| Literature DB >> 33413419 |
Yann Cheli1, Meri K Tulic2, Najla El Hachem3, Nicolas Nottet4, Arnaud Jacquel5, Maeva Gesson6, Thomas Strub4, Karine Bille4, Alexandra Picard-Gauci7, Henri Montaudié7, Guillaume E Beranger4,2, Thierry Passeron2,7, Pierre Close3, Corine Bertolotto4, Robert Ballotti4.
Abstract
Resistances to immunotherapies remains a major hurdle towards a cure for melanoma in numerous patients. An increase in the mesenchymal phenotype and a loss of differentiation have been clearly associated with resistance to targeted therapies. Similar phenotypes have been more recently also linked to resistance to immune checkpoint therapies. We demonstrated here that the loss of MIcrophthalmia associated Transcription Factor (MITF), a pivotal player in melanocyte differentiation, favors the escape of melanoma cells from the immune system. We identified Integrin beta-like protein 1 (ITGBL1), a secreted protein, upregulated in anti-PD1 resistant patients and in MITFlow melanoma cells, as the key immunomodulator. ITGBL1 inhibited immune cell cytotoxicity against melanoma cells by inhibiting NK cells cytotoxicity and counteracting beneficial effects of anti-PD1 treatment, both in vitro and in vivo. Mechanistically, MITF inhibited RUNX2, an activator of ITGBL1 transcription. Interestingly, VitaminD3, an inhibitor of RUNX2, improved melanoma cells to death by immune cells. In conclusion, our data suggest that inhibition of ITGBL1 might improve melanoma response to immunotherapies.Entities:
Keywords: ITGBL1; MITF; Melanoma
Year: 2021 PMID: 33413419 PMCID: PMC7789764 DOI: 10.1186/s12943-020-01306-2
Source DB: PubMed Journal: Mol Cancer ISSN: 1476-4598 Impact factor: 27.401