Prospective identification of neoantigen-specific lymphocytes in the peripheral blood of melanoma patients

Gros, Alena; Parkhurst, Maria R.; Tran, Eric; Pasetto, Anna; Robbins, Paul F.; Ilyas, Sadia; Prickett, Todd D.; Gartner, Jared J.; Crystal, Jessica S.; Roberts, Ilana M.; Trebska-McGowan, Kasia; Wunderlich, John R.; Yang, James Chih‐Hsin; Rosenberg, Steven A.

doi:10.1038/nm.4051

Cited by 733 publications

(649 citation statements)

References 41 publications

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“…7 Furthermore, Gros and colleagues were able to recently identify PD1 + CD8 + T cells in circulation of three melanoma patients that targeted unique patient-specific neoantigens. 31 Our findings, that tumor antigen specific T-cells (including EGFR, MAGE and HPV) in the periphery express PD-1 and CTLA-4, support these observations. Thus, circulating TA-specific T cells can be identified in peripheral blood with important consequences for the development of individualized TCR analyses and therefore personalized therapies.…”

Section: Discussionsupporting

confidence: 82%

T cell receptor richness in peripheral blood increases after cetuximab therapy and correlates with therapeutic response

et al. 2018

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The role of T cell receptor (TCR) signaling for adaptive immune responses is essential. The ability to respond to a broad spectrum of tumor antigens requires an adaptive selection of various TCR. So far, little is known about the role of TCR richness and clonality in the cellular immune response to head and neck cancer (HNC), though the Endothelial Growth Factor Receptor (EGFR)-specific CD8+ T cell response can be enhanced by cetuximab therapy. Therefore, we investigated differences in TCR sequences between human papillomavirus (HPV)+ and HPV− HNC patients, as well as differences in TCR sequence characteristics between T cells of peripheral blood mononuclear cells (PBMC) and tumor infiltrating lymphocytes (TIL). Additionally, we were able to investigate the TCR richness and clonality in samples pre- and post- treatment in a prospective clinical trial of neoadjuvant cetuximab. Interestingly, HPV+ and HPV− HNSCC did not significantly differ in the extent of TCR clonality and richness in PBMC or TIL. However, neoadjuvant cetuximab treatment increased the number of unique TCR sequences in PBMC (p = 0.0003), which was more prominent in the clinical responder patients compared to non-responders (p = 0.04). A trend toward TCR gene focusing was observed in TIL (p = 0.1) post-treatment. Thus, an increase in richness of TCR sequences in the periphery with a focusing at the tumor site is associated with an improved treatment response, suggesting an influence of peripheral quantity and intratumoral quality on adaptive immunity in cetuximab treated patients.

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Section: Discussionsupporting

confidence: 82%

T cell receptor richness in peripheral blood increases after cetuximab therapy and correlates with therapeutic response

et al. 2018

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“…34 Moreover, expression of checkpoint molecules such as PD1 on circulating CD8 + T-cells is a biomarker of tumor antigen specificity. 35 We therefore dichotomized the HPV+ HNSCC data set based on median LAG3, PD1, TIGIT, or TIM3 expression and calculated the impact of high versus low expression on overall patient survival (Figure 7, black and red curves). Higher than median expression of any of these genes predicted markedly improved survival in HPV+ HNSCC over those patients with tumors expressing these markers at levels below the median.…”

Section: Resultsmentioning

confidence: 99%

Treatment-naïve HPV+ head and neck cancers display a T-cell-inflamed phenotype distinct from their HPV- counterparts that has implications for immunotherapy

et al. 2018

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Cancers progress when the immune system fails to identify and eliminate malignant cells. Recognition of this, combined with advances in tumor immunology, has allowed development of therapies that induce effective anti-tumor immune responses. For incompletely-understood reasons, effective responses to immunotherapy occur in some patients and not others. Head and neck squamous cell carcinomas (HNSCC) are a common cancer type that can be divided into two subsets based on human papillomavirus (HPV) status. HPV status is a strong predictor of positive clinical outcome. Expression of exogenous viral antigens by HPV+, but not HPV-, HNSCC allows direct comparison of the immune status (immune cell presence and characteristics) between these two otherwise anatomically-similar tumors. Using TCGA data, we compared the immune landscape between HPV+ and HPV- treatment-naïve HNSCC. As compared to HPV- samples, HPV+ HNSCC exhibited a strong Th1 response characterized by increased infiltration with multiple types of immune cells and expression of their effector molecules. HPV+ HNSCC also expressed higher levels of CD39 and multiple T-cell exhaustion markers including LAG3, PD1, TIGIT, and TIM3 compared to HPV- HNSCC. Importantly, patients with higher expression of these exhaustion markers–indicative of a T-cell-inflamed tumor–correlated with markedly improved survival in HPV+, but not HPV-, HNSCC. Thus, profound differences exist between the immune landscape of HPV+ and HPV- HNSCC. These results suggest that immune checkpoint inhibitor therapy is a promising treatment strategy for HPV+ HNSCC, and that expression of immune checkpoint molecules could serve as a predictive biomarker of patient outcome in HPV+ HNSCC.

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“…Consistently, Simon et al have recently showed that PD-1 expression identifies Ag-specific T-cell clones with high avidity, 28 and Gros et al described PD-1 + neoantigen-specific anti-tumor CD8 + T cells, either circulating or intratumoral. 56 …”

Section: Discussionmentioning

confidence: 99%

Antigen-specificity and DTIC before peptide-vaccination differently shape immune-checkpoint expression pattern, anti-tumor functionality and TCR repertoire in melanoma patients

et al. 2018

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We have recently described that DNA-damage inducing drug DTIC, administered before peptide (Melan-A and gp100)-vaccination, improves anti-tumor CD8+ Melan-A-specific T-cell functionality, enlarges the Melan-A+ TCR repertoire and impacts the overall survival of melanoma patients. To identify whether the two Ags employed in the vaccination differently shape the anti-tumor response, herein we have carried out a detailed analysis of phenotype, anti-tumor functionality and TCR repertoire in treatment-driven gp100-specific CD8+ T cells, in the same patients previously analyzed for Melan-A. We found that T-cell clones isolated from patients treated with vaccination alone possessed an Early/intermediate differentiated phenotype, whereas T cells isolated after DTIC plus vaccination were late-differentiated. Sequencing analysis of the TCRBV chains of 29 treatment-driven gp100-specific CD8+ T-cell clones revealed an oligoclonal TCR repertoire irrespective of the treatment schedule. The high anti-tumor activity observed in T cells isolated after chemo-immunotherapy was associated with low PD-1 expression. Differently, T-cell clones isolated after peptide-vaccination alone expressed a high level of PD-1, along with LAG-3 and TIM-3, and were neither tumor-reactive nor polyfunctional. Blockade of PD-1 reversed gp100-specific CD8+ T-cell dysfunctionality, confirming the direct role of this co-inhibitory molecule in suppressing anti-tumor activity, differently from what we have previously observed for Melan-A+CD8+ T cells, expressing PD-1 but highly functional. These findings indicate that the functional advantage induced by combined chemo-immunotherapy is determined by the tumor antigen nature, T-cell immune-checkpoints phenotype, TCR repertoire diversity and anti-tumor T-cell quality and highlights the importance of integrating these parameters to develop effective immunotherapeutic strategies.

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Prospective identification of neoantigen-specific lymphocytes in the peripheral blood of melanoma patients

Cited by 733 publications

References 41 publications

T cell receptor richness in peripheral blood increases after cetuximab therapy and correlates with therapeutic response

T cell receptor richness in peripheral blood increases after cetuximab therapy and correlates with therapeutic response

Treatment-naïve HPV+ head and neck cancers display a T-cell-inflamed phenotype distinct from their HPV- counterparts that has implications for immunotherapy

Antigen-specificity and DTIC before peptide-vaccination differently shape immune-checkpoint expression pattern, anti-tumor functionality and TCR repertoire in melanoma patients

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