The Netrin-4/Neogenin-1 axis promotes neuroblastoma cell survival and migration

Villanueva, Andrea A.; Falcón, Paulina; Espinoza, Natalie; Solano, R. Luis; Milla, Luis A.; Hernandez-SanMiguel, Esther; Torres, Vicente A.; Sanchez-Gomez, Pilar; Palma, Verónica

Artículos de revistas

Fecha

2017

Registro en:

Oncotarget, Volumen 8, Issue 6, 2018, Pages 9767-9782

19492553

10.18632/oncotarget.14213

https://repositorio.uchile.cl/handle/2250/167032

Autor

Villanueva, Andrea A.

Falcón, Paulina

Espinoza, Natalie

Solano, R. Luis

Milla, Luis A.

Hernandez-SanMiguel, Esther

Torres, Vicente A.

Sanchez-Gomez, Pilar

Palma, Verónica

Institución

Universidad de Chile

Resumen

Neogenin-1 (NEO1) is a transmembrane receptor involved in axonal guidance, angiogenesis, neuronal cell migration and cell death, during both embryonic development and adult homeostasis. It has been described as a dependence receptor, because it promotes cell death in the absence of its ligands (Netrin and Repulsive Guidance Molecule (RGM) families) and cell survival when they are present. Although NEO1 and its ligands are involved in tumor progression, their precise role in tumor cell survival and migration remain unclear. Public databases contain extensive information regarding the expression of NEO1 and its ligands Netrin-1 (NTN1) and Netrin-4 (NTN4) in primary neuroblastoma (NB) tumors. Analysis of this data revealed that patients with high expression levels of both NEO1 and NTN4 have a poor survival rate. Accordingly, our analyses in NB cell lines with different genetic backgrounds revealed that knocking-down NEO1 reduces cell migration, whereas silencing of endogenous NTN4 induced

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