Abstract 187P
Background
Uveal melanoma (UM), an uncommon but aggressive eye cancer, exhibits genetic diversity, classifying into M3 (poor prognosis) and D3 (better outcome) subsets. Despite low mutation rates, metastatic UM patients have detectable CD4 and CD8 T cells, suggesting an immune response. We recently identified public neo-antigens generated by SF3B1 mutations in D3 tumors, triggering CD8+ T cell responses. In M3 tumors with BAP1 inactivation, immune infiltration increases, but CD8 T cell specificity remains unclear.
Methods
We collected blood and tumor samples from uveal melanoma patients at Institut Curie. Specific peptide-loaded HLA-A2 tetramers were labeled and used for staining blood and tumor cells. Single-cell RNA-Seq experiments were performed on TILs.
Results
In our analysis of 24 enucleated patient samples, we observed an enrichment of CD8+ T cells over CD4+ T cells within the tumor microenvironment. A notable fraction of CD8+ T cells exhibited exhaustion markers like PD-1 and CD39, suggesting the presence of an Ag-specific immune response. Among these exhausted CD8+ T cells, 1-10% were specific for HLA-A2: Melan-A. By using scRNA-seq and VDJ TCR-seq we explored T cells response within 3 primary HLA-A2+ M3 tumors. Our analysis identified nine distinct clusters, notably Cluster 0, which displayed upregulation of genes such as PDCD1 (PD-1), ENTPD1 (CD39), HAVCR2 (TIM3), LAG3, GZMB, and GZMK. This gene expression profile suggests chronic activation due to exposure to tumor antigens. Melan-A tetramer-positive cells predominantly localized to Cluster C0, and the largest clonotype was associated with this cluster. We also assessed systemic recirculation by sequencing TCRs in PBMCs, revealing varying recirculation levels among different T-cell clusters. While chronically activated (C0) T cells displayed limited recirculation, T cells with a memory phenotype (C2), cytotoxic functions (C4), and effector T-cell responses (C6) were more present in the peripheral blood.
Conclusions
These findings challenge the notion of the eye as an immune-privileged site, as we consistently observed immune responses within UM tumors. The mechanism by which tumor antigens prime naïve T cells in this site remains mysterious.
Legal entity responsible for the study
F. Lucibello.
Funding
Ligue Contre le Cancer.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
60P - Adaptive NK cells as a therapeutic option for childhood leukaemia
Presenter: Zoya Eskandarian
Session: Poster Display
61P - Unlocking the Power of Natural Killer Cells: Precision Selection with Cutting-Edge Microfluidics
Presenter: Neelima KC
Session: Poster Display
63TiP - A phase I study of tumor-infiltrating lymphocytes (TILs) in advanced solid tumors used an optimized regimen: MIZAR trial
Presenter: Qing Xu
Session: Poster Display
68P - Real-world (rw) outcomes in patients (pts) with metastatic (m) NSCLC and STK11, KEAP1 and/or KRAS mutations (mut) receiving PD-(L)1-based treatment (tx): CORRELATE
Presenter: Solange Peters
Session: Poster Display
70P - LIST (Lung Initiative on Sequence Therapy), a real-world study of nivolumab for advanced NSCLC in France: first effectiveness, safety, and IO-rechallenge results
Presenter: Benoît GODBERT
Session: Poster Display
72P - Camrelizumab plus apatinib after chemoradiotherapy in unresectable stage III non-small-cell lung cancer?A multi-center, single-arm, phase 2 study
Presenter: Hui Zhouguang
Session: Poster Display
74P - A single-center, Phase II study of surufatinib combined with toripalimab, pemetrexed(A), and platinum (P) in patients with advanced non-squamous non-small cell lung cancer (nsq-NSCLC)
Presenter: Wen Feng Fang
Session: Poster Display
75P - Patient-reported outcomes (PROs) of cemiplimab + chemotherapy in advanced non-small cell lung cancer (NSCLC): EMPOWER-lung 3 liver metastases subpopulation
Presenter: Ana Baramidze
Session: Poster Display