Ser Zheng, Gao Xia, Johnson Christelle, Mehrmohamadi Mahya, Liu Xiaojing, Li Siqi, Locasale Jason W
Tri-Institutional Training Program in Chemical Biology, Weill Cornell Medical College, Rockefeller University, Memorial Sloan-Kettering Cancer Center, New York, NY 10065, USA.
Department of Pharmacology and Cancer Biology, Duke Cancer Institute, Duke Molecular Physiology Institute, Duke University School of Medicine, Durham, NC 27710, USA.
Cell Rep. 2016 Jun 14;15(11):2367-76. doi: 10.1016/j.celrep.2016.05.035. Epub 2016 Jun 2.
Antimetabolites that affect nucleotide metabolism are frontline chemotherapy agents in several cancers and often successfully target one carbon metabolism. However, the precise mechanisms and resulting determinants of their therapeutic value are unknown. We show that 5-fluorouracil (5-FU), a commonly used antimetabolite therapeutic with varying efficacy, induces specific alterations to nucleotide metabolism by disrupting pyrimidine homeostasis. An integrative metabolomics analysis of the cellular response to 5-FU reveals intracellular uracil accumulation, whereas deoxyuridine levels exhibited increased flux into the extracellular space, resulting in an induction of overflow metabolism. Subsequent analysis from mice bearing colorectal tumors treated with 5-FU show specific secretion of metabolites in tumor-bearing mice into serum that results from alterations in nucleotide flux and reduction in overflow metabolism. Together, these findings identify a determinant of an antimetabolite response that may be exploited to more precisely define the tumors that could respond to targeting cancer metabolism.
影响核苷酸代谢的抗代谢物是多种癌症的一线化疗药物,且常常成功靶向一碳代谢。然而,其治疗价值的确切机制及相关决定因素尚不清楚。我们发现,5-氟尿嘧啶(5-FU)作为一种疗效各异的常用抗代谢物疗法,通过破坏嘧啶稳态诱导核苷酸代谢发生特定改变。对细胞对5-FU反应的综合代谢组学分析揭示了细胞内尿嘧啶积累,而脱氧尿苷水平则显示进入细胞外空间的通量增加,从而导致溢流代谢的诱导。随后对用5-FU治疗的结直肠癌小鼠的分析表明,荷瘤小鼠体内的代谢物会因核苷酸通量改变和溢流代谢减少而特异性分泌到血清中。总之,这些发现确定了一种抗代谢物反应的决定因素,可利用该因素更精确地界定可能对靶向癌症代谢有反应的肿瘤。
