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Gain of glucose-independent growth upon metastasis of breast cancer cells to the brain

Cancer Research. 2014; 
Jinyu Chen , Ho-Jeong Lee *, Xuefeng Wu *, Lei Huo *, Sun-Jin Kim *, Lei Xu , Yan Wang , Junqing He , Lakshmi Reddy Bollu , Guang Gao , Fei Su , James Briggs , Xiaojing Liu , Tamar Melman , John M. Asara, Isaiah J. Fidler , Lewis C. Cantley , Jason W. Locasale and Zhang Weihua†
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Peptide Synthesis Peptides, CYRIGHHSTSDDSS and CYRIGHHpSTSDDSS were used for productions of rabbit polyclonal antibodies against the total BCKDH-E1 and pSer293-BCKDH-E1 respectively (36). The antibodies were produced by Genscript USA Inc. (Piscataway, NJ). Recombinant BCKDH-E1 and BCKD were purchased from Globozymes (Carlsbad, CA). Get A Quote

摘要

Breast cancer brain metastasis is resistant to therapy and a particularly poor prognostic feature in patient survival. Altered metabolism is a common feature of cancer cells but little is known as to what metabolic changes benefit breast cancer brain metastases. We found that brain-metastatic breast cancer cells evolved the ability to survive and proliferate independent of glucose due to enhanced gluconeogenesis and oxidations of glutamine and branched chain amino acids, which together sustain the non-oxidative pentose pathway for purine synthesis. Silencing expression of fructose-1,6- bisphosphatases (FBPs) in brain metastatic cells reduced their viability and improved the survival of metastasis-bearing immuno... More

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