Immunotherapy of Acute MYELOID LEUKEMIA: ANTI-LEUKEMIC EFFECTS by Unprimed or Primed, Selected or Unselected Effector T-CELLS.

1) Blast- and DC-characterization: Blasts can be characterized by blast phenotypes or LAA-RNA-PCR(WT1,PR1 or PRAME).An LAA-overexpression was found in 70-94% of 88AML-samples compared to healthy controls. Ex vivo DC_leu can regularly be generated independent from karyotypes and quantified in every AML-case and used to prime T-cells(Schmetzer 2005-2009).

2) Effectorcell characterization: a)In 6 patients after preemptive DLI-therapy between 0.1 and 0.5% LAA-specific T-cells with a highly Vβ-restricted T-cellprofil were found(Tetramer/Spectratyping). B)Compared to unprimed T-cells (with no or low antileukemic ex vivo function) selected from a patient after SCT IFNg-selected unprimed and even more primed T-cells have an improved antileukemic function compared to non-IFNg-selected primed T-cells. C) DC-priming (more than blast-priming) increases the antileukemic T-cell reactivity (shown in 20 cases) and is associated with highest Vβ-restriction, but is not in every case successful C) By spectratyping identical clone was found after DC-priming ex vivo and in vivo prepared from patient proving the value of DC-culturing for ‘simulating’ in vivo reactions.

3)Predictive and prognostic significance: a)Composition of DC-subtypes (high proportions of mature and leukemia-derived DC) and of T-cells (ratios>1 of CD4:CD8 and CD45RO:CD45RA)and microenvironment (high concentrations of CXCL8 and CCL2 in DC-culture supernatans,IL6 and IFNg in DC/T-MLC-supernatans) arepredictive for effectful antileukemic functionalityof primed T-cells b) Composition of DC-subtypes (high proportions of mature, leukemia-derived DC and convertibility of blasts to DC) predicts the clinical response to immunotherapy (SCT (n=18) or DLI-relapse therapy (n=17)):cases with higher proportions of mature DC/ DC_leu /better blastconvertibility to DC_leu had a higher chance to respond to immunotherapy (SCT/DLI) and had an improved overall survival.

In summary blasts can be characterized (LAA/blast phenotype) and DC/DC_leu be generated in any given case independent from karyotype. A DC priming of T cells improves the antileukemic CTL, but not in every case. The composition of DC and T cells and the microenvironment in MLC are predictive for the ex vivo lytic efficiency of DC-primed T cells and for patients' response to immunotherapy (SCT or DLI). Effector T-cells can be identified, characterized or selected by their Vβ-profil, their LAA-specifity or IFNg-release (before or after blast- or DC-priming). Although the reactive differences or the therapeutic benefit of those different T-cellsubsets are not clear at the moment we hope to contribute to understand biological mechanisms behind cytotoxic reactions, to identify reactive T-cells (and identify best stemcell donors), to learn about escape mechanisms and to develop adoptive immunotherapies with specific, antileukemia directed T-cells without side effects.

No relevant conflicts of interest to declare.