B cell receptor silencing reveals the origin of high-grade B cell lymphomas with MYC and BCL2 rearrangements
Preprint 2024 en
Authors
PS
Paola Sindaco
SL
Silvia Lonardi
GV
Gabriele Varano
Abstract
1 min read
Abstract The B cell receptor (BCR) is essential for mature B cell lymphomas, serving as therapeutic target. Here, we show that high-grade B cell lymphomas with MYC and BCL2 rearrangements (HGBCL-DH- BCL2 ) predominantly exhibit immunoglobulin heavy (IGH) chain silencing, leading to BCR shutdown. HGBCL-DH- BCL2 with undetectable IGH (IGH UND ) differ from IGH-expressing counterparts for germinal center-zone gene programs, MYC expression and T cell infiltration. While IGH + HGBCL-DH- BCL2 prefer IGM/IG-Kappa expression, IGH UND counterparts have completed IGH class-switching, favoring IG-Lambda (IGL) light chains. IGH UND HGBCL-DH- BCL2 preserve IGHV gene integrity, overcoming antigen-driven selection. IGH silencing precedes onset and shapes evolution of HGBCL-DH- BCL2 from Follicular Lymphoma (FL) or FL/HGBCL-DH- BCL2 common precursor. In FL/HGBCL-DH- BCL2 pairs and HGBCL-DH- BCL2 models, BCR silencing promoted RAG1/2-dependent IG light chain editing, causing t(8;22)(q24;q11)/ IGL :: MYC . IGH silencing protected HGBCL-DH- BCL2 models from killing by CD79B-targeting Polatuzumab-Vedotin. Collectively, HGBCL-DH- BCL2 primarily originate from BCR-silenced isotype-switched t(14;18)/ IGH::BCL2 -positive (pre)FL cells acquiring I GL::MYC translocations during IG light chain revision, with clinical implications. Significance These findings link BCR silencing in isotype-switched t(14;18) + Follicular Lymphoma cells (or their precursors) to RAG1/2 re-expression, promoting IGL::MYC translocations responsible for transformation into high-grade B cell lymphomas (HGBCL). Predominant silencing of the BCR complex in HGBCL with MYC and BCL2 rearrangements protects tumor cells from CD79B-directed Polatuzumab-Vedotin killing.
Silvia Brambillasca, Nicara Chantal Parr, Adriana Palmeri, A. Andronache, Hiroshi Arima, Giovanni Faga’, Brian Leuzzi, Laura Perucho, M. Robusto, Maurizio Pasi, Federica Mainoldi, D. Fancelli, M. Varasi, Gabriele Varano, C. Mercurio, Stefano Casola
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