Peripheral T-cell lymphoma, not otherwise specified (PTCL-NOS) is a heterogeneous group of malignancies with poor outcome. Here, we identify a subgroup, PTCL-NOSSMARCB1-, which is characterized by the lack of the SMARCB1 protein and occurs more frequently in young patients. Human and murine PTCL-NOSSMARCB1- show similar DNA methylation profiles, with hypermethylation of T-cell-related genes and hypomethylation of genes involved in myeloid development. Single-cell analyses of human and murine tumors revealed a rich and complex network of interactions between tumor cells and an immunosuppressive and exhausted tumor microenvironment (TME). In a drug screen, we identified histone deacetylase inhibitors (HDACi) as a class of drugs effective against PTCL-NOSSmarcb1-. In vivo treatment of mouse tumors with SAHA, a pan-HDACi, triggered remodeling of the TME, promoting replenishment of lymphoid compartments and reversal of the exhaustion phenotype. These results provide a rationale for further exploration of HDACi combination therapies targeting PTCL-NOSSMARCB1- within the TME.
Lack of SMARCB1 expression characterizes a subset of human and murine peripheral T-cell lymphomas / Fischer, Anja; Albert, Thomas K.; Moreno, Natalia; Interlandi, Marta; Mormann, Jana; Glaser, Selina; Patil, Paurnima; de Faria, Flavia W.; Richter, Mathis; Verma, Archana; Balbach, Sebastian T.; Wagener, Rabea; Bens, Susanne; Dahlum, Sonja; Göbel, Carolin; Münter, Daniel; Inserte, Clara; Graf, Monika; Kremer, Eva; Melcher, Viktoria; Di Stefano, Gioia; Santi, Raffaella; Chan, Alexander; Dogan, Ahmet; Bush, Jonathan; Hasselblatt, Martin; Cheng, Sylvia; Spetalen, Signe; Fosså, Alexander; Hartmann, Wolfgang; Herbrüggen, Heidi; Robert, Stella; Oyen, Florian; Dugas, Martin; Walter, Carolin; Sandmann, Sarah; Varghese, Julian; Rossig, Claudia; Schüller, Ulrich; Tzankov, Alexandar; Pedersen, Martin B.; d'Amore, Francesco A.; Mellgren, Karin; Kontny, Udo; Kancherla, Venkatesh; Veloza, Luis; Missiaglia, Edoardo; Fataccioli, Virginie; Gaulard, Philippe; Burkhardt, Birgit; Soehnlein, Oliver; Klapper, Wolfram; de Leval, Laurence; Siebert, Reiner; Kerl, Kornelius. - In: NATURE COMMUNICATIONS. - ISSN 2041-1723. - STAMPA. - 15:(2024), pp. 8571.1-8571.18. [10.1038/s41467-024-52826-0]
Lack of SMARCB1 expression characterizes a subset of human and murine peripheral T-cell lymphomas
Di Stefano, Gioia;Santi, Raffaella;
2024
Abstract
Peripheral T-cell lymphoma, not otherwise specified (PTCL-NOS) is a heterogeneous group of malignancies with poor outcome. Here, we identify a subgroup, PTCL-NOSSMARCB1-, which is characterized by the lack of the SMARCB1 protein and occurs more frequently in young patients. Human and murine PTCL-NOSSMARCB1- show similar DNA methylation profiles, with hypermethylation of T-cell-related genes and hypomethylation of genes involved in myeloid development. Single-cell analyses of human and murine tumors revealed a rich and complex network of interactions between tumor cells and an immunosuppressive and exhausted tumor microenvironment (TME). In a drug screen, we identified histone deacetylase inhibitors (HDACi) as a class of drugs effective against PTCL-NOSSmarcb1-. In vivo treatment of mouse tumors with SAHA, a pan-HDACi, triggered remodeling of the TME, promoting replenishment of lymphoid compartments and reversal of the exhaustion phenotype. These results provide a rationale for further exploration of HDACi combination therapies targeting PTCL-NOSSMARCB1- within the TME.
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