Effect of Krebs cycle intermediates and inhibitors on toad gastric mucosa.

Chacín, Jesús; Rincón, R; Inciarte, Douglas J.; Canizales, A.; Martínez, Guillermo; Alonso, D

doi:10.1152/ajpendo.1979.236.6.e692

Cited by 4 publications

(1 citation statement)

References 17 publications

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“…The differences in the kinetics of oxoglutarate oxidation might be related to different permeability rates in the process of penetration of oxoglutarate into the cells. In the isolated toad gastric mucosa, cell permeability is a ratelimiting factor for oxoglutarate oxidation, and lowering the nutrient pH from 7.4 to 5 0 facilitates penetration and oxidation (Chacin et al 1979).…”

Section: Discussionmentioning

confidence: 99%

Interactions between oxoglutarate oxidation and acid secretion in isolated rabbit gastric glands

Chacín¹,

Hernández²

1995

Experimental Physiology

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SUMMARYThe effects of gastric secretagogues, and other agents that modify H+,K+-ATPase activity and cell calcium concentration, on the rate of oxoglutarate oxidation were investigated in isolated gastric glands. Oxoglutarate was oxidized in a dose-dependent manner by gastric glands, with an apparent Km for oxoglutarate of 3 9 + 0 5 mM. Oxoglutarate progressively inhibited the rate of glucose oxidation. In the presence of 0 5 mM oxoglutarate plus 10 mM glucose, the latter substrate was preferentially oxidized and contributed most to oxygen uptake. With 10 mM oxoglutarate plus 10 mM glucose, the rate of glucose oxidation was greatly inhibited and oxoglutarate oxidation accounted for most of the oxygen consumption. Acid secretion (aminopyrine accumulation) was significantly increased by 0.1 mM histamine in glands oxidizing 10 mM oxoglutarate, although this stimulation was significantly lower than that observed in the presence of 0-5 mM oxoglutarate plus 10 mM glucose. Omeprazole, an inhibitor of the H+,K+-ATPase, significantly reduced the oxidation of oxoglutarate, whereas NH4+, an activator of the enzyme, stimulated the oxidation of a submaximal dose of oxoglutarate. Carbachol at 0.1 mm significantly increased the rate of oxidation of non-saturating concentrations of oxoglutarate. The calcium ionophore ionomycin at 10 /M produced a similar effect. Chelation of intracellular calcium by BAPTA AM caused a significant inhibition of oxoglutarate oxidation. The results provide further evidence that changes in the ATP: ADP ratio resulting from activation of the H+,K+-ATPase, and calcium ions are involved in the mechanisms of activation of oxidative metabolism in the parietal cell.

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Section: Discussionmentioning

confidence: 99%

Interactions between oxoglutarate oxidation and acid secretion in isolated rabbit gastric glands

Chacín¹,

Hernández²

1995

Experimental Physiology

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Stimulation of pyruvate carboxylation by gastric secretagogues

Bohórquez

Chacín

1980

Experientia

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Pyruvate carboxylation was stimulated by 2 gastric secretagogues, histamine and dibutyryl cyclic AMP, and by butyrate. Thiocyanate, an inhibitor of acid secretion, produced a slight decrease. Avidin significantly reduced acid secretion and this effect was overcome by biotin and oxalacetate. The results suggest that carboxylation of pyruvate is one of the reactions controlling oxidative metabolism and acid secretion in toad gastric mucosa.

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