4.3 Article

Mitochondrial bioenergetic profile and responses to metabolic inhibition in human hepatocarcinoma cell lines with distinct differentiation characteristics

期刊

JOURNAL OF BIOENERGETICS AND BIOMEMBRANES
卷 43, 期 5, 页码 493-505

出版社

SPRINGER/PLENUM PUBLISHERS
DOI: 10.1007/s10863-011-9380-5

关键词

Tumor metabolism; Mitochondria; ATP synthase; Inhibitor Factor 1; Mitochondrial membrane potential; Human hepatocarcinoma

资金

  1. Italian Ministero dell'Universita e della Ricerca Scientifica (MIUR)

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The classical view of tumour cell bioenergetics has been recently revised. Then, the definition of the mitochondrial profile is considered of fundamental importance for the development of anti-cancer therapies, but it still needs to be clarified. We investigated two human hepatocellular carcinoma cell lines: the partially differentiated HepG2 and the undifferentiated JHH-6. High resolution respirometry revealed a marked impairment/uncoupling of OXPHOS in JHH-6 compared with HepG2, with the phosphorylation system limiting the capacity for electron transport much more in JHH-6. Blocking glycolysis or mitochondrial ATP synthase we demonstrated that in JHH-6 ATP synthase functions in reverse and consumes glycolytic ATP, thereby sustaining Delta Psi m. A higher expression level of ATP synthase Inhibitor Factor 1 (IF1), a higher extent of IF1 bound to ATP synthase and a lower ATPase/synthase capacity were documented in JHH-6. Thus, here IF1 appears to down-regulate the reverse mode of ATPsynthase activity, thereby playing a crucial role in controlling energy waste and Delta Psi m. These results, while confirming the over-expression of IF1 in cancer cells, are the first to indicate an inverse link between cell differentiation status and IF1 (expression level and regulatory function).

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