Deciphering the Roles of MEIS Transcription Factors in Brain Tumors through Integrative Literature and Bioinformatics Analyses

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Year-Number: 2026-1
Language : İngilizce
Subject : Moleküler Biyoloji ve Genetik
Number of pages: 88-97
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Abstract

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Abstract

Brain cancers, particularly glioblastoma and lower-grade glioma, remain major clinical

challenges due to their molecular heterogeneity, invasive behavior, treatment resistance, and

recurrence potential. MEIS1, MEIS2, and MEIS3 are TALE-class homeobox transcription

factors functioning within MEIS–PBX–HOX regulatory networks, yet their roles in brain

cancers remain incompletely understood. This thesis aimed to evaluate the biological

and clinical relevance of MEIS family members in brain cancers by integrating current literature

with exploratory bioinformatics analyses using publicly available platforms, including

GEPIA2, cBioPortal, UALCAN, STRING, TIMER3, and the Human Protein Atlas.

The findings suggest that MEIS family members show member-specific and context-

dependent patterns in glioma biology rather than behaving as a single uniform group. MEIS1

emerged as the most evidence-supported candidate, with associations related to glioma

aggressiveness, survival, and stemness-related features. MEIS2 showed a more limited profile,

suggesting a possible neural-lineage or cell-cycle-associated role without strong prognostic

support. MEIS3 displayed a distinct pattern, indicating a potential progression-related signal

that requires further validation. Overall, this thesis provides a comparative framework for

understanding the possible roles of MEIS1, MEIS2, and MEIS3 in brain cancer and supports

future experimental studies using glioma stem cell models, IDH-stratified cohorts, and MEIS-

directed therapeutic approaches.

 

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