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Chromosomal instability upregulates interferon in acute myeloid leukemia.

染色体不稳定性上调急性髓系白血病的干扰素。

  • 影响因子:3.04
  • DOI:10.1002/gcc.22880
  • 作者列表:"Jin N","Lera RF","Yan RE","Guo F","Oxendine K","Horner VL","Hu Y","Wan J","Mattison RJ","Weaver BA","Burkard ME
  • 发表时间:2020-06-17
Abstract

:Chromosome instability (CIN) generates genetic and karyotypic diversity that is common in hematological malignancies. Low to moderate levels of CIN are well tolerated and can promote cancer proliferation. However, high levels of CIN are lethal. Thus, CIN may serve both as a prognostic factor to predict clinical outcome and as a predictive biomarker. A retrospective study was performed to evaluate CIN in acute myeloid leukemia (AML). Chromosome mis-segregation frequency was correlated with clinical outcome in bone marrow core biopsy specimens from 17 AML cases. Additionally, we induced chromosome segregation errors in AML cell lines with AZ3146, an inhibitor of the Mps1 mitotic checkpoint kinase, to quantify the phenotypic effects of high CIN. We observed a broad distribution of chromosome mis-segregation frequency in AML bone marrow core specimens. High CIN correlated with complex karyotype in AML, as expected, although there was no clear survival effect. In addition to CIN, experimentally inducing chromosome segregation errors by Mps1 inhibition in AML cell lines causes DNA damage, micronuclei formation and upregulation of interferon stimulated genes. High levels of CIN appear to be immunostimulatory, suggesting an opportunity to combine mitotic checkpoint inhibitors with immunotherapy in treatment of AML. This article is protected by copyright. All rights reserved.

摘要

: 染色体不稳定性 (CIN) 产生遗传和核型多样性,常见于血液系统恶性肿瘤。低至中度水平的 CIN 耐受性良好,可促进癌症增殖。然而,高水平的 CIN 是致命的。因此,CIN 既可以作为预测临床结果的预后因素,也可以作为预测生物标志物。本文回顾性研究急性髓系白血病 (AML) 的 CIN。染色体错分频率与 17 例 AML 骨髓核心活检标本的临床结局相关。此外,我们用 Mps1 有丝分裂检查点激酶的抑制剂 AZ3146 在 AML 细胞系中诱导染色体分离错误,以量化高 CIN 的表型效应。我们在 AML 骨髓核心标本中观察到染色体错分频率的广泛分布。高 CIN 与 AML 中复杂核型相关,不出所料,尽管没有明确的生存效应。除 CIN 外,AML 细胞系中通过 Mps1 抑制实验诱导染色体分离错误引起 DNA 损伤、微核形成和干扰素刺激基因的上调。高水平的 CIN 似乎具有免疫刺激作用,提示有丝分裂检查点抑制剂与免疫疗法联合治疗 AML 的机会。本文受版权保护。保留所有权利。

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