The cell-intrinsic nature of tumor metabolism has become increasingly well characterized. The impact that tumors have on systemic metabolism, however, has received less attention. Here, we used adult zebrafish harboring BRAF(V600E)-driven melanoma to study the effect of cancer on distant tissues. By applying metabolomics and isotope tracing, we found that melanoma consume ~15 times more glucose than other tissues measured. Despite this burden, circulating glucose levels were maintained in disease animals by a tumor-liver alanine cycle. Excretion of glucose-derived alanine from tumors provided a source of carbon for hepatic gluconeogenesis and allowed tumors to remove excess nitrogen from branched-chain amino acid catabolism, which we found to be activated in zebrafish and human melanoma. Pharmacological inhibition of the tumor-liver alanine cycle in zebrafish reduced tumor burden. Our findings underscore the significance of metabolic crosstalk between tumors and distant tissues and establish the adult zebrafish as an attractive model to study such processes.
Isotope tracing in adult zebrafish reveals alanine cycling between melanoma and liver.
成年斑马鱼的同位素示踪显示,丙氨酸在黑色素瘤和肝脏之间循环
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作者:Naser Fuad J, Jackstadt Madelyn M, Fowle-Grider Ronald, Spalding Jonathan L, Cho Kevin, Stancliffe Ethan, Doonan Steven R, Kramer Eva T, Yao Lijun, Krasnick Bradley, Ding Li, Fields Ryan C, Kaufman Charles K, Shriver Leah P, Johnson Stephen L, Patti Gary J
| 期刊: | Cell Metabolism | 影响因子: | 30.900 |
| 时间: | 2021 | 起止号: | 2021 Jul 6; 33(7):1493-1504 |
| doi: | 10.1016/j.cmet.2021.04.014 | 研究方向: | 肿瘤 |
| 疾病类型: | 黑色素瘤 | ||
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