Splenic marginal zone lymphoma (SMZL) is a distinct clinical and pathological entity among marginal zone lymphomas. Genetic and microenvironmental factors leading to aberrant activation of the NF-κB pathway have been implicated in SMZL pathogenesis. CYLD is a negative regulator of NF-κB and other signaling pathways acting as a deubiquitinase of regulatory molecules and has been reported as a tumor suppressor in different types of cancer, including B-cell malignancies. To assess whether CYLD is implicated in the natural history of SMZL, we profiled primary cells from patients with SMZL and SMZL cell lines for CYLD expression and functionality. We report that CYLD is downregulated in patients with SMZL and that CYLD ablation in vitro leads to NF-κB pathway hyperactivation, promoting the proliferation of SMZL cells. In addition, we found that CYLD deficiency was associated with increased migration of SMZL cells in vitro, through CCR7 receptor signaling, and with increased dissemination in vivo. CYLD loss was sufficient to induce BcR signaling, conferring increased resistance to ibrutinib treatment in vitro. In summary, our work uncovers a novel role of CYLD as a key regulator in SMZL pathogenesis, dissemination, and resistance to targeted agents. On these grounds, CYLD could be proposed as a novel target for patient stratification and personalized interventions.
Loss of CYLD promotes splenic marginal zone lymphoma / Pseftogas, A.; Bordini, J.; Heltai, S.; Bonfiglio, F.; Gavriilidis, G.; Vasileiou, V.; Keisaris, S.; Belloni, D.; Taccetti, C.; Ranghetti, P.; Perotta, E.; Frenquelli, M.; Sarkar, U. A.; Albi, E.; Martini, F.; Sant'Antonio, E.; Mavilia, F.; Psomopoulos, F.; Daibata, M.; Martinez Climent, J. A.; Mosialos, G.; Rossi, D.; Campanella, A.; Scarfo', L.; Stamatopoulos, K.; Xanthopoulos, K.; Ghia, P.. - In: HEMASPHERE. - ISSN 2572-9241. - 9:3(2025). [10.1002/hem3.70098]
Loss of CYLD promotes splenic marginal zone lymphoma
Bordini J.Secondo
;Taccetti C.;Campanella A.;Scarfo' L.;Ghia P.
Ultimo
2025-01-01
Abstract
Splenic marginal zone lymphoma (SMZL) is a distinct clinical and pathological entity among marginal zone lymphomas. Genetic and microenvironmental factors leading to aberrant activation of the NF-κB pathway have been implicated in SMZL pathogenesis. CYLD is a negative regulator of NF-κB and other signaling pathways acting as a deubiquitinase of regulatory molecules and has been reported as a tumor suppressor in different types of cancer, including B-cell malignancies. To assess whether CYLD is implicated in the natural history of SMZL, we profiled primary cells from patients with SMZL and SMZL cell lines for CYLD expression and functionality. We report that CYLD is downregulated in patients with SMZL and that CYLD ablation in vitro leads to NF-κB pathway hyperactivation, promoting the proliferation of SMZL cells. In addition, we found that CYLD deficiency was associated with increased migration of SMZL cells in vitro, through CCR7 receptor signaling, and with increased dissemination in vivo. CYLD loss was sufficient to induce BcR signaling, conferring increased resistance to ibrutinib treatment in vitro. In summary, our work uncovers a novel role of CYLD as a key regulator in SMZL pathogenesis, dissemination, and resistance to targeted agents. On these grounds, CYLD could be proposed as a novel target for patient stratification and personalized interventions.| File | Dimensione | Formato | |
|---|---|---|---|
|
HemaSphere - 2025 - Pseftogas - Loss of CYLD promotes splenic marginal zone lymphoma-1.pdf
accesso aperto
Tipologia:
Submitted manuscript (manoscritto inviato all’editore)
Licenza:
Creative commons
Dimensione
1.97 MB
Formato
Adobe PDF
|
1.97 MB | Adobe PDF | Visualizza/Apri |
I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
