The B-cell receptor (BCR) is critical for mature B-cell lymphomas (BCL), serving as a therapeutic target. We show that high-grade BCLs with MYC and BCL2 rearrangements [HGBCL-double-hit (DH)-BCL2] predominantly exhibit immunoglobulin heavy (IGH) chain silencing, leading to BCR shutdown. IGH-silenced HGBCL-DH-BCL2 (IGHUND) tumors differ from IGH+ counterparts in germinal center (GC) zone programs, MYC expression, and immune infiltrate. Whereas IGH+ HGBCL-DH-BCL2 tumors favor IGM/IG-κ expression, IGHUND counterparts complete IGH isotype switching and IG-λ rearrangements. IGHUND lymphomas retain productive IGHV rearrangements and require IGH for optimal fitness. BCR silencing, caused by accelerated IGH turnover and reduced IGH expression, precedes HGBCL-DH-BCL2 onset, inducing RAG1/2-dependent IG light chain editing and facilitating t(8;22)/IGL::MYC translocations. IGHUND HGBCL-DH-BCL2 models exhibit reduced sensitivity to the CD79B-targeting antibody-drug conjugate polatuzumab vedotin. Collectively, HGBCL-DH-BCL2 commonly arises from isotype-switched t(14;18)+ GC B cells, which edit IG light chains, fueling intraclonal diversification, BCR extinction, and t(8;22) while maintaining IGH dependence, with clinical implications. SIGNIFICANCE: These findings link BCR silencing in IGH isotype-switched t(14;18)+ GC B cells to RAG1/2 expression, which triggers IG light chain editing and predisposes to IGL::MYC translocations, promoting HGBCL. In HGBCL with MYC and BCL2 rearrangements, BCR silencing protects from polatuzumab vedotin killing. See related commentary by Shevchenko and Hodson, p. 284.
B-cell Receptor Silencing Reveals the Origin and Dependencies of High-Grade B-cell Lymphomas with MYC and BCL2 Rearrangements.
B 细胞受体沉默揭示了具有 MYC 和 BCL2 重排的高级别 B 细胞淋巴瘤的起源和依赖性
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作者:Varano Gabriele, Lonardi Silvia, Sindaco Paola, Pietrini Ilaria, Morello Gaia, Balzarini Piera, Vit Filippo, Neuman Hadas, Bertolazzi Giorgio, Brambillasca Silvia, Parr Nicara C, Chiarini Marco, Bellesi Silvia, Maiolo Elena, Giampaolo Sabrina, Mainoldi Federica, Selvarasa Viveka, Arima Hiroshi, Pellegrini Vilma, Pagani Chiara, Bugatti Mattia, Ranise Cecilia, Taddei Tommaso M, Sonoki Takashi, Thanasi Hajdica, Morlacchi Elena, Segura-Garzon Daniel, Albertini Emma, Daffini Rosa, Sivacegaram Anojan, Yang Henry, Li Ying, Cancila Valeria, Cicio Giada, Robusto Michela, Leuzzi Brian, Andronache Adrian, Trifiro Paolo, Riboni Mirko, Minardi Simone P, Bonnal Raoul J P, Gonzalez Cristina Lopez, Visco Euplio, Capaccio Pasquale, Torretta Sara, Pignataro Lorenzo, Almici Camillo, Varasi Mario, Larocca Luigi M, Siebert Reiner, Falini Brunangelo, Ferreri Andres J M, Tucci Alessandra, Lorenzini Daniele, Cabras Antonello D, Pruneri Giancarlo, Di Napoli Arianna, Ungari Marco, Pizzi Marco, Hohaus Stefan, Mercurio Ciro, Song Joo Y, Chan Wing C, Lorenzi Luisa, Bomben Riccardo, Ponzoni Maurilio, Mehr Ramit, Tripodo Claudio, Facchetti Fabio, Casola Stefano
| 期刊: | Blood Cancer Discovery | 影响因子: | 11.500 |
| 时间: | 2025 | 起止号: | 2025 Jul 1; 6(4):364-393 |
| doi: | 10.1158/2643-3230.BCD-25-0099 | 靶点: | BCL2 |
| 研究方向: | 细胞生物学 | 疾病类型: | 淋巴瘤 |
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