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2. Enantiospecific antitrypanosomal in vitro activity of eflornithine.

Author

Mikael Boberg, Monica Cal, Marcel Kaiser, Rasmus Jansson-Löfmark, Pascal Mäser, and Michael Ashton

Subjects
Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270
Abstract

The polyamine synthesis inhibitor eflornithine is a recommended treatment for the neglected tropical disease Gambian human African trypanosomiasis in late stage. This parasitic disease, transmitted by the tsetse fly, is lethal unless treated. Eflornithine is administered by repeated intravenous infusions as a racemic mixture of L-eflornithine and D-eflornithine. The study compared the in vitro antitrypanosomal activity of the two enantiomers with the racemic mixture against three Trypanosoma brucei gambiense strains. Antitrypanosomal in vitro activity at varying drug concentrations was analysed by non-linear mixed effects modelling. For all three strains, L-eflornithine was more potent than D-eflornithine. Estimated 50% inhibitory concentrations of the three strains combined were 9.1 μM (95% confidence interval [8.1; 10]), 5.5 μM [4.5; 6.6], and 50 μM [42; 57] for racemic eflornithine, L-eflornithine and D-eflornithine, respectively. The higher in vitro potency of L-eflornithine warrants further studies to assess its potential for improving the treatment of late-stage Gambian human African trypanosomiasis.

Published
2021
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3. Population pharmacodynamic modeling of eflornithine-based treatments against late-stage gambiense human African trypanosomiasis and efficacy predictions of l-eflornithine-based therapy

Author

Carl Amilon, Mikael Boberg, Joel Tarning, Angela Äbelö, Michael Ashton, and Rasmus Jansson-Löfmark

Subjects
Eflornithine, Trypanosomiasis, African, Trypanosoma brucei gambiense, Animals, Humans, Pharmaceutical Science, Drug Therapy, Combination, Nifurtimox, Trypanocidal Agents
Abstract

Eflornithine is a recommended treatment against late-stage gambiense human African trypanosomiasis, a neglected tropical disease. Standard dosing of eflornithine consists of repeated intravenous infusions of a racemic mixture of L- and D-eflornithine. Data from three clinical studies, (i) eflornithine intravenous monotherapy, (ii) nifurtimox-eflornithine combination therapy, and (iii) eflornithine oral monotherapy, were pooled and analyzed using a time-to-event pharmacodynamic modeling approach, supported by in vitro activity data of the individual enantiomers. Our aim was to assess (i) the efficacy of the eflornithine regimens in a time-to-event analysis and (ii) the feasibility of an L-eflornithine-based therapy integrating clinical and preclinical data. A pharmacodynamic time-to-event model was used to estimate the total dose of eflornithine, associated with 50% reduction in baseline hazard, when administered as monotherapy or in the nifurtimox-eflornithine combination therapy. The estimated total doses were 159, 60 and 291 g for intravenous eflornithine monotherapy, nifurtimox-eflornithine combination therapy and oral eflornithine monotherapy, respectively. Simulations suggested that L-eflornithine achieves a higher predicted median survival, compared to when racemate is administered, as treatment against late-stage gambiense human African trypanosomiasis. Our findings showed that oral L-eflornithine-based monotherapy would not result in adequate efficacy, even at high dose, and warrants further investigations to assess the potential of oral L-eflornithine-based treatment in combination with other treatments such as nifurtimox. An all-oral eflornithine-based regimen would provide easier access to treatment and reduce burden on patients and healthcare systems in gambiense human African trypanosomiasis endemic areas.

Published
2022
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4. Chiral Chromatographic Isolation on Milligram Scale of the Human African Trypanosomiasis Treatment d- and l‑Eflornithine

Author

Michael Ashton, Hanna Leek, Mikael Boberg, Anna C. Jonson, and Rasmus Jansson-Löfmark

Subjects
Chromatography, General Chemical Engineering, General Chemistry, medicine.disease, High-performance liquid chromatography, Article, chemistry.chemical_compound, Chemistry, chemistry, Eflornithine, medicine, Supercritical fluid chromatography, Racemic mixture, African trypanosomiasis, Enantiomer, Derivatization, Nifurtimox, QD1-999, medicine.drug
Abstract

Eflornithine is a recommended treatment against the otherwise fatal parasitic disease late stage human African trypanosomiasis (HAT), also known as Gambian sleeping sickness. It is administered repeatedly as a racemic mixture intravenously (IV) together with oral nifurtimox. Racemic eflornithine has been investigated in clinical trials for oral dosing. However, due to low systemic exposures at a maximum tolerated oral dose, the drug is continued to be administered IV. The eflornithine enantiomers, d- and l-eflornithine, have different affinities to the target enzyme ornithine decarboxylase, suggesting that the pharmacodynamics of the enantiomers may differ. The aim of this study was to develop a method for isolation of d- and l-eflornithine from a racemic mixture. Several chiral stationary phases (CSPs) were evaluated for enantioselectivity using supercritical fluid chromatography (SFC) or high-performance liquid chromatography (HPLC). None of the tested CSPs rendered separation of the enantiomers in SFC mode. Separation of the enantiomers with SFC on the CSP Chiralpak IG was only achieved on an analytical scale after derivatization with ortho-phthalaldehyde (OPA). This was the first reported enantioselective SFC method for an eflornithine derivate. However, due to poor stability, the eflornithine-OPA derivates degraded and no chemically pure enantiomers were obtained. The CSP that showed enantioselectivity in HPLC mode was Chirobiotic R, which resulted in a successful isolation on a semipreparative milligram scale. The isolated eflornithine enantiomers will be tested in nonclinical in vitro and in vivo studies to support and assess the feasibility of a future clinical program with an oral HAT treatment.

Published
2020

6. Enantiospecific antitrypanosomal in vitro activity of eflornithine

Author

Monica Cal, Marcel Kaiser, Rasmus Jansson-Löfmark, Pascal Mäser, Mikael Boberg, and Michael Ashton

Subjects
0301 basic medicine, Physiology, Trypanosoma brucei gambiense, RC955-962, Pharmacology, Toxicology, Pathology and Laboratory Medicine, Nervous System, Isomers, 0302 clinical medicine, Medical Conditions, Stereochemistry, Arctic medicine. Tropical medicine, Zoonoses, Medicine and Health Sciences, African trypanosomiasis, Stereoisomers, Cerebrospinal Fluid, Protozoans, Cytotoxicity Assay, biology, Chemistry, Eukaryota, Trypanocidal Agents, Body Fluids, Infectious Diseases, Physical Sciences, Public aspects of medicine, RA1-1270, Anatomy, medicine.drug, Research Article, Neglected Tropical Diseases, Trypanosoma, Eflornithine, 030231 tropical medicine, 030106 microbiology, African Trypanosomiasis, 03 medical and health sciences, Isomerism, Trypanosomiasis, medicine, Parasitic Diseases, Potency, Humans, Protozoan Infections, Public Health, Environmental and Occupational Health, Chemical Compounds, Organisms, Biology and Life Sciences, medicine.disease, biology.organism_classification, Tropical Diseases, In vitro, Parasitic Protozoans, Enantiomers, Racemic mixture, Enantiomer
Abstract

The polyamine synthesis inhibitor eflornithine is a recommended treatment for the neglected tropical disease Gambian human African trypanosomiasis in late stage. This parasitic disease, transmitted by the tsetse fly, is lethal unless treated. Eflornithine is administered by repeated intravenous infusions as a racemic mixture of L-eflornithine and D-eflornithine. The study compared the in vitro antitrypanosomal activity of the two enantiomers with the racemic mixture against three Trypanosoma brucei gambiense strains. Antitrypanosomal in vitro activity at varying drug concentrations was analysed by non-linear mixed effects modelling. For all three strains, L-eflornithine was more potent than D-eflornithine. Estimated 50% inhibitory concentrations of the three strains combined were 9.1 μM (95% confidence interval [8.1; 10]), 5.5 μM [4.5; 6.6], and 50 μM [42; 57] for racemic eflornithine, L-eflornithine and D-eflornithine, respectively. The higher in vitro potency of L-eflornithine warrants further studies to assess its potential for improving the treatment of late-stage Gambian human African trypanosomiasis., Author summary The neglected tropical disease human African trypanosomiasis is lethal unless treated. One of the treatments for the late stage–i.e. when parasites have invaded the central nervous system–of Gambian human African trypanosomiasis is the drug eflornithine, which is dosed as 50:50 racemic mixture of the two enantiomers L-eflornithine and D-eflornithine. This study showed that L-eflornithine was better than D-eflornithine at inhibiting the growth of parasites in vitro. The 50% inhibitory concentration for L-eflornithine was 5.5 μM in comparison to 50 μM for D-eflornithine. This higher in vitro potency for L-eflornithine warrants further studies to assess its potential as an improved treatment for late-stage Gambian human African trypanosomiasis.

Published
2021
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7. Age-Dependent Absolute Abundance of Hepatic Carboxylesterases (CES1 and CES2) by LC-MS/MS Proteomics: Application to PBPK Modeling of Oseltamivir In Vivo Pharmacokinetics in Infants

Author

Bhagwat Prasad, Mikael Boberg, Robin E. Pearce, Aanchal Mehrotra, J. Steven Leeder, Marc Vrana, Andrea Gaedigk, and Deepak Kumar Bhatt

Subjects
Adult, Proteomics, 0301 basic medicine, Aging, Pharmaceutical Science, In Vitro Techniques, Pharmacology, Biology, Tandem mass spectrometry, Models, Biological, 030226 pharmacology & pharmacy, Carboxylesterase, 03 medical and health sciences, Cytosol, Oseltamivir, 0302 clinical medicine, Pharmacokinetics, Tandem Mass Spectrometry, In vivo, Humans, Area under the curve, Infant, Articles, 030104 developmental biology, Liver, Biochemistry, Microsomes, Liver, Microsome, Carboxylic Ester Hydrolases, Chromatography, Liquid
Abstract

The age-dependent absolute protein abundance of carboxylesterase (CES) 1 and CES2 in human liver was investigated and applied to predict infant pharmacokinetics (PK) of oseltamivir. The CES absolute protein abundance was determined by liquid chromatography-tandem mass spectrometry proteomics in human liver microsomal and cytosolic fractions prepared from tissue samples obtained from 136 pediatric donors and 35 adult donors. Two surrogate peptides per protein were selected for the quantification of CES1 and CES2 protein abundance. Purified CES1 and CES2 protein standards were used as calibrators, and the heavy labeled peptides were used as the internal standards. In hepatic microsomes, CES1 and CES2 abundance (in picomoles per milligram total protein) increased approximately 5-fold (315.2 vs. 1664.4) and approximately 3-fold (59.8 vs. 174.1) from neonates to adults, respectively. CES1 protein abundance in liver cytosol also showed age-dependent maturation. Oseltamivir carboxylase activity was correlated with protein abundance in pediatric and adult liver microsomes. The protein abundance data were then used to model in vivo PK of oseltamivir in infants using pediatric physiologically based PK modeling and incorporating the protein abundance–based ontogeny function into the existing pediatric Simcyp model. The predicted pediatric area under the curve, maximal plasma concentration, and time for maximal plasma concentration values were below 2.1-fold of the clinically observed values, respectively.

Published
2016
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8. Characterization of acoustic emission analysis in applications for inhalation device performance assessment

Author

Mats Josefson, Roland Greguletz, Lisa Holmstén, Lars Karlsson, Staffan Folestad, Kyrre Thalberg, and Mikael Boberg

Subjects
Inhalation, Computer science, business.industry, Process analytical technology, Pharmaceutical Science, Dry Powder Inhalers, 02 engineering and technology, Acoustics, Equipment Design, 021001 nanoscience & nanotechnology, 030226 pharmacology & pharmacy, Dry-powder inhaler, Chemometrics, 03 medical and health sciences, 0302 clinical medicine, Acoustic emission, Dry powder, Principal component analysis, Multivariate Analysis, Performance monitoring, Powders, 0210 nano-technology, Process engineering, business
Abstract

Acoustic Emission (AE) measurement technology has gained wide appreciation in material sciences and process monitoring. In inhalation research, AE has been used for adherence indicating applications in clinical studies. Promising results from feasibility studies using AE combined with multivariate data analysis (AE-MVDA) in the analysis of devices for inhalation have prompted a broader study reported in this paper. This work presents the novel application of AE-MVDA for assessment of the combined inhalation device and formulation performance. The purpose is to evaluate the benefits that this technology can provide to inhalation product development programs. The work was carried out using two different dry powder inhaler device model systems while investigating different performance features. The devices were filled with dry powder formulations with both placebo and with active pharmaceutical ingredient (API). The acquired AE data was analyzed using multivariate data analysis tools such as Principal component analysis (PCA) and orthogonal projections to latent structures (OPLS). The AE profiles were indicative for device and formulation performance. Normal and deviating performances were readily picked up in the AE data. Moreover, performance trends between doses withdrawn from the inhalers were also observable. Lastly, differences in the AE profile between the formulations could be detected. The overall conclusion from the AE-MVDA measurement approach evaluation is that it has the potential to add value as a cost-effective, non-invasive quality and performance monitoring technology both in development and in production of inhaled medicines.

Published
2018

9. Age- and Genotype-Dependent Variability in the Protein Abundance and Activity of Six Major Uridine Diphosphate-Glucuronosyltransferases in Human Liver

Author

J. Steven Leeder, Revathi Chapa, Deepak Kumar Bhatt, Andrea Gaedigk, Ulrich Broeckel, Robin E. Pearce, Haeyoung Zhang, Roger Gaedigk, Aanchal Mehrotra, Abdul Basit, Bhagwat Prasad, Mikael Boberg, and Prachi Choudhari

Subjects
UGT1A6, medicine.medical_specialty, UGT1A4, Adolescent, Genotype, Antimetabolites, Biology, Tandem mass spectrometry, Proteomics, digestive system, 030226 pharmacology & pharmacy, Article, 03 medical and health sciences, chemistry.chemical_compound, Young Adult, 0302 clinical medicine, Internal medicine, medicine, Humans, Pharmacology (medical), Glucuronosyltransferase, Child, Pharmacology, Morphine, Age Factors, Infant, Newborn, Infant, Uridine, UGT2B7, Analgesics, Opioid, Enzyme Activation, Uridine diphosphate, Endocrinology, chemistry, 030220 oncology & carcinogenesis, Child, Preschool, Microsome, Microsomes, Liver, Zidovudine
Abstract

The ontogeny of hepatic uridine diphosphate-glucuronosyltransferases (UGTs) was investigated by determining their protein abundance in human liver microsomes isolated from 136 pediatric (0-18 years) and 35 adult (age >18 years) donors using liquid chromatography / tandem mass spectrometry (LC-MS/MS) proteomics. Microsomal protein abundances of UGT1A1, UGT1A4, UGT1A6, UGT1A9, UGT2B7, and UGT2B15 increased by ∼8, 55, 35, 33, 8, and 3-fold from neonates to adults, respectively. The estimated age at which 50% of the adult protein abundance is observed for these UGT isoforms was between 2.6-10.3 years. Measured in vitro activity was generally consistent with the protein data. UGT1A1 protein abundance was associated with multiple single nucleotide polymorphisms exhibiting noticeable ontogeny-genotype interplay. UGT2B15 rs1902023 (*2) was associated with decreased protein activity without any change in protein abundance. Taken together, these data are invaluable to facilitate the prediction of drug disposition in children using physiologically based pharmacokinetic modeling as demonstrated here for zidovudine and morphine.

Published
2017

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