己糖激酶
线粒体
生产(经济)
细胞生物学
瓦博格效应
糖酵解
化学
ATP合酶
三磷酸腺苷
生物
生物化学
酶
经济
宏观经济学
作者
Kimberly S. Huggler,Carlos A. Mellado Fritz,Kyle M. Flickinger,Gavin Chang,Maura McGuire,Jason R. Cantor
标识
DOI:10.1101/2025.02.07.637120
摘要
ABSTRACT Hexokinase (HK) catalyzes the synthesis of glucose-6-phosphate, marking the first committed step of glucose metabolism. Most cancer cells express two homologous isoforms (HK1 and HK2) that can each bind to the outer mitochondrial membrane (OMM). CRISPR screens across hundreds of cancer cell lines indicate that both are dispensable for cell growth in traditional culture media. By contrast, HK2 deletion impairs cell growth in Human Plasma-Like Medium (HPLM). Here, we find that HK2 is required to maintain sufficient cytosolic (OMM-detached) HK activity under conditions that enhance HK1 binding to the OMM. Notably, OMM-detached rather than OMM-docked HK promotes “aerobic glycolysis” (Warburg effect), an enigmatic phenotype displayed by most proliferating cells. We show that several proposed theories for this phenotype cannot explain the HK2 dependence and instead find that HK2 deletion severely impairs glycolytic ATP production with little impact on total ATP yield for cells in HPLM. Our results reveal a basis for conditional HK2 essentiality and suggest that demand for compartmentalized ATP synthesis underlies the Warburg effect.
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