Advanced Age in Humans and Mouse Models of Glioblastoma Show Decreased Survival from Extratumoral Influence.

dc.contributor.author

Johnson, Margaret

dc.contributor.author

Bell, April

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Lauing, Kristen L

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Ladomersky, Erik

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Zhai, Lijie

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Penco-Campillo, Manon

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Shah, Yajas

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Mauer, Elizabeth

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Xiu, Joanne

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Nicolaides, Theodore

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Drumm, Michael

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McCortney, Kathleen

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Elemento, Olivier

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Kim, Miri

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Bommi, Prashant

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Low, Justin T

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Memon, Ruba

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Wu, Jennifer

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Zhao, Junfei

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Mi, Xinlei

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Glantz, Michael J

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Sengupta, Soma

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Castro, Brandyn

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Yamini, Bakhtiar

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Horbinski, Craig

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Baker, Darren J

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Walunas, Theresa L

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Schiltz, Gary E

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Lukas, Rimas V

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Wainwright, Derek A

dc.date.accessioned

2026-04-02T17:59:26Z

dc.date.available

2026-04-02T17:59:26Z

dc.date.issued

2023-12

dc.description.abstract

Purpose

Glioblastoma (GBM) is the most common aggressive primary malignant brain tumor in adults with a median age of onset of 68 to 70 years old. Although advanced age is often associated with poorer GBM patient survival, the predominant source(s) of maladaptive aging effects remains to be established. Here, we studied intratumoral and extratumoral relationships between adult patients with GBM and mice with brain tumors across the lifespan.

Experimental design

Electronic health records at Northwestern Medicine and the NCI SEER databases were evaluated for GBM patient age and overall survival. The commercial Tempus and Caris databases, as well as The Cancer Genome Atlas were profiled for gene expression, DNA methylation, and mutational changes with varying GBM patient age. In addition, gene expression analysis was performed on the extratumoral brain of younger and older adult mice with or without a brain tumor. The survival of young and old wild-type or transgenic (INK-ATTAC) mice with a brain tumor was evaluated after treatment with or without senolytics and/or immunotherapy.

Results

Human patients with GBM ≥65 years of age had a significantly decreased survival compared with their younger counterparts. While the intra-GBM molecular profiles were similar between younger and older patients with GBM, non-tumor brain tissue had a significantly different gene expression profile between young and old mice with a brain tumor and the eradication of senescent cells improved immunotherapy-dependent survival of old but not young mice.

Conclusions

This work suggests a potential benefit for combining senolytics with immunotherapy in older patients with GBM.
dc.identifier

729127

dc.identifier.issn

1078-0432

dc.identifier.issn

1557-3265

dc.identifier.uri

https://hdl.handle.net/10161/34375

dc.language

eng

dc.publisher

American Association for Cancer Research (AACR)

dc.relation.ispartof

Clinical cancer research : an official journal of the American Association for Cancer Research

dc.relation.isversionof

10.1158/1078-0432.ccr-23-0834

dc.rights.uri

https://creativecommons.org/licenses/by-nc/4.0

dc.subject

Animals

dc.subject

Humans

dc.subject

Mice

dc.subject

Glioblastoma

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Brain Neoplasms

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DNA Methylation

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Mutation

dc.subject

Aged

dc.subject

Senotherapeutics

dc.title

Advanced Age in Humans and Mouse Models of Glioblastoma Show Decreased Survival from Extratumoral Influence.

dc.type

Journal article

duke.contributor.orcid

Johnson, Margaret|0000-0003-1208-622X|0009-0005-5596-3407

pubs.begin-page

4973

pubs.end-page

4989

pubs.issue

23

pubs.organisational-group

Duke

pubs.organisational-group

School of Medicine

pubs.organisational-group

Clinical Science Departments

pubs.organisational-group

Institutes and Centers

pubs.organisational-group

Duke Cancer Institute

pubs.organisational-group

Neurology

pubs.organisational-group

Neurology, General & Community Neurology

pubs.organisational-group

Neurosurgery

pubs.organisational-group

Neurosurgery

pubs.publication-status

Published

pubs.volume

29

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