Targeting CXCR4 reverts the suppressive activity of T-regulatory cells in renal cancer

Sara Santagata; Maria Napolitano; Crescenzo D'Alterio; Sonia Desicato; Salvatore Di Maro; Luciana Marinelli; Alessandra Fragale; Maria Buoncervello; Francesco Persico; Lucia Gabriele; Ettore Novellino; Nicola Longo; Sandro Pignata; Sisto Perdonà; Stefania Scala

doi:10.18632/oncotarget.20363

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Research Papers:

Targeting CXCR4 reverts the suppressive activity of T-regulatory cells in renal cancer

Sara Santagata, Maria Napolitano, Crescenzo D'Alterio, Sonia Desicato, Salvatore Di Maro, Luciana Marinelli, Alessandra Fragale, Maria Buoncervello, Francesco Persico, Lucia Gabriele, Ettore Novellino, Nicola Longo, Sandro Pignata, Sisto Perdonà and Stefania Scala _

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Oncotarget. 2017; 8:77110-77120. https://doi.org/10.18632/oncotarget.20363

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Abstract

Sara Santagata1, Maria Napolitano1, Crescenzo D'Alterio1, Sonia Desicato2, Salvatore Di Maro3, Luciana Marinelli3, Alessandra Fragale4, Maria Buoncervello4, Francesco Persico5, Lucia Gabriele4, Ettore Novellino3, Nicola Longo5, Sandro Pignata2, Sisto Perdonà2 and Stefania Scala1

1Functional Genomics, Istituto Nazionale per lo Studio e la Cura dei Tumori, Fondazione “G. Pascale”-IRCCS, 80131 Naples, Italy

2Uro-Gynecological Department, Istituto Nazionale per lo Studio e la Cura dei Tumori, Fondazione “G. Pascale”-IRCCS, 80131 Naples, Italy

3Department of Pharmacy, University of Naples Federico II, 80131 Naples, Italy

4Department of Hematology, Oncology and Molecular Medicine, Istituto Superiore di Sanità, 00161 Rome, Italy

5Urology Division, University Federico II, 80131 Naples, Italy

Correspondence to:

Stefania Scala, email: [email protected], [email protected]

Keywords: CXCR4, immune suppression, renal cell carcinoma, T regulatory cells, tumor microenvironment

Received: May 07, 2017 Accepted: June 25, 2017 Published: August 19, 2017

ABSTRACT

With the intent to identify biomarkers in renal cell carcinoma (RCC) the functional status of T-regulatory cells (Tregs) was investigated in primary RCC. Tregs were isolated from tumoral-(TT), peritumoral tissue-(PT) and peripheral blood-(PB) of 42 primary RCC patients and function evaluated through effector T cells (Teff) proliferation, cytokines release and demethylation of Treg Specific Region (TSDR). The highest value of Tregs was detected in TT with the uppermost amount of effector-Tregs-(CD4⁺CD25^hiFOXP3^hiCD45RA^-). PB-RCC Tregs efficiently suppress Teff proliferation compared to healthy donor (HD)-Tregs and, at the intrapatient evaluation, TT-derived Tregs were the most suppressive. Higher demethylation TSDR was detected in TT- and PB-RCC Tregs vs HD-Tregs (P <0,001). CXCR4 is highly expressed on Tregs, thus we wished to modulate Tregs function through CXCR4 inhibition. CXCR4 antagonism, elicited by a new peptidic antagonist, Peptide-R29, efficiently reversed Tregs suppression of Teff proliferation. Thus Tregs functional evaluation precisely reflects Tregs status and may be a reliable biomarker of tumoral immune response. In addition, treatment with CXCR4 antagonist, impairing Tregs function, could improve the anticancer immune response, in combination with conventional therapy and/or immunotherapy such as checkpoints inhibitors.

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Research Papers:

Targeting CXCR4 reverts the suppressive activity of T-regulatory cells in renal cancer

Abstract