Publication:
Switchable CAR T cell strategy against osteosarcoma

dc.contributor.authorHidalgo, Laura
dc.contributor.authorSomovilla-Crespo, Beatriz
dc.contributor.authorGarcía-Rodriguez, Patricia
dc.contributor.authorMorales-Molina, Alvaro
dc.contributor.authorRodriguez-Milla, Miguel A
dc.contributor.authorGarcia-Castro, Javier
dc.contributor.funderInstituto de Salud Carlos III
dc.contributor.funderAsociación Pablo Ugarte contra el cáncer infantil
dc.contributor.funderFundación Oncohematología Infantil
dc.contributor.funderAsociación de Familias de Niños con Cáncer de Castilla-La Mancha
dc.contributor.funderComunidad de Madrid (España)
dc.date.accessioned2023-05-12T13:06:24Z
dc.date.available2023-05-12T13:06:24Z
dc.date.issued2023-04-16
dc.description.abstractImmunotherapy with chimeric antigen receptor T (CAR T) cells has changed the treatment of hematological malignances, but they are still a challenge for solid tumors, including pediatric sarcomas. Here, we report a switchable CAR T cell strategy based on anti-FITC CAR T cells and a switch molecule conjugated with FITC for targeting osteosarcoma (OS) tumors. As a potential target, we analyzed the expression of B7-H3, an immune checkpoint inhibitor, in OS cell lines. In addition, we evaluate the capacity of an anti-B7-H3 monoclonal antibody conjugated with FITC (anti-B7-H3-FITC mAb) to control the antitumor activity of anti-FITC CAR T cells. The effector functions of anti-FITC CAR T cells against OS, measured in vitro by tumor cell killing activity and cytokine production, are dependent on the presence of the anti-B7-H3-FITC mAb switch. Moreover, OS cells stimulate anti-FITC CAR T cells migration. In vivo, anti-B7-H3 mAb penetrates in the tumor and binds 143B OS tumor cells. Furthermore, anti-FITC CAR T cells reach tumor region and exert antitumor effect in an OS NSG mouse model only in the presence of the switch molecule. We demonstrate that anti-B7-H3-FITC mAb redirects the cytotoxic activity of anti-FITC CAR T cells against OS tumors suggesting that switchable CAR T cell platforms might be a plausible strategy against OS.es_ES
dc.description.peerreviewedes_ES
dc.description.sponsorshipThis research was funded by Instituto de Salud Carlos III (ISCIII): PI20CIII-00040 and RD21/0017/0005, Red Española de Terapias Avanzadas TERAV-ISCIII (NextGenerationEU. Plan de Recuperación Transformación y Resiliencia), the Asociación Pablo Ugarte, the Fundación Oncohematología Infantil and AFANION for grants support. LH is benefciary of a grant under the Talent Attraction Program of the Comunidad de Madrid (2018-T2/BMD-10337). AM-M is benefciary of a grant under the PhD ISCIII-PFIS program (FI18CIII/00017) and is a member of the PhD Program in Molecular Biosciences of Universidad Autónoma de Madrid. PR-G is enrolled in the Doctoral Program in Biomedical Sciences and Public Health as a trainee researcher at the UNED International Doctoral School. AntiFITC CAR single chain variable fragment (scFv) encoding plasmid was kindly provided by Dr. Michael Jensen from Seattle Children´s Research Institute, Washington, USA. The authors wish to thank the donors, and the Biobank Hospital Universitario Puerta de Hierro Majadahonda (HUPHM)/Instituto de Investigación Sanitaria Puerta de Hierro-Segovia de Arana (IDIPHISA) (PT17/0015/0020 in the Spanish National Biobanks Network) for the human specimens used in this study. Images for the graphical scheme of experiments were obtained and modifed from SMART—Servier Medical Art under a Creative Common Attribution 3.0 Unported License.es_ES
dc.format.number8
dc.format.page2623-2633
dc.format.volume72
dc.identifier.citationCancer Immunol Immunother. 2023 Aug;72(8):2623-2633.es_ES
dc.identifier.doi10.1007/s00262-023-03437-zes_ES
dc.identifier.e-issn1432-0851es_ES
dc.identifier.journalCancer immunology, immunotherapy : CIIes_ES
dc.identifier.pubmedID37062034es_ES
dc.identifier.urihttp://hdl.handle.net/20.500.12105/16059
dc.language.isoenges_ES
dc.publisherSpringer
dc.relation.projectFECYTinfo:eu-repo/grantAgreement/ES/PT17/0015/0020es_ES
dc.relation.projectFISinfo:fis/Instituto de Salud Carlos III/Programa Estatal de Generación de Conocimiento y Fortalecimiento del Sistema Español de I+D+I/Subprograma Estatal de Generación de Conocimiento/PI20-ISCIII Modalidad Proyectos de Investigacion en Salud Intramurales. (2020)/PI20CIII/00040es_ES
dc.relation.projectFISinfo:eu-repo/grantAgreement/ES/RD21/0017/0005es_ES
dc.relation.projectFISinfo:eu-repo/grantAgreement/ES/FI18CIII/00017es_ES
dc.relation.publisherversionhttps://doi.org/10.1007/s00262-023-03437-zes_ES
dc.repisalud.centroISCIII::Instituto de Investigación de Enfermedades Raras (IIER)es_ES
dc.repisalud.institucionISCIIIes_ES
dc.rights.accessRightsopen accesses_ES
dc.rights.licenseAtribución 4.0 Internacional*
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/*
dc.subjectB7-H3es_ES
dc.subjectCAR Tes_ES
dc.subjectImmunotherapyes_ES
dc.subjectOsteosarcomaes_ES
dc.titleSwitchable CAR T cell strategy against osteosarcomaes_ES
dc.typeresearch articlees_ES
dc.type.hasVersionVoRes_ES
dspace.entity.typePublication
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