MicroRNA-221 Enhances MYCN Via Targeting Nemo-like Kinase and Functions As an Oncogene Related to Poor Prognosis in Neuroblastoma

Overview

Journal Clin Cancer Res

Specialty Oncology

Date 2016 Dec 23

PMID 28003306

Citations 18

Authors

Xiao-Yan He

Zheng-Lan Tan

Qin Mou

Fang-Jie Liu

Shan Liu

Chao-Wen Yu

Jin Zhu

Lin-Ya Lv

Jun Zhang

Shan Wang

Li-Ming Bao

Bin Peng

Hui Zhao

Lin Zou

Affiliations

Soon will be listed here.

Abstract

is one of the most well-characterized genetic markers of neuroblastoma. However, the mechanisms as to how mediate neuroblastoma tumorigenesis are not fully clear. Increasing evidence has confirmed that the dysregulation of miRNAs is involved in MYCN-mediated neuroblastoma tumorigenesis, supporting their potential as therapeutic targets for neuroblastoma. Although miR-221 has been reported as one of the upregulated miRNAs, the interplay between miR-221 and MYCN-mediated neuroblastoma progression remains largely elusive. The expression of miR-221 in the formalin-fixed, paraffin-embedded tissues from 31 confirmed patients with neuroblastoma was detected by locked nucleic acid- hybridization and qRT-PCR. The correlation between miR-221 expression and clinical features in patients with neuroblastoma was assessed. The mechanisms as to how miR-221 regulate MYCN in neuroblastoma were addressed. The effect of miR-221 on cellular proliferation in neuroblastoma was determined both and miR-221 was significantly upregulated in neuroblastoma tumor cells and tissues that overexpress MYCN, and high expression of miR-221 was positively associated with poor survival in patients with neuroblastoma. Nemo-like kinase (NLK) as a direct target of miR-221 in neuroblastoma was verified. In addition, overexpression of miR-221 decreased LEF1 phosphorylation but increased the expression of MYCN via targeting of NLK and further regulated cell cycle, particularly in S-phase, promoting the growth of neuroblastoma cells. This study provides a novel insight for miR-221 in the control of neuroblastoma cell proliferation and tumorigenesis, suggesting potentials of miR-221 as a prognosis marker and therapeutic target for patients with MYCN overexpressing neuroblastoma. .

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