Literature DB >> 6846528

Functional compartmentalization of oxidative and glycolytic metabolism in vascular smooth muscle.

R J Paul.   

Abstract

The metabolism of vascular smooth muscle is characterized by an unusual component of aerobic glycolysis. Lactate production, even under fully oxygenated conditions, is of similar magnitude to the rate of oxygen consumption when compared on a molar basis. Although the underlying mechanisms are unknown, the ratio of glycolytic to oxidative metabolism has been suggested to be an index of vascular myopathy. Measurements of the rate of O2 consumption (JO2), lactate production (Jlac), and isometric force in porcine coronary arteries were made under conditions known to alter both active force (delta Po) and Na+-K+ transport. As previously reported, JO2 was strongly correlated with delta Po; Jlac, however, was correlated with conditions that alter Na+-K+ transport. Under conditions known to inhibit Na+-K+ transport (10(-5) M ouabain, absence of extracellular K+ or Na+), Jlac was inhibited even though delta Po and JO2 were increased. The coupling of Na+-K+ transport with aerobic glycolysis was not dependent on tonicity or the major anion species, nor was it an effect simply on tissue lactate permeability as indicated by studies of tissue lactate content. Metabolic measurements made at similar levels of delta Po indicate that Jlac is markedly inhibited by ouabain, whereas JO2 shows little effect. Thus the unusual aerobic glycolysis observed in vascular smooth muscle appears to be linked to Na+-K+ transport processes and not to some nonspecific metabolic deficiency. Experiments on both systemic and pulmonary arteries from rat, rabbit, dog, and pig indicate that these results are not limited solely to porcine coronary vessels.

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Year:  1983        PMID: 6846528     DOI: 10.1152/ajpcell.1983.244.5.C399

Source DB:  PubMed          Journal:  Am J Physiol        ISSN: 0002-9513


  45 in total

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3.  Effects of exercise on plasma lipoprotein levels and endothelium-dependent vasodilatation in young and old rats.

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5.  Importance of various types of metabolic inhibition for cell damage caused by direct membrane damage.

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7.  The focal adhesion protein paxillin regulates contraction in canine tracheal smooth muscle.

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8.  Effects of hypoxia on relationships between cytosolic and mitochondrial NAD(P)H redox and superoxide generation in coronary arterial smooth muscle.

Authors:  Qun Gao; Michael S Wolin
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9.  Functional compartmentation of glycolytic versus oxidative metabolism in isolated rabbit heart.

Authors:  J Weiss; B Hiltbrand
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10.  Cardiac ischemia. Part I--Metabolic and physiologic responses.

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