Inhibition of GPR158 by microRNA-449a suppresses neural lineage of glioma stem/progenitor cells and correlates with higher glioma grades.
Inhibition of GPR158 by microRNA-449a suppresses neural lineage of glioma stem/progenitor cells and correlates with higher glioma grades.
To identify biomarkers for glioma growth, invasion and progression, we used a candidate gene approach in mouse models with two complementary brain tumour phenotypes, developing either slow-growing, diffusely infiltrating gliomas or highly proliferative, non-invasive primitive neural tumours. In a microRNA screen we first identified microRNA-449a as most significantly differentially expressed between these two tumour types. miR-449a has a target dependent effect, inhibiting cell growth and migration by downregulation of CCND1 and suppressing neural phenotypes by inhibition of G protein coupled-receptor (GPR) 158. GPR158 promotes glioma stem cell differentiation and induces apoptosis and is highest expressed in the cerebral cortex and in oligodendrogliomas, lower in IDH mutant astrocytomas and lowest in the most malignant form of glioma, IDH wild-type glioblastoma. The correlation of GPR158 expression with molecular subtypes, patient survival and therapy response suggests a possible role of GPR158 as prognostic biomarker in human gliomas.
4313-4333
Li, Ning Ning
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Zhang, Ying
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Sidlauskas, Kastyutis
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Ellis, Matthew
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Evans, Ian
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Frankel, Paul
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Lau, Joanne
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El-Hassan, Tedani
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Guglielmi, Loredana
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Broni, Jessica
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Richard-Loendt, Angela
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Brandner, Sebastian
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Li, Ning Ning
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Zhang, Ying
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Sidlauskas, Kastyutis
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Ellis, Matthew
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Evans, Ian
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Frankel, Paul
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Lau, Joanne
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El-Hassan, Tedani
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Guglielmi, Loredana
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Broni, Jessica
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Richard-Loendt, Angela
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Brandner, Sebastian
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Li, Ning Ning, Zhang, Ying, Sidlauskas, Kastyutis, Ellis, Matthew, Evans, Ian, Frankel, Paul, Lau, Joanne, El-Hassan, Tedani, Guglielmi, Loredana, Broni, Jessica, Richard-Loendt, Angela and Brandner, Sebastian
(2018)
Inhibition of GPR158 by microRNA-449a suppresses neural lineage of glioma stem/progenitor cells and correlates with higher glioma grades.
Oncogene, 37 (31), .
(doi:10.1038/s41388-018-0277-1).
Abstract
To identify biomarkers for glioma growth, invasion and progression, we used a candidate gene approach in mouse models with two complementary brain tumour phenotypes, developing either slow-growing, diffusely infiltrating gliomas or highly proliferative, non-invasive primitive neural tumours. In a microRNA screen we first identified microRNA-449a as most significantly differentially expressed between these two tumour types. miR-449a has a target dependent effect, inhibiting cell growth and migration by downregulation of CCND1 and suppressing neural phenotypes by inhibition of G protein coupled-receptor (GPR) 158. GPR158 promotes glioma stem cell differentiation and induces apoptosis and is highest expressed in the cerebral cortex and in oligodendrogliomas, lower in IDH mutant astrocytomas and lowest in the most malignant form of glioma, IDH wild-type glioblastoma. The correlation of GPR158 expression with molecular subtypes, patient survival and therapy response suggests a possible role of GPR158 as prognostic biomarker in human gliomas.
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Inhibition of GPR158
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e-pub ahead of print date: 3 May 2018
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Local EPrints ID: 427641
URI: http://eprints.soton.ac.uk/id/eprint/427641
ISSN: 0950-9232
PURE UUID: 160d067d-4776-445d-98d9-bc0b98c06bdc
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Date deposited: 24 Jan 2019 17:30
Last modified: 15 Mar 2024 23:48
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Author:
Ning Ning Li
Author:
Ying Zhang
Author:
Kastyutis Sidlauskas
Author:
Matthew Ellis
Author:
Ian Evans
Author:
Paul Frankel
Author:
Joanne Lau
Author:
Tedani El-Hassan
Author:
Loredana Guglielmi
Author:
Jessica Broni
Author:
Angela Richard-Loendt
Author:
Sebastian Brandner
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