NF1 mutation-driven neuronal hyperexcitability sets a threshold for tumorigenesis and therapeutic targeting of murine optic glioma

Corina Anastasaki; Jit Chatterjee; Joshua P. Koleske; Yunqing Gao; Stephanie L. Bozeman; Chloe M. Kernan; Lara I. Marco Y Marquez; Ji Kang Chen; Caitlin E. Kelly; Connor J. Blair; Dennis J. Dietzen; Robert A. Kesterson; David H. Gutmann

doi:10.1093/neuonc/noae054

NF1 mutation-driven neuronal hyperexcitability sets a threshold for tumorigenesis and therapeutic targeting of murine optic glioma

Corina Anastasaki, Jit Chatterjee, Joshua P. Koleske, Yunqing Gao, Stephanie L. Bozeman, Chloe M. Kernan, Lara I. Marco Y Marquez, Ji Kang Chen, Caitlin E. Kelly, Connor J. Blair, Dennis J. Dietzen, Robert A. Kesterson, David H. Gutmann

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

7 Scopus citations

Abstract

Background: With the recognition that noncancerous cells function as critical regulators of brain tumor growth, we recently demonstrated that neurons drive low-grade glioma initiation and progression. Using mouse models of neurofibromatosis type 1 (NF1)-associated optic pathway glioma (OPG), we showed that Nf1 mutation induces neuronal hyperexcitability and midkine expression, which activates an immune axis to support tumor growth, such that high-dose lamotrigine treatment reduces Nf1-OPG proliferation. Herein, we execute a series of complementary experiments to address several key knowledge gaps relevant to future clinical translation. Methods: We leverage a collection of Nf1-mutant mice that spontaneously develop OPGs to alter both germline and retinal neuron-specific midkine expression. Nf1-mutant mice harboring several different NF1 patient-derived germline mutations were employed to evaluate neuronal excitability and midkine expression. Two distinct Nf1-OPG preclinical mouse models were used to assess lamotrigine effects on tumor progression and growth in vivo. Results: We establish that neuronal midkine is both necessary and sufficient for Nf1-OPG growth, demonstrating an obligate relationship between germline Nf1 mutation, neuronal excitability, midkine production, and Nf1-OPG proliferation. We show anti-epileptic drug (lamotrigine) specificity in suppressing neuronal midkine production. Relevant to clinical translation, lamotrigine prevents Nf1-OPG progression and suppresses the growth of existing tumors for months following drug cessation. Importantly, lamotrigine abrogates tumor growth in two Nf1-OPG strains using pediatric epilepsy clinical dosing. Conclusions: Together, these findings establish midkine and neuronal hyperexcitability as targetable drivers of Nf1-OPG growth and support the use of lamotrigine as a potential chemoprevention or chemotherapy agent for children with NF1-OPG.

Original language	English
Pages (from-to)	1496-1508
Number of pages	13
Journal	Neuro-oncology
Volume	26
Issue number	8
DOIs	https://doi.org/10.1093/neuonc/noae054
State	Published - Aug 1 2024

Keywords

NF1
lamotrigine
midkine
neuronal excitability
optic glioma

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10.1093/neuonc/noae054

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Anastasaki, C., Chatterjee, J., Koleske, J. P., Gao, Y., Bozeman, S. L., Kernan, C. M., Marco Y Marquez, L. I., Chen, J. K., Kelly, C. E., Blair, C. J., Dietzen, D. J., Kesterson, R. A., & Gutmann, D. H. (2024). NF1 mutation-driven neuronal hyperexcitability sets a threshold for tumorigenesis and therapeutic targeting of murine optic glioma. Neuro-oncology, 26(8), 1496-1508. https://doi.org/10.1093/neuonc/noae054

@article{36b0684232c64a6e8efcf38a450dfca4,

title = "NF1 mutation-driven neuronal hyperexcitability sets a threshold for tumorigenesis and therapeutic targeting of murine optic glioma",

abstract = "Background: With the recognition that noncancerous cells function as critical regulators of brain tumor growth, we recently demonstrated that neurons drive low-grade glioma initiation and progression. Using mouse models of neurofibromatosis type 1 (NF1)-associated optic pathway glioma (OPG), we showed that Nf1 mutation induces neuronal hyperexcitability and midkine expression, which activates an immune axis to support tumor growth, such that high-dose lamotrigine treatment reduces Nf1-OPG proliferation. Herein, we execute a series of complementary experiments to address several key knowledge gaps relevant to future clinical translation. Methods: We leverage a collection of Nf1-mutant mice that spontaneously develop OPGs to alter both germline and retinal neuron-specific midkine expression. Nf1-mutant mice harboring several different NF1 patient-derived germline mutations were employed to evaluate neuronal excitability and midkine expression. Two distinct Nf1-OPG preclinical mouse models were used to assess lamotrigine effects on tumor progression and growth in vivo. Results: We establish that neuronal midkine is both necessary and sufficient for Nf1-OPG growth, demonstrating an obligate relationship between germline Nf1 mutation, neuronal excitability, midkine production, and Nf1-OPG proliferation. We show anti-epileptic drug (lamotrigine) specificity in suppressing neuronal midkine production. Relevant to clinical translation, lamotrigine prevents Nf1-OPG progression and suppresses the growth of existing tumors for months following drug cessation. Importantly, lamotrigine abrogates tumor growth in two Nf1-OPG strains using pediatric epilepsy clinical dosing. Conclusions: Together, these findings establish midkine and neuronal hyperexcitability as targetable drivers of Nf1-OPG growth and support the use of lamotrigine as a potential chemoprevention or chemotherapy agent for children with NF1-OPG.",

keywords = "NF1, lamotrigine, midkine, neuronal excitability, optic glioma",

author = "Corina Anastasaki and Jit Chatterjee and Koleske, {Joshua P.} and Yunqing Gao and Bozeman, {Stephanie L.} and Kernan, {Chloe M.} and {Marco Y Marquez}, {Lara I.} and Chen, {Ji Kang} and Kelly, {Caitlin E.} and Blair, {Connor J.} and Dietzen, {Dennis J.} and Kesterson, {Robert A.} and Gutmann, {David H.}",

year = "2024",

month = aug,

day = "1",

doi = "10.1093/neuonc/noae054",

language = "English",

volume = "26",

pages = "1496--1508",

journal = "Neuro-oncology",

issn = "1522-8517",

number = "8",

}

Anastasaki, C, Chatterjee, J, Koleske, JP, Gao, Y, Bozeman, SL, Kernan, CM, Marco Y Marquez, LI, Chen, JK, Kelly, CE, Blair, CJ, Dietzen, DJ, Kesterson, RA & Gutmann, DH 2024, 'NF1 mutation-driven neuronal hyperexcitability sets a threshold for tumorigenesis and therapeutic targeting of murine optic glioma', Neuro-oncology, vol. 26, no. 8, pp. 1496-1508. https://doi.org/10.1093/neuonc/noae054

TY - JOUR

T1 - NF1 mutation-driven neuronal hyperexcitability sets a threshold for tumorigenesis and therapeutic targeting of murine optic glioma

AU - Anastasaki, Corina

AU - Chatterjee, Jit

AU - Koleske, Joshua P.

AU - Gao, Yunqing

AU - Bozeman, Stephanie L.

AU - Kernan, Chloe M.

AU - Marco Y Marquez, Lara I.

AU - Chen, Ji Kang

AU - Kelly, Caitlin E.

AU - Blair, Connor J.

AU - Dietzen, Dennis J.

AU - Kesterson, Robert A.

AU - Gutmann, David H.

PY - 2024/8/1

Y1 - 2024/8/1

N2 - Background: With the recognition that noncancerous cells function as critical regulators of brain tumor growth, we recently demonstrated that neurons drive low-grade glioma initiation and progression. Using mouse models of neurofibromatosis type 1 (NF1)-associated optic pathway glioma (OPG), we showed that Nf1 mutation induces neuronal hyperexcitability and midkine expression, which activates an immune axis to support tumor growth, such that high-dose lamotrigine treatment reduces Nf1-OPG proliferation. Herein, we execute a series of complementary experiments to address several key knowledge gaps relevant to future clinical translation. Methods: We leverage a collection of Nf1-mutant mice that spontaneously develop OPGs to alter both germline and retinal neuron-specific midkine expression. Nf1-mutant mice harboring several different NF1 patient-derived germline mutations were employed to evaluate neuronal excitability and midkine expression. Two distinct Nf1-OPG preclinical mouse models were used to assess lamotrigine effects on tumor progression and growth in vivo. Results: We establish that neuronal midkine is both necessary and sufficient for Nf1-OPG growth, demonstrating an obligate relationship between germline Nf1 mutation, neuronal excitability, midkine production, and Nf1-OPG proliferation. We show anti-epileptic drug (lamotrigine) specificity in suppressing neuronal midkine production. Relevant to clinical translation, lamotrigine prevents Nf1-OPG progression and suppresses the growth of existing tumors for months following drug cessation. Importantly, lamotrigine abrogates tumor growth in two Nf1-OPG strains using pediatric epilepsy clinical dosing. Conclusions: Together, these findings establish midkine and neuronal hyperexcitability as targetable drivers of Nf1-OPG growth and support the use of lamotrigine as a potential chemoprevention or chemotherapy agent for children with NF1-OPG.

AB - Background: With the recognition that noncancerous cells function as critical regulators of brain tumor growth, we recently demonstrated that neurons drive low-grade glioma initiation and progression. Using mouse models of neurofibromatosis type 1 (NF1)-associated optic pathway glioma (OPG), we showed that Nf1 mutation induces neuronal hyperexcitability and midkine expression, which activates an immune axis to support tumor growth, such that high-dose lamotrigine treatment reduces Nf1-OPG proliferation. Herein, we execute a series of complementary experiments to address several key knowledge gaps relevant to future clinical translation. Methods: We leverage a collection of Nf1-mutant mice that spontaneously develop OPGs to alter both germline and retinal neuron-specific midkine expression. Nf1-mutant mice harboring several different NF1 patient-derived germline mutations were employed to evaluate neuronal excitability and midkine expression. Two distinct Nf1-OPG preclinical mouse models were used to assess lamotrigine effects on tumor progression and growth in vivo. Results: We establish that neuronal midkine is both necessary and sufficient for Nf1-OPG growth, demonstrating an obligate relationship between germline Nf1 mutation, neuronal excitability, midkine production, and Nf1-OPG proliferation. We show anti-epileptic drug (lamotrigine) specificity in suppressing neuronal midkine production. Relevant to clinical translation, lamotrigine prevents Nf1-OPG progression and suppresses the growth of existing tumors for months following drug cessation. Importantly, lamotrigine abrogates tumor growth in two Nf1-OPG strains using pediatric epilepsy clinical dosing. Conclusions: Together, these findings establish midkine and neuronal hyperexcitability as targetable drivers of Nf1-OPG growth and support the use of lamotrigine as a potential chemoprevention or chemotherapy agent for children with NF1-OPG.

KW - NF1

KW - lamotrigine

KW - midkine

KW - neuronal excitability

KW - optic glioma

UR - http://www.scopus.com/inward/record.url?scp=85200722309&partnerID=8YFLogxK

U2 - 10.1093/neuonc/noae054

DO - 10.1093/neuonc/noae054

M3 - Article

C2 - 38607967

AN - SCOPUS:85200722309

SN - 1522-8517

VL - 26

SP - 1496

EP - 1508

JO - Neuro-oncology

JF - Neuro-oncology

IS - 8

ER -

NF1 mutation-driven neuronal hyperexcitability sets a threshold for tumorigenesis and therapeutic targeting of murine optic glioma

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