A Perivascular Niche for Brain Tumor Stem Cells

Christopher Calabrese; Helen Poppleton; Mehmet Kocak; Twala L. Hogg; Christine Fuller; Blair Hamner; Eun Young Oh; M. Waleed Gaber; David Finklestein; Meredith Allen; Adrian Frank; Ildar T. Bayazitov; Stanislav S. Zakharenko; Amar Gajjar; Andrew Davidoff; Richard J. Gilbertson

doi:10.1016/j.ccr.2006.11.020

A Perivascular Niche for Brain Tumor Stem Cells

Christopher Calabrese
, Helen Poppleton
, Mehmet Kocak
, Twala L. Hogg
, Christine Fuller
, Blair Hamner
, Eun Young Oh
, M. Waleed Gaber
, David Finklestein
, Meredith Allen
, Adrian Frank
, Ildar T. Bayazitov
, Stanislav S. Zakharenko
, Amar Gajjar
, Andrew Davidoff
, Richard J. Gilbertson

Pathology

Upstate Medical University

St. Jude Children Research Hospital

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

1939 Scopus citations

Abstract

Cancers are believed to arise from cancer stem cells (CSCs), but it is not known if these cells remain dependent upon the niche microenvironments that regulate normal stem cells. We show that endothelial cells interact closely with self-renewing brain tumor cells and secrete factors that maintain these cells in a stem cell-like state. Increasing the number of endothelial cells or blood vessels in orthotopic brain tumor xenografts expanded the fraction of self-renewing cells and accelerated the initiation and growth of tumors. Conversely, depletion of blood vessels from xenografts ablated self-renewing cells from tumors and arrested tumor growth. We propose that brain CSCs are maintained within vascular niches that are important targets for therapeutic approaches.

Original language	English
Pages (from-to)	69-82
Number of pages	14
Journal	Cancer Cell
Volume	11
Issue number	1
DOIs	https://doi.org/10.1016/j.ccr.2006.11.020
State	Published - Jan 2007

Keywords

STEMCELL

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10.1016/j.ccr.2006.11.020

Cite this

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title = "A Perivascular Niche for Brain Tumor Stem Cells",

abstract = "Cancers are believed to arise from cancer stem cells (CSCs), but it is not known if these cells remain dependent upon the niche microenvironments that regulate normal stem cells. We show that endothelial cells interact closely with self-renewing brain tumor cells and secrete factors that maintain these cells in a stem cell-like state. Increasing the number of endothelial cells or blood vessels in orthotopic brain tumor xenografts expanded the fraction of self-renewing cells and accelerated the initiation and growth of tumors. Conversely, depletion of blood vessels from xenografts ablated self-renewing cells from tumors and arrested tumor growth. We propose that brain CSCs are maintained within vascular niches that are important targets for therapeutic approaches.",

keywords = "STEMCELL",

author = "Christopher Calabrese and Helen Poppleton and Mehmet Kocak and Hogg, \{Twala L.\} and Christine Fuller and Blair Hamner and Oh, \{Eun Young\} and Gaber, \{M. Waleed\} and David Finklestein and Meredith Allen and Adrian Frank and Bayazitov, \{Ildar T.\} and Zakharenko, \{Stanislav S.\} and Amar Gajjar and Andrew Davidoff and Gilbertson, \{Richard J.\}",

year = "2007",

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doi = "10.1016/j.ccr.2006.11.020",

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journal = "Cancer Cell",

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T1 - A Perivascular Niche for Brain Tumor Stem Cells

AU - Calabrese, Christopher

AU - Poppleton, Helen

AU - Kocak, Mehmet

AU - Hogg, Twala L.

AU - Fuller, Christine

AU - Hamner, Blair

AU - Oh, Eun Young

AU - Gaber, M. Waleed

AU - Finklestein, David

AU - Allen, Meredith

AU - Frank, Adrian

AU - Bayazitov, Ildar T.

AU - Zakharenko, Stanislav S.

AU - Gajjar, Amar

AU - Davidoff, Andrew

AU - Gilbertson, Richard J.

PY - 2007/1

Y1 - 2007/1

N2 - Cancers are believed to arise from cancer stem cells (CSCs), but it is not known if these cells remain dependent upon the niche microenvironments that regulate normal stem cells. We show that endothelial cells interact closely with self-renewing brain tumor cells and secrete factors that maintain these cells in a stem cell-like state. Increasing the number of endothelial cells or blood vessels in orthotopic brain tumor xenografts expanded the fraction of self-renewing cells and accelerated the initiation and growth of tumors. Conversely, depletion of blood vessels from xenografts ablated self-renewing cells from tumors and arrested tumor growth. We propose that brain CSCs are maintained within vascular niches that are important targets for therapeutic approaches.

AB - Cancers are believed to arise from cancer stem cells (CSCs), but it is not known if these cells remain dependent upon the niche microenvironments that regulate normal stem cells. We show that endothelial cells interact closely with self-renewing brain tumor cells and secrete factors that maintain these cells in a stem cell-like state. Increasing the number of endothelial cells or blood vessels in orthotopic brain tumor xenografts expanded the fraction of self-renewing cells and accelerated the initiation and growth of tumors. Conversely, depletion of blood vessels from xenografts ablated self-renewing cells from tumors and arrested tumor growth. We propose that brain CSCs are maintained within vascular niches that are important targets for therapeutic approaches.

KW - STEMCELL

UR - https://www.scopus.com/pages/publications/33846029123

U2 - 10.1016/j.ccr.2006.11.020

DO - 10.1016/j.ccr.2006.11.020

M3 - Article

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SN - 1535-6108

VL - 11

SP - 69

EP - 82

JO - Cancer Cell

JF - Cancer Cell

IS - 1

ER -

A Perivascular Niche for Brain Tumor Stem Cells

Abstract

Keywords

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