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. 2021 Mar;35(3):823-834.
doi: 10.1038/s41375-020-0947-1. Epub 2020 Jul 6.

miR-21 antagonism abrogates Th17 tumor promoting functions in multiple myeloma

Marco Rossi #  1 Emanuela Altomare #  2 Cirino Botta  3 Maria Eugenia Gallo Cantafio  2 Sarai Sarvide  4 Daniele Caracciolo  2 Caterina Riillo  2 Marco Gaspari  2 Domenico Taverna  2 Francesco Conforti  5 Paola Critelli  2 Bernardo Bertucci  6 Michelangelo Iannone  7 Nicoletta Polerà  2 Domenica Scumaci  2 Mariamena Arbitrio  7 Nicola Amodio  2 Maria Teresa Di Martino  2 Bruno Paiva  4 Pierosandro Tagliaferri  2 Pierfrancesco Tassone  2   8
Affiliations

miR-21 antagonism abrogates Th17 tumor promoting functions in multiple myeloma

Marco Rossi et al. Leukemia. 2021 Mar.

Abstract

Multiple myeloma (MM) is tightly dependent on inflammatory bone marrow microenvironment. IL-17 producing CD4+ T cells (Th17) sustain MM cells growth and osteoclasts-dependent bone damage. In turn, Th17 differentiation relies on inflammatory stimuli. Here, we investigated the role of miR-21 in Th17-mediated MM tumor growth and bone disease. We found that early inhibition of miR-21 in naive T cells (miR-21i-T cells) impaired Th17 differentiation in vitro and abrogated Th17-mediated MM cell proliferation and osteoclasts activity. We validated these findings in NOD/SCID-g-NULL mice, intratibially injected with miR-21i-T cells and MM cells. A Pairwise RNAseq and proteome/phosphoproteome analysis in Th17 cells demonstrated that miR-21 inhibition led to upregulation of STAT-1/-5a-5b, STAT-3 impairment and redirection of Th17 to Th1/Th2 like activated/polarized cells. Our findings disclose the role of miR-21 in pathogenic Th17 activity and open the avenue to the design of miR-21-targeting strategies to counteract microenvironment dependence of MM growth and bone disease.

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