Epigenetic regulation of cell state by H2AFY governs immunogenicity in high-risk neuroblastoma.

Divya Nagarajan,Rebeca T Parracho,David Corujo,Minglu Xie,Ginte Kutkaite,Thale K Olsen,Marta Rúbies Bedós,Maede Salehi,Ninib Baryawno,Michael P Menden,Xingqi Chen,Marcus Buschbeck,Yumeng Mao
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Abstract

Childhood neuroblastoma with MYCN-amplification is classified as high-risk and often relapses after intensive treatments. Immune checkpoint blockade therapy against the PD-1/L1 axis shows limited efficacy in neuroblastoma patients and the cancer intrinsic immune regulatory network is poorly understood. Here, we leverage genome-wide CRISPR/Cas9 screens and identify H2AFY as a resistance gene to the clinically approved PD-1 blocking antibody, nivolumab. Analysis of single-cell RNA sequencing datasets reveals that H2AFY mRNA is enriched in adrenergic cancer cells and is associated with worse patient survival. Genetic deletion of H2afy in MYCN-driven neuroblastoma cells reverts in vivo resistance to PD-1 blockade by eliciting activation of the adaptive and innate immunity. Mapping of the epigenetic and translational landscape demonstrates that H2afy deletion promotes cell transition to a mesenchymal-like state. With a multi-omics approach, we uncover H2AFY-associated genes that are functionally relevant and prognostic in patients. Altogether, our study elucidates the role of H2AFY as an epigenetic gatekeeper for cell states and immunogenicity in high-risk neuroblastoma.
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H2AFY对细胞状态的表观遗传调控制约着高危神经母细胞瘤的免疫原性。
MYCN扩增的儿童神经母细胞瘤被列为高危肿瘤,在接受强化治疗后往往会复发。针对PD-1/L1轴的免疫检查点阻断疗法对神经母细胞瘤患者的疗效有限,而且人们对癌症内在免疫调节网络知之甚少。在这里,我们利用全基因组CRISPR/Cas9筛选,确定了H2AFY是临床批准的PD-1阻断抗体nivolumab的抗性基因。对单细胞 RNA 测序数据集的分析表明,H2AFY mRNA 在肾上腺素能癌细胞中富集,并与患者生存率降低有关。在MYCN驱动的神经母细胞瘤细胞中遗传性删除H2afy可通过激活适应性免疫和先天性免疫来恢复体内对PD-1阻断剂的抗性。表观遗传学和翻译图谱显示,H2afy缺失会促进细胞向间充质样状态转化。通过多组学方法,我们发现了与H2AFY相关的基因,这些基因与患者的功能和预后相关。总之,我们的研究阐明了 H2AFY 在高风险神经母细胞瘤中作为细胞状态和免疫原性的表观遗传看门人的作用。
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