Detection of pancreatic ductal adenocarcinoma with galectin-9 serum levels

Adrian M. Seifert(German Cancer Research Center), Charlotte Reiche(University Hospital Carl Gustav Carus), Max Heiduk(German Cancer Research Center), Anna Tannert(University Hospital Carl Gustav Carus), Ann-Christin Meinecke(University Hospital Carl Gustav Carus), Stephanie Baier(University Hospital Carl Gustav Carus), Janusz von Renesse(University Hospital Carl Gustav Carus), Christoph Kahlert(German Cancer Research Center), Marius Distler(University Hospital Carl Gustav Carus), Thilo Welsch(German Cancer Research Center), Christoph Reißfelder(Heidelberg University), Daniela E. Aust(University Hospital Carl Gustav Carus), George Miller(New York University), Jürgen Weitz(German Cancer Research Center), Lena Seifert(German Cancer Research Center)
Oncogene
February 13, 2020
Cited by 110Open Access
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Abstract

Abstract Pancreatic ductal adenocarcinoma (PDAC) responds poorly to checkpoint blockade, such as anti-CTLA-4 and anti-PD-1. Galectin-9, a β-galactoside-binding lectin, promotes immune suppression through T-cell inhibition, and programming of tolerogenic macrophages. Of all cancers tested, PDAC showed the highest expression of LGALS9 (galectin-9) mRNA. We analyzed formalin-fixed and paraffin-embedded specimens from 83 patients with PDAC stained for galectin-9. Using flow cytometry, we determined galectin-9 expression on immune cells from tumor and matched blood samples from 12 patients with resectable PDAC. Furthermore, we analyzed galectin-9 serum levels by enzyme-linked immunosorbent assay using serum samples from 70 patients with PDAC, from 36 individuals with benign pancreatic disease, and from 28 healthy controls. Galectin-9 was highly expressed in human PDAC compared with normal pancreas and present on both tumor and immune cells. Tumor-infiltrating immune cells, especially CD3 + T cells, showed upregulation of galectin-9 compared with immune cells from matched blood. Blood γδ T cells from PDAC patients had higher galectin-9 expression than γδ T cells from healthy individuals. Galectin-9 polarized macrophages toward a protumoral M2 phenotype leading to suppressed T-cell cytokine secretion. Furthermore, serum concentration of galectin-9 was able to discriminate PDAC from benign pancreatic disease and healthy individuals, and was prognostic for stage IV patients. Galectin-9 is a new biomarker for the detection of PDAC.


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