| Literature DB >> 28791558 |
Yosuke Watanabe1, Yoshiaki Ishizuka1, Takayuki Hirano1, Eri Nagasaki-Maeoka1, Reina Hoshi1, Shinsuke Yoshizawa1, Shota Uekusa1, Hiroyuki Kawashima1, Kiminobu Sugito1, Kenichi Shinohara2, Noboru Fukuda3, Hiroki Nagase4, Masayoshi Soma5, Tsugumichi Koshinaga6, Kyoko Fujiwara7.
Abstract
Although DNA hypermethylation at non-promoter region of the Zygote arrest 1 (ZAR1) gene has been observed in many types of tumor, including neuroblastoma (NB), the role of this gene in tumor development and/or progression is unclear. One reason is that knowledge about the function of ZAR1 protein is limited. Although it has been reported that ZAR1 plays a crucial role in early embryogenesis and may act as a transcriptional repressor for some transcripts, the detailed mechanism is still elusive. In the present study, we analyzed public data of NB patients and found that higher expression levels of ZAR1 were significantly associated with a shorter survival period. Consistent with this result, ZAR1-depleted NB cells showed well-differentiated phenotypes with elongated neurites and upregulated expression of TRKA and RET, which are markers for differentiated NB. Moreover, the expression level of MYCN protein was markedly suppressed in ZAR1-depleted NB cells. MYCN-depleted cells showed similar phenotypes to ZAR1-depleted cells. The present findings indicate that ZAR1 has oncogenic effects in NB by suppressing cell differentiation via regulation of MYCN expression.Entities:
Keywords: Cell differentiation; MYCN; Neuroblastoma; Oncogene; ZAR1
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Year: 2017 PMID: 28791558 DOI: 10.1007/s12032-017-0999-x
Source DB: PubMed Journal: Med Oncol ISSN: 1357-0560 Impact factor: 3.064