Data from Natural Killer Cell–Mediated Cytotoxicity Shapes the Clonal Evolution of B-cell Leukemia

细胞毒性 细胞 自然(考古学) 自然杀伤细胞 白血病 生物 癌症的体细胞进化 癌症研究 免疫学 遗传学 癌症 体外 古生物学
作者
Michelle C. Buri,Mohamed R. Shoeb,Aleksandr Bykov,Peter Repiščák,Hayeon Baik,Alma Dupanovic,Faith O. David,Boris Kovacic,Faith Hall‐Glenn,Sara Dopa,Jos Urbanus,Lisa Sippl,Susanne Stofner,Dominik Emminger,Jason Cosgrove,Dagmar Schinnerl,Anna R. Poetsch,Manfred Lehner,Xaver Koenig,Leïla Perié
标识
DOI:10.1158/2326-6066.c.7702665
摘要

<div>Abstract<p>The term cancer immunoediting describes the dual role by which the immune system can suppress and promote tumor growth and is divided into three phases: elimination, equilibrium, and escape. The role of NK cells has mainly been attributed to the elimination phase. Here, we show that NK cells play a role in all three phases of cancer immunoediting. Extended co-culturing of DNA-barcoded mouse BCR/ABL<sup>p185+</sup> B-cell acute lymphoblastic leukemia (B-ALL) cells with NK cells allowed for a quantitative measure of NK cell–mediated immunoediting. Although most tumor cell clones were efficiently eliminated by NK cells, a certain fraction of tumor cells harbored an intrinsic primary resistance. Furthermore, DNA barcoding revealed tumor cell clones with secondary resistance, which stochastically acquired resistance to NK cells. NK cell–mediated cytotoxicity put a selective pressure on B-ALL cells, which led to an outgrowth of primary and secondary resistant tumor cell clones, which were characterized by an IFNγ signature. Besides well-known regulators of immune evasion, our analysis of NK cell–resistant tumor cells revealed the upregulation of genes, including lymphocyte antigen 6 complex, locus A (<i>Ly6a</i>), which we found to promote leukemic cell resistance to NK cells. Translation of our findings to the human system showed that high expression of <i>LY6E</i> on tumor cells impaired their physical interaction with NK cells and led to worse prognosis in patients with leukemia. Our results demonstrate that tumor cells are actively edited by NK cells during the equilibrium phase and use different avenues to escape NK cell–mediated eradication.</p></div>
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