Using arterial-venous analysis to characterize cancer metabolic consumption in patients.
Nan-Xiang XiongXiaofei GaoHongyang ZhaoFeng CaiFang-Cheng ZhangYe YuanWeichao LiuFangping HeLauren G ZachariasHong LinHieu S VuChao XingDong-Xiao YaoFei ChenBenyan LuoWenzhi SunRalph J DeBerardinisHao XuWoo-Ping GePublished in: Nature communications (2020)
Understanding tumor metabolism holds the promise of new insights into cancer biology, diagnosis and treatment. To assess human cancer metabolism, here we report a method to collect intra-operative samples of blood from an artery directly upstream and a vein directly downstream of a brain tumor, as well as samples from dorsal pedal veins of the same patients. After performing targeted metabolomic analysis, we characterize the metabolites consumed and produced by gliomas in vivo by comparing the arterial supply and venous drainage. N-acetylornithine, D-glucose, putrescine, and L-acetylcarnitine are consumed in relatively large amounts by gliomas. Conversely, L-glutamine, agmatine, and uridine 5-monophosphate are produced in relatively large amounts by gliomas. Further we verify that D-2-hydroxyglutarate (D-2HG) is high in venous plasma from patients with isocitrate dehydrogenases1 (IDH1) mutations. Through these paired comparisons, we can exclude the interpatient variation that is present in plasma samples usually taken from the cubital vein.
Keyphrases
- end stage renal disease
- high grade
- ejection fraction
- newly diagnosed
- squamous cell
- chronic kidney disease
- prognostic factors
- peritoneal dialysis
- endothelial cells
- spinal cord
- type diabetes
- squamous cell carcinoma
- ms ms
- machine learning
- artificial intelligence
- cancer therapy
- single molecule
- weight loss
- deep learning
- skeletal muscle
- aqueous solution
- living cells