Proliferation and survival of embryonic sympathetic neuroblasts by MYCN and activated ALK signaling

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Abstract

Neuroblastoma (NB) is a childhood tumor that arises from the sympathoadrenal lineage.MYCNamplification is the most reliable marker for poor prognosis andMYCNoverexpression in embryonic mouse sympathetic ganglia results in NB-like tumors.MYCNcooperates with mutational activation of anaplastic lymphoma kinase (ALK), which promotes progression to NB, but the role of MYCN and ALK in tumorigenesis is still poorly understood. Here, we use chick sympathetic neuroblasts to examine the normal function of MYCN and MYC in the control of neuroblast proliferation, as well as effects of overexpression of MYCN, MYC, and activated ALK, alone and in combination. We demonstrate that MYC is more strongly expressed than MYCN during neurogenesis and is important for in vitro neuroblast proliferation. MYC and MYCN overexpression elicits increased proliferation but does not sustain neuroblast survival. Unexpectedly, long-term expression of activated ALKF1174L leads to cell-cycle arrest and promotes differentiation and survival of postmitotic neurons. ALKF1174L induces NEFM, RET, and VACHT and results in decreased expression of proapototic (BMF, BIM), adrenergic (TH), and cell-cycle genes (e.g., CDC25A, CDK1). In contrast, neuroblast proliferation is maintained when MYCN and ALKF1174L are coexpressed. Proliferating MYCN/ALKF1174L neuroblasts display a differentiated phenotype but differ from ALK-expressing neurons by the upregulation of SKP2, CCNA2, E2F8, and DKC1. Inhibition of the ubiquitin ligase SKP2 (S-phase kinase-associated protein 2), which targets the CDK inhibitor p27 for degradation, reduces neuroblast proliferation, implicating SKP2 in the maintained proliferation of MYCN/ ALKF1174L neuroblasts. Together, our results characterize MYCN/ALK cooperation leading to neuroblast proliferation and survival that may represent initial steps toward NB development.

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APA

Kramer, M., Ribeiro, D., Arsenian-Henriksson, M., Deller, T., & Rohrer, H. (2016). Proliferation and survival of embryonic sympathetic neuroblasts by MYCN and activated ALK signaling. Journal of Neuroscience, 36(40), 10425–10439. https://doi.org/10.1523/JNEUROSCI.0183-16.2016

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