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The determination of the rate constant for the efflux of an amine from efflux curves for amine and metabolite (1978)

Bönisch, H. ; Graefe, K. -H. ; Trendelenburg, U.

Springer

Naunyn-Schmiedeberg's archives of pharmacology 304 (1978), S. 147-155

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ISSN: 1432-1912

Keywords: Rate constant for efflux of amine ; Isoprenaline ; Simulated efflux curves ; Extraneuronal mechanism ; Mathematical model

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary 1. Rat hearts were perfused with 0.1 μM 3H-isoprenaline for 10 min in the presence of 10 μM U-0521 to inhibit catechol-O-methyl transferase (COMT) and then washed out with amine-free solution. Analysis of efflux curves revealed a preferential filling of one (compartment III) of the two extraneuronal compartments described by Bönisch et al. (1974). U-0521 inhibited the efflux of isoprenaline from compartment III. Omission of U-0521 from the wash out solution quickly restored COMT activity. It was then possible to determine the rate constant for the efflux (k s) of isoprenaline from rate of efflux and amine content of tissue. 2. A procedure is developed which permits the calculation of k s from efflux curves for amine and metabolite without any need for determining the amine content of the tissue. With this procedure, k s can be determined even when there is a “bound fraction” (i.e., a second compartment, the amine content of which does not contribute to the experimentally determined efflux). The procedure is based on the fact that, for a single compartment in which the amine is metabolized and from which there is efflux of amine and metabolite, parallel efflux curves (i.e., plots of log rate of efflux against time) are obtained, if the rate constant for the efflux of the metabolite (k p) is higher than the rate constant for the loss of amine from the compartment (k system). The activity of the metabolizing enzyme determines k system and the ratio “initial rate of efflux of metabolite/initial rate of efflux of amine” (F 0). 3. A mathematical model (simulating metabolism in, and efflux of amine and metabolite from a single compartment) was used to determine the distortion of F 0 by “k system/k P” (when k P limits the efflux of the metabolite). An estimate of k s obtained from F 0 and from k system agrees well with the estimate of k s obtained directly (see 1, above).

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00495551

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Analysis of the compartments involved in the extraneuronal storage and metabolism of isoprenaline in the perfused heart (1974)

Bönisch, H. ; Uhlig, W. ; Trendelenburg, U.

Springer

Naunyn-Schmiedeberg's archives of pharmacology 283 (1974), S. 223-244

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ISSN: 1432-1912

Keywords: Isoprenaline ; Extraneuronal COMT ; Uptake2 ; Corticosterone ; Extraneuronal Compartments

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary 1. Rat hearts were perfused with various concentrations of 3H-(±)-isoprenaline, and initial rates were determined for the removal of the amine from the perfusion fluid and for its O-methylation. Both removal and O-methylation obeyed Michaelis-Menten kinetics, K m and V max being 21 μM and 38 nmoles · g−1 · min−1 for the former, and 2.9 μM and 1.7 nmoles · g−1 · min−1 for the latter. After block of COMT the kinetic constants for removal (which equals accumulation under these conditions) were about the same as before. The kinetics of O-methylation seem to differ strikingly from those of accumulation of unchanged amine. 2. Corticosterone and 3-O-methylisoprenaline were about equipotent in antagonizing the accumulation and O-methylation of isoprenaline in the rat heart during perfusion with 3H-isoprenaline. 3. U-0521 (dihydroxy-2-methyl propiophenone; 100 μM) was used as a blocker of COMT. In addition it was found to be a weak inhibitor of the extraneuronal uptake of isoprenaline (K i =230 μM). 4. After block of COMT and subsequent to perfusion of the heart with 0.95 μM 3H-isoprenaline, efflux curves were determined during wash out with amine-free solution. Four compartments were detected (in order of increasing half time of efflux): I represented the fluid in dead space, cardiac cavities and large vessels; II equalled the extracellular space; III and IV represented extraneuronal storage sites. Corticosterone impaired the filling of compartments III and IV when present during filling. Both corticosterone and 3-O-methylisoprenaline (OMI) delayed the efflux from compartment III when present in the wash out solution only. 5. Experiments with guinea-pig hearts showed qualitative similarities between these and rat hearts. However, the storage and the O-methylating capacity of the guinea-pig heart was considerably smaller than that of the rat heart. 6. Rat ventricle slices (exposed to 0.95 μM 3H-(±)-isoprenaline for 30 min) were compared with perfused hearts. While the accumulation of 3H-isoprenaline was about 1/4, the total formation of 3H-OMI was only 1/50 of that determined for the perfused heart. This low rate of formation of 3H-OMI was also observed for slices of aorta, vas deferens and spleen, while slices of salivary glands had a high O-methylating capacity. Apparently, perfusion of the heart provides optimal access to the O-methylating compartment which may be located in vascular smooth muscle.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00499185

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Further studies on the extraneuronal uptake and metabolism of isoprenaline in the perfused rat heart (1978)

Bönisch, H.

Springer

Naunyn-Schmiedeberg's archives of pharmacology 303 (1978), S. 121-131

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ISSN: 1432-1912

Keywords: Isoprenaline ; Extraneuronal uptake ; Corticosterone ; Inhibition of extraneuronal uptake ; Extraneuronal efflux ; Steady-state kinetics

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary To simultaneously determine the kinetics of removal, O-methylation and accumulation of 3H-isoprenaline, isolated rat hearts were perfused for 4 min with various concentrations of 3H-isoprenaline. The apparent K m for the O-methylation of 3H-isoprenaline (3.3±0.5 μM) was more than one order of magnitude lower than the corresponding value for the accumulation of unchanged amine (71.3±7.1 μM). The apparent K m for removal was very similar to that for accumulation (63.2±5.9 μM). At perfusion concentrations higher than 25 μM, i.e. when O-methylation was saturated, removal virtually equalled accumulation. However, at low substrate concentrations removal of 3H-isoprenaline was overwhelmingly followed by O-methylation; this led to a marked difference between rates of removal and those of accumulation. When initial rates of uptake of 3H-isoprenaline were determined after 1.5 min of perfusion of the hearts by the method of Graefe et al. (1978), the uptake of 3H-isoprenaline consisted of two components: a nonsaturable and a saturable (after subtraction of the nonsaturable component from the total uptake). The kinetic constants of the saturable component of uptake were higher than those obtained after 4 min perfusion (see above) (K m : 110±19 μM; V max: 80±4 nmoles·g−1·min−1). Corticosterone competitively inhibited the saturable component of uptake of 3H-isoprenaline (K m : 1.2 μM). During wash out of accumulated 3H-isoprenaline, O-methylation took place predominantly in one of the two extraneuronal compartments. The efflux of 3-O-methyl-3H-isoprenaline (3H-OMI), the O-methylated metabolite of 3H-isoprenaline, was characterized by a half time of about 1.2 min. O-methylation accelerated the loss of radioactivity from the tissue during wash out. The extraneuronal uptake of 3H-isoprenaline was characterized as a “pump and leak” system by means of steady-state kinetics of accumulation of 3H-isoprenaline. Half saturation of the steady-state accumulation was observed at a concentration of 104.5 ±18.5 μM 3H-isoprenaline; the leak component was characterized by a rate constant of 0.0359 min−1.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00508057

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The O-methylation of extraneuronally stored isoprenaline in the perfused heart (1974)

Uhlig, W. ; Bönisch, H. ; Trendelenburg, U.

Springer

Naunyn-Schmiedeberg's archives of pharmacology 283 (1974), S. 245-261

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ISSN: 1432-1912

Keywords: Isoprenaline ; Extraneuronal COMT ; Uptake2 ; Corticosterone ; Extraneuronal Compartments

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary 1. Rat hearts were perfused with 0.95 or 23.8 μM 3H-(±)-isoprenaline for 30 min; efflux curves were determined for total radioactivity, 3H-isoprenaline and 3H-O-methylisoprenaline during wash out with amine-free solution. 2. The efflux curves indicated that most or all of the COMT activity was associated with compartment III of Bönisch et al. (1974). Most of the metabolite appearing in the wash out solution was formed during wash out. 3. The efflux curves for the metabolite (3H-OMI) were convex. The convexity was much more pronounced after perfusion with 23.8 μM than after perfusion with 0.95 μM 3H-isoprenaline. 4. On addition of 20 μM corticosterone to the wash out solution, the rate of efflux of 3H-isoprenaline was reduced but not that of 3H-OMI; in addition, the appearance of the convexity of the efflux curve for 3H-OMI was delayed. 5. In order to explain these phenomena, it is suggested that, during perfusion with 0.95 μm or more of catecholamine, the rate of uptake into compartment III is substantially higher than the rate of O-methylation. Consequently, unchanged amine can accumulate in compartment III and saturate COMT. During wash out the enzyme becomes desaturated, and the convex shape of the efflux curve for the product (3H-OMI) ensues. 6. The O-methylating capacity of the guinea-pig hearts is considerably smaller than that of the rat heart.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00499186

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Extraneuronal removal, accumulation and O-methylation of isoprenaline in the perfused heart (1974)

Bönisch, H. ; Trendelenburg, U.

Springer

Naunyn-Schmiedeberg's archives of pharmacology 283 (1974), S. 191-218

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ISSN: 1432-1912

Keywords: Isoprenaline ; Extraneuronal Uptake ; Extraneuronal O-Methylation ; Rat Heart ; Removal of Isoprenaline

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary 1. Isolated rat and guinea-pig hearts were perfused with 0.95 μM (±)-isoprenaline or 3H(±)-isoprenaline, a catecholamine which is taken up by extraneuronal mechanisms only. From measurements of the arterio-nevous difference (by fluorimetry and by scintillation counting, respectively) the rate of removal of the amine from the perfusion fluid was measured; in addition, the rate of appearance of its metabolite (3-O-methyl-3H-isoprenaline; 3H-OMI) was determined in the venous effluent as well as the accumulation of 3H-isoprenaline and 3H-OMI in the heart. 2. Experiments with sodium thiocyanate and 14C-sorbitol showed that these agents distributed into the extracellular space (about 350 μl/g; t/2 for efflux of about 1.2 min) and into ventricular and atrial cavities (about 1500 μl/g; t/2 for efflux of 0.1 to 0.2 min). 3. The removal of 3H-isoprenaline from the perfusion fluid declined biphasically with time; after an initial rapid decline the rate of removal approached steadystate levels within about 30 min. After block of COMT (by the presence of 100 μM U-0521) the second phase of decline approached zero. In the absence of U-0521 the steady-state rate of removal was 10 times higher in rat than in guinea-pig hearts; in the presence of U-0521 the approach to zero was faster for guinea-pig than for rat hearts. 4. When COMT was intact, 3H-OMI appeared in the venous effluent, first at a rapidly increasing rate, from the 9th minute of perfusion onward at a steady rate which was identical with the steady-state rate of removal of 3H-isoprenaline. No 3H-OMI was detected after block of COMT. 5. The accumulation of 3H-isoprenaline in the heart reached a steady level within about 30 min; block of COMT increased the time required for approach to steady levels and increased the accumulation of 3H-isoprenaline in the rat (but not in the guinea-pig) heart. When COMT was intact, the accumulation of 3H-OMI in the heart reached steady-state levels within 10 min. 6. The time-dependent decline of the rate of removal of 3H-isoprenaline by hearts whose COMT had been inhibited was due to a time-dependent increase of the rate of efflux of the amine from the stores; there did not seem to be any change in the rate of gross influx. 7. Isoprenaline-induced ventricular fibrillation reduced the rate of O-methylation of 3H-isoprenaline significantly. 8. Perfusion of hearts with 0.095 μM (±)-isoprenaline resulted in a significantly greater accumulation of the amine in rat than in guinea-pig and rabbit hearts.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00501145

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