Literature DB >> 31413910

Targeting the C-terminus of galectin-9 induces mesothelioma apoptosis and M2 macrophage depletion.

Pietro Bertino1, Thomas A Premeaux2, Tsuyoshi Fujita2, Brien K Haun1, Michael P Marciel1, Fukun W Hoffmann1, Alan Garcia3, Haining Yiang4, Sandra Pastorino4, Michele Carbone4, Toshiro Niki5,6, John Berestecky3, Peter R Hoffmann1, Lishomwa C Ndhlovu2.   

Abstract

Galectin-9 has emerged as a promising biological target for cancer immunotherapy due to its role as a regulator of macrophage and T-cell differentiation. In addition, its expression in tumor cells modulates tumor cell adhesion, metastasis, and apoptosis. Malignant mesothelioma (MM) is an aggressive neoplasm of the mesothelial cells lining the pleural and peritoneal cavities, and in this study, we found that both human MM tissues and mouse MM cells express high levels of galectin-9. Using a novel monoclonal antibody (mAb) (Clone P4D2) that binds the C-terminal carbohydrate recognition domain (CRD) of galectin-9, we demonstrate unique agonistic properties resulting in MM cell apoptosis. Furthermore, the P4D2 mAb reduced tumor-associated macrophages differentiation toward a protumor phenotype. Importantly, these effects exerted by the P4D2 mAb were observed in both human and mouse in vitro experiments and not observed with another antigalectin-9 specific mAb (clone P1D9) that engages the N-terminus CRD of galectin-9. In syngeneic murine models of MM, P4D2 mAb treatment inhibited tumor growth and improved survival, with tumors from P4D2-treated mice exhibited reduced infiltration of tumor-associated M2 macrophages. This was consistent with an increased production of inducible nitric oxide synthase, which is a major enzyme-regulating macrophage inflammatory response to cancer. These data suggest that using an antigalectin 9 mAb with agonistic properties similar to those exerted by galectin-9 may provide a novel multitargeted strategy for the treatment of mesothelioma and possibly other galectin-9 expressing tumors.

Entities:  

Keywords:  Lectins; agonist monoclonal antibody; galectin 9; immunotherapy; macrophages; mesothelioma

Year:  2019        PMID: 31413910      PMCID: PMC6682368          DOI: 10.1080/2162402X.2019.1601482

Source DB:  PubMed          Journal:  Oncoimmunology        ISSN: 2162-4011            Impact factor:   8.110


  48 in total

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4.  Development of highly stable galectins: truncation of the linker peptide confers protease-resistance on tandem-repeat type galectins.

Authors:  Nozomu Nishi; Aiko Itoh; Aimi Fujiyama; Naoko Yoshida; Shin-ichi Araya; Mitsuomi Hirashima; Hiroki Shoji; Takanori Nakamura
Journal:  FEBS Lett       Date:  2005-04-11       Impact factor: 4.124

5.  The Tim-3 ligand galectin-9 negatively regulates T helper type 1 immunity.

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Review 6.  Multivalent protein-carbohydrate interactions. A new paradigm for supermolecular assembly and signal transduction.

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Journal:  Biochemistry       Date:  2001-03-13       Impact factor: 3.162

7.  Macrophage arginase promotes tumor cell growth and suppresses nitric oxide-mediated tumor cytotoxicity.

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Journal:  Cancer Res       Date:  2001-02-01       Impact factor: 12.701

8.  Galectin-9 induces apoptosis through the calcium-calpain-caspase-1 pathway.

Authors:  Yumiko Kashio; Kazuhiro Nakamura; Mohammad J Abedin; Masako Seki; Nozomu Nishi; Naoko Yoshida; Takanori Nakamura; Mitsuomi Hirashima
Journal:  J Immunol       Date:  2003-04-01       Impact factor: 5.422

9.  Up-regulation of tumor interleukin-8 expression by infiltrating macrophages: its correlation with tumor angiogenesis and patient survival in non-small cell lung cancer.

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10.  Establishment of a murine model of malignant mesothelioma.

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Journal:  Int J Cancer       Date:  1992-12-02       Impact factor: 7.396

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3.  Development and characterization of anti-galectin-9 antibodies that protect T cells from galectin-9-induced cell death.

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4.  Unraveling tumor microenvironment heterogeneity in malignant pleural mesothelioma identifies biologically distinct immune subtypes enabling prognosis determination.

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Review 5.  Mouse models for mesothelioma drug discovery and development.

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6.  The molecular landscape and microenvironment of salivary duct carcinoma reveal new therapeutic opportunities.

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Review 7.  The Immune Microenvironment in Mesothelioma: Mechanisms of Resistance to Immunotherapy.

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