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The soluble form of CD160 acts as a tumor mediator of immune escape in melanoma

Marie-Léa Gauci, Jérôme Giustiniani, C. Lepelletier, Christian Garbar, Nicolas Thonnart, Nicolas Dumaz, Arnaud Foussat, Célèste Lebbé, Armand Bensussan, Anne Marie‐Cardine

2022Cancer Immunology Immunotherapy13 citationsDOIOpen Access PDF

Abstract

Abstract Melanoma is responsible for 90% of skin cancer-related deaths. Major therapeutic advances have led to a considerable improvement in the prognosis of patients, with the development of targeted therapies (BRAF or MEK inhibitors) and immunotherapy (anti-CTLA-4 or -PD-1 antibodies). However, the tumor constitutes an immunosuppressive microenvironment that prevents the therapeutic efficacy and/or promotes the development of secondary resistances. CD160 is an activating NK-cell receptor initially described as delineating the NK and CD8 + T -cell cytotoxic populations. Three forms of CD160 have been described: (1) the GPI isoform, constitutively expressed and involved in the initiation of NK-cells' cytotoxic activity, (2) the transmembrane isoform, neo-synthesized upon cell activation, allowing the amplification of NK cells' cytotoxic functions and (3) the soluble form, generated after cleavage of the GPI isoform, which presents an immuno-suppressive activity. By performing immunohistochemistry analyses, we observed a strong expression of CD160 at the primary cutaneous tumor site of melanoma patients. We further demonstrated that melanoma cells express CD160-GPI isoform and constitutively release the soluble form (sCD160) into the tumor environment. sCD160 was shown to inhibit the cytotoxic activity of NK-cells towards their target cells. In addition, it was found in the serum of melanoma patients and associated with increased tumor dissemination. Altogether these results support a role for sCD160 in the mechanisms leading to the inhibition of anti-tumor response and immune surveillance in melanoma.

Topics & Concepts

MelanomaCytotoxic T cellImmunotherapyCancer researchImmune systemCD8Cancer immunotherapyImmunologyGene isoformTumor microenvironmentBiologyIn vitroGeneBiochemistryImmune Cell Function and InteractionImmunotherapy and Immune ResponsesT-cell and B-cell Immunology
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