AML中NUP98重排的分子机制及其临床意义

Onco Pub Date : 2023-07-18 DOI:10.3390/onco3030011
Sagarajit Mohanty
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引用次数: 0

摘要

NUP98融合构成了AML患者的一个小亚组,并且仍然是一个高风险的AML亚型。在AML患者中发现了大约30种类型的NUP98融合。这些患者表现出对现有治疗方法的耐药性和较差的临床结果。NUP98与不同融合伙伴的融合具有致癌转化潜能。这篇综述描述了NUP98基因如何在与多个伙伴重排后获得致癌特性。在机制部分,强调了核体的形成和HoxA/Meis1通路的失调。本文还讨论了NUP98融合体的突变特征及其在白血病发生中的意义。它还讨论了NUP98融合及其相关突变在AML患者中的临床意义。此外,它强调了这些白血病的治疗脆弱性,可以作为治疗策略加以利用。最后,本文讨论了我们在AML中关于NUP98融合的知识差距,以及未来的研究机会。
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NUP98 Rearrangements in AML: Molecular Mechanisms and Clinical Implications
NUP98 fusions constitute a small subgroup of AML patients and remain a high-risk AML subtype. There are approximately 30 types of NUP98 fusions identified in AML patients. These patients show resistance to currently available therapies and poor clinical outcomes. NUP98 fusions with different fusion partners have oncogenic transformation potential. This review describes how the NUP98 gene acquires oncogenic properties after rearrangement with multiple partners. In the mechanistic part, the formation of nuclear bodies and dysregulation of the HoxA/Meis1 pathway are highlighted. This review also discusses mutational signatures among NUP98 fusions and their significance in leukemogenesis. It also discusses the clinical implications of NUP98 fusions and their associated mutations in AML patients. Furthermore, it highlights therapeutic vulnerabilities in these leukemias that can be exploited as therapeutic strategies. Lastly, this review discusses the gaps in our knowledge regarding NUP98 fusions in AML, as well as future research opportunities.
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