| Literature DB >> 28329685 |
Xiaoling Zhang1, Zhiwei Dong1, Cheng Zhang2, Choong Yong Ung2, Shuning He3, Ting Tao3, Andre M Oliveira4, Alexander Meves5, Baoan Ji1, A Thomas Look3, Hu Li2, Benjamin G Neel6, Shizhen Zhu7.
Abstract
Growing evidence suggests a major role for Src-homology-2-domain-containing phosphatase 2 (SHP2/PTPN11) in MYCN-driven high-risk neuroblastoma, although biologic confirmation and a plausible mechanism for this contribution are lacking. Using a zebrafish model of MYCN-overexpressing neuroblastoma, we demonstrate that mutant ptpn11 expression in the adrenal gland analog of MYCN transgenic fish promotes the proliferation of hyperplastic neuroblasts, accelerates neuroblastomagenesis, and increases tumor penetrance. We identify a similar mechanism in tumors with wild-type ptpn11 and dysregulated Gab2, which encodes a Shp2 activator that is overexpressed in human neuroblastomas. In MYCN transgenic fish, Gab2 overexpression activated the Shp2-Ras-Erk pathway, enhanced neuroblastoma induction, and increased tumor penetrance. We conclude that MYCN cooperates with either GAB2-activated or mutant SHP2 in human neuroblastomagenesis. Our findings further suggest that combined inhibition of MYCN and the SHP2-RAS-ERK pathway could provide effective targeted therapy for high-risk neuroblastoma patients with MYCN amplification and aberrant SHP2 activation.Entities:
Keywords: Gab2; MYCN; RAS-ERK pathway; Shp2; neuroblastoma; ptpn11; zebrafish
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Year: 2017 PMID: 28329685 PMCID: PMC5393048 DOI: 10.1016/j.celrep.2017.02.065
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423