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Specifically activated memory T cell subsets from cancer patients recognize and reject xenotransplanted autologous tumors
113
Citations
35
References
2004
Year
Cell TherapyT-regulatory CellImmunologyImmune RegulationImmunoeditingImmunotherapeuticsCancer PatientsImmunotherapyCancer BiologyTumor BiologyTumor ImmunityCancer Cell BiologyBone MarrowRadiation OncologyCell TransplantationCancer ResearchTumor InfiltrationMedicineImmune SurveillanceT Cell ImmunityTumor TargetingCell BiologyMalignant DiseaseTumor MicroenvironmentCancer ImmunosurveillanceAutologous TumorsCd8+ T CellsDendritic Cell BiologyCellular Immune ResponseOncology
Bone marrow of breast cancer patients was found to contain CD8+ T cells specific for peptides derived from breast cancer–associated proteins MUC1 and Her-2/neu. Most of these cells had a central or effector memory phenotype (CD45RA–CD62L+ or CD45RA–CD62L–, respectively). To test their in vivo function, we separated bone marrow–derived CD45RA+ naive or CD45RA–CD45RO+ memory T cells, stimulated them with autologous dendritic cells pulsed with tumor lysate, and transferred them into NOD/SCID mice bearing autologous breast tumors and normal skin transplants. CD45RA– memory but not CD45RA+ naive T cells infiltrated autologous tumor but not skin tissues after the transfer. These tumor-infiltrating cells had a central or effector memory phenotype and produced perforin. Many of them expressed the P-selectin glycoprotein ligand 1 and were found around P-selectin+ tumor endothelium. Tumor infiltration included cluster formation in tumor tissue by memory T cells with cotransferred dendritic cells. It was associated with the induction of tumor cell apoptosis and significant tumor reduction. We thus demonstrate selective homing of memory T cells to human tumors and suggest that tumor rejection is based on the recognition of tumor-associated antigens on tumor cells and dendritic cells by autologous specifically activated central and effector memory T cells.
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