Gene-expression profiling elucidates molecular signaling networks that can be therapeutically targeted in vestibular schwannoma

Sameer Agnihotri; Isabel Gugel; Marc Remke; Antje Bornemann; Georgios Pantazis; Stephen C. Mack; David Shih; Sanjay K. Singh; Nesrin Sabha; Michael D. Taylor; Marcos Tatagiba; Gelareh Zadeh; Boris Krischek

doi:10.3171/2014.6.JNS131433

Gene-expression profiling elucidates molecular signaling networks that can be therapeutically targeted in vestibular schwannoma

Sameer Agnihotri, Isabel Gugel, Marc Remke, Antje Bornemann, Georgios Pantazis, Stephen C. Mack, David Shih, Sanjay K. Singh, Nesrin Sabha, Michael D. Taylor, Marcos Tatagiba, Gelareh Zadeh, Boris Krischek

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

30 Scopus citations

Abstract

Object. Vestibular schwannomas (VS) are common benign tumors of the vestibular nerve that cause significant morbidity. The current treatment strategies for VS include surgery or radiation, with each treatment option having associated complications and side effects. The transcriptional landscape of schwannoma remains largely unknown. Methods. In this study the authors performed gene-expression profiling of 49 schwannomas and 7 normal control vestibular nerves to identify tumor-specific gene-expression patterns. They also interrogated whether schwannomas comprise several molecular subtypes using several transcription-based clustering strategies. The authors also performed in vitro experiments testing therapeutic inhibitors of over-activated pathways in a schwannoma cell line, namely the PI3K/AKT/mTOR pathway. Results. The authors identified over 4000 differentially expressed genes between controls and schwannomas with network analysis, uncovering proliferation and anti-apoptotic pathways previously not implicated in VS. Furthermore, using several distinct clustering technologies, they could not reproducibly identify distinct VS subtypes or significant differences between sporadic and germline NF2-associated schwannomas, suggesting that they are highly similar entities. The authors identified overexpression of PI3K/AKT/mTOR signaling networks in their geneexpression study and evaluated this pathway for therapeutic targeting. Testing the compounds BEZ235 and PKI-587, both novel dual inhibitors of PI3K and mTOR, attenuated tumor growth in a preclinical cell line model of schwannoma (HEI-293). In vitro findings demonstrated that pharmacological inhibition of the PI3K/AKT/mTOR pathway with next-generation compounds led to decreased cell viability and increased cell death. Conclusions. These findings implicate aberrant activation of the PI3K/AKT/mTOR pathway as a molecular mechanism of pathogenesis in VS and suggest inhibition of this pathway as a potential treatment strategy.

Original language	English (US)
Pages (from-to)	1434-1445
Number of pages	12
Journal	Journal of neurosurgery
Volume	121
Issue number	6
DOIs	https://doi.org/10.3171/2014.6.JNS131433
State	Published - Dec 1 2014
Externally published	Yes

Keywords

Molecular profiling
Pi3k-akt inhibitors
Therapeutics
Vestibular schwannoma

ASJC Scopus subject areas

Surgery
Clinical Neurology

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10.3171/2014.6.JNS131433

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Agnihotri, S., Gugel, I., Remke, M., Bornemann, A., Pantazis, G., Mack, S. C., Shih, D., Singh, S. K., Sabha, N., Taylor, M. D., Tatagiba, M., Zadeh, G., & Krischek, B. (2014). Gene-expression profiling elucidates molecular signaling networks that can be therapeutically targeted in vestibular schwannoma. Journal of neurosurgery, 121(6), 1434-1445. https://doi.org/10.3171/2014.6.JNS131433

Agnihotri, S, Gugel, I, Remke, M, Bornemann, A, Pantazis, G, Mack, SC, Shih, D, Singh, SK, Sabha, N, Taylor, MD, Tatagiba, M, Zadeh, G & Krischek, B 2014, 'Gene-expression profiling elucidates molecular signaling networks that can be therapeutically targeted in vestibular schwannoma', Journal of neurosurgery, vol. 121, no. 6, pp. 1434-1445. https://doi.org/10.3171/2014.6.JNS131433

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title = "Gene-expression profiling elucidates molecular signaling networks that can be therapeutically targeted in vestibular schwannoma",

abstract = "Object. Vestibular schwannomas (VS) are common benign tumors of the vestibular nerve that cause significant morbidity. The current treatment strategies for VS include surgery or radiation, with each treatment option having associated complications and side effects. The transcriptional landscape of schwannoma remains largely unknown. Methods. In this study the authors performed gene-expression profiling of 49 schwannomas and 7 normal control vestibular nerves to identify tumor-specific gene-expression patterns. They also interrogated whether schwannomas comprise several molecular subtypes using several transcription-based clustering strategies. The authors also performed in vitro experiments testing therapeutic inhibitors of over-activated pathways in a schwannoma cell line, namely the PI3K/AKT/mTOR pathway. Results. The authors identified over 4000 differentially expressed genes between controls and schwannomas with network analysis, uncovering proliferation and anti-apoptotic pathways previously not implicated in VS. Furthermore, using several distinct clustering technologies, they could not reproducibly identify distinct VS subtypes or significant differences between sporadic and germline NF2-associated schwannomas, suggesting that they are highly similar entities. The authors identified overexpression of PI3K/AKT/mTOR signaling networks in their geneexpression study and evaluated this pathway for therapeutic targeting. Testing the compounds BEZ235 and PKI-587, both novel dual inhibitors of PI3K and mTOR, attenuated tumor growth in a preclinical cell line model of schwannoma (HEI-293). In vitro findings demonstrated that pharmacological inhibition of the PI3K/AKT/mTOR pathway with next-generation compounds led to decreased cell viability and increased cell death. Conclusions. These findings implicate aberrant activation of the PI3K/AKT/mTOR pathway as a molecular mechanism of pathogenesis in VS and suggest inhibition of this pathway as a potential treatment strategy.",

keywords = "Molecular profiling, Pi3k-akt inhibitors, Therapeutics, Vestibular schwannoma",

author = "Sameer Agnihotri and Isabel Gugel and Marc Remke and Antje Bornemann and Georgios Pantazis and Mack, {Stephen C.} and David Shih and Singh, {Sanjay K.} and Nesrin Sabha and Taylor, {Michael D.} and Marcos Tatagiba and Gelareh Zadeh and Boris Krischek",

note = "Publisher Copyright: {\textcopyright}AANS, 2014.",

year = "2014",

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doi = "10.3171/2014.6.JNS131433",

language = "English (US)",

volume = "121",

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T1 - Gene-expression profiling elucidates molecular signaling networks that can be therapeutically targeted in vestibular schwannoma

AU - Agnihotri, Sameer

AU - Gugel, Isabel

AU - Remke, Marc

AU - Bornemann, Antje

AU - Pantazis, Georgios

AU - Mack, Stephen C.

AU - Shih, David

AU - Singh, Sanjay K.

AU - Sabha, Nesrin

AU - Taylor, Michael D.

AU - Tatagiba, Marcos

AU - Zadeh, Gelareh

AU - Krischek, Boris

PY - 2014/12/1

Y1 - 2014/12/1

N2 - Object. Vestibular schwannomas (VS) are common benign tumors of the vestibular nerve that cause significant morbidity. The current treatment strategies for VS include surgery or radiation, with each treatment option having associated complications and side effects. The transcriptional landscape of schwannoma remains largely unknown. Methods. In this study the authors performed gene-expression profiling of 49 schwannomas and 7 normal control vestibular nerves to identify tumor-specific gene-expression patterns. They also interrogated whether schwannomas comprise several molecular subtypes using several transcription-based clustering strategies. The authors also performed in vitro experiments testing therapeutic inhibitors of over-activated pathways in a schwannoma cell line, namely the PI3K/AKT/mTOR pathway. Results. The authors identified over 4000 differentially expressed genes between controls and schwannomas with network analysis, uncovering proliferation and anti-apoptotic pathways previously not implicated in VS. Furthermore, using several distinct clustering technologies, they could not reproducibly identify distinct VS subtypes or significant differences between sporadic and germline NF2-associated schwannomas, suggesting that they are highly similar entities. The authors identified overexpression of PI3K/AKT/mTOR signaling networks in their geneexpression study and evaluated this pathway for therapeutic targeting. Testing the compounds BEZ235 and PKI-587, both novel dual inhibitors of PI3K and mTOR, attenuated tumor growth in a preclinical cell line model of schwannoma (HEI-293). In vitro findings demonstrated that pharmacological inhibition of the PI3K/AKT/mTOR pathway with next-generation compounds led to decreased cell viability and increased cell death. Conclusions. These findings implicate aberrant activation of the PI3K/AKT/mTOR pathway as a molecular mechanism of pathogenesis in VS and suggest inhibition of this pathway as a potential treatment strategy.

AB - Object. Vestibular schwannomas (VS) are common benign tumors of the vestibular nerve that cause significant morbidity. The current treatment strategies for VS include surgery or radiation, with each treatment option having associated complications and side effects. The transcriptional landscape of schwannoma remains largely unknown. Methods. In this study the authors performed gene-expression profiling of 49 schwannomas and 7 normal control vestibular nerves to identify tumor-specific gene-expression patterns. They also interrogated whether schwannomas comprise several molecular subtypes using several transcription-based clustering strategies. The authors also performed in vitro experiments testing therapeutic inhibitors of over-activated pathways in a schwannoma cell line, namely the PI3K/AKT/mTOR pathway. Results. The authors identified over 4000 differentially expressed genes between controls and schwannomas with network analysis, uncovering proliferation and anti-apoptotic pathways previously not implicated in VS. Furthermore, using several distinct clustering technologies, they could not reproducibly identify distinct VS subtypes or significant differences between sporadic and germline NF2-associated schwannomas, suggesting that they are highly similar entities. The authors identified overexpression of PI3K/AKT/mTOR signaling networks in their geneexpression study and evaluated this pathway for therapeutic targeting. Testing the compounds BEZ235 and PKI-587, both novel dual inhibitors of PI3K and mTOR, attenuated tumor growth in a preclinical cell line model of schwannoma (HEI-293). In vitro findings demonstrated that pharmacological inhibition of the PI3K/AKT/mTOR pathway with next-generation compounds led to decreased cell viability and increased cell death. Conclusions. These findings implicate aberrant activation of the PI3K/AKT/mTOR pathway as a molecular mechanism of pathogenesis in VS and suggest inhibition of this pathway as a potential treatment strategy.

KW - Molecular profiling

KW - Pi3k-akt inhibitors

KW - Therapeutics

KW - Vestibular schwannoma

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Gene-expression profiling elucidates molecular signaling networks that can be therapeutically targeted in vestibular schwannoma

Abstract

Keywords

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