替莫唑胺
PTEN公司
脱甲基酶
基因敲除
癌症研究
甲基转移酶
生物
PI3K/AKT/mTOR通路
胶质母细胞瘤
细胞生物学
表观遗传学
DNA
信号转导
细胞培养
遗传学
甲基化
基因
作者
Vivien Ullrich,Sarah Ertmer,Anna Baginska,Madeleine Dorsch,Hanah Gull,Igor Cima,Pia Berger,Celia Dobersalske,Sarah Langer,Loona Meyer,Philip Dujardin,Sied Kebir,Martin Glas,Tobias Blau,Kathy Keyvani,Laurèl Rauschenbach,Ulrich Sure,Alexander Roesch,Barbara M. Grüner,Björn Scheffler
出处
期刊:iScience
[Elsevier]
日期:2024-01-01
卷期号:27 (1): 108596-108596
标识
DOI:10.1016/j.isci.2023.108596
摘要
Adaptive plasticity to the standard chemotherapeutic temozolomide (TMZ) leads to glioblastoma progression. Here, we examine early stages of this process in patient-derived cellular models, exposing the human lysine-specific demethylase 5B (KDM5B) as a prospective indicator for subclonal expansion. By integration of a reporter, we show its preferential activity in rare, stem-like ALDH1A1+ cells, immediately increasing expression upon TMZ exposure. Naive, genetically unmodified KDM5Bhigh cells phosphorylate AKT (pAKT) and act as slow-cycling persisters under TMZ. Knockdown of KDM5B reverses pAKT levels, simultaneously increasing PTEN expression and TMZ sensitivity. Pharmacological inhibition of PTEN rescues the effect. Interference with KDM5B subsequent to TMZ decreases cellular vitality, and clonal tracing with DNA barcoding demonstrates high individual levels of KDM5B to predict subclonal expansion already before TMZ exposure. Thus, KDM5Bhigh treatment-naive cells preferentially contribute to the dynamics of drug resistance under TMZ. These findings may serve as a cornerstone for future biomarker-assisted clinical trials.
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