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Identifying off-target effects of etomoxir reveals that carnitine palmitoyltransferase I is essential for cancer cell proliferation independent of β-oxidation.

PLoS Biol.. 2018-03; 
YaoCong-Hui,LiuGao-Yuan,WangRencheng,MoonSung Ho,GrossRichard W,PattiGa
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Codon Optimization … Cells given scrambled siRNA were used as a negative control. For overexpression of human CPT1A, the cDNA was cloned in the pcDNA3.1+ vector (GenScript) under a constitutive CMV promoter. The codon was optimized to be resistant to the siRNA added … Get A Quote

摘要

It has been suggested that some cancer cells rely upon fatty acid oxidation (FAO) for energy. Here we show that when FAO was reduced approximately 90% by pharmacological inhibition of carnitine palmitoyltransferase I (CPT1) with low concentrations of etomoxir, the proliferation rate of various cancer cells was unaffected. Efforts to pharmacologically inhibit FAO more than 90% revealed that high concentrations of etomoxir (200 μM) have an off-target effect of inhibiting complex I of the electron transport chain. Surprisingly, however, when FAO was reduced further by genetic knockdown of CPT1, the proliferation rate of these same cells decreased nearly 2-fold and could not be restored by acetate or octan... More

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