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The effect of the addition of ouabain to the nutrient solution was determined on resistance, potential difference (p.d.) and H+ secretion rate. In NaCl media, 10?3 M ouabain decreased significantly the p.d. from 25.6 mV to 16.1 mV in 30 min and to 11.0 mV in 60 min. NO significant changes occurred in resistance and H+ secretion rate. In Na2SO4 (Cl?-free) media, ouabain produced a biphasic effect on p.d. The p.d. changed from ?28.0 mV (nutrient-negative) to a nadir of ?37.4 mV in 7 min and then increased to ?16.4 mV in 60 min. At the nadir there was no significant change in resistance or H+ secretion rate but at 60 min, unlike Cl? media, resistance increased by 36% and H+ secretion rate decreased by 43%. To decide whether the ouabain-caused decrease in H+ rate in Na2SO4 media was due to an effect on the H+ pump or on resistance of the return pathways, the voltage was clamped at 0 and 40 mV. Clamping the voltage showed that in the case of a marked decrease in the H+ secretion rate, the H+ transport mechanism itself was inhibited (and not the parallel pathway). The decrease in p.d. due to ouabain in Cl? and SO42? media indicates that the (Na+ + K+)-ATPase mechanism may be electrogenic.  相似文献   

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The frog gastric mucosa has been shown to be sensitive to amytal. At 2 mM acid secretion was completely inhibited with a rise of resistance, fall in short-circuit current and no significant change in potential difference. Simultaneously there was 75% inhibition of O2 consumption and 50% depression of ATP levels. Dual-beam spectrophotometric studies of intact mucosa with amytal showed a crossover point between NAD+ and FAD. The microsomal NADH oxidase ferricyanide reductase has also been shown to be amytal sensitive. Cl transport was relatively insensitive to amytal, suggesting a qualitative distinction between the mechanisms underlying the transport of H+ and Cl in the mucosa. This was further brought out by the effects of anoxia in which H+ transport was inhibited at 5 min but Cl transport at minimally 20 min following the onset of anoxia.  相似文献   

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Water flow through frog gastric mucosa   总被引:2,自引:0,他引:2       下载免费PDF全文
To elucidate the role of protein synthesis in DNA formation, E. coli R2 infected with phage T2 was studed as a model, employing chloramphenicol to inhibit protein synthesis. The following results were obtained. 1. Chloramphenicol inhibited protein synthesis but not synthesis of nucleic acids in uninfected bacteria. 2. Studies of the effect of chloramphenicol on phage maturation indicated a delay of 2 minutes between time of addition and cessation of phage growth. 3. The increase of DNA in phage-infected bacteria was completely suppressed by the addition of chloramphenicol within 2 minutes following infection. Addition at later times showed progressively less inhibitory action depending upon the time interval, and addition after the 10th or 12th minute showed no appreciable effect on DNA synthesis despite the cessation of intracellular phage formation and protein synthesis. 4. When chloramphenicol was added to infected cells the increase of resistance to UV stopped within 2 minutes, whether or not DNA synthesis continued. Thus evolution of resistance paralleled the rate of DNA synthesis achieved, but not the amount of DNA accumulated. 5. We conclude that in infected bacteria, protein synthesis is necessary to initiate DNA synthesis but is not essential for its continuation. The resistance to UV that characterizes infected cells near the midpoint of the latent period is not due to accumulation of DNA, but depends on some chloramphenicol-sensitive process (probably protein synthesis) completed at about the time the rate of DNA synthesis becomes maximal.  相似文献   

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The effects of Ba2+ were studied in vitro on the isolated frog spinal cord. Ba2+ (25 microM-5 mM) caused a concentration-dependent depolarization of ventral (VR) and dorsal (DR) roots. TTX and Mg2+ substantially reduced the depolarization suggesting that interneuronal effects were involved. Ba2+ (25-500 microM) markedly increased the frequency and duration of spontaneous VR and DR potentials and substantially enhanced the duration (and frequently the amplitude) of VR and DR potentials evoked by DR stimulation. Higher concentrations of Ba2+ (1-5 mM) reduced both spontaneous and evoked potentials. Ba2+ (25-500 microM) enhanced the amount of K+ released by a DR volley and by application of L-glutamate and L-aspartate. The cation reduced VR and DR root depolarizations produced by elevated [K+]0. VR potentials induced by L-glutamate, L-aspartate, GABA and glycine and DR depolarizations caused by GABA were reduced by Ba2+. These results show that Ba2+ has complex actions on reflex transmission, interneuronal activity, the postsynaptic actions of excitatory and inhibitory amino acids and the evoked release of K+.  相似文献   

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An adenosine triphosphatase from frog gastric mucosa   总被引:6,自引:0,他引:6  
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Production of ulcers in isolated frog gastric mucosa   总被引:3,自引:0,他引:3  
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Active transport and ATP in frog gastric mucosa   总被引:1,自引:0,他引:1  
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Serosal-to-mucosal and mucosal-to-serosal diffusion of 14C-labelled inulin, sucrose, erythritol and propionamide was compared with 3HHO diffusion in mucosae incubated with isosmotic solutions at both surfaces, as well as isosmotic solution at serosal surface and hyperosmotic solution at the mucosal surface. The use of a hyperosmotic solution at the mucosal surface significantly increases unidirectional diffusion fluxes of inulin and of sucrose. To a nonsignificant extent, it affects the fluxes of erythritol and propionamide and significantly reduces the 3HHO diffusion. A size increment of the diffusion path utilized by the larger molecules is proposed.  相似文献   

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A method of estimation of pH in frog gastric mucosa by measuring the apparent creatine kinase equilibrium was studied. In a resting, in vitro preparation of frog stomach the intracellular pH was found to increase linearly with an increase in the serosal pH. This increase was also accompanied by an increase in the apparent equilibrium constant of the creatine kinase reaction. A similar increase was found when the resting mucosa was stimulated with histamine plus theophylline. During this procedure the total content of adenine nucleotides and creatine plus creatine phosphate remained constant.  相似文献   

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ATP, added to the solution bathing the nutrient (serosal) surface of isolated frog gastric mucosa, was found to break down rapidly to ADP, inorganic phosphate and other products. This activity is due to an ectoenzyme, i.e., to an enzyme system easily accessible to the bathing solution. This conclusion follows from experiments which showed that penetration of ATP into the mucosal cells occurred at a much slower rate: leakage of inorganic phosphate and adenine nucleotides from mucosal cells was also minor. The surface ATPase may reflect the operation of a mechanism at the nutrient surface involved in acid secretion.  相似文献   

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The unidirectional fluxes of Cl- and Na+ across the frog gastric mucosa in vitro were investigated with radioactive isotopes, and related to the secretory and electrical properties of the normal, and metabolically inhibited, mucosa. The flux of Cl- from nutrient to secretory surface of the mucosa was observed to rise sharply with increasing acid secretion, while the corresponding flux of Na+ did not change appreciably. Lowering [NaCl] in the secretory solution caused a proportional drop in the fluxes from secretory to nutrient surface, of both Cl- and Na+. Under the same conditions, the flux of Cl- from nutrient to secretory surface fell by nearly the same amount as did the flux of Cl- in the opposite direction, while the flux of Na+ from nutrient to secretory surface remained essentially unchanged. Electrical and hydrodynamic causes for this observation could be excluded. Metabolic inhibitors, including cyanide, azide, DNP, and anaerobiosis depressed Cl- flux in both directions distinctly below the corresponding values observed with the normal, non-secreting mucosa. At the same time, a decrease in electrical potential difference and conductance was observed under inhibition. The flux of Na+ was little changed by metabolic inhibition. The relationship between fluxes and conductance of Cl- during metabolic inhibition differs markedly from that observed under normal conditions, and is consistent with the view that during metabolic inhibition most of the Cl- moving across the mucosa does so as a free ion. From the above data it is concluded that Cl- is normally transported across the mucosa in combination with a carrier, the supply of which is impaired under metabolic inhibition. According to the behavior of the Na+ flux, the passive permeability of the mucosa appeared to be little affected by the metabolic inhibition applied, but seemed to rise considerably after death of the mucosa, probably due to structural damage.  相似文献   

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