Your search keyword '"Degen PH"' showing total 3 results

1. Correlated nerve conduction, somatosensory evoked potential and neuropathological studies in clioquinol and 2,5-hexanedione neurotoxicity in the baboon.

Author

Thomas PK, Bradley DJ, Bradley WA, Degen PH, Krinke G, Muddle J, Schaumburg HH, Skelton-Stroud PN, Thomann P, and Tzebelikos E

Subjects

Administration, Oral, Animals, Axons drug effects, Cerebellum drug effects, Dose-Response Relationship, Drug, Female, Male, Motor Neurons drug effects, Myelin Sheath drug effects, Optic Nerve drug effects, Papio, Peripheral Nerves drug effects, Sensation drug effects, Spinal Cord drug effects, Clioquinol toxicity, Evoked Potentials, Somatosensory drug effects, Hexanones toxicity, Hydroxyquinolines toxicity, Ketones toxicity, Nervous System drug effects, Neural Conduction drug effects

Abstract

Observations have been made on 10 baboons receiving a high-dose regimen of clioquinol administered orally, 6 receiving a low-dose regimen and 6 treated with 2,5-hexanedione. The results were compared with those obtained from 10 control animals. Motor and sensory nerve conduction velocity was markedly reduced in the hexanedione-treated animals but only very minor abnormalities were detected in the clioquinol-treated baboons. Cervical and Rolandic somatosensory evoked potentials to lower and upper limb stimulation were delayed in both the high-dose clioquinol-treated and the hexanedione-treated animals, particularly in the latter. Histopathological studies in the low-dose clioquinol-treated group showed no abnormalities. In the high-dose group; axonal degeneration was confined to the spinal cord, cerebellar vermis and optic tract. It was most marked in the rostral portions of the dorsal spinal columns and the caudal parts of the direct and crossed corticospinal tracts. Occasional dorsal column fibres had degenerated back to the root entry zone in the cord. The distribution was that of a selective central distal axonopathy. There appeared to be no correlation with estimated blood levels of unaltered clioquinol. In hexanedione-treated animals there was also degeneration in the distal optic tracts and peripheral nerves in a pattern of central-peripheral distal axonopathy.

Published

1984

2. Percutaneous absorption of clioquinol (Vioform).

Author

Degen PH, Moppert J, Schmid K, and Weirich EG

Subjects

Administration, Oral, Administration, Topical, Adult, Clioquinol administration & dosage, Clioquinol urine, Humans, Middle Aged, Ointments, Clioquinol metabolism, Skin Absorption

Abstract

The percutaneous absorption of clioquinol from three different preparations for skin treatment (Vioform cream, Locacorten-Vioform cream and Vioform-Hydrocortisone cream) was evaluated. After topical dosages corresponding to 30 mg clioquinol, concentrations in the blood were below the detection limit of the analytical procedure, i.e., smaller than 0.02 micrograms/ml; therefore the percutaneous absorption was evaluated by measuring cumulative urinary excretion of clioquinol and was compared to that found after an equivalent oral dose. The study was carried out in 4 healthy volunteers. The topical preparations were applied under occlusive dressings. Following epicutaneous application of the three topicals in quantities containing 30 mg clioquinol each, the urinary excretion of the drug was between 1.2 and 3.6% of the applied dose. When the same dose of clioquinol was administered orally to two volunteers, 52.4 and 92.9% of the dose was excreted in the urine. Taking the urinary elimination as the minimal amount of drug absorbed, the extent of percutaneous absorption from the three dermatological preparations amounted to 1.2-3.6% of the applied dose. There was no difference in the pattern of urinary excretion products among the three topicals and the oral formulation. The bulk of clioquinol was excreted as glucuronide (mean: 96 +/- 3%) and only a small fraction was excreted as sulfate (mean: 3.8 +/- 3%). A small amount of free clioquinol (1.1%) was measured in 1 subject only after the oral dose.

Published

1979

3. The determination of clioquinol in biological materials by extractive alkylation and gas-liquid chromatography.

Author

Degen PH, Schneider W, Vuillard P, Geiger UP, and Riess W

Subjects

Adipose Tissue analysis, Alkylation, Animals, Chromatography, Liquid, Clioquinol blood, Clioquinol urine, Humans, Methods, Methylation, Swine, Chromatography, Gas, Clioquinol analysis

Abstract

Clioquinol, or 5-chloro-7-iodo-8-hydroxyquinoline (Vioform), and the internal standard, 5,7-dichloro-8-hydroxyquinoline are extracted from biological material in the form of their tetrahexylammonium salts into dichloromethane, where, in the presence of a methylating agent, both clioquinol and the standard are spontaneously transformed into their O-methyl derivatives. These derivatives can be purified by base-specific extraction and subsequently determined by gas chromatography; concentrations down to 10 ng per sample may be assayed. The method is compared with a previously reported procedure based on the O-acetyl derivatives.

Published

1976