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Extensive and saturable accumulation of paclitaxel by the human platelet (1995)

Wild, Mark D. ; Walle, U. Kristina ; Walle, T.

Springer

Cancer chemotherapy and pharmacology 36 (1995), S. 41-44

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ISSN: 1432-0843

Keywords: Key words Taxol ; Paclitaxel ; Platelets

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Little is known about the cellular distribution of paclitaxel in humans. In the present study we examined the distribution of [3H]-paclitaxel in human blood. When 1 μM paclitaxel was incubated with fresh blood at 37°C, the platelet/plasma concentration ratio was 240±17 (mean±SEM), whereas the red blood cell (RBC)/plasma concentration ratio was only 0.59±0.05. In kinetics experiments using platelet-rich plasma, we observed that the platelet accumulation of paclitaxel was highly temperature- and concentration-dependent. Scatchard analysis of the 37° C uptake data demonstrated a dissociation constant (K app) of 0.80± 0.10 μM and a maximal binding capacity of 672± 102 pmol/109 platelets. It is proposed that the platelet accumulation of paclitaxel reflects binding to microtubules and may serve as a useful model for binding to less accessible cellular sites.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00685730

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Extensive and saturable accumulation of paclitaxel by the human platelet (1995)

Wild, Mark D. ; Walle, U. Kristina ; Walle, Thomas

Springer

Cancer chemotherapy and pharmacology 36 (1995), S. 41-44

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ISSN: 1432-0843

Keywords: Taxol ; Paclitaxel ; Platelets

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Little is known about the cellular distribution of paclitaxel in humans. In the present study we examined the distribution of [3H]-paclitaxel in human blood. When 1 μM paclitaxel was incubated with fresh blood at 37°C, the platelet/plasma concentration ratio was 240±17 (mean±SEM), whereas the red blood cell (RBC)/plasma concentration ratio was only 0.59±0.05. In kinetics experiments using platelet-rich plasma, we observed that the platelet accumulation of paclitaxel was highly temperature- and concentration-dependent. Scatchard analysis of the 37°C uptake data demonstrated a dissociation constant (K app) of 0.80±0.10 μM and a maximal binding capacity of 672±102 pmol/109 platelets. It is proposed that the platelet accumulation of paclitaxel reflects binding to microtubules and may serve as a useful model for binding to less accessible cellular sites.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00685730

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Induction of UDP-Glucuronosyl-Transferase by the Flavonoids Chrysin and Quercetin in Caco-2 Cells (2000)

Galijatovic, Alema ; Walle, U. Kristina ; Walle, Thomas

Springer

Pharmaceutical research 17 (2000), S. 21-26

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ISSN: 1573-904X

Keywords: flavonoids ; chrysin ; quercetin ; induction ; glucuronidation ; UDP-glucuronosyltransferase ; Caco-2 cells

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract Purpose. Dietary flavonoids have been reported to be potent inhibitorsof drug metabolizing enzymes. In the present study we examined theinducing effect of three of these compounds, chrysin, quercetin andgenistein, on UDP-glucuronosyltransferase (UGT) in the humanintestinal cell line Caco-2. Methods. The induction of UGT by flavonoid pretreatment was studiedboth in the intact cells and cell homogenates, measured as theglucuronidation of chrysin, and by immunoblot analysis of the UGT 1A protein. Results. Exposure of Caco-2 cells to 50 μM chrysin resulted in a3.8-fold increase in chrysin glucuronidation in intact cells (p 〈 0.0001)with a 38% decrease in sulfation (p 〈 0.01). In the cell homogenatethe induction was much larger, 14-fold. The induction was slow todevelop with maximum induction after 3–4 days. Interestingly, theisoflavonoid genistein was without effect. Immunoblot analysis ofCaco-2 cell microsomes with a UGT1A subfamily-selective antibodyshowed a markedly increased band at about 59 kDa, consistent withinduction of one or more UGT1A isoforms. A 5-week exposure ofCaco-2 cells to low concentrations (10 μM) of chrysin or quercetinalso showed markedly increased glucuronidation activity. Conclusions. Diet-mediated induction of intestinal UGT may beimportant for the bioavailability of carcinogens and other toxicchemicals as well as therapeutic drugs.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1007506222436

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Stereochemistry of tissue distribution of racemic propranolol in the dog (1989)

Walle, U. Kristina ; Thibodeaux, Harold ; Privitera, Philip J. ; [et al.]

New York, NY [u.a.] : Wiley-Blackwell

Chirality 1 (1989), S. 192-196

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ISSN: 0899-0042

Keywords: propranolol enantiomers ; enantiomers ; propranolol ; β-receptor-blocking drugs ; Chemistry ; Organic Chemistry

Source: Wiley InterScience Backfile Collection 1832-2000

Topics: Chemistry and Pharmacology

Notes: Only limited information is available on the stereochemistry of the in vivo distribution of β-receptor-blocking drugs. In this study we determined the levels of the propranolol enantiomers in plasma, cerebrospinal fluid (CSF) and central nervous system (CNS), and peripheral tissues in the dog following an intravenous dose of a deuterium-labeled pseudoracemate. The appearance of the propranolol enantiomers in the CSF was rapid and nonstereoselective, with maximum concentrations reached at 15 min after dosing. The levels of the enantiomers in both CSF and plasma then declined in a parallel biphasic fashion, with a terminal t1/2 of about 125 min. Except for an early high CSF/plasma concentration ratio of 0.35, the CSF propranolol levels corresponded to the unbound concentration in plasma, CSF/plasma 0.20. All areas of the brain showed a similar uptake of propranolol, with a tissue concentration exceeding that in plasma about 10-fold during the terminal phase of elimination. The uptake of propranolol by peripheral tissues varied widely, ranging from a 50-fold accumulation by the lungs compared to plasma to no accumulation by adipose tissue. However, as for the CSF, there was no evidence of stereoselective uptake of propranolol by any CNS or peripheral tissue except for the liver. A significantly higher level of (+)- vs. (-)-propranolol in liver tissue presumably was a reflection of stereoselective hepatic metabolism of (-)-propranolol by this tissue. The slight stereoselectivity in plasma binding of propranolol known to exist in the dog had no significant influence on tissue or CSF distribution.

Additional Material: 2 Ill.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1002/chir.530010303

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Stereoselective sulfation of terbutaline by the rat liver cytosol: evaluation of experimental approaches (1989)

Walle, U. Kristina ; Walle, Thomas

New York, NY [u.a.] : Wiley-Blackwell

Chirality 1 (1989), S. 121-126

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ISSN: 0899-0042

Keywords: stereoselective metabolism ; sulfate conjugation ; in vitro sulfation ; sympathomimetic amines ; chiral separation ; Chemistry ; Organic Chemistry

Source: Wiley InterScience Backfile Collection 1832-2000

Topics: Chemistry and Pharmacology

Notes: Little is known about the stereochemistry of sulfation of chiral phenolic drugs. In this study we examined several in vitro approaches to this question, using (+)-, (-)-, or (±)-terbutaline as the substrate and the rat liver cytosol as the phenolsulfotransferase enzyme source. The cosubstrate PAPS was either generated by the cytosol from inorganic sulfate and ATP or added to the cytosol. The intact sulfate conjugates formed were determined by HPLC. Using the PAPS generating system, which is best suited for the production of relatively large quantities of sulfate conjugates, with the individual enantiomers as substrates, (+)-terbutaline was conjugated to a much greater extent than (-)-terbutaline; the (+)/(-)-enantiomer ratio was 7.3 ± 0.3 (mean ± SE). When (±)-terbutaline was the substrate and chiral derivatization was employed to separate the sulfate enantiomers formed, a similar (+)/(-)-enantiomer ratio of 7.9 ± 0.2 was obtained. With PAP35S added to the cytosol, an approach best suited for kinetic studies, the substrate concentration dependence of sulfation could be determined. The Km app for this reaction was identical for (+)- and (-)-terbutaline. However, the Vmax app was 8.1 ± 0.4 times greater for (+)-terbutaline. This study for the first time shows enantioselectivity in sulfation of a chiral phenolic drug. The experimental approaches used should be valuable for human studies of stereoselectiven sulfation of terbutaline and other chiral drugs.

Additional Material: 4 Ill.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1002/chir.530010205

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Influence of food on the intravenous and oral dose kinetics of propranolol in the dog (1985)

Bai, Stephen A. ; Walle, U. Kristina ; Walle, Thomas

Springer

Journal of pharmacokinetics and pharmacodynamics 13 (1985), S. 229-241

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ISSN: 1573-8744

Keywords: food effects ; propranolol ; kinetics ; dogs ; oral and intravenous doses

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract The intravenous and oral dose kinetics of propranolol were studied in the dog both in a fasted state and immediately after a meal consisting of 100 g of cooked beef liver. Fifty ΜCi of3H-propranolol was administered intravenously simultaneously with a 40-mg oral dose of unlabeled propranolol. Plasma3H-propranolol was measured by specific extraction and liquid scintillation spectrometry, and unlabeled plasma propranolol was determined by gas chromatography-mass spectrometry. Feeding significantly reduced (25%) the elimination half-life and increased (52%) the systemic clearance of intravenous propranolol. The increase in the systemic clearance of propranolol after feeding was mostly due to an increase (60%) in apparent hepatic blood flow, which appeared to remain elevated for 5–7 hr. The meal had no influence on the apparent volume of distribution or plasma binding. Feeding did not affect the area under the concentration-time curve of oral propranolol, but significantly delayed the rate of oral propranolol absorption, shifting the time to reach peak plasma levels from 60 to 158 min. The results of this study suggest that feeding alters the disposition of propranolol in the dog by producing a sustained increase in hepatic blood flow.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01065654

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Propranolol, alprenolol and oxprenolol metabolism in the dog. Identification of N-Methylated metabolites (1981)

Walle, U. Kristina ; Wilson, Michael J. ; Walle, Thomas

Chichester : Wiley-Blackwell

Biological Mass Spectrometry 8 (1981), S. 78-84

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ISSN: 1052-9306

Keywords: Chemistry ; Analytical Chemistry and Spectroscopy

Source: Wiley InterScience Backfile Collection 1832-2000

Topics: Chemistry and Pharmacology

Notes: The metabolism of propranolol, alprenolol and oxprenolol was studied in the dog and rat; propranolol in five additional species, including man. Basic, phenolic and neutral metabolites were extracted from urine at pH 9.6 after enzymatic hydrolysis. Separation and identification of parent drug and seven metabolites each for propranolol, alprenolol and oxprenolol in the dog were accomplished by gas chromatography mass spectrometry as the trifluoroacetyl derivatives. A very uniform and predictable fragmentation pattern was observed for all 24 compounds. Seven new metabolites were identified. The metabolism of all three drugs was qualitatively the same, including N-dealkylation followed by N-methylation or deamination of the primary amines. The parent drugs as well as all of their sidechain metabolism products were also partially ring hydroxylated. N-Methylation was only found in the dog and is a minor metabolic pathway. The stereochemical composition of N-methyldesisopropylpropranolol and its immediate precursor N-desisopropylpropranolol showed a marked enrichment of the (+)-isomer.

Additional Material: 6 Ill.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1002/bms.1200080206

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