Nectin-4 reduces T cell effector function and is a therapeutic target in pancreatic cancer
Max Heiduk, Carolin Beer, Sarah Cronjaeger, Emily A. Kawaler, Ulrich Sommer, Franziska Baenke, David Digomann, Loreen Natusch Bufe, Charlotte Reiche, Jessica Glück, Franziska Hoffmann, Sungsik Kim, Daniel E. Stange, Diane M. Simeone, Jürgen Weitz, Lena Seifert, Adrian M. Seifert
Max Heiduk, Carolin Beer, Sarah Cronjaeger, Emily A. Kawaler, Ulrich Sommer, Franziska Baenke, David Digomann, Loreen Natusch Bufe, Charlotte Reiche, Jessica Glück, Franziska Hoffmann, Sungsik Kim, Daniel E. Stange, Diane M. Simeone, Jürgen Weitz, Lena Seifert, Adrian M. Seifert
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Research Article Gastroenterology Oncology

Nectin-4 reduces T cell effector function and is a therapeutic target in pancreatic cancer

Abstract

Pancreatic ductal adenocarcinoma (PDAC) has a dismal prognosis, and current therapies show limited efficacy. Ligands and receptors of the TIGIT axis were analyzed using multicolor flow cytometry of tumor and blood samples, IHC from primary tumors, and single-cell RNA-Seq from primary tumors and liver metastasis from patients with various stages of PDAC. The effect of soluble and plate-bound Nectin-4 on T cell function was tested in vitro. Furthermore, patient-derived PDAC organoids were treated with the standard-of-care therapies FOLFIRINOX, gemcitabine plus paclitaxel, or the antibody-drug conjugate enfortumab vedotin. TIGIT expression was increased on tumor-infiltrating conventional T cells and Tregs compared with T cells from matched blood. Nectin-4 but not CD155 expression was associated with poor outcome. Nectin-4 was exclusively expressed by tumor cells and correlated with low immune infiltration. Notably, Nectin-4 inhibited T cell effector cytokine production in vitro. Targeting Nectin-4 with the antibody-drug conjugate enfortumab vedotin inhibited tumor growth in multiple patient-derived PDAC organoids. Collectively, our data underscore Nectin-4 as a potential novel therapeutic target and provide the rationale to test this agent in patients with PDAC.

Authors

Max Heiduk, Carolin Beer, Sarah Cronjaeger, Emily A. Kawaler, Ulrich Sommer, Franziska Baenke, David Digomann, Loreen Natusch Bufe, Charlotte Reiche, Jessica Glück, Franziska Hoffmann, Sungsik Kim, Daniel E. Stange, Diane M. Simeone, Jürgen Weitz, Lena Seifert, Adrian M. Seifert

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Figure 5

Nectin-4 is exclusively expressed by tumor cells in PDAC.

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Nectin-4 is exclusively expressed by tumor cells in PDAC. (A) Dot plot d...
(A) Dot plot depicting gene expression of TIGIT family receptors and ligands in several compartments within human primary PDAC (n = 17). The dot size represents the percentage of cells expressing the gene, and the color represents the average expression within those cells. (B) Violin plot of PVRL4 expression in all malignant epithelial cells in primary PDAC (n = 11) compared with PDAC liver metastases (n = 9) from treatment-naive patients. (C) Scatter plot showing the correlation between PVRL4 expression in malignant epithelial cells and percentage of T cells among all analyzed cells per sample in treatment-naive (n = 11) and chemotherapeutically-treated (n = 6) primary PDAC. Pearson correlation coefficients and P values are depicted. Each dot represents 1 sample. Wilcoxon signed-rank test for comparison of expression levels. ****P < 0.0001.