CD44-mediated metabolic rewiring is a targetable dependency of IDH-mutant leukemia.

CD44 介导的代谢重编程是 IDH 突变型白血病的一个可靶向依赖性因素

阅读:5
作者:Lyu Junhua, Liu Yuxuan, Liu Ningning, Vu Hieu S, Cai Feng, Cao Hui, Kaphle Pranita, Wu Zheng, Botten Giovanni A, Zhang Yuannyu, Wang Jin, Achyutuni Sarada, Gao Xiaofei, Iacobucci Ilaria, Mullighan Charles G, Chung Stephen S, Ni Min, DeBerardinis Ralph J, Xu Jian
期刊:Blood影响因子:23.100
时间:2025起止号:2025 Apr 3; 145(14):1553-1567
doi:10.1182/blood.2024027207靶点: CD44
研究方向: 代谢疾病类型: 白血病
Recurrent isocitrate dehydrogenase (IDH) mutations catalyze nicotinamide adenine dinucleotide phosphate (NADPH)-dependent production of oncometabolite (R)-2-hydroxyglutarate (R-2HG) for tumorigenesis. IDH inhibition provides clinical response in a subset of acute myeloid leukemia (AML) cases; however, most patients develop resistance, highlighting the need for more effective IDH-targeting therapies. By comparing transcriptomic alterations in isogenic leukemia cells harboring CRISPR base-edited IDH mutations, we identify the activation of adhesion molecules including CD44, a transmembrane glycoprotein, as a shared feature of IDH-mutant leukemia, consistent with elevated CD44 expression in IDH-mutant AML patients. CD44 is indispensable for IDH-mutant leukemia cells through activating pentose phosphate pathway and inhibiting glycolysis by phosphorylating glucose-6-phosphate dehydrogenase and pyruvate kinase muscle isozyme M2, respectively. This metabolic rewiring ensures efficient NADPH generation for mutant IDH-catalyzed R-2HG production. Combining IDH inhibition with CD44 blockade enhances the elimination of IDH-mutant leukemia cells. Hence, we describe an oncogenic feedforward pathway involving CD44-mediated metabolic rewiring for oncometabolite production, representing a potentially targetable dependency of IDH-mutant malignancies.

特别声明

1、本页面内容包含部分的内容是基于公开信息的合理引用;引用内容仅为补充信息,不代表本站立场。

2、若认为本页面引用内容涉及侵权,请及时与本站联系,我们将第一时间处理。

3、其他媒体/个人如需使用本页面原创内容,需注明“来源:[生知库]”并获得授权;使用引用内容的,需自行联系原作者获得许可。

4、投稿及合作请联系:info@biocloudy.com。