The netrin-1 receptors UNC5H are putative tumor suppressors controlling cell death commitment

Karine Thiébault, Laetitia Mazelin, Laurent Pays, Fabien Llambi, Marie Odile Joly, Jean Yves Scoazec, Jean Christophe Saurin, Giovanni Romeo, Patrick Mehlen

Résultats de recherche: Contribution à un journalArticleRevue par des pairs

173 Citations (Scopus)

Résumé

The three mammalian receptors UNC5H1, UNC5H2, and UNC5H3 (also named UNC5A, UNC5B, and UNC5C in human) that belong to the family of the netrin-1 receptors, UNC5H, were initially proposed as mediators of the chemorepulsive effect of netrin-1 on specific axons. However, they were also recently shown to act as dependence receptors. Such receptors induce apoptosis when unbound to their ligand. We show here that the expression of the human UNC5A, UNC5B, or UNC5C is down-regulated in multiple cancers including colorectal, breast, ovary, uterus, stomach, lung, or kidney cancers. In colorectal tumors, this down-regulation is associated with loss of heterozygosity occurring within UNC5A, UNC5B, and UNC5C genes but may also be partially related to epigenetic processes because histone deacetylase inhibitor increased UNC5C expression in various cancer cell lines. Moreover, sequencing of UNC5C gene in patients with colorectal tumors revealed the presence of missense mutations. The loss/reduction of expression may be a crucial mechanism for tumorigenicity because the expression of UNC5H1, UNC5H2, or UNC5H3 inhibits tumor cell anchorage-independent growth and invasion. Moreover, these hallmarks of malignant transformation can be restored by netrin-1 addition or apoptosis inhibition. Hence, UNC5H1, UNC5H2, and UNC5H3 receptors may represent tumor suppressors that inhibit tumor extension outside the region of netrin-1 availability by inducing apoptosis.

langue originaleAnglais
Pages (de - à)4173-4178
Nombre de pages6
journalProceedings of the National Academy of Sciences of the United States of America
Volume100
Numéro de publication7
Les DOIs
étatPublié - 1 avr. 2003
Modification externeOui

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