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Oncolytic vaccinia virus immunotherapy antagonizes image-guided radiotherapy in mouse mammary tumor models. | LitMetric

AI Article Synopsis

  • Ionizing radiation and oncolytic viruses, like the vaccinia virus (VACV), both aim to trigger an immune response to fight cancer, and this study investigates their combined effects.
  • The combination of image-guided ionizing radiation (IG-IR) and VACV showed some effectiveness in killing cancer cells but delayed use of VACV after IG-IR improved results, suggesting timing is crucial.
  • The presence of VACV after IG-IR altered the immune environment, inhibiting the anti-tumor immune response possibly due to VACV's immunosuppressive properties, indicating careful timing and further research are needed for effective treatment strategies.

Article Abstract

Ionizing radiation (IR) and oncolytic viruses are both used to treat cancer, and the effectiveness of both agents depends upon stimulating an immune response against the tumor. In this study we tested whether combining image guided ionizing radiation (IG-IR) with an oncolytic vaccinia virus (VACV) could yield a better therapeutic response than either treatment alone. ΔF4LΔJ2R VACV grew well on irradiated human and mouse breast cancer cells, and the virus can be combined with 4 or 8 Gy of IR to kill cells in an additive or weakly synergistic manner. To test efficacy in vivo we used immune competent mice bearing orthotopic TUBO mammary tumors. IG-IR worked well with 10 Gy producing 80% complete responses, but this was halved when the tumors were treated with VACV starting 2 days after IG-IR. VACV monotherapy was ineffective in this model. The antagonism was time dependent as waiting for 21 days after IG-IR eliminated the inhibitory effect but without yielding any further benefits over IR alone. In irradiated tumors, VACV replication was also lower, suggesting that irradiation created an environment that did not support infection as well in vivo as in vitro. A study of how four different treatment regimens affected the immune composition of the tumor microenvironment showed that treating irradiated tumors with VACV altered the immunological profiles in tumors exposed to IR or VACV alone. We detected more PD-1 and PD-L1 expression in tumors exposed to IR+VACV but adding an αPD-1 antibody to the protocol did not change the way VACV interferes with IG-IR therapy. VACV encodes many immunosuppressive gene products that may interfere with the ability of radiotherapy to induce an effective anti-tumor immune response through the release of danger-associated molecular patterns. These data suggest that infecting irradiated tumors with VACV, too soon after exposure, may interfere in the innate and linked adaptive immune responses that are triggered by radiotherapy to achieve a beneficial impact.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10947714PMC
http://journals.plos.org/plosone/article?id=10.1371/journal.pone.0298437PLOS

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