Publication:
Pulsed radiotherapy to mitigate high tumor burden and generate immune memory

dc.contributor.coauthorBarsoumian, H.B.
dc.contributor.coauthorHe, K.
dc.contributor.coauthorHu, Y.
dc.contributor.coauthorWang, Q.
dc.contributor.coauthorAbana, C.O.
dc.contributor.coauthorPuebla-Osorio, N.
dc.contributor.coauthorHsu, E.Y.
dc.contributor.coauthorWasley, M.
dc.contributor.coauthorMasrorpour, F.
dc.contributor.coauthorWang, J.
dc.contributor.coauthorCortez, M.A.
dc.contributor.coauthorWelsh, J.W.
dc.contributor.departmentSchool of Medicine
dc.contributor.kuauthorSezen, Duygu
dc.contributor.schoolcollegeinstituteSCHOOL OF MEDICINE
dc.date.accessioned2024-11-09T12:14:24Z
dc.date.issued2022
dc.description.abstractRadiation therapy (XRT) has a well-established role in cancer treatment. Given the encouraging results on immunostimulatory effects, radiation has been increasingly used with immune-check-point inhibitors in metastatic disease, especially when immunotherapy fails due to tumor immune evasion. We hypothesized that using high-dose stereotactic radiation in cycles (pulses) would increase T-cell priming and repertoire with each pulse and build immune memory in an incremental manner. To prove this hypothesis, we studied the combination of anti-CTLA-4 and Pulsed radiation therapy in our 344SQ non-small cell lung adenocarcinoma murine model. Primary and secondary tumors were bilaterally implanted in 129Sv/Ev mice. In the Pulsed XRT group, both primary and secondary tumors received 12Gyx2 radiation one week apart, and blood was collected seven days afterwards for TCR repertoire analysis. As for the delayed-Pulse group, primary tumors received 12Gyx2, and after a window of two weeks, the secondary tumors received 12Gyx2. Blood was collected seven days after the second cycle of radiation. The immunotherapy backbone for both groups was anti-CTLA-4 antibody to help with priming. Treatment with Pulsed XRT + anti-CTLA-4 led to significantly improved survival and resulted in a delayed tumor growth, where we observed enhanced antitumor efficacy at primary tumor sites beyond XRT + anti-CTLA-4 treatment group. More importantly, Pulsed XRT treatment led to increased CD4+ effector memory compared to single-cycle XRT. Pulsed XRT demonstrated superior efficacy to XRT in driving antitumor effects that were largely dependent on CD4+ T cells and partially dependent on CD8+ T cells. These results suggest that combinatorial strategies targeting multiple points of tumor immune evasion may lead to a robust and sustained antitumor response.
dc.description.fulltextYES
dc.description.indexedbyWOS
dc.description.indexedbyScopus
dc.description.indexedbyPubMed
dc.description.openaccessYES
dc.description.publisherscopeInternational
dc.description.sponsoredbyTubitakEuN/A
dc.description.sponsorshipThis work was supported in part by Cancer Center Support (Core) Grant P30 CA016672 from the National Cancer Institute, National Institutes of Health, to The University of Texas MD Anderson Cancer Center.
dc.description.versionPublisher version
dc.description.volume13
dc.identifier.doi10.3389/fimmu.2022.984318
dc.identifier.embargoNO
dc.identifier.filenameinventorynoIR04048
dc.identifier.issn1664-3224
dc.identifier.quartileQ1
dc.identifier.scopus2-s2.0-85140268792
dc.identifier.urihttps://hdl.handle.net/20.500.14288/1289
dc.identifier.wos874226400001
dc.keywordsImmune memory
dc.keywordsImmunotherapy
dc.keywordsLung cancer
dc.keywordsPulsed radiation
dc.keywordsRadiotherapy
dc.language.isoeng
dc.publisherFrontiers
dc.relation.grantnoNA
dc.relation.ispartofFrontiers in Immunology
dc.relation.urihttp://cdm21054.contentdm.oclc.org/cdm/ref/collection/IR/id/10923
dc.subjectImmunology
dc.titlePulsed radiotherapy to mitigate high tumor burden and generate immune memory
dc.typeJournal Article
dspace.entity.typePublication
local.contributor.kuauthorSezen, Duygu
local.publication.orgunit1SCHOOL OF MEDICINE
local.publication.orgunit2School of Medicine
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