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  • Low energy costs of F1Fo ATP synthase reversal in colon carcinoma cells deficient in mitochondrial complex IV.

Low energy costs of F1Fo ATP synthase reversal in colon carcinoma cells deficient in mitochondrial complex IV.

Free radical biology & medicine (2017-02-13)
Alexander V Zhdanov, Dmitry E Andreev, Pavel V Baranov, Dmitri B Papkovsky
摘要

Mitochondrial polarisation is paramount for a variety of cellular functions. Under ischemia, mitochondrial membrane potential (ΔΨm) and proton gradient (ΔpH) are maintained via a reversal of mitochondrial F1Fo ATP synthase (mATPase), which can rapidly deplete ATP and drive cells into energy crisis. We found that under normal conditions in cells with disassembled cytochrome c oxidase complex (COX-deficient HCT116), mATPase maintains ΔΨm at levels only 15-20% lower than in WT cells, and for this utilises relatively little ATP. For a small energy expenditure, mATPase enables mitochondrial ΔpH, protein import, Ca

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羰基氰化物 4-(三氟甲氧基)苯腙, ≥98% (HPLC), powder
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BPTES, ≥95% (HPLC)
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四甲基罗丹明甲酯高氯酸盐, ≥95%