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:Gabriele Varano #,Silvia Lonardi #,Paola Sindaco #,Ilaria Pietrini #,Gaia Morello,Piera Balzarini,Filippo Vit,Hadas Neuman,Giorgio Bertolazzi,Silvia Brambillasca,Nicara C Parr,Marco Chiarini,Silvia Bellesi,Elena Maiolo,Sabrina Giampaolo,Federica Mainoldi,Viveka Selvarasa,Hiroshi Arima,Vilma Pellegrini,Chiara Pagani,Mattia Bugatti,Cecilia Ranise,Tommaso M Taddei,Takashi Sonoki,Hajdica Thanasi,Elena Morlacchi,Daniel Segura-Garzon,Emma Albertini,Rosa Daffini,Anojan Sivacegaram,Henry Yang,Ying Li,Valeria Cancila,Giada Cicio,Michela Robusto,Brian Leuzzi,Adrian Andronache,Paolo Trifiro,Mirko Riboni,Simone P Minardi,Raoul J P Bonnal,Cristina Lopez Gonzalez,Euplio Visco,Pasquale Capaccio,Sara Torretta,Lorenzo Pignataro,Camillo Almici,Mario Varasi,Luigi M Larocca,Reiner Siebert,Brunangelo Falini,Andres J M Ferreri,Alessandra Tucci,Daniele Lorenzini,Antonello D Cabras,Giancarlo Pruneri,Arianna Di Napoli,Marco Ungari,Marco Pizzi,Stefan Hohaus,Ciro Mercurio,Joo Y Song,Wing C Chan,Luisa Lorenzi,Riccardo Bomben,Maurilio Ponzoni,Ramit Mehr,Claudio Tripodo #,Fabio Facchetti #,Stefano Casola #
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

Abstract

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.

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