TY - JOUR
T1 - Dependence receptor TrkC is a putative colon cancer tumor suppressor
AU - Genevois, Anne Laure
AU - Ichim, Gabriel
AU - Coissieux, Marie May
AU - Lambert, Marie Pierre
AU - Lavial, Fabrice
AU - Goldschneider, David
AU - Jarrosson-Wuilleme, Loraine
AU - Lepinasse, Florian
AU - Gouysse, Géraldine
AU - Herceg, Zdenko
AU - Scoazec, Jean Yves
AU - Tauszig-Delamasure, Servane
AU - Mehlen, Patrick
PY - 2013/2/19
Y1 - 2013/2/19
N2 - The TrkC neurotrophin receptor belongs to the functional dependence receptor family, members of which share the ability to induce apoptosis in the absence of their ligands. Such a trait has been hypothesized to confer tumor-suppressor activity. Indeed, cells that express these receptors are thought to be dependent on ligand availability for their survival, a mechanism that inhibits uncontrolled tumor cell proliferation and migration. TrkC is a classic tyrosine kinase receptor and therefore generally considered to be a protooncogene. We show here that TrkC expression is down-regulated in a large fraction of human colorectal cancers, mainly through promoter methylation. Moreover, we show that TrkC silencing by promoter methylation is a selective advantage for colorectal cell lines to limit tumor cell death. Furthermore, reestablished TrkC expression in colorectal cancer cell lines is associated with tumor cell death and inhibition of in vitro characteristics of cell transformation, as well as in vivo tumor growth. Finally, we provide evidence that a mutation of TrkC detected in a sporadic cancer is a loss-ofproapoptotic function mutation. Together, these data support the conclusion that TrkC is a colorectal cancer tumor suppressor.
AB - The TrkC neurotrophin receptor belongs to the functional dependence receptor family, members of which share the ability to induce apoptosis in the absence of their ligands. Such a trait has been hypothesized to confer tumor-suppressor activity. Indeed, cells that express these receptors are thought to be dependent on ligand availability for their survival, a mechanism that inhibits uncontrolled tumor cell proliferation and migration. TrkC is a classic tyrosine kinase receptor and therefore generally considered to be a protooncogene. We show here that TrkC expression is down-regulated in a large fraction of human colorectal cancers, mainly through promoter methylation. Moreover, we show that TrkC silencing by promoter methylation is a selective advantage for colorectal cell lines to limit tumor cell death. Furthermore, reestablished TrkC expression in colorectal cancer cell lines is associated with tumor cell death and inhibition of in vitro characteristics of cell transformation, as well as in vivo tumor growth. Finally, we provide evidence that a mutation of TrkC detected in a sporadic cancer is a loss-ofproapoptotic function mutation. Together, these data support the conclusion that TrkC is a colorectal cancer tumor suppressor.
KW - Caspase-3
KW - Epigenetic
KW - Genetic
KW - Neurotrophin-3
UR - http://www.scopus.com/inward/record.url?scp=84874283320&partnerID=8YFLogxK
U2 - 10.1073/pnas.1212333110
DO - 10.1073/pnas.1212333110
M3 - Article
C2 - 23341610
AN - SCOPUS:84874283320
SN - 0027-8424
VL - 110
SP - 3017
EP - 3022
JO - Proceedings of the National Academy of Sciences of the United States of America
JF - Proceedings of the National Academy of Sciences of the United States of America
IS - 8
ER -