Engineered T cells secreting αB7-H3-αCD3 bispecific engagers for enhanced anti-tumor activity against B7-H3 positive multiple myeloma: a novel therapeutic approach

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dc.contributor.authorRujirachaivej P.
dc.contributor.authorSiriboonpiputtana T.
dc.contributor.authorChoomee K.
dc.contributor.authorSupimon K.
dc.contributor.authorSangsuwannukul T.
dc.contributor.authorSongprakhon P.
dc.contributor.authorNatungnuy K.
dc.contributor.authorLuangwattananun P.
dc.contributor.authorYuti P.
dc.contributor.authorJunking M.
dc.contributor.authorYenchitsomanus P.T.
dc.contributor.correspondenceRujirachaivej P.
dc.contributor.otherMahidol University
dc.date.accessioned2025-01-28T18:18:18Z
dc.date.available2025-01-28T18:18:18Z
dc.date.issued2025-01-13
dc.description.abstractBACKGROUND: Multiple myeloma (MM) is an incurable plasma cell malignancy with increasing global incidence. Chimeric antigen receptor (CAR) T-cell therapy targeting BCMA has shown efficacy in relapsed or refractory MM, but it faces resistance due to antigen loss and the tumor microenvironment. Bispecific T-cell engaging (BITE) antibodies also encounter clinical challenges, including short half-lives requiring continuous infusion and potential toxicities. METHODS: To address these issues, we developed a lentiviral system to engineer T cells that secrete αB7-H3-αCD3 bispecific engager molecules (αB7-H3-αCD3 ENG-T cells). We evaluated their effectiveness against MM cells with varying B7-H3 expression levels, from B7-H3neg to B7-H3high. RESULTS: The αB7-H3-αCD3 ENG-T cells demonstrated significant anti-tumor activity against MM cell lines expressing B7-H3. SupT-1 cells (B7-H3neg) served as controls and exhibited minimal cytotoxicity from αB7-H3-αCD3 ENG T cells. In contrast, these engineered T cells showed dose-dependent killing of B7-H3-expressing MM cells: NCI-H929 (B7-H3low), L-363 (B7-H3medium), and KMS-12-PE (B7-H3high). For NCI-H929 cells, cytotoxicity reached 38.5 ± 7.4% (p = 0.0212) and 54.0 ± 9.2% (p = 0.0317) at effector-to-target (E:T) ratios of 5:1 and 10:1, respectively. Against L-363 cells, cytotoxicity was 56.6 ± 3.2% (p < 0.0001) and 71.4 ± 5.2% (p = 0.0002) at E:T ratios of 5:1 and 10:1, respectively. For KMS-12-PE cells, significant cytotoxic effects were observed even at an E:T ratio of 1:1, with 27.2 ± 3.7% (p = 0.0004), 44.4 ± 3.7% (p < 0.0001), and 68.6 ± 9.2% (p = 0.0004) cytotoxicity at E:T ratios of 1:1, 5:1, and 10:1, respectively. CONCLUSIONS: These results indicate that αB7-H3-αCD3 ENG T cells could be a promising therapy for B7-H3-positive MM. They may enhance current MM treatments and improve overall outcomes. Additional preclinical and clinical research is required to fully assess their therapeutic potential.
dc.identifier.citationJournal of translational medicine Vol.23 No.1 (2025) , 54
dc.identifier.doi10.1186/s12967-024-05923-z
dc.identifier.eissn14795876
dc.identifier.pmid39806405
dc.identifier.scopus2-s2.0-85215558670
dc.identifier.urihttps://repository.li.mahidol.ac.th/handle/20.500.14594/103092
dc.rights.holderSCOPUS
dc.subjectBiochemistry, Genetics and Molecular Biology
dc.titleEngineered T cells secreting αB7-H3-αCD3 bispecific engagers for enhanced anti-tumor activity against B7-H3 positive multiple myeloma: a novel therapeutic approach
dc.typeArticle
mu.datasource.scopushttps://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85215558670&origin=inward
oaire.citation.issue1
oaire.citation.titleJournal of translational medicine
oaire.citation.volume23
oairecerif.author.affiliationSiriraj Hospital
oairecerif.author.affiliationMayo Clinic in Rochester, Minnesota
oairecerif.author.affiliationFaculty of Medicine Ramathibodi Hospital, Mahidol University

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