The MicroRNA Landscape of MYCN-Amplified Neuroblastoma

Misiak, Danny; Hagemann, Sven; Bell, Jessica L.; Busch, Bianca; Lederer, Marcell; Bley, Nadine; Schulte, Johannes H.; Hüttelmaier, Stefan

doi:10.3389/fonc.2021.647737

Cited by 19 publications

(30 citation statements)

References 51 publications

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“…MiRNAs targeting MYCN were found to be particularly important in regulating its expression in neuroblastoma in different ways [ 8 , 226 ]. Some miRNAs targeting MYCN, such as the let-7 family, work as inhibitors [ 227 ] and are down-regulated in neuroblastoma, inducing N-Myc protein expression [ 228 , 229 , 230 ]. These miRNA types are considered the most common, but other miRNAs were found to work with the opposite mechanism.…”

Section: Mycn Determines High-risk Neuroblastomamentioning

confidence: 99%

“…For instance, miRNAs such as the family of miR-17-92 are substantially employed as MYCN up-regulators. Interestingly N-Myc is able to stimulate the expression of miR-17-92 cluster, suggesting the presence of a positive feedback mechanism of regulation between MYCN and the miR-17-92 cluster itself [ 230 , 231 , 232 ].…”

Section: Mycn Determines High-risk Neuroblastomamentioning

confidence: 99%

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MYCN Impact on High-Risk Neuroblastoma: From Diagnosis and Prognosis to Targeted Treatment

Bartolucci

Montemurro

Raieli³

et al. 2022

Cancers

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Among childhood cancers, neuroblastoma is the most diffuse solid tumor and the deadliest in children. While to date, the pathology has become progressively manageable with a significant increase in 5-year survival for its less aggressive form, high-risk neuroblastoma (HR-NB) remains a major issue with poor outcome and little survivability of patients. The staging system has also been improved to better fit patient needs and to administer therapies in a more focused manner in consideration of pathology features. New and improved therapies have been developed; nevertheless, low efficacy and high toxicity remain a staple feature of current high-risk neuroblastoma treatment. For this reason, more specific procedures are required, and new therapeutic targets are also needed for a precise medicine approach. In this scenario, MYCN is certainly one of the most interesting targets. Indeed, MYCN is one of the most relevant hallmarks of HR-NB, and many studies has been carried out in recent years to discover potent and specific inhibitors to block its activities and any related oncogenic function. N-Myc protein has been considered an undruggable target for a long time. Thus, many new indirect and direct approaches have been discovered and preclinically evaluated for the interaction with MYCN and its pathways; a few of the most promising approaches are nearing clinical application for the investigation in HR-NB.

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Section: Mycn Determines High-risk Neuroblastomamentioning

confidence: 99%

Section: Mycn Determines High-risk Neuroblastomamentioning

confidence: 99%

MYCN Impact on High-Risk Neuroblastoma: From Diagnosis and Prognosis to Targeted Treatment

Bartolucci

Montemurro

Raieli³

et al. 2022

Cancers

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“…The result from the interaction between miRNAs and mRNAs is the silencing of the second, through three main processes; The first concerns mRNA cleavage, the second concerns the destabilization of the mRNA through shortening of its poly(A) tail, and finally the third concerns the inhibition of translation in the ribosomes [ 123 ]. Similarly, the MYCN gene is known to be regulated by miRNAs [ 124 ]. A search for possible miRNA targets of MYCN revealed a total of 234 miRNAs, using the miRDB database [ 125 , 126 , 127 , 128 ], which we present in the Supplementary Materials Table S1 .…”

Section: Molecular Mechanistics Of the Mycn Genementioning

confidence: 99%

MYCN in Neuroblastoma: “Old Wine into New Wineskins”

et al. 2021

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MYCN Proto-Oncogene, BHLH Transcription Factor (MYCN) has been one of the most studied genes in neuroblastoma. It is known for its oncogenetic mechanisms, as well as its role in the prognosis of the disease and it is considered one of the prominent targets for neuroblastoma therapy. In the present work, we attempted to review the literature, on the relation between MYCN and neuroblastoma from all possible mechanistic sites. We have searched the literature for the role of MYCN in neuroblastoma based on the following topics: the references of MYCN in the literature, the gene’s anatomy, along with its transcripts, the protein’s anatomy, the epigenetic mechanisms regulating MYCN expression and function, as well as MYCN amplification. MYCN plays a significant role in neuroblastoma biology. Its functions and properties range from the forming of G-quadraplexes, to the interaction with miRNAs, as well as the regulation of gene methylation and histone acetylation and deacetylation. Although MYCN is one of the most primary genes studied in neuroblastoma, there is still a lot to be learned. Our knowledge on the exact mechanisms of MYCN amplification, etiology and potential interventions is still limited. The knowledge on the molecular mechanisms of MYCN in neuroblastoma, could have potential prognostic and therapeutic advantages.

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“…However, in vivo treatment with single-agent binimetinib in various neuroblastoma cell line-derived xenograft models demonstrated inhibition of tumor growth and extended survival in NRAS or NF1 mutated xenografts while ALK mutated tumors did not respond, likely due to persistent or alternative tyrosine kinase pathway activation [ 8 , 93 ]. Moreover, there may be a role for microRNAs such as the let-7 microRNA family for contributing to ALK inhibitor therapy resistance by regulating RAS expression [ 94 , 95 ]. Therefore, these findings suggest the need for combined targeting of pathways.…”

Section: Yap and Its Role In High-risk Neuroblastomamentioning

confidence: 99%

A New Player in Neuroblastoma: YAP and Its Role in the Neuroblastoma Microenvironment

Shim

Goldsmith

2021

Cancers

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Neuroblastoma is the most common extra-cranial pediatric solid tumor that accounts for more than 15% of childhood cancer-related deaths. High risk neuroblastomas that recur during or after intense multimodal therapy have a <5% chance at a second sustained remission or cure. The solid tumor microenvironment (TME) has been increasingly recognized to play a critical role in cancer progression and resistance to therapy, including in neuroblastoma. The Yes-Associated Protein (YAP) in the Hippo pathway can regulate cancer proliferation, tumor initiation, and therapy response in many cancer types and as such, its role in the TME has gained interest. In this review, we focus on YAP and its role in neuroblastoma and further describe its demonstrated and potential effects on the neuroblastoma TME. We also discuss the therapeutic strategies for inhibiting YAP in neuroblastoma.

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The MicroRNA Landscape of MYCN-Amplified Neuroblastoma

Cited by 19 publications

References 51 publications

MYCN Impact on High-Risk Neuroblastoma: From Diagnosis and Prognosis to Targeted Treatment

MYCN Impact on High-Risk Neuroblastoma: From Diagnosis and Prognosis to Targeted Treatment

MYCN in Neuroblastoma: “Old Wine into New Wineskins”

A New Player in Neuroblastoma: YAP and Its Role in the Neuroblastoma Microenvironment

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