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Molecular characteristics of incidental lower-grade glioma for treatment decision-making

Authors
 Jeongman Park  ;  Jeongmin Sim  ;  Juwon Ahn  ;  Yu Jin Kim  ;  Sojung Hwang  ;  Kyunggi Cho  ;  Da-Young Chang  ;  Jin-Hwa Jung  ;  Ju Hyung Moon  ;  KyoungSu Sung  ;  Jaejoon Lim 
Citation
 JOURNAL OF NEUROSURGERY, Vol.138(3) : 629-638, 2023-03 
Journal Title
JOURNAL OF NEUROSURGERY
ISSN
 0022-3085 
Issue Date
2023-03
MeSH
Brain Neoplasms* / pathology ; Carmustine ; Glioma* / pathology ; Humans ; Isocitrate Dehydrogenase / genetics ; Mutation ; Prognosis ; Retrospective Studies
Keywords
chemoresistance ; incidental lower-grade glioma ; mutation analysis ; oncology ; symptomatic lower-grade glioma ; transcriptomic analysis
Abstract
Objective: Several limitations are associated with the early diagnosis and treatment of incidental lower-grade glioma (iLGG), and due to its unknown molecular features, its management is categorized as either the "wait-and-see" strategy or immediate treatment. Therefore, in this study the authors explored iLGG's clinical and molecular landscape to improve its management.

Methods: The authors retrospectively assessed the differences between the molecular and clinical characteristics of iLGG and symptomatic lower-grade glioma (sLGG) samples filtered based on symptom data corresponding to The Cancer Genome Atlas cohort with mutations. Thereafter, genomic and transcriptomic analysis was performed.

Results: There was no significant difference between iLGG and sLGG with respect to mutation status; however, there was an increase in the interaction between major mutations in sLGG, depending on the histological subtype and the IDH1 mutation status. Furthermore, the IDH1 mutation characteristics corresponding to wild-type glioma were much more obvious in sLGG than in iLGG. Additionally, in sLGG, genes associated with malignancy, including cell proliferation-related, cell migration-related, epithelial-to-mesenchymal transition-related, and negative regulation of cell death-related genes, were significantly upregulated, and groups showing higher expression levels of these genes were associated with worse prognosis. Also, 8 of the 75 identified upregulated genes showed positive correlation with resistance to the drugs that are normally used for glioma treatment, including procarbazine, carmustine, vincristine, and temozolomide.

Conclusions: The new insights regarding the different molecular features of iLGG and sLGG indicated that the immediate management of iLGG could result in better prognosis than the wait-and-see strategy.
Full Text
https://thejns.org/view/journals/j-neurosurg/138/3/article-p629.xml
DOI
10.3171/2022.6.JNS22967.
Appears in Collections:
1. College of Medicine (의과대학) > Dept. of Neurosurgery (신경외과학교실) > 1. Journal Papers
Yonsei Authors
Moon, Ju Hyung(문주형)
URI
https://ir.ymlib.yonsei.ac.kr/handle/22282913/196412
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