Multiple myeloma (MM) is an incurable plasma cell malignancy that exploits transcriptional networks driven by IRF4. We employ a multi-omics approach to discover IRF4 vulnerabilities, integrating functional genomics screening, spatial proteomics, and global chromatin mapping. ARID1A, a member of the SWI/SNF chromatin remodeling complex, is required for IRF4 expression and functionally associates with IRF4 protein on chromatin. Deleting Arid1a in activated murine B cells disrupts IRF4-dependent transcriptional networks and blocks plasma cell differentiation. Targeting SWI/SNF activity leads to rapid loss of IRF4-target gene expression and quenches global amplification of oncogenic gene expression by MYC, resulting in profound toxicity to MM cells. Notably, MM patients with aggressive disease bear the signature of SWI/SNF activity, and SMARCA2/4 inhibitors remain effective in immunomodulatory drug (IMiD)-resistant MM cells. Moreover, combinations of SWI/SNF and MEK inhibitors demonstrate synergistic toxicity to MM cells, providing a promising strategy for relapsed/refractory disease.
IRF4 requires ARID1A to establish plasma cell identity in multiple myeloma.
IRF4 需要 ARID1A 来确立多发性骨髓瘤中浆细胞的身份
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作者:Bolomsky Arnold, Ceribelli Michele, Scheich Sebastian, Rinaldi Kristina, Huang Da Wei, Chakraborty Papiya, Pham Lisette, Wright George W, Hsiao Tony, Morris Vivian, Choi Jaewoo, Phelan James D, Holewinski Ronald J, Andresson Thorkell, Wisniewski Jan, Riley Deanna, Pittaluga Stefania, Hill Elizabeth, Thomas Craig J, Muppidi Jagan, Young Ryan M
| 期刊: | Cancer Cell | 影响因子: | 44.500 |
| 时间: | 2024 | 起止号: | 2024 Jul 8; 42(7):1185-1201 |
| doi: | 10.1016/j.ccell.2024.05.026 | 研究方向: | 细胞生物学 |
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