Your search keyword '"Charman, S."' showing total 5 results

1. Lymphatic absorption is a significant contributor to the subcutaneous bioavailability of insulin in a sheep model.

Author

Charman SA, McLennan DN, Edwards GA, and Porter CJ

Subjects

Absorption, Animals, Area Under Curve, Biological Availability, Enzyme-Linked Immunosorbent Assay, Hypoglycemic Agents administration & dosage, Injections, Intravenous, Injections, Subcutaneous, Insulin administration & dosage, Lymph metabolism, Reproducibility of Results, Sheep, Hypoglycemic Agents pharmacokinetics, Insulin pharmacokinetics, Lymphatic System metabolism

Abstract

Purpose: This study was conducted to explore the role of the peripheral lymphatics in insulin absorption following subcutaneous (SC) administration using a sheep model that allows continuous collection of peripheral lymph and simultaneous assessment of systemic bioavailability., Methods: In a parallel group design, soluble human insulin (0.5 IU/kg) was administered by bolus SC injection into the interdigital space of the hind leg of non-cannulated control sheep, and sheep in which the efferent popliteal lymph duct was cannulated. A separate group received a bolus IV injection (0.15 IU/kg). Blood was sampled from all animals, and lymph was collected continuously over 12 h postdosing. Samples were assayed for insulin by ELISA., Results: The SC bioavailability of insulin in control sheep was 31.5+/-3.2%, which was significantly higher than when the peripheral lymph was continuously collected (18.4+/-1.7%). In the lymph-cannulated animals, 17.3+/-1.0% of the dose was collected in peripheral lymph., Conclusions: Based on the direct measurement of insulin in regional lymph and on the decrease in the systemic bioavailability when regional lymph was continuously collected, the results demonstrate that lymphatic absorption contributed significantly to the overall insulin bioavailability following SC administration to sheep.

Published

2001

2. Validation of a peptide map for recombinant porcine growth hormone and application to stability assessment.

Author

Charman SA, McCrossin LE, and Charman WN

Subjects

Amino Acid Sequence, Animals, Chromatography, High Pressure Liquid, Growth Hormone metabolism, Mass Spectrometry, Molecular Sequence Data, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Reproducibility of Results, Swine, Trypsin metabolism, Growth Hormone chemistry, Peptide Mapping

Abstract

A reverse-phase HPLC method for the analysis of tryptic digests of recombinant porcine growth hormone (pGH) has been developed and validated. Digestion was performed at 4 degrees C for a 20-hr period with TPCK-treated trypsin at a 1:20 (w/w) trypsin:pGH ratio. Gradient elution HPLC, using an Aquapore RP300 C8 column, was incorporated for separation of the digestion products and peak identification was carried out by mass spectrometry (MS). The digestion procedure and subsequent chromatography were linear in the initial concentration range of 4.55-45.46 microM (100 to 1000 micrograms/mL) pGH. The variability in the fragment retention times was low and the normalized peak area variability was less than 5% for all but three of the fragments. The utility of the trypsin digestion and chromatography procedures has been demonstrated by assessing chemical changes in pGH induced by incubation at elevated pH. Upon incubation of pGH in 0.2 M Tris buffer at pH 9 (ionic strength adjusted to 0.5 with NaCl) and 37 degrees C over a period of 400 hr, significant degradation in the regions corresponding to the digestion fragments T23-T25 (residues 181-182 linked by a disulfide bond to residues 184-191), T9 (residues 96-108), and T5-T18 (residues 43-64 linked by a disulfide bond to residues 158-166) was observed. The disappearance of the peaks corresponding to fragments T23-T25 and T9 both displayed apparent first-order degradation kinetics over the time period investigated with half-lives of 131 and 154 hr, respectively.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1993

3. Techniques for assessing the effects of pharmaceutical excipients on the aggregation of porcine growth hormone.

Author

Charman SA, Mason KL, and Charman WN

Subjects

Animals, Buffers, Cellulose analogs & derivatives, Chromatography, Gel, Electrophoresis, Polyacrylamide Gel, Growth Hormone drug effects, Guanidines chemistry, Hot Temperature, Isoelectric Focusing, Polysorbates, Protein Denaturation, Solubility, Solutions, Sorbitol, Spectrophotometry, Ultraviolet, Swine, Temperature, Excipients pharmacology, Growth Hormone chemistry

Abstract

Three denaturing techniques have been evaluated for their ability to induce irreversible aggregation and precipitation of recombinant porcine growth hormone (pGH). The denaturing stimuli included thermal denaturation, interfacial denaturation through the introduction of a high air/water interface by vortex agitation, and a guanidine (Gdn) HCl technique which involved rapid dilution of a partially unfolded state of pGH to nondenaturing conditions. Soluble and insoluble pGH fractions were evaluated for the presence of covalently modified species and soluble aggregates by size exclusion chromatography (SEC), sodium dodecyl sulfate-polyacrylamide gel electrophoresis (SDS-PAGE), and isoelectric focusing (IEF). In each of the three denaturation methods, precipitation was found to be irreversible, as the precipitated pellet could not be solubilized upon resuspending in buffer. The soluble pGH fractions consisted of only monomeric material and the insoluble protein pellet could be completely solubilized with Gdn HCl or SDS. There was no evidence of detectable covalent modifications in the precipitated protein pellet following any of the three denaturation techniques. Three excipients, Tween 20, hydroxypropyl-beta-cyclodextrin (HPCD), and sorbitol were evaluated for their stabilizing ability using each of the three denaturation methods and the degree of stabilization was found to be dependent upon the denaturing stimulus incorporated. Tween 20 was found to be highly effective in preventing pGH precipitation using the interfacial and Gdn techniques and was moderately effective using the thermal denaturation method. Inclusion of HPCD in the sample buffer significantly reduced precipitation using the thermal and interfacial methods but was ineffective in the Gdn technique.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1993

4. Analysis of pilocarpine and its degradation products by micellar electrokinetic capillary chromatography.

Author

Charman WN, Humberstone AJ, and Charman SA

Subjects

Drug Stability, Micelles, Ophthalmic Solutions chemistry, Pilocarpine chemistry, Reproducibility of Results, Sodium Dodecyl Sulfate, Chromatography methods, Electrophoresis methods, Pilocarpine analysis

Published

1992

5. Self-emulsifying drug delivery systems: formulation and biopharmaceutic evaluation of an investigational lipophilic compound.

Author

Charman SA, Charman WN, Rogge MC, Wilson TD, Dutko FJ, and Pouton CW

Subjects

Administration, Oral, Animals, Dogs, Drug Evaluation, Preclinical, Drugs, Investigational administration & dosage, Excipients, Injections, Intravenous, Isoxazoles administration & dosage, Male, Particle Size, Polyethylene Glycols administration & dosage, Postural Balance physiology, Capsules, Drug Delivery Systems, Drugs, Investigational pharmacokinetics, Gelatin, Isoxazoles pharmacokinetics, Lipids chemistry, Polyethylene Glycols pharmacokinetics

Abstract

Self-emulsifying drug delivery systems (SEDDSs) represent a possible alternative to traditional oral formulations of lipophilic compounds. In the present study, a lipophilic compound, WIN 54954, was formulated in a medium chain triglyceride oil/nonionic surfactant mixture which exhibited self-emulsification under conditions of gentle agitation in an aqueous medium. The efficiency of emulsification was studied using a laser diffraction sizer to determine particle size distributions of the resultant emulsions. An optimized formulation which consisted of 25% (w/w) surfactant, 40% (w/w) oil, and 35% (w/w) WIN 54954 emulsified rapidly with gentle agitation in 0.1 N HCl (37 degrees C), producing dispersions with mean droplet diameters of less than 3 microns. The self-emulsifying preparation was compared to a polyethylene glycol 600 (PEG 600) solution formulation by administering each as prefilled soft gelatin capsules to fasted beagle dogs in a parallel crossover study. Pharmacokinetic parameters were determined and the absolute bioavailability of the drug was calculated by comparison to an i.v. injection. The SEDDS improved the reproducibility of the plasma profile in terms of the maximum plasma concentration (Cmax) and the time to reach the maximum concentration (tmax). There was no significant difference in the absolute bioavailability of WIN 54954 from either the SEDDS or the PEG formulations.

Published

1992