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  • Epithelial transport  (6)
  • Sulfate transport  (4)
  • Kidney Micropuncture  (2)
  • 1
    Electronic Resource
    Electronic Resource
    Transport of inorganic and organic substances in the renal proximal tubule (1982)
    Springer
    Journal of molecular medicine 60 (1982), S. 1165-1172 
    Details
    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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  • 2
    Electronic Resource
    Electronic Resource
    Contraluminal sulfate transport in the proximal tubule of the rat kidney (1985)
    Springer
    Pflügers Archiv 404 (1985), S. 300-306 
    Details
    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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  • 3
    Electronic Resource
    Electronic Resource
    Contraluminal sulfate transport in the proximal tubule of the rat kidney (1984)
    Springer
    Pflügers Archiv 402 (1984), S. 264-271 
    Details
    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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  • 4
    Electronic Resource
    Electronic Resource
    Active sulfate reabsorption in the proximal convolution of the rat kidney: Specificity, Na+ and HCO 3 − dependence (1980)
    Springer
    Pflügers Archiv 383 (1980), S. 159-163 
    Details
    ISSN: 1432-2013
    Keywords: Renal tubule ; Sulfate transport ; Na+ coupled transport ; Thiosulfate ; Molybdate
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract Using the standing droplet technique in the proximal convolution and simultaneous microperfusion of the peritubular capillaries, the decrease in luminal sulfate concentration with time and the zero net flux transtubular concentration difference of sulfate ( $$\Delta c_{{\text{SO}}_{\text{4}}^{{\text{2 - }}} } $$ ) at 45 s was determined — the latter being taken as a measure of the rate of active sulfate reabsorption. Starting with 0.5 mmol/l sulfate in both perfusates the $$\Delta c_{{\text{SO}}_{\text{4}}^{{\text{2 - }}} } $$ value of 0.35 mmol/l was approached exponentially with a half value time of 4.3 s. The $$\Delta c_{{\text{SO}}_{\text{4}}^{{\text{2 - }}} } $$ values in the early proximal and late proximal convolution did not deviate from each other. If the Na+ concentration in the perfusates was reduced, the $$\Delta c_{{\text{SO}}_{\text{4}}^{{\text{2 - }}} } $$ approached zero and extrapolated to a slightly negative value (c i〉c o). When 1 mmol/l ouabain was added to the perfusates $$\Delta c_{{\text{SO}}_{\text{4}}^{{\text{2 - }}} } $$ decreased by 66% (the latter experiments were performed in the golden hamster which is more sensitive to ouabain than the rat). 1 mmol/l thiosulfate diminished $$\Delta c_{{\text{SO}}_{\text{4}}^{{\text{2 - }}} } $$ by 68% and 1 mmol/l molybdate by 24%. Omitting or replacing bicarbonate by HEPES or glycodiazine reduced the sulfate reabsorption significantly, while acetazolamide (0.1 mmol/l) and increasing the CO2-pressure from 4.66 to 14.0 kPa (i.e. 5–15% CO2) had no effect. SITS 1 mmol/l had no effect on sulfate reabsorption. The data indicate that the sulfate reabsorption is driven by a Na+ gradient and inhibited by thiosulfate and molybdate, i.e. molecules which have a similar tetrahedral molecule structure. The sulfate reabsorption depends in an undefined manner on the presence of bicarbonate ions.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF00581877
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  • 5
    Electronic Resource
    Electronic Resource
    Bidirectional active transport of thiosulfate in the proximal convolution of the rat kidney (1980)
    Springer
    Pflügers Archiv 387 (1980), S. 127-132 
    Details
    ISSN: 1432-2013
    Keywords: Renal tubule ; Thiosulfate transport ; Na+ coupled transport ; Sulfate transport ; Paraaminohippurate transport
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract Using the standing droplet method in the late proximal convolution and simultaneous microperfusion of the peritubular capillaries, the zero net flux transtubular concentration difference of thiosulfate at 45 s was determined, the latter being taken as a measure of active thiosulfate transport. Under control conditions, in the presence of Na+, near zero Δc values were observed. When 1 mmol/l carinamide or paraaminohippurate (PAH) were added to the perfusates significant reabsorptive Δc arose. However, when 7.5 mmol/l sulfate was added to the Na+-free secretory Δc values were observed. Tested under Na+-free conditions, the secretory Δc was not influenced by simultaneously present 5 mmol/l of SO 4 2− but was diminished by 50 mmol/l SO 4 2− . PAH (1 mmol/l), carinamide (0.2 mmol/l) and probenecid (1 mmol/l) decreased the secretory Δc by 48, 65 and 48%, respectively. The PAH secretion was not influenced, when thiosulfate or sulfate up to 50 mmol/l was added to both perfusates. Under Na+-free conditions the Δc of thiosulfate in early loops of the proximal convolution is higher than in late loops, while for PAH this pattern is reversed. Taken together with the previously published inhibition of sulfate reabsorption by thiosulfate the data indicate 1. thiosulfate is reabsorved by the Na+-dependent sulfate transport system and 2. thiosulfate is simultaneously secreted by a carinamide-, probenecid-and PAH-sensitive secretory system. The secretory system might also be shared by sulfate. The thiosulfate net flux is the result of the difference in the activity of the counteracting transporters, located at the luminal and contraluminal cell side. Is is possible that the higher activity of the transporter at one cell side leads to a reversal of the flux through the transporter at the other cell side.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF00584263
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  • 6
    Electronic Resource
    Electronic Resource
    Contraluminal sulfate transport in the proximal tubule of the rat kidney (1985)
    Springer
    Pflügers Archiv 404 (1985), S. 293-299 
    Details
    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 sulfate esters and sulfonate compounds on the35SO 4 2− influx from the interstitium into cortical tubular cells in situ has been determined. The following was found: 1. From 10 sulfate monoesters tested 9 inhibited contraluminal sulfate influx with an app.K i between 0.6 and 6 mmol/l; the two sulfate diesters tested, however, did not. 2. Out of 8 aliphatic sulfonate compounds only three, having a NH- or OH-group in a suitable position, exerted a moderate inhibition (app.K i ca. 2–6 mmol/l). 3. Amongst 14 benzene sulfonates tested only 2 compounds (5-nitrobenzene-sulfonate and 2-hydroxy-5-nitrobenzenesulfonate) inhibited with aK i〈5 mmol/l. 4. Out of 10 naphthalene sulfonates tested 8 inhibited with aK i〈5; the highest inhibition was seen with the NH-containing 8-anilinonaphthalene-1-sulfonate (ANS), but no inhibition with 2 compounds containing an amino group. 5. From the polycyclic sulfonates pyrene-3-sulfonate and anthracene-1-sulfonate inhibited with aK i of approximately 2 mmol/l, while no inhibition was seen with anthracene-2-sulfonate. 6. Out of 4 amino-sulfonates tested benzene-1-amino-sulfonate and a similar benzyl-analog inhibited with aK i of 1 mmol/l and smaller; cyclohexyl-1-amino-sulfonate (cyclamate), however, inhibited only slightly (app.K i of 6 mmol/l). The data indicate that sulfate monoesters are well accepted by the contraluminal sulfate transport system. The affinity of sulfonate compounds to this system depends on neighbouring OH-groups −NH-groups, meta-positioned electronegative groups or a hydrophobic moiety in an appropriate position.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF00585338
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  • 7
    Electronic Resource
    Electronic Resource
    Contraluminal sulfate transport in the proximal tubule of the rat kidney (1985)
    Springer
    Pflügers Archiv 404 (1985), S. 311-318 
    Details
    ISSN: 1432-2013
    Keywords: Epithelial transport ; Contraluminal cell membrane
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract In order to evaluate the specificity for the contraluminal sulfate transport system the inhibitory potency of phenol- and sulfonphthaleins, of sulfamoyl-compounds (diuretics) as well as diphenylamine-2-carboxylates (Cl− channel blockers) on the35SO 4 2− influx from the interstitium into cortical tubular cells in situ has been determined. The following was found: 1) Phenolsulfonphthalein (phenol-red) inhibited with an app.K i-value of 1.7 mmol/l, while analogs which had additional Br-atoms in position 3 and/or 5, i.e. bromphenol-blue, bromcresol-purple and bromcresol-green, inhibited with an apparentK i of 0.1 and 0.5 mmol/l respectively. 2) Phenolphthalein and tetrabromphenolphthalein did not inhibit, while the disulfonate dyes bromsulfalein, fuchsin acid and indigocarmine inhibited with aK i between ≈1 and 3 mmol/l. The highest inhibitory potency in this class of compounds was seen with orange G (app.K i 0.07 mmol/l). The monosulfonate dyes tested, fluoresceinsulfonate and orange I inhibited moderately with an app.K i of ≈5 mmol/l. 3) The 3-sulfamoyl compounds inhibited to a varying degree, when they had a neighbouring −NH-group (furylmethylamino-group), i.e. in position 6 to the COOH or SO3H-group, or when they had a phenoxy-group in position 4. 4) 4-sulfamoylbenzoate and the related compounds probenecid, acetazolamide and hydrochlorothiazide inhibited with an app.K i between 4 and 7 mmol/l. 5) All diphenylamine-2-carboxylate analogs inhibited with an app.K i between 3 and 5 mmol/l, even when the −NH-group was replaced by an =O-group or the benzene ring was replaced by a pyrimidine ring, but not when it was replaced by a thiophen ring. In contrast, 4-phenylaminepyridine-3-sulfonate was ineffective, while diphenylamine-2-amino sulfonate exerted the highest inhibition of this group with an app.K i of 1.4 mmol/l. When, however, the aminosulfonate group was replaced by a methylsulfonamide, the inhibitory potency disappeared. The data can be explained by inhibitory patterns found in previous papers for disulfonates [29], sulfonates with a hydrophobic moiety [28] or neighbouring OH-group [28, 29], carboxylates with a neighbouring −NH- or OH-group in position 2- and an electron-attracting group in position 5 [30].
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF00585341
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  • 8
    Electronic Resource
    Electronic Resource
    Specificity and sodium dependence of the active sugar tansport in the proximal convolution of the rat kidney (1974)
    Springer
    Pflügers Archiv 351 (1974), S. 35-48 
    Details
    ISSN: 1432-2013
    Keywords: Hexose Transport ; Sodium Cotransport ; Kidney Tubules ; Sugar Specificity ; Kidney Micropuncture
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Summary With the technique of stop flow microperfusion with simultaneous capillary perfusion, the zero net flux transtubular concentration difference (Δc) of labelled sugars was measured. The following sequence of Δc values, which are a measure for the active transtubular transport rate, were evaluated:d-glucose ≅β methyl-d-glycoside 〉α-methyl-d-glycoside 〉d-galactose 〉3-O-methyl-glucose 〉d-allose. When 10−4 M phlorrhizin was given in the luminal perfusate the Δc's dropped to zero (±8%). Δc-values in the same range i.e. indicating no active transport, were found for:l-glucose,d-mannose, 2-deoxy-d-glucose,d-fructose,d-glucosamine, 6-deoxy-d-galactose (=d-fucose),d-ribose and the reference polyalcohold-mannitol. Inhibition of thed-galactose δc was achieved by 15 mmol/l of the following sugars: α-methyl-d-glycoside ≅d-glucose ≅ 6-deoxy-d-glucose 〉3-O-methyl-d-glucose an no significant inhibition byd-xylose andd-mannose. Against Δc of α-methyl-d-glucose the following inhibitory potency was observed:d-glucose 〉6-deoxy-d-glucose 〉3-O-methyl-d-glucose ≅d-galactose 〉d-xylose and no inhibition byd-mannose. When the ambient sodium was replaced by choline, the Δc values of all actively transported sugars dropped toward zero. An analysis of the Na+ dependence of the α-methyl-d-glycoside transport revealed that the sodium dependence is of the affinity type i.e. that onlyK m increased with increasing Na+ concentration whileV max remained almost constant. From these data one can conclude: 1. The Crane specificity, i.e. that only the α-position of the OH-group on carbon atom 2 is essential, which was found for the intestinal hexose transport holds for the rat proximal kidney tubule, too. 2. The hexose transport system in the rat works only when Na+-ions are present. The sodium ions augment the affinity of the hexose transport system for the hexoses.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF00603509
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  • 9
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    Electronic Resource
    Contraluminal para-aminohippurate transport in the proximal tubule of the rat kidney (1987)
    Springer
    Pflügers Archiv 409 (1987), S. 547-554 
    Details
    ISSN: 1432-2013
    Keywords: Dicarboxylate transport ; Sulfate transport ; Benzoyl compounds ; Phenoxy compounds ; Valproate
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract In order to study the specificity of the contraluminal para-aminohippurate (PAH) transport system, the inhibitory potency of monocarboxylates on the3H-PAH influx from the interstitium into cortical tubular cells in situ has been determined. The following was found: if a homologous series of fatty acids with increasing chain length is tested, inhibition of contraluminal PAH influx is first seen with valerate (app.K i 1.4 mmol/l), increasing up to nonanoate (app.K i 0.06 mmol/l) and remaining in this range up to duodecanoate, the last compound of this series which is sufficiently water-soluble. Similarly, the inhibitory potency of aromatic monocarboxylates increases with increasing hydrophobicity. If the fatty acids are esterified, their inhibitory potency is lost. If they are transformed to the respective aldehydes their inhibitory potency is preserved at a reduced degree. Introduction of a hydrophobic methyl-, ethyl-, or propyl-group increases the inhibitory potency. A β-, but not an α-oxo-group augments the inhibitory potency of phenylpropionate analogs, an OH group diminishes it, and a NH2 group abolishes it. Among phenyl-fatty acids an increase in affinity is observed from phenyl- 〈 benzoylamine-〈 phenoxy- 〈 benzoyl-acetate and-propionate. All monocarboxylate compounds, so far tested, do not inhibit contraluminal sulfate and Na+/succinate influx. The data indicate that the PAH transporter interacts with monocarboxylates and also with aldehydes which have a hydrophobic moiety. An additional oxo-group facilitates the interaction. Thus, the benzoyl compounds show the highest affinity observed.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF00584652
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  • 10
    Electronic Resource
    Electronic Resource
    Sodium dependence of the amino acid transport in the proximal convolution of the rat kidney (1974)
    Springer
    Pflügers Archiv 351 (1974), S. 49-60 
    Details
    ISSN: 1432-2013
    Keywords: Amino Acid Transport ; Sodium Cotransport ; Kidney Tubules ; Kidney Micropuncture
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Summary With the technique of stop flow microperfusion with simultaneous capillary microperfusion the zero net flux transtubular concentration differences (Δc) of labelled amino acids which are equivalent to their active transport rates were measured. Alll-amino acids tested (phenylalanine, histidine, aminobicycloheptane-carboxylic acid, aminoisobutyric acid; lysine, ornithine, arginine; aspartic acid; proline and glycine) showed a considerable Δc, i.e. active transport rate. When, however, the ambient sodium was replaced by choline the Δc values dropped to zero. An analysis of the Na+ dependence of the ornithine transport revealed that the sodium-dependence is of the mixed type, i.e. thatK m decreased andV max increased with increasing Na+ concentration to the same extent. In contrast to other biological systems no mutual interaction between the Na+-dependentd-glucose andl-histidine transport could be observed. Incidental to these studies it was observed that the active transport rate ofd-histidine was in the range of 40% of that of thel-isomer while ford-phenylalanine it was only in the range of 10% of the active transport of thel-isomer. Furthermore it was found that thel-aspartic acid transport was already saturated at a luminall-aspartic acid concentration of 0.05 mmol/l while that ofl-phenylalanine was not saturated even at a luminal concentration of 9 mmol/l.
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    URL: http://dx.doi.org/10.1007/BF00603510
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