (Massachusetts General Hospital), Fares Nigim (Massachusetts General Hospital), and Kiyoto Takehara (Okayama University) for providing advice on experiments and Dr. Yoichiro Kawamura (MGH) for scientific discussionsen_US
dc.language.isoengen_US
dc.publisherCancer Lettersen_US
dc.rightsinfo:eu-repo/semantics/embargoedAccessen_US
dc.subjectOncolytic herpes simplex virusen_US
dc.subjectOnkolitik herpes simpleks virüsütr_TR
dc.subjectPhotodynamic therapyen_US
dc.subjectFotodinamik terapitr_TR
dc.subjectKillerReden_US
dc.subjectKatilKırmızıtr_TR
dc.subjectGlioblastomaen_US
dc.subjectGlioblastomatr_TR
dc.subjectMalignant meningiomaen_US
dc.subjectMalign menenjiyomtr_TR
dc.titlePhotodynamic augmentation of oncolytic virus therapy for central nervous system malignanciesen_US
dc.typeinfo:eu-repo/semantics/articleen_US
dc.relation.publicationcategoryInternational publicationen_US
dc.identifier.volume572
dc.contributor.orcid0000-0001-8045-8641 [Turna Demir, Fatma]
dc.contributor.abuauthorTurna Demir, Fatma
dc.contributor.yokid166754 [Turna Demir, Fatma]
dc.identifier.PubMedID37619813
dc.identifier.doi10.1016/j.canlet.2023.216363


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