Therapeutic targeting in pediatric acute myeloid leukemia with aberrant HOX/MEIS1 expression

IF 1.6 4区医学 Q3 GENETICS & HEREDITY

European journal of medical genetics Pub Date : 2023-10-29 DOI:10.1016/j.ejmg.2023.104869

Kristian L. Juul-Dam , Neerav N. Shukla , Todd M. Cooper , Branko Cuglievan , Olaf Heidenreich , E Anders Kolb , Milad Rasouli , Henrik Hasle , C Michel Zwaan

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引用次数: 0

Abstract

Despite advances in the clinical management of childhood acute myeloid leukemia (AML) during the last decades, outcome remains fatal in approximately one third of patients. Primary chemoresistance, relapse and acute and long-term toxicities to conventional myelosuppressive therapies still constitute significant challenges and emphasize the unmet need for effective targeted therapies. Years of scientific efforts have translated into extensive insights on the heterogeneous spectrum of genetics and oncogenic signaling pathways of AML and identified a subset of patients characterized by upregulation of HOXA and HOXB homeobox genes and myeloid ecotropic virus insertion site 1 (MEIS1). Aberrant HOXA/MEIS1 expression is associated with genotypes such as rearrangements in Histone-lysine N-methyltransferase 2A (KMT2A-r), nucleoporin 98 (NUP98-r) and mutated nucleophosmin (NPM1c) that are found in approximately one third of children with AML. AML with upregulated HOXA/MEIS1 shares a number of molecular vulnerabilities amenable to recently developed molecules targeting the assembly of protein complexes or transcriptional regulators. The interaction between the nuclear scaffold protein menin and KMT2A has gained particular interest and constitutes a molecular dependency for maintenance of the HOXA/MEIS1 transcription program. Menin inhibitors disrupt the menin-KMT2A complex in preclinical models of KMT2A-r, NUP98-r and NPM1c acute leukemias and its occupancy at target genes leading to leukemic cell differentiation and apoptosis. Early-phase clinical trials are either ongoing or in development and preliminary data suggests tolerable toxicities and encouraging efficacy of menin inhibitors in adults with relapsed or refractory KMT2A-r and NPM1c AML. The Pediatric Acute Leukemia/European Pediatric Acute Leukemia (PedAL/EUPAL) project is focused to advance and coordinate informative clinical trials with new agents and constitute an ideal framework for testing of menin inhibitors in pediatric study populations. Menin inhibitors in combination with standard chemotherapy or other targeting agents may enhance anti-leukemic effects and constitute rational treatment strategies for select genotypes of childhood AML, and provide enhanced safety to avoid differentiation syndrome. In this review, we discuss the pathophysiological mechanisms in KMT2A-r, NUP98-r and NPM1c AML, emerging molecules targeting the HOXA/MEIS1 transcription program with menin inhibitors as the most prominent examples and future therapeutic implications of these agents in childhood AML.

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儿童急性髓系白血病HOX/MEIS1异常表达的治疗靶向

尽管在过去的几十年里，儿童急性髓性白血病(AML)的临床治疗取得了进展，但大约三分之一的患者的结局仍然是致命的。传统骨髓抑制疗法的原发性化疗耐药、复发以及急性和长期毒性仍然是重大挑战，并强调了有效靶向治疗的未满足需求。多年的科学努力已经转化为对AML遗传异质性谱和致癌信号通路的广泛见解，并确定了以HOXA和HOXB同源盒基因和髓系嗜生态病毒插入位点1 (MEIS1)上调为特征的患者亚群。异常的HOXA/MEIS1表达与组蛋白赖氨酸n -甲基转移酶2A (KMT2A-r)、核孔蛋白98 (NUP98-r)和核磷蛋白突变(NPM1c)等基因型重排相关，这些基因型在大约三分之一的AML患儿中发现。HOXA/MEIS1上调的AML与最近开发的靶向蛋白质复合物组装或转录调节因子的分子具有许多相同的分子脆弱性。核支架蛋白menin和KMT2A之间的相互作用引起了人们的特别关注，并构成了HOXA/MEIS1转录程序维持的分子依赖性。在KMT2A-r、NUP98-r和NPM1c急性白血病的临床前模型中，Menin抑制剂破坏Menin - kmt2a复合物及其在靶基因上的占据，导致白血病细胞分化和凋亡。早期临床试验正在进行或正在进行中，初步数据表明，menin抑制剂对复发或难治性KMT2A-r和NPM1c AML的成人患者具有可耐受的毒性和令人鼓舞的疗效。儿科急性白血病/欧洲儿科急性白血病(PedAL/EUPAL)项目的重点是推进和协调新药物的信息性临床试验，并构成儿科研究人群中menin抑制剂测试的理想框架。Menin抑制剂联合标准化疗或其他靶向药物可增强抗白血病效果，可为选择基因型的儿童AML提供合理的治疗策略，并提高安全性，避免分化综合征。在这篇综述中，我们讨论了KMT2A-r、NUP98-r和NPM1c AML的病理生理机制，以menin抑制剂为最突出的例子，讨论了针对HOXA/MEIS1转录程序的新兴分子以及这些药物在儿童AML中的未来治疗意义。

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

European journal of medical genetics 医学-遗传学

CiteScore

4.10

自引率

0.00%

发文量

193

审稿时长

66 days

期刊介绍： The European Journal of Medical Genetics (EJMG) is a peer-reviewed journal that publishes articles in English on various aspects of human and medical genetics and of the genetics of experimental models. Original clinical and experimental research articles, short clinical reports, review articles and letters to the editor are welcome on topics such as : • Dysmorphology and syndrome delineation • Molecular genetics and molecular cytogenetics of inherited disorders • Clinical applications of genomics and nextgen sequencing technologies • Syndromal cancer genetics • Behavioral genetics • Community genetics • Fetal pathology and prenatal diagnosis • Genetic counseling.