Expansion of a neural crest gene signature following ectopic MYCN expression in sympathoadrenal lineage cells in vivo
Rodrigo Ibarra-García-Padilla, Annika Nambiar, Thomas A. Hamre, Eileen W. Singleton, Rosa A. Uribe, Michael Klymkowsky, Tao Liu, Tao Liu

TL;DR
Overexpression of MYCN in zebrafish SAP cells leads to abnormal gene expression patterns similar to neural crest cells, potentially contributing to neuroblastoma development.
Contribution
This study reveals that MYCN overexpression disrupts SAP differentiation by inducing an aberrant neural crest gene signature and dampening BMP signaling.
Findings
MYCN overexpression in SAP cells causes transient expansion of NCC markers alongside SAP and neuronal markers.
BMP signaling activity is reduced in MYCN-overexpressing SAP cells.
Pharmacological BMP inhibition phenocopies the effects of MYCN overexpression in SAP cells.
Abstract
Neural crest cells (NCC) are multipotent migratory stem cells that originate from the neural tube during early vertebrate embryogenesis. NCCs give rise to a variety of cell types within the developing organism, including neurons and glia of the sympathetic nervous system. It has been suggested that failure in correct NCC differentiation leads to several diseases, including neuroblastoma (NB). During normal NCC development, MYCN is transiently expressed to promote NCC migration, and its downregulation precedes neuronal differentiation. Overexpression of MYCN has been linked to high-risk and aggressive NB progression. For this reason, understanding the effect overexpression of this oncogene has on the development of NCC-derived sympathoadrenal progenitors (SAP), which later give rise to sympathetic nerves, will help elucidate the developmental mechanisms that may prime the onset of NB.…
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Taxonomy
TopicsNeuroblastoma Research and Treatments · Congenital heart defects research · Congenital Diaphragmatic Hernia Studies
