ARID1A mutations protect follicular lymphoma from FAS-dependent immune surveillance by reducing RUNX3/ETS1-driven FAS-expression

IF 13.7 1区生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY

Cell Death and Differentiation Pub Date : 2025-01-23 DOI:10.1038/s41418-025-01445-3

Martina Antoniolli, Maria Solovey, Johannes Adrian Hildebrand, Tabea Freyholdt, Carolin Dorothea Strobl, Deepak Bararia, William David Keay, Louisa Adolph, Michael Heide, Verena Passerini, Lis Winter, Lucas Wange, Wolfgang Enard, Susanne Thieme, Helmut Blum, Martina Rudelius, Julia Mergner, Christina Ludwig, Sebastian Bultmann, Marc Schmidt-Supprian, Heinrich Leonhardt, Marion Subklewe, Michael von Bergwelt-Baildon, Maria Colomé-Tatché, Oliver Weigert

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Abstract

The cell death receptor FAS and its ligand (FASLG) play crucial roles in the selection of B cells during the germinal center (GC) reaction. Failure to eliminate potentially harmful B cells via FAS can lead to lymphoproliferation and the development of B cell malignancies. The classic form of follicular lymphoma (FL) is a prototypic GC-derived B cell malignancy, characterized by the t(14;18)(q32;q21)IGH::BCL2 translocation and overexpression of antiapoptotic BCL2. Additional alterations were shown to be clinically relevant, including mutations in ARID1A. ARID1A is part of the SWI/SNF nucleosome remodeling complex that regulates DNA accessibility (“openness”). However, the mechanism how ARID1A mutations contribute to FL pathogenesis remains unclear. We analyzed 151 FL biopsies of patients with advanced-stage disease at initial diagnosis and found that ARID1A mutations were recurrent and mainly disruptive, with an overall frequency of 18%. Additionally, we observed that ARID1A mutant FL showed significantly lower FAS protein expression in the FL tumor cell population. Functional experiments in BCL2-translocated lymphoma cells demonstrated that ARID1A is directly involved in the regulation of FAS, and ARID1A loss leads to decreased FAS protein and gene expression. However, ARID1A loss did not affect FAS promotor openness. Instead, we identified and experimentally validated a previously unknown co-transcriptional complex consisting of RUNX3 and ETS1 that regulates FAS expression, and ARID1A loss leads to reduced RUNX3 promotor openness and gene expression. The reduced FAS levels induced by ARID1A loss rendered lymphoma cells resistant to both soluble and T cell membrane-anchored FASLG-induced apoptosis, and significantly diminished CAR T cell killing in functional experiments. In summary, we have identified a functionally and clinically relevant mechanism how FL cells can escape FAS-dependent immune surveillance, which may also impact the efficacy of T cell-based therapies, including CAR T cells.

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ARID1A突变通过降低RUNX3/ ets1驱动的fas表达来保护滤泡性淋巴瘤免受fas依赖性免疫监视

细胞死亡受体FAS及其配体（FASLG）在生发中心（GC）反应中对B细胞的选择起着至关重要的作用。不能通过FAS消除潜在有害的B细胞可导致淋巴细胞增殖和B细胞恶性肿瘤的发展。滤泡性淋巴瘤（FL）的典型形式是一种典型的gc源性B细胞恶性肿瘤，其特征是t(14;18)(q32;q21)IGH::BCL2易位和抗凋亡BCL2过表达。其他改变被证明与临床相关，包括ARID1A突变。ARID1A是调节DNA可及性（“开放性”）的SWI/SNF核小体重塑复合体的一部分。然而，ARID1A突变导致FL发病的机制尚不清楚。我们分析了151例初始诊断为晚期疾病的FL活检患者，发现ARID1A突变是复发性的，主要是破坏性的，总频率为18%。此外，我们观察到ARID1A突变体FL在FL肿瘤细胞群中FAS蛋白表达显著降低。在bcl2易位淋巴瘤细胞中的功能实验表明，ARID1A直接参与FAS的调控，ARID1A缺失导致FAS蛋白和基因表达下降。然而，ARID1A缺失并不影响FAS启动子的开放程度。相反，我们鉴定并实验验证了一个由RUNX3和ETS1组成的先前未知的共转录复合物，该复合物调节FAS表达，ARID1A缺失导致RUNX3启动子开放度降低和基因表达降低。在功能实验中，ARID1A缺失导致的FAS水平降低使淋巴瘤细胞对可溶性和T细胞膜锚定的fassg诱导的凋亡产生抗性，并显著减少CAR - T细胞的杀伤。总之，我们已经确定了FL细胞如何逃避fas依赖的免疫监视的功能和临床相关机制，这也可能影响T细胞疗法（包括CAR - T细胞）的疗效。

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来源期刊

Cell Death and Differentiation 生物-生化与分子生物学

CiteScore

24.70

自引率

1.60%

发文量

181

审稿时长

3 months

期刊介绍： Mission, vision and values of Cell Death & Differentiation: To devote itself to scientific excellence in the field of cell biology, molecular biology, and biochemistry of cell death and disease. To provide a unified forum for scientists and clinical researchers It is committed to the rapid publication of high quality original papers relating to these subjects, together with topical, usually solicited, reviews, meeting reports, editorial correspondence and occasional commentaries on controversial and scientifically informative issues.