Lactate in breast cancer cells is associated with evasion of hypoxia-induced cell cycle arrest and adverse patient outcome

被引:0
|
作者
Yamin Liu
Yasir Suhail
Ashkan Novin
Junaid Afzal
Aditya Pant
机构
[1] University of Connecticut Health,Department of Biomedical Engineering
[2] University of Connecticut Health,Center for Cell Analysis and Modeling
[3] University of California San Francisco,Department of Medicine
[4] University of Connecticut Health,NEAG Comprehensive Cancer Center
来源
Human Cell | 2024年 / 37卷
关键词
Lactate; Hypoxia; Tumor hypoxia; Patient prognosis; Breast cancer invasion;
D O I
暂无
中图分类号
学科分类号
摘要
Tumor hypoxia is a common microenvironmental factor in breast cancers, resulting in stabilization of Hypoxia-Inducible Factor 1 (HIF-1), the master regulator of hypoxic response in cells. Metabolic adaptation by HIF-1 results in inhibition of citric acid cycle, causing accumulation of lactate in large concentrations in hypoxic cancers. Lactate can therefore serve as a secondary microenvironmental factor influencing cellular response to hypoxia. Presence of lactate can alter the hypoxic response of breast cancers in many ways, sometimes in opposite manners. Lactate stabilizes HIF-1 in oxidative condition, as well as destabilizes HIF-1 in hypoxia, increases cellular acidification, and mitigates HIF-1-driven inhibition of cellular respiration. We therefore tested the effect of lactate in MDA-MB-231 under hypoxia, finding that lactate can activate pathways associated with DNA replication, and cell cycling, as well as tissue morphogenesis associated with invasive processes. Using a bioengineered nano-patterned stromal invasion assay, we also confirmed that high lactate and induced HIF-1α gene overexpression can synergistically promote MDA-MB-231 dissemination and stromal trespass. Furthermore, using The Cancer Genome Atlas, we also surprisingly found that lactate in hypoxia promotes gene expression signatures prognosticating low survival in breast cancer patients. Our work documents that lactate accumulation contributes to increased heterogeneity in breast cancer gene expression promoting cancer growth and reducing patient survival.
引用
收藏
页码:768 / 781
页数:13
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