NHE7 IMPLICATION IN GLIOMA PROGNOSIS: AN <EM>IN SILICO</EM> AND AN <EM>IN VITRO</EM> APPROACH
University of Barcelona
Presentation
Date TBA
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Poster Board
PS05-09AM-442
Poster
View posterAbstract
To address this knowledge gap, we performed an integrative analysis of NHE7 expression across the TCGA, CGGA693, and CGGA325 cohorts. Across all cohorts, NHE7 expression was consistently reduced in high-grade gliomas relative to low-grade tumors and was significantly associated with decreased overall survival and adverse clinical outcome (HR [95% CI] = 0.650, p < 0.001). Functional enrichment analyses (KEGG and GO) revealed significant alterations in pathways related to exocytosis, calcium signaling, ion channel activity, and neurotransmitter release, implicating NHE7 in vesicle-dependent signaling and intercellular communication.
To translate these observations into functional insight, NHE7 expression is being modulated in IDH-wildtype glioblastoma cell lines (U373, U87-MG, T98G). Ongoing in vitro studies aim to elucidate the mechanistic contribution of NHE7 to the dysregulated pathways identified in silico. Collectively, these findings identify NHE7 as a previously underappreciated regulator of glioma progression and prognosis, and support its further exploration as a mechanistic and therapeutic target in glioblastoma.
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