Genetic Aberrations and Interaction of NEK2 and TP53 Accelerate Aggressiveness of Multiple Myeloma
Abstract: It has been previously shown that (never in mitosis gene A)‐related kinase 2 (NEK2) is upregulated in multiple myeloma (MM) and contributes to drug resistance. However, the mechanisms behind this upregulation remain poorly understood. In this study, it is found that amplification of NEK2 and hypermethylation of distal CpG islands in its promoter correlate strongly with increased NEK2 expression. Patients with NEK2 amplification have a poor rate of survival and often exhibit TP53 deletion, which is an independent prognostic factor in MM. This combination of TP53 knockout and NEK2 overexpression induces asymmetric mitosis, proliferation, drug resistance, and tumorigenic behaviors in MM in vitro and in vivo. In contrast, delivery of wild type p53 and suppression of NEK2 in TP53−/− MM cell lines inhibit tumor formation and enhance the effect of Bortezomib against MM. It is also discovered that inactivating p53 elevates NEK2 expression genetically by inducing NEK2 amplification, transcriptionally by increased activity of cell cycle‐related genes like E2F8 and epigenetically by upregulating DNA methyltransferases. Dual defects of TP53 and NEK2 may define patients with the poorest outcomes in MM with p53 inactivation, and NEK2 may serve as a novel therapeutic target in aggressive MM with p53 abnormalities.
- Location
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Deutsche Nationalbibliothek Frankfurt am Main
- Extent
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Online-Ressource
- Language
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Englisch
- Bibliographic citation
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Genetic Aberrations and Interaction of NEK2 and TP53 Accelerate Aggressiveness of Multiple Myeloma ; day:27 ; month:01 ; year:2022 ; extent:19
Advanced science ; (27.01.2022) (gesamt 19)
- Creator
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Feng, Xiangling
Guo, Jiaojiao
An, Gang
Wu, Yangbowen
Liu, Zhenhao
Meng, Bin
He, Nihan
Zhao, Xinying
Chen, Shilian
Zhu, Yinghong
Xia, Jiliang
Li, Xin
Yu, Zhiyong
Li, Ruixuan
Ren, Guofeng
Chen, Jihua
Wu, Minghua
He, Yanjuan
Qiu, Lugui
Zhou, Jiaxi
Zhou, Wen
- DOI
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10.1002/advs.202104491
- URN
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urn:nbn:de:101:1-2022012814174677366093
- Rights
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Open Access; Der Zugriff auf das Objekt ist unbeschränkt möglich.
- Last update
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15.08.2025, 7:22 AM CEST
Data provider
Deutsche Nationalbibliothek. If you have any questions about the object, please contact the data provider.
Associated
- Feng, Xiangling
- Guo, Jiaojiao
- An, Gang
- Wu, Yangbowen
- Liu, Zhenhao
- Meng, Bin
- He, Nihan
- Zhao, Xinying
- Chen, Shilian
- Zhu, Yinghong
- Xia, Jiliang
- Li, Xin
- Yu, Zhiyong
- Li, Ruixuan
- Ren, Guofeng
- Chen, Jihua
- Wu, Minghua
- He, Yanjuan
- Qiu, Lugui
- Zhou, Jiaxi
- Zhou, Wen
Other Objects (12)
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Pathogenic germline aberrations in TP53 and BRCA1/2-negative breast cancer patients suggestive of Li-Fraumeni syndrome
Clonal evolution after treatment pressure in multiple myeloma: heterogenous genomic aberrations and transcriptomic convergence
Microbiota-driven interleukin-17-producing cells and eosinophils synergize to accelerate multiple myeloma progression
Aggressiveness and Redistribution
Identifying novel mechanisms of biallelic TP53 loss refines poor outcome for patients with multiple myeloma
Hyperhaploid plasma cell myeloma characterized by poor outcome and monosomy 17 with frequently co-occurring TP53 mutations
Alterations of gut microbiome accelerate multiple myeloma progression by increasing the relative abundances of nitrogen-recycling bacteria
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Sexual aberrations, Vol. 2.
Epigenetic aberrations and cancer
Comparison of acute myeloid leukemia and myelodysplastic syndromes with TP53 aberrations
The clinical characteristics and prognosis in adult Ph negative acute lymphoblastic leukemia with TP53 aberrations
Pathogenic germline aberrations in TP53 and BRCA1/2-negative breast cancer patients suggestive of Li-Fraumeni syndrome
Clonal evolution after treatment pressure in multiple myeloma: heterogenous genomic aberrations and transcriptomic convergence
Microbiota-driven interleukin-17-producing cells and eosinophils synergize to accelerate multiple myeloma progression
Aggressiveness and Redistribution
Identifying novel mechanisms of biallelic TP53 loss refines poor outcome for patients with multiple myeloma
Hyperhaploid plasma cell myeloma characterized by poor outcome and monosomy 17 with frequently co-occurring TP53 mutations
Alterations of gut microbiome accelerate multiple myeloma progression by increasing the relative abundances of nitrogen-recycling bacteria
Sexual aberrations, Vol. 1.
Sexual aberrations, Vol. 2.
Epigenetic aberrations and cancer
Comparison of acute myeloid leukemia and myelodysplastic syndromes with TP53 aberrations
The clinical characteristics and prognosis in adult Ph negative acute lymphoblastic leukemia with TP53 aberrations
Pathogenic germline aberrations in TP53 and BRCA1/2-negative breast cancer patients suggestive of Li-Fraumeni syndrome
Clonal evolution after treatment pressure in multiple myeloma: heterogenous genomic aberrations and transcriptomic convergence
Microbiota-driven interleukin-17-producing cells and eosinophils synergize to accelerate multiple myeloma progression
Aggressiveness and Redistribution
Identifying novel mechanisms of biallelic TP53 loss refines poor outcome for patients with multiple myeloma
Hyperhaploid plasma cell myeloma characterized by poor outcome and monosomy 17 with frequently co-occurring TP53 mutations
Alterations of gut microbiome accelerate multiple myeloma progression by increasing the relative abundances of nitrogen-recycling bacteria
Sexual aberrations, Vol. 1.
Sexual aberrations, Vol. 2.