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

Authors
 Park, Jeongman  ;  Sim, Jeongmin  ;  Ahn, Juwon  ;  Kim, Yu Jin  ;  Hwang, Sojung  ;  Cho, Kyunggi  ;  Chang, Da-Young  ;  Jung, Jin-Hwa  ;  Moon, Ju Hyung  ;  Sung, KyoungSu  ;  Lim, Jaejoon 
Citation
 Journal of Neurosurgery, Vol.138(3) : 629-638, 2023-03 
Journal Title
JOURNAL OF NEUROSURGERY
ISSN
 0022-3085 
Issue Date
2023-03
Keywords
incidental lower-grade glioma ; symptomatic lower-grade glioma ; mutation analysis ; transcriptomic analysis ; chemoresistance ; oncology
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 obvi-ous 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 im-mediate management of iLGG could result in better prognosis than the wait-and-see strategy.
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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