Inactivation of NF1 in CNS causes increased glial progenitor proliferation and optic glioma formation

Yuan Zhu; Takayuki Harada; Li Liu; Mark E. Lush; Frantz Guignard; Chikako Harada; Dennis K. Burns; M. Livia Bajenaru; David H. Gutmann; Luis F. Parada

doi:10.1242/dev.02162

Inactivation of NF1 in CNS causes increased glial progenitor proliferation and optic glioma formation

Yuan Zhu, Takayuki Harada, Li Liu, Mark E. Lush, Frantz Guignard, Chikako Harada, Dennis K. Burns, M. Livia Bajenaru, David H. Gutmann, Luis F. Parada

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151 Scopus citations

Abstract

The gene responsible for neurofibromatosis type 1 (NF1) encodes a tumor suppressor that functions as a negative regulator of the Ras proto-oncogene. Individuals with germline mutations in NF1 are predisposed to the development of benign and malignant tumors of the peripheral and central nervous system (CNS). Children with this disease suffer a high incidence of optic gliomas, a benign but potentially debilitating tumor of the optic nerve; and an increased incidence of malignant astrocytoma, reactive astrogliosis and intellectual deficits. In the present study, we have sought insight into the molecular and cellular basis of NF1-associated CNS pathologies. We show that mice genetically engineered to lack NF1 in CNS exhibit a variety of defects in glial cells. Primary among these is a developmental defect resulting in global reactive astrogliosis in the adult brain and increased proliferation of glial progenitor cells leading to enlarged optic nerves. As a consequence, all of the mutant optic nerves develop hyperplastic lesions, some of which progress to optic pathway gliomas. These data point to hyperproliferative glial progenitors as the source of the optic tumors and provide a genetic model for NF1-associated astrogliosis and optic glioma.

Original language	English (US)
Pages (from-to)	5577-5588
Number of pages	12
Journal	Development
Volume	132
Issue number	24
DOIs	https://doi.org/10.1242/dev.02162
State	Published - Dec 2005

Keywords

Astrocyte
Glial progenitor
Mouse
Neurofibromatosis type 1
Optic glioma
Tumor suppressor gene

ASJC Scopus subject areas

Molecular Biology
Developmental Biology

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10.1242/dev.02162

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title = "Inactivation of NF1 in CNS causes increased glial progenitor proliferation and optic glioma formation",

abstract = "The gene responsible for neurofibromatosis type 1 (NF1) encodes a tumor suppressor that functions as a negative regulator of the Ras proto-oncogene. Individuals with germline mutations in NF1 are predisposed to the development of benign and malignant tumors of the peripheral and central nervous system (CNS). Children with this disease suffer a high incidence of optic gliomas, a benign but potentially debilitating tumor of the optic nerve; and an increased incidence of malignant astrocytoma, reactive astrogliosis and intellectual deficits. In the present study, we have sought insight into the molecular and cellular basis of NF1-associated CNS pathologies. We show that mice genetically engineered to lack NF1 in CNS exhibit a variety of defects in glial cells. Primary among these is a developmental defect resulting in global reactive astrogliosis in the adult brain and increased proliferation of glial progenitor cells leading to enlarged optic nerves. As a consequence, all of the mutant optic nerves develop hyperplastic lesions, some of which progress to optic pathway gliomas. These data point to hyperproliferative glial progenitors as the source of the optic tumors and provide a genetic model for NF1-associated astrogliosis and optic glioma.",

keywords = "Astrocyte, Glial progenitor, Mouse, Neurofibromatosis type 1, Optic glioma, Tumor suppressor gene",

author = "Yuan Zhu and Takayuki Harada and Li Liu and Lush, {Mark E.} and Frantz Guignard and Chikako Harada and Burns, {Dennis K.} and Bajenaru, {M. Livia} and Gutmann, {David H.} and Parada, {Luis F.}",

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language = "English (US)",

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T1 - Inactivation of NF1 in CNS causes increased glial progenitor proliferation and optic glioma formation

AU - Zhu, Yuan

AU - Harada, Takayuki

AU - Liu, Li

AU - Lush, Mark E.

AU - Guignard, Frantz

AU - Harada, Chikako

AU - Burns, Dennis K.

AU - Bajenaru, M. Livia

AU - Gutmann, David H.

AU - Parada, Luis F.

PY - 2005/12

Y1 - 2005/12

N2 - The gene responsible for neurofibromatosis type 1 (NF1) encodes a tumor suppressor that functions as a negative regulator of the Ras proto-oncogene. Individuals with germline mutations in NF1 are predisposed to the development of benign and malignant tumors of the peripheral and central nervous system (CNS). Children with this disease suffer a high incidence of optic gliomas, a benign but potentially debilitating tumor of the optic nerve; and an increased incidence of malignant astrocytoma, reactive astrogliosis and intellectual deficits. In the present study, we have sought insight into the molecular and cellular basis of NF1-associated CNS pathologies. We show that mice genetically engineered to lack NF1 in CNS exhibit a variety of defects in glial cells. Primary among these is a developmental defect resulting in global reactive astrogliosis in the adult brain and increased proliferation of glial progenitor cells leading to enlarged optic nerves. As a consequence, all of the mutant optic nerves develop hyperplastic lesions, some of which progress to optic pathway gliomas. These data point to hyperproliferative glial progenitors as the source of the optic tumors and provide a genetic model for NF1-associated astrogliosis and optic glioma.

AB - The gene responsible for neurofibromatosis type 1 (NF1) encodes a tumor suppressor that functions as a negative regulator of the Ras proto-oncogene. Individuals with germline mutations in NF1 are predisposed to the development of benign and malignant tumors of the peripheral and central nervous system (CNS). Children with this disease suffer a high incidence of optic gliomas, a benign but potentially debilitating tumor of the optic nerve; and an increased incidence of malignant astrocytoma, reactive astrogliosis and intellectual deficits. In the present study, we have sought insight into the molecular and cellular basis of NF1-associated CNS pathologies. We show that mice genetically engineered to lack NF1 in CNS exhibit a variety of defects in glial cells. Primary among these is a developmental defect resulting in global reactive astrogliosis in the adult brain and increased proliferation of glial progenitor cells leading to enlarged optic nerves. As a consequence, all of the mutant optic nerves develop hyperplastic lesions, some of which progress to optic pathway gliomas. These data point to hyperproliferative glial progenitors as the source of the optic tumors and provide a genetic model for NF1-associated astrogliosis and optic glioma.

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Inactivation of NF1 in CNS causes increased glial progenitor proliferation and optic glioma formation

Abstract

Keywords

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