Effects of <scp>dl</scp>-2-bromopalmitoyl-CoA and bromoacetyl-CoA in rat liver and heart mitochondria. Inhibition of carnitine palmitoyltransferase and displacement of [14C]malonyl-CoA from mitochondrial binding sites

Edwards, Michael R.; Bird, Michael I.; Saggerson, E D

doi:10.1042/bj2300169

Cited by 24 publications

(1 citation statement)

References 30 publications

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“…The conclusion that fatty acyl-CoA elongation activity is not detectable in the heart leads to the abandonment of the suggestion in [10] that the condensing enzyme of this system could act as the cellular binding ' sink ' for malonyl-CoA. Therefore other undefined cellular components must constitute this ' sink ', which is absolutely necessary because ' global ' concentrations of malonyl-CoA in the heart are very much higher than those that inhibit heart CPT " [3][4][5]35,36].…”

Section: Discussionmentioning

confidence: 99%

Malonyl-CoA metabolism in cardiac myocytes

HAMILTON

Saggerson

2000

Biochem. J.

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(1) Malonyl-CoA is thought to play a signalling role in fuel-selection in cardiac muscle, but the rate at which the concentration of this potential signal can be changed has not previously been investigated. (2) Rapid changes in cellular malonyl-CoA could be observed when rat cardiac myocytes were incubated in glucose-free medium followed by re-addition of 5 mM glucose, or when cells were transferred from a medium containing glucose to a glucose-free medium. On addition of glucose, malonyl-CoA increased by 62% to a new steady-state level, at a rate of at least 0.4 nmol/g dry wt. per min. The half-time of this change was less than 3 min. After removal of glucose the malonyl-CoA content was estimated to decline by 0.43-0.55 nmol/g dry wt. per min. (3) Malonyl-CoA decarboxylase (MDC) is a possible route for disposal of malonyl-CoA. No evidence was obtained for a cytosolic activity of MDC in rat heart where most of the activity was found in the mitochondrial fraction. MDC in the mitochondrial matrix was not accessible to extramitochondrial malonyl-CoA. However, approx. 16% of the MDC activity in mitochondria was overt, in a manner that could not be explained by mitochondrial leakage. It is suggested that this, as yet uncharacterized, overt MDC activity could provide a route for disposal of cytosolic malonyl-CoA in the heart. (4) No activity of the condensing enzyme for the fatty acid elongation system could be detected in any heart subcellular fraction using two assay systems. A previous suggestion [Awan and Saggerson (1993) Biochem. J. 295, 61-66] that this could provide a route for disposal of cytosolic malonyl-CoA in heart should therefore be abandoned.

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