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1

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EFFECT OF INHIBITORS AND THE MECHANISMS OF ANION TRANSPORT IN THE PROXIMAL RENAL TUBULE OF RATS (1980)

Frömter, E. ; Ullrich, K. J.

Oxford, UK : Blackwell Publishing Ltd

Annals of the New York Academy of Sciences 341 (1980), S. 0

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ISSN: 1749-6632

Source: Blackwell Publishing Journal Backfiles 1879-2005

Topics: Natural Sciences in General

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1111/j.1749-6632.1980.tb47164.x

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2

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„Anatomie” eines Epithels (1973)

Ullrich, K. J.

Springer

Naturwissenschaften 60 (1973), S. 290-297

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ISSN: 1432-1904

Source: Springer Online Journal Archives 1860-2000

Topics: Biology , Chemistry and Pharmacology , Natural Sciences in General

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00624443

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3

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Transport of inorganic and organic substances in the renal proximal tubule (1982)

Ullrich, K. J. ; Rumrich, G. ; Klöss, S.

Springer

Journal of molecular medicine 60 (1982), S. 1165-1172

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ISSN: 1432-1440

Keywords: Epithelial transport ; Kidney ; Lactate transport ; Electrolyte transport ; Epithelialer Transport ; Niere ; Laktattransport ; Elektrolyttransport

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Description / Table of Contents: Zusammenfassung Resorption bzw. Sekretion im proximalen Nierentubulus läuft einmal passiv auf dem parazellulären Weg, d.i. zwischen den Zellen hindurch, ab, zum anderen aktiv, transzellulär, durch die Zellen hindurch. Der transzelluläre aktive Transport ist in der Regel sekundär aktiv. Er verläuft gekoppelt an den Fluß von Na+-Ionen, wobei ein transzellulärer Gradient von Na+-Ionen, der seinerseits durch die kontraluminal gelegene (Na+-K+)-ATPase geschaffen wird, die Triebkraft liefert. Einmal in der Zelle, verlassen die Substanzen die kontraluminale Zellseite vermittels Karrier, die Na+-unabhängig sind. Mit Hilfe von Mikroperfusions- und elektrophysiologischen Techniken sowie mit Hilfe von Bürstensaumvesikeln wurde der Na+-Kotransport von Aminosäuren, Phosphat, Sulfat, Thiosulfat, Gallensäuren, aliphatischen und aromatischen Monokarboxylsäuren (Laktat) sowie der von Dikarboxylsäuren untersucht. Besonderes Augenmerk wurde dem bidirektionalen Transport von Thiosulfat sowie der Spezifität des Mono- und Dikarboxylsäure-Transportsystems gewidmet.

Notes: Summary The transport through the epithelial cell layer of the renal proximal tubule proceeds in principle by passive paracellular and active transcellular transport. The active transcellular transport is mostly secondary active. This means it proceeds coupled with the flux of Na+ ions, where-by the transcellular gradient of sodium, created by the (Na++K+)-ATPase, located at the contraluminal cell side, provides the main driving force. Once in the cell the substances leave the other cell side by a Na+-independent, but carrier-mediated transport system. Using microperfusion and electrophysiological techniques as well as brush border membrane vesicle preparation the Na+-H+ countertransport and the Na+-cotransport of amino acids, phosphate, sulfate, thiosulfate, bile acids, aliphatic-aromatic monocarboxylic acids (lactate) and dicarboxylic acids was studied. Special emphasis will be given to the bidirectional transport of thiosulfate as well as to the specificity of the monocarboxylic acid and dicarboxylic acid transport system.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01716718

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4

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Bicarbonate reabsorption in the papillary collecting duct of rats (1981)

Ullrich, K. J. ; Papavassiliou, F.

Springer

Pflügers Archiv 389 (1981), S. 271-275

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ISSN: 1432-2013

Keywords: Adaptation, HCO 3 − transport ; Glycodiazine transport ; Metabolic acidosis ; Metabolic alkalosis ; Acetazolamide ; SITS ; Potassium deficiency

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Using the technique of capillary perfusion and simultaneous luminal stop flow microperfusion the reabsorption of bicarbonate and glycodiazine from the papillary collecting duct was evaluated. Starting with equal H14CO 3 − and3H-glycodiazine concentrations in the luminal and peritubular perfusates, the decrease in the luminal concentration at 10 and 45 s contact time was measured. In control rats with 25 mmol/l HCO 3 − in the perfusates the rate of HCO 3 − reabsorption calculated from the 10 s values was 0.34 nmol cm−2s−1. In acute metabolic acidosis, the rate of bicarbonate reabsorption was 2,3 times higher. In metabolic alkalosis, the rate of bicarbonate absorption dropped to 13% of the control values. Also the 45 s values of acidotic and alkalotic animals differed significantly from each other. With 25 mmol/l glycodiazine in both perfusates the rate of biffer reabsorption as calculated from the 10 s values was 0.76 nmol cm−2s−1 in control rats and did not deviate significantly from this value in acidotic and alkalotic animals. In control rats the bicarbonate reabsorption in % was the same, no matter whether both luminal and capillary perfusate contained 25 mmol/l bicarbonate or 10 mmol/l. In acidotic rats the rate of HCO 3 − reabsorption did not change significantly if all Na+ in the perfusates was replaced by choline (0.88 versus 0.79 nmol cm−2s−1 at 25 mmol/l HCO 3 − ). When in acidotic rats 0.1 mmol/l acetazolamide or 1 mmol/l SITS (4-acetamido-4′-isothiocyanatostilbene-2,2′-disulfonic acid) was added to both perfusates the rate of HCO 3 − reabsorption dropped by 75 and 58%, respectively. A potassium deficient diet for one week and DOCA administration had no influence on the bicarbonate reabsorption of rats which were on standard diet. The data indicate that (1) the buffer reabsorption from the papillary collecting duct is rather due to H+ ion secretion than to buffer anion reabsorption. (2) The adaptation to metabolic acidosis and alkalosis is specific for bicarbonate and not seen with glycodiazine. (3) Within the concentration range tested the HCO 3 − reabsorption rises linearly with the HCO 3 t- concentration. (4) The HCO 3 − reabsorption in the papillary collecting duct is Na+-independent, it can be inhibited by acetazolamide and SITS, but is not influenced by K+-deficient diet plus DOCA.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00584789

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5

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Contraluminal sulfate transport in the proximal tubule of the rat kidney (1985)

Ullrich, K. J. ; Rumrich, G. ; Klöss, S.

Springer

Pflügers Archiv 404 (1985), S. 300-306

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ISSN: 1432-2013

Keywords: Epithelial transport ; Contraluminal cell membrane

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract In order to study the specificity for the contraluminal sulfate transport system the inhibitory potency of disulfonates, di-, tricarboxylates and sulfocarboxylates on the35SO 4 2− influx from the interstitium into cortical tubular cells in situ has been determined. The following was found: 1) Methane- and ethane-disulfonate as well as benzene-1,3-disulfonate inhibit contraluminal35SO 4 2− influx (with an (app.K i of 〈6 mmol/l), while benzene-1,2- and 1,4-disulfonate do not. 2) The inhibitory potency of 1,3-benzene disulfonate is slightly augmented by an additional NH2 − or OH-group in position 4. However, OH-groups at position 4 and 5 or 4 and 6 abolish the inhibitory potency. 3) The naphthalene disulfonates tested inhibit only if they have an OH-group in ortho-position to one SO3H group. 4) The stilbene disulfonates H2DIDS and DNDS inhibit the contraluminal35SO 4 2− influx with high (app.K i≈0.8 mmol/l), DADS with lower potency (app.K i≈6 mmol/l). 5) Amongst the tested aliphatic di- and tricarboxylates inhibition was exerted by oxalate (app.K i 1.1 mmol/l) and maleate (app.K i 3.8 mmol/l), but not by malonate, hydroxymalonate and citrate. 6) Out of the tested benzenedicarboxylates only those inhibit which have the COO−-groups directly on the ring in 1,2 and 1,3 position (app.K i 4.0 and 2.7 mmol/l), but not in the 1,4 position. An additional OH-group in position 4 augments the inhibitory potency of 1,3 benzene-dicarboxylates (app.K i 0.8 mmol/l), while an OH group on position 5 abolishes it. 7) The benzene tricarboxylates (BTC) inhibit in the sequence 1,2,3-BTC〉1,3,5-BTC〉1,2,4-BTC (app.K i 0.9, 1.5 and 4.2 mmol/l, respectively). 8) The carboxy-benzene-sulfonates inhibit also in the 1,2 and 1,3 position only (app.K i 6.7 and 5 mmol/l), but not in the 1,4 position. Addition of an −OH-group to the 3-carboxy-1-benzene-sulfonate forming 4-hydroxy-3-carboxy-1-benzene-sulfate augments the inhibitory potency drastically (app.K i 0.32 mmol/l), while a NH2 substitution at the same position leaves it unchanged (app.K i 4.7 mmol/l). If, however, ethylamine instead of NH2 is used as substituent, the inhibitory potency is almost as high as of 4-hydroxy-3-carboxy-1-benzene-sulfonate (app.K i≈0.6 mmol/l). Amongst the dicarboxy-benzene-sulfonates, 3,4-carboxy-benzene-1-sulfonate inhibits (app.K i ca. 2 mmol/l), while 3,5-carboxy-benzene-1-sulfonate does not. The data indicate that a strong interaction of substrate with the sulfate transporter is given, when two charged groups (COO− and/or SO 3 − ) are present in a distance equivalent to the meta-position on the benzene ring and an additional hydrogen bond forming OH- or −NH-group. Hydrogen bond forming groups and charged groups in other positions usually abolish the inhibitory potency.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00585339

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6

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A stopped flow capillary perfusion method to evaluate contraluminal transport parameters of methylsuccinate from interstitium into renal proximal tubular cells (1984)

Fritzsch, G. ; Haase, W. ; Rumrich, G. ; [et al.]

Springer

Pflügers Archiv 400 (1984), S. 250-256

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ISSN: 1432-2013

Keywords: Kidney cortex structure ; Tissue compartments ; Transport models ; Inhibitory kinetics ; Facilitated diffusion

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract In order to study the transport of dicarboxylic acids through the contraluminal cell membrane of proximal tubular cells,3H-methylsuccinate has been synthetized by catalytic hydration of methylfumarate. As the chromatography of radioactive material excreted in the urine after i.v. injection of3H-methylsuccinate shows, no metabolite is detectable during the first 3 min. After 10 min, less than 10% of the excreted radiolabel is metabolized. To measure the contraluminal influx of3H-methylsuccinate from the interstitium into cortical tubular cells, the renal vessels were clamped so that the proximal tubular lumina collapsed. Then Ringer solution was injected into the blood capillaries. It contained different concentrations of3H-methylsuccinate and14C-inulin as extracellular space marker. After contact times between 1 and 10 s, this fluid was withdrawn from the capillaries and the disappearance of3H-methylsuccinate relative to14C-inulin was measured. The morphological compartments in the outer cortex of the clamped glutaraldehyde-fixed kidney were evaluated by a stereological method. For proximal tubular cells a ratio of extracellular water space to intracellular space of 1:3.1 and a ratio extracellular water space to free cell water space of 1:2 was found. It was tested whether the experimental disappearance curves with 4 different starting concentrations of3H-methylsuccinate fit with the data from four model calculations. It was found that the data and the conditions of transport are consistent with the predictions of a facilitated diffusion model. In this model, a transport coefficient occurs which depends on the concentration of3H-methylsuccinate following saturation kinetics. The calculated parameters wer:K m for3H-methylsuccinate=0.12 mmol/l,J max=0.50 pmol/s ·cm (related to tubular length in cm). Furthermore, equations are given to calculate inhibitory constantsK i of competing dicarboxylic acids.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00581555

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7

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Contraluminal transport of small aliphatic carboxylates in the proximal tubule of the rat kidney in situ (1986)

Ullrich, K. J. ; Papavassiliou, F.

Springer

Pflügers Archiv 407 (1986), S. 488-492

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ISSN: 1432-2013

Keywords: Lactate ; Pyruvate ; 3-hydroxybutyrate ; Acetoacetate ; Nonspecific anion channel

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract In order to study the characteristic of contraluminal transport of hydrophylic small fatty acids the in situ stopped flow microperfusion technique [12] has been applied. By measuring with 4 s contact time the decrease in the contraluminal concentration of the respective radiolabelled substances the concentration dependence of the influx into the cortical cells was tested. The 4 s decrease in contraluminal concentration of chloroacetate,l-lactate,d-lactate, 3-hydroxybutyrate and acetoacetate was between 26% and 31%. For each substance the percent decrease was the same, no matter whether it was offered in a concentration of 0.1 or 10 mmol/l. Contraluminal disappearance of 0.1 mmol/ll-lactate was not influenced by 5 mmol/l H2DIDS, probenecid, phloretin, mersalyl or cyanocinnamate, but it was significantly (37%) inhibited by 5-nitro-2-(phenyl-propyl-amino) benzoate, a blocker of the nonspecific anion channel. The percent decrease in propionate uptake was somewhat larger — between 36% and 39% — but again not different at 0.01, 0.1, 1.0 and 10 mmol/l. With pyruvate the contraluminal decrease was 20% at 0.1 mmol/l and 31% at 10 mmol/l. The percent disappearance of the aromatic pyrazinoate was 38% and 34% at 0.1 and 10 mmol/l and for nicotinate 42% and 22%, respectively. The disappearance of nicotinate (0.1 mmol/l) was significantly inhibited by 10 mmol/l pyrazinoate and paraaminohippurate (PAH). The data are in agreement with the hypothesis that the hydrophilic small fatty acids traverse the contraluminal cell side by simple diffusion, possibly via the unspecific anion channel [14], pyruvate via the dicarboxylic acid pathway in a cooperative manner and pyrazinoate, as well as nicotinate, via the PAH pathway.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00657505

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Contraluminal para-aminohippurate (PAH) transport in the proximal tubule of the rat kidney (1987)

Ullrich, K. J. ; Rumrich, G. ; Fritzsch, G. ; [et al.]

Springer

Pflügers Archiv 408 (1987), S. 38-45

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ISSN: 1432-2013

Keywords: Oxalate ; Succinate ; Glutarate ; 2-Oxoglutarate ; Citrate ; Sulfate

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract In order to study the specificity for contraluminal para-aminohippurate (PAH) transport, the inhibitory potency of aliphatic dicarboxylates on3H-PAH influx, as well as the inhibitory effect on35SO 4 2− - and3H-succinate influx, from the interstitium into cortical tubular cells in situ has been determined. The following was found: 1. Testing a homologous series of dicarboxylates-ranging from the 2 C oxalate to the 10 C sebacate — PAH transport was inhibited by succinate (app.K i 1.35 mmol/l), and all longer dicarboxylates, with high potency (app.K i 0.05–0.35 mmol/l). Sulfate transport was inhibited only by oxalate (app.K i 1.1 mmol/l), while dicarboxylate transport was inhibited by succinate, glutarate, adipate and pimelate with decreasing potency (app.K i 0.04, 0.24, 0.91, 4.0 mmol/l, respectively). 2. PAH transport was inhibited by succinate and glutarate with high potency (app.K i 1.35 and 0.05 mmol/l), by the correspondent monomethylester to a lesser extent (app.K i 1.7 and 0.74 mmol/l), but not by the dimethylester. On the other hand, the semialdehyde of succinate with aK i-value of 1.2 mmol/l, had the same inhibitory potency as succinate itself, while the dialdehyde of glutarate (app.K i 1.4 mmol/l) was much less potent as glutarate. 3. Introduction of an oxo-, methyl- or sulfhydroxylgroup onto the 2-position of succinate, or of an oxo-group onto the 2-position of glutarate moderately augmented the inhibitory potency against PAH-uptake. However, introduction of a 2-hydroxy group onto succinate or glutarate in thel-position reduced the inhibitory potency more than in thed-position. Introduction of two methyl-, sulfhydryl- or hydroxyl-groups in the 2–3-position of succinate reduced or abolished its inhibitory potency. The introduction of a 2-amino group onto succinate or glutarate abolished its effect on PAH transport. However, N-acetylation or N-benzoylation led to a restitution in inhibitory potency. 4. The trans-isomers fumarate and mesaconate inhibited PAH- and methylsuccinate transport, while the cis-isomers maleate and citraconate did so to a lesser extent or not at all. The effect was reversed with the tricarboxylic aconitates, because cis-aconitate bears a CH2-extended COOH-group in trans-position and trans-aconitate in cis-position. The data indicate that there exist three different anion transport systems at the contraluminal cell side of the proximal renal tubule: 1. a sulfate-oxalate transporter, 2. a sodium-dependent dicarboxylate transporter, and 3. a paraaminohippurate transporter. The PAH transport system accepts dicarboxylates with chain length higher than 7.5 Å (=distance between the terminal oxygen atoms), while the dicarboxylate transport interacts with dicarboxylates with a chain length between 6.5 and 10 Å. Both transport systems prefer the transconfiguration. The effect of side groups on the interaction of dicarboxylates with the PAH-transport system is due mainly to hydrophobicity and electron configuration.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00581838

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Contraluminal sulfate transport in the proximal tubule of the rat kidney (1984)

Ullrich, K. J. ; Rumrich, G. ; Klöss, S.

Springer

Pflügers Archiv 402 (1984), S. 264-271

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ISSN: 1432-2013

Keywords: Epithelial transport ; Contraluminal cell membrane ; Anion exchange

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract In order to study contraluminal sulfate transport the influx rate of35SO 4 2− from the interstitium into cortical tubular cells has been determined. Preloading of the rat with sulfate augmented contraluminal35SO 4 2− influx; preperfusion with sulfate-free solutions diminished it. The contraluminal35SO 4 2− influx in sulfate-loaded animals followed two parameter kinetics (K m 1.4 mmol/l,J max 1.2 pmol·s−1·cm−1). The contraluminal35SO 4 2− influx (starting concentration 10 μmol/l) did not change when the K+ concentration was varied between 4 and 40 mmol/l and the Ca2+ concentration from zero to 3 mmol/l. Omission of Na+ from the perfusates augmented contraluminal35SO 4 2− influx markedly. The increase is larger at pH 6 than at pH 7.4. Changes of pH affect contraluminal35SO 4 2− influx only when the solutions are Na+- and K+-free. Under these conditions the35SO 4 2− influx decreased when the ambient pH was raised from pH 6.0 to pH 8.0. Thiosulfate, selenate, molybdate, oxalate, phosphate, arsenate, and bicarbonate exerted competitive inhibition, while formate, 2-oxoglutarate and paraaminohippurate showed a biphasic response: inhibition at 50 mmol/l, no inhibition at 150 mmol/l. Chloride and bicarbonate inhibited35SO 4 2− influx at 10 μmol/l35SO 4 2− , but augmented sulfate influx at 5 mmol/l35SO 4 2− concentration in rats not preloaded with sulfate. The data indicate the presence of a contraluminal sulfate transport system which is shared by a variety of inorganic and organic anions. The biphasic behaviour of some anions suggests parallel pathways leading to a cis-inhibition at small and trans-stimulation at high anion concentrations. Na+ and H+ may be cotransported or interact with the transport system at a modifier site.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00585509

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Reabsorption of monocarboxylic acids in the proximal tubule of the rat kidney (1982)

Ullrich, K. J. ; Rumrich, G. ; Klöss, S.

Springer

Pflügers Archiv 395 (1982), S. 212-219

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ISSN: 1432-2013

Keywords: SITS ; Probenecid ; Phloretin ; Acetazolamide ; Lactate ; Renal tubule

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract The transport ofd-lactate across the epithelium of the late proximal convolution was investigated by two methods: 1. by measuring the zero net flux transtubular concentration difference (Δc tt,45s) and the permeability (P) ofd-lactate and calculating from both the transtubular active transport rate (J lac act ). 2. By measuring the 3.5 s efflux ofd-lactate from the tubular lumen, while blood was flowing through the capillaries. The 3.5 s efflux comprises two components, one going through the brush border (J lac bb ) and one going the paracellular pathway (J lac paracell =P lac·c lac lumen). Both,J lac act andJ lac bb ofd-lactate gave the sameK m 1.9 and 1.7 mmol/l and the same maximal transport rate 3.2 and 2.9 pmol cm−1 s−1. TheK i ofl-lactate tested againstJ lac act andJ lac bb ofd-lactate was also the same: 1.1 and 1.0 mmol/l. These data indicate that under our experimental conditions only the flux through the brush border seems to be rate limiting and thatd-lactate uses the same transport system asl-lactate. When Na+ was omitted from the perfusatesJ lac act disappeared completely, whileJ lac bb was reduced by 64%. These data reflect the Na+ dependence of thed-lactate transport through the brush border. Variation of intra-and extracellular pH by raisingpCO2, omitting HCO 3 − from the perfusates or adding acetazolamide had no effect on the transport ofd-lactate when α-ketoglutarate was used as fuel. However, when acetate was used as fuel, intracellular acidosis brought the reducedJ lac act back to the values obtained with α-ketoglutarate as fuel. It is suggested that this is an effect on a contraluminal transport step. Probenecid (5 mmol/l) and phloretin (0.25 mmol/l) inhibitedJ lac act significantly.J lac bb , however, was only inhibited by probenecid when acetate was used as fuel. These data indicate that both compounds act on thed-lactate exit at the contraluminal cell side, but that probenecid acts in addition at the luminal cell side. SITS (1 mmol/l) augmentedJ lac bb when acetate was used as fuel and is similar to the effect of lowering intracellular pH as described above. The SH reagents mersalyl (1.0 mmol/l) and maleolylglycine (1 mmol/l) did not influenceJ lac bb .

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00584812

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