EphB receptor activity suppresses colorectal cancer progression

Eduard Batlle; Julinor Bacani; Harry Begthel; Suzanne Jonkeer; Alexander Gregorieff; Maaike Van De Born; Núria Malats; Elena Sancho; Elles Boon; Tony Pawson; Steven Gallinger; Steven Pals; Hans Clevers; Suzanne Jonkheer

doi:https://doi.org/10.1038/nature03626

EphB receptor activity suppresses colorectal cancer progression

Eduard Batlle, Julinor Bacani, Harry Begthel, Suzanne Jonkeer, Alexander Gregorieff, Maaike Van De Born, Núria Malats, Elena Sancho, Elles Boon, Tony Pawson, Steven Gallinger, Steven Pals, Hans Clevers, Suzanne Jonkheer

Research output: Contribution to journal › Article › Academic › peer-review

351 Citations (Scopus)

Abstract

Most sporadic colorectal cancers are initiated by activating Wnt pathway mutations¹, characterized by the stabilization of β-catenin and constitutive transcription by the β-catenin/T cell factor-4 (Tcf-4) complex^2'3. EphB guidance receptors are Tcf4 target genes that control intestinal epithelial architecture through repulsive interactions with Ephrin-B ligands^4'5. Here we show that, although Wnt signalling remains constitutively active, most human colorectal cancers lose expression of EphB at the adenoma-carcinoma transition. Loss of EphB expression strongly correlates with degree of malignancy. Furthermore, reduction of EphB activity accelerates tumorigenesis in the colon and rectum of Apc^Min/+ mice, and results in the formation of aggressive adenocarcinomas. Our data demonstrate that loss of EphB expression represents a critical step in colorectal cancer progression.

Original language	English
Pages (from-to)	1126-1130
Number of pages	5
Journal	NATURE
Volume	435
Issue number	7045
DOIs	https://doi.org/10.1038/nature03626
Publication status	Published - 23 Jun 2005

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title = "EphB receptor activity suppresses colorectal cancer progression",

abstract = "Most sporadic colorectal cancers are initiated by activating Wnt pathway mutations1, characterized by the stabilization of β-catenin and constitutive transcription by the β-catenin/T cell factor-4 (Tcf-4) complex2'3. EphB guidance receptors are Tcf4 target genes that control intestinal epithelial architecture through repulsive interactions with Ephrin-B ligands4'5. Here we show that, although Wnt signalling remains constitutively active, most human colorectal cancers lose expression of EphB at the adenoma-carcinoma transition. Loss of EphB expression strongly correlates with degree of malignancy. Furthermore, reduction of EphB activity accelerates tumorigenesis in the colon and rectum of ApcMin/+ mice, and results in the formation of aggressive adenocarcinomas. Our data demonstrate that loss of EphB expression represents a critical step in colorectal cancer progression.",

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T1 - EphB receptor activity suppresses colorectal cancer progression

AU - Batlle, Eduard

AU - Bacani, Julinor

AU - Begthel, Harry

AU - Jonkeer, Suzanne

AU - Gregorieff, Alexander

AU - Van De Born, Maaike

AU - Malats, Núria

AU - Sancho, Elena

AU - Boon, Elles

AU - Pawson, Tony

AU - Gallinger, Steven

AU - Pals, Steven

AU - Clevers, Hans

AU - Jonkheer, Suzanne

PY - 2005/6/23

Y1 - 2005/6/23

N2 - Most sporadic colorectal cancers are initiated by activating Wnt pathway mutations1, characterized by the stabilization of β-catenin and constitutive transcription by the β-catenin/T cell factor-4 (Tcf-4) complex2'3. EphB guidance receptors are Tcf4 target genes that control intestinal epithelial architecture through repulsive interactions with Ephrin-B ligands4'5. Here we show that, although Wnt signalling remains constitutively active, most human colorectal cancers lose expression of EphB at the adenoma-carcinoma transition. Loss of EphB expression strongly correlates with degree of malignancy. Furthermore, reduction of EphB activity accelerates tumorigenesis in the colon and rectum of ApcMin/+ mice, and results in the formation of aggressive adenocarcinomas. Our data demonstrate that loss of EphB expression represents a critical step in colorectal cancer progression.

AB - Most sporadic colorectal cancers are initiated by activating Wnt pathway mutations1, characterized by the stabilization of β-catenin and constitutive transcription by the β-catenin/T cell factor-4 (Tcf-4) complex2'3. EphB guidance receptors are Tcf4 target genes that control intestinal epithelial architecture through repulsive interactions with Ephrin-B ligands4'5. Here we show that, although Wnt signalling remains constitutively active, most human colorectal cancers lose expression of EphB at the adenoma-carcinoma transition. Loss of EphB expression strongly correlates with degree of malignancy. Furthermore, reduction of EphB activity accelerates tumorigenesis in the colon and rectum of ApcMin/+ mice, and results in the formation of aggressive adenocarcinomas. Our data demonstrate that loss of EphB expression represents a critical step in colorectal cancer progression.

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DO - https://doi.org/10.1038/nature03626

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SN - 0028-0836

VL - 435

SP - 1126

EP - 1130

JO - NATURE

JF - NATURE

IS - 7045

ER -

EphB receptor activity suppresses colorectal cancer progression

Abstract

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