Dissociation of EphB2 Signaling Pathways Mediating Progenitor Cell Proliferation and Tumor Suppression

Maria Genander; Michael M. Halford; Nan Jie Xu; Malin Eriksson; Zuoren Yu; Zhaozhu Qiu; Anna Martling; Gedas Greicius; Sonal Thakar; Timothy Catchpole; Michael J. Chumley; Sofia Zdunek; Chenguang Wang; Torbjörn Holm; Stephen P. Goff; Sven Pettersson; Richard G. Pestell; Mark Henkemeyer; Jonas Frisén

doi:10.1016/j.cell.2009.08.048

Dissociation of EphB2 Signaling Pathways Mediating Progenitor Cell Proliferation and Tumor Suppression

Maria Genander, Michael M. Halford, Nan Jie Xu, Malin Eriksson, Zuoren Yu, Zhaozhu Qiu, Anna Martling, Gedas Greicius, Sonal Thakar, Timothy Catchpole, Michael J. Chumley, Sofia Zdunek, Chenguang Wang, Torbjörn Holm, Stephen P. Goff, Sven Pettersson, Richard G. Pestell, Mark Henkemeyer, Jonas Frisén

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

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Abstract

Signaling proteins driving the proliferation of stem and progenitor cells are often encoded by proto-oncogenes. EphB receptors represent a rare exception; they promote cell proliferation in the intestinal epithelium and function as tumor suppressors by controlling cell migration and inhibiting invasive growth. We show that cell migration and proliferation are controlled independently by the receptor EphB2. EphB2 regulated cell positioning is kinase-independent and mediated via phosphatidylinositol 3-kinase, whereas EphB2 tyrosine kinase activity regulates cell proliferation through an Abl-cyclin D1 pathway. Cyclin D1 regulation becomes uncoupled from EphB signaling during the progression from adenoma to colon carcinoma in humans, allowing continued proliferation with invasive growth. The dissociation of EphB2 signaling pathways enables the selective inhibition of the mitogenic effect without affecting the tumor suppressor function and identifies a pharmacological strategy to suppress adenoma growth.

Original language	English
Pages (from-to)	679-692
Number of pages	14
Journal	Cell
Volume	139
Issue number	4
DOIs	https://doi.org/10.1016/j.cell.2009.08.048
Publication status	Published - 13 Nov 2009
Externally published	Yes

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Genander, M., Halford, M. M., Xu, N. J., Eriksson, M., Yu, Z., Qiu, Z., Martling, A., Greicius, G., Thakar, S., Catchpole, T., Chumley, M. J., Zdunek, S., Wang, C., Holm, T., Goff, S. P., Pettersson, S., Pestell, R. G., Henkemeyer, M., & Frisén, J. (2009). Dissociation of EphB2 Signaling Pathways Mediating Progenitor Cell Proliferation and Tumor Suppression. Cell, 139(4), 679-692. https://doi.org/10.1016/j.cell.2009.08.048

@article{52666a0c931f493497a3bdfb6e12ae6c,

title = "Dissociation of EphB2 Signaling Pathways Mediating Progenitor Cell Proliferation and Tumor Suppression",

abstract = "Signaling proteins driving the proliferation of stem and progenitor cells are often encoded by proto-oncogenes. EphB receptors represent a rare exception; they promote cell proliferation in the intestinal epithelium and function as tumor suppressors by controlling cell migration and inhibiting invasive growth. We show that cell migration and proliferation are controlled independently by the receptor EphB2. EphB2 regulated cell positioning is kinase-independent and mediated via phosphatidylinositol 3-kinase, whereas EphB2 tyrosine kinase activity regulates cell proliferation through an Abl-cyclin D1 pathway. Cyclin D1 regulation becomes uncoupled from EphB signaling during the progression from adenoma to colon carcinoma in humans, allowing continued proliferation with invasive growth. The dissociation of EphB2 signaling pathways enables the selective inhibition of the mitogenic effect without affecting the tumor suppressor function and identifies a pharmacological strategy to suppress adenoma growth.",

keywords = "CELLBIO, HUMDISEASE, SIGNALING",

author = "Maria Genander and Halford, {Michael M.} and Xu, {Nan Jie} and Malin Eriksson and Zuoren Yu and Zhaozhu Qiu and Anna Martling and Gedas Greicius and Sonal Thakar and Timothy Catchpole and Chumley, {Michael J.} and Sofia Zdunek and Chenguang Wang and Torbj{\"o}rn Holm and Goff, {Stephen P.} and Sven Pettersson and Pestell, {Richard G.} and Mark Henkemeyer and Jonas Fris{\'e}n",

note = "Funding Information: We thank F. Granath, J. Holmberg, L. Huminiecki, J. Lindholm, A. Simon, and members of the Fris{\'e}n lab for valuable discussions, M.-L. Sp{\aa}ngberg and M. Toro for technical assistance, and Novartis for providing Gleevec and AEW-541. This study was supported by grants from the NIH (R01CA70896, R01CA75503, and R01CA86072 to R.G.P. and 2R01 MH66332 to M.H.), the Dr. Ralph and Marian C. Falk Medical Research Trust, the Pennsylvania Department of Health (which specifically disclaims responsibility for analyses, interpretations, or conclusions) (R.G.P.), the Swedish Cancer Society, the Swedish Research Council, Knut och Alice Wallenbergs Stiftelse, the Karolinska Institute, and the Tobias Foundation (J.F.). The Kimmel Cancer Center was supported by the NIH Cancer Center Core grant P30CA56036 (R.G.P). ",

year = "2009",

month = nov,

day = "13",

doi = "10.1016/j.cell.2009.08.048",

language = "English",

volume = "139",

pages = "679--692",

journal = "Cell",

issn = "0092-8674",

publisher = "Cell Press",

number = "4",

}

Genander, M, Halford, MM, Xu, NJ, Eriksson, M, Yu, Z, Qiu, Z, Martling, A, Greicius, G, Thakar, S, Catchpole, T, Chumley, MJ, Zdunek, S, Wang, C, Holm, T, Goff, SP, Pettersson, S, Pestell, RG, Henkemeyer, M & Frisén, J 2009, 'Dissociation of EphB2 Signaling Pathways Mediating Progenitor Cell Proliferation and Tumor Suppression', Cell, vol. 139, no. 4, pp. 679-692. https://doi.org/10.1016/j.cell.2009.08.048

TY - JOUR

T1 - Dissociation of EphB2 Signaling Pathways Mediating Progenitor Cell Proliferation and Tumor Suppression

AU - Genander, Maria

AU - Halford, Michael M.

AU - Xu, Nan Jie

AU - Eriksson, Malin

AU - Yu, Zuoren

AU - Qiu, Zhaozhu

AU - Martling, Anna

AU - Greicius, Gedas

AU - Thakar, Sonal

AU - Catchpole, Timothy

AU - Chumley, Michael J.

AU - Zdunek, Sofia

AU - Wang, Chenguang

AU - Holm, Torbjörn

AU - Goff, Stephen P.

AU - Pettersson, Sven

AU - Pestell, Richard G.

AU - Henkemeyer, Mark

AU - Frisén, Jonas

N1 - Funding Information: We thank F. Granath, J. Holmberg, L. Huminiecki, J. Lindholm, A. Simon, and members of the Frisén lab for valuable discussions, M.-L. Spångberg and M. Toro for technical assistance, and Novartis for providing Gleevec and AEW-541. This study was supported by grants from the NIH (R01CA70896, R01CA75503, and R01CA86072 to R.G.P. and 2R01 MH66332 to M.H.), the Dr. Ralph and Marian C. Falk Medical Research Trust, the Pennsylvania Department of Health (which specifically disclaims responsibility for analyses, interpretations, or conclusions) (R.G.P.), the Swedish Cancer Society, the Swedish Research Council, Knut och Alice Wallenbergs Stiftelse, the Karolinska Institute, and the Tobias Foundation (J.F.). The Kimmel Cancer Center was supported by the NIH Cancer Center Core grant P30CA56036 (R.G.P).

PY - 2009/11/13

Y1 - 2009/11/13

N2 - Signaling proteins driving the proliferation of stem and progenitor cells are often encoded by proto-oncogenes. EphB receptors represent a rare exception; they promote cell proliferation in the intestinal epithelium and function as tumor suppressors by controlling cell migration and inhibiting invasive growth. We show that cell migration and proliferation are controlled independently by the receptor EphB2. EphB2 regulated cell positioning is kinase-independent and mediated via phosphatidylinositol 3-kinase, whereas EphB2 tyrosine kinase activity regulates cell proliferation through an Abl-cyclin D1 pathway. Cyclin D1 regulation becomes uncoupled from EphB signaling during the progression from adenoma to colon carcinoma in humans, allowing continued proliferation with invasive growth. The dissociation of EphB2 signaling pathways enables the selective inhibition of the mitogenic effect without affecting the tumor suppressor function and identifies a pharmacological strategy to suppress adenoma growth.

AB - Signaling proteins driving the proliferation of stem and progenitor cells are often encoded by proto-oncogenes. EphB receptors represent a rare exception; they promote cell proliferation in the intestinal epithelium and function as tumor suppressors by controlling cell migration and inhibiting invasive growth. We show that cell migration and proliferation are controlled independently by the receptor EphB2. EphB2 regulated cell positioning is kinase-independent and mediated via phosphatidylinositol 3-kinase, whereas EphB2 tyrosine kinase activity regulates cell proliferation through an Abl-cyclin D1 pathway. Cyclin D1 regulation becomes uncoupled from EphB signaling during the progression from adenoma to colon carcinoma in humans, allowing continued proliferation with invasive growth. The dissociation of EphB2 signaling pathways enables the selective inhibition of the mitogenic effect without affecting the tumor suppressor function and identifies a pharmacological strategy to suppress adenoma growth.

KW - CELLBIO

KW - HUMDISEASE

KW - SIGNALING

UR - http://www.scopus.com/inward/record.url?scp=70350780571&partnerID=8YFLogxK

U2 - 10.1016/j.cell.2009.08.048

DO - 10.1016/j.cell.2009.08.048

M3 - Article

C2 - 19914164

AN - SCOPUS:70350780571

SN - 0092-8674

VL - 139

SP - 679

EP - 692

JO - Cell

JF - Cell

IS - 4

ER -

Dissociation of EphB2 Signaling Pathways Mediating Progenitor Cell Proliferation and Tumor Suppression

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