CRISPR-GEMM Pooled Mutagenic Screening Identifies KMT2D as a Major Modulator of Immune Checkpoint Blockade

生物 清脆的 癌症研究 免疫检查点 染色质重塑 染色质 突变 免疫系统 遗传学 突变 计算生物学 免疫疗法 基因
作者
Guangchuan Wang,Ryan D. Chow,Lvyun Zhu,Zhigang Bai,Lupeng Ye,Feifei Zhang,Paul Renauer,Matthew B. Dong,Xiaoyun Dai,Xiaoya Zhang,Yaying Du,Yujing Cheng,Leilei Niu,Zhiyuan Chu,Kristin Kim,Cun Liao,Paul Clark,Youssef Errami,Sidi Chen
出处
期刊:Cancer Discovery [American Association for Cancer Research]
卷期号:10 (12): 1912-1933 被引量:109
标识
DOI:10.1158/2159-8290.cd-19-1448
摘要

Abstract Immune checkpoint blockade (ICB) has shown remarkable clinical efficacy in several cancer types. However, only a fraction of patients will respond to ICB. Here, we performed pooled mutagenic screening with CRISPR-mediated genetically engineered mouse models (CRISPR-GEMM) in ICB settings, and identified KMT2D as a major modulator of ICB response across multiple cancer types. KMT2D encodes a histone H3K4 methyltransferase and is among the most frequently mutated genes in patients with cancer. Kmt2d loss led to increased DNA damage and mutation burden, chromatin remodeling, intron retention, and activation of transposable elements. In addition, Kmt2d-mutant cells exhibited increased protein turnover and IFNγ-stimulated antigen presentation. In turn, Kmt2d-mutant tumors in both mouse and human were characterized by increased immune infiltration. These data demonstrate that Kmt2d deficiency sensitizes tumors to ICB by augmenting tumor immunogenicity, and also highlight the power of CRISPR-GEMMs for interrogating complex molecular landscapes in immunotherapeutic contexts that preserve the native tumor microenvironment. Significance: ICB is ineffective in the majority of patients. Through direct in vivo CRISPR mutagenesis screening in GEMMs of cancer, we find Kmt2d deficiency sensitizes tumors to ICB. Considering the prevalence of KMT2D mutations, this finding potentially has broad implications for patient stratification and clinical decision-making. This article is highlighted in the In This Issue feature, p. 1775
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