Cellular carcinogenesis in preleukemic conditions:drivers and defenses.

IF 0.7 Q3 MEDICINE, GENERAL & INTERNAL

Fukushima Journal of Medical Science Pub Date : 2024-01-27 Epub Date: 2023-11-11 DOI:10.5387/fms.2023-17

Koki Ueda, Kazuhiko Ikeda

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Abstract

Acute myeloid leukemia (AML) arises from preleukemic conditions. We have investigated the pathogenesis of typical preleukemia, myeloproliferative neoplasms, and clonal hematopoiesis. Hematopoietic stem cells in both preleukemic conditions harbor recurrent driver mutations; additional mutation provokes further malignant transformation, leading to AML onset. Although genetic alterations are defined as the main cause of malignant transformation, non-genetic factors are also involved in disease progression. In this review, we focus on a non-histone chromatin protein, high mobility group AT-hook2 (HMGA2), and a physiological p53 inhibitor, murine double minute X (MDMX). HMGA2 is mainly overexpressed by dysregulation of microRNAs or mutations in polycomb components, and provokes expansion of preleukemic clones through stem cell signature disruption. MDMX is overexpressed by altered splicing balance in myeloid malignancies. MDMX induces leukemic transformation from preleukemia via suppression of p53 and p53-independent activation of WNT/β-catenin signaling. We also discuss how these non-genetic factors can be targeted for leukemia prevention therapy.

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白血病前期的细胞癌变:驱动因素和防御因素。

急性髓性白血病(AML)起源于白血病前期。我们研究了典型的白血病前期、骨髓增生性肿瘤和克隆造血的发病机制。两种白血病前期的造血干细胞都有反复发生的驱动突变;额外的突变引起进一步的恶性转化，导致AML发病。虽然遗传改变被定义为恶性转化的主要原因，但非遗传因素也参与疾病进展。在这篇综述中，我们重点研究了一种非组蛋白染色质蛋白，高迁移率组AT-hook2 (HMGA2)和一种生理p53抑制剂，小鼠双分钟X (MDMX)。HMGA2主要通过microrna的失调或多梳组分的突变而过度表达，并通过干细胞特征破坏引起白血病前克隆的扩增。MDMX在髓系恶性肿瘤中通过剪接平衡的改变而过表达。MDMX通过抑制p53和p53独立的WNT/β-catenin信号激活诱导白血病前期转化。我们还讨论了这些非遗传因素如何靶向白血病预防治疗。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Fukushima Journal of Medical Science MEDICINE, GENERAL & INTERNAL-

CiteScore

1.70

自引率

12.50%

发文量