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5 results on '"Ott, J L"'

1. Disposition kinetics and tissue residues of tilmicosin following intravenous, subcutaneous, single and multiple oral dosing in geese (Anser anser domesticus).

Author

Bourdo K, Fadel C, Giorgi M, Šitovs A, Poapolathep A, and Łebkowska-Wieruszewska B

Subjects
Animals, Male, Administration, Oral, Injections, Intravenous veterinary, Half-Life, Injections, Subcutaneous veterinary, Biological Availability, Area Under Curve, Tissue Distribution, Drug Residues pharmacokinetics, Drug Residues analysis, Geese, Tylosin pharmacokinetics, Tylosin analogs & derivatives, Tylosin administration & dosage, Tylosin blood, Anti-Bacterial Agents pharmacokinetics, Anti-Bacterial Agents administration & dosage, Anti-Bacterial Agents blood
Abstract

Tilmicosin (TMC), a semi-synthetic macrolide antibiotic, is widely used in veterinary medicine due to its broad-spectrum, bacteriostatic properties. Frequently administered in various birds species, it is likely used off-label in geese as well. The study sought to investigate TMC's pharmacokinetics, tissue residues, in geese through in vivo experiments. The study involved longitudinal open studies on 15 healthy adult males, with three phases separated by one-month washout periods. Geese were administered TMC through intravenous (IV, 5 mg/kg), subcutaneous (SC, 10 mg/kg), and oral (PO, 25 mg/kg for five consecutive days) routes, with blood samples drawn at specific intervals. Tissue samples were also collected for subsequent analysis at pre-assigned times. TMC in goose plasma was quantified by a fully validated HPLC method. Plasma concentrations were quantified up to 4 hr for the PO and IV routes, and up to 10 hr in the SC route. Significant variations in bioavailability were observed between SC (87%) and PO (4%) routes. The body extraction ratio was low at 0.03, suggesting minimal ability of the liver and kidneys to eliminate TMC. Multiple oral doses showed no plasma accumulation, but tissue data revealed extensive distribution and prolonged residence, up to 120 h, suggesting a sustained therapeutic effect despite the brief plasma half-life. Regarding the multiple PO doses, provisional withdrawal times of 6, 7.5, and 8 days were suggested for the liver, muscles, and kidneys, respectively, according to the MRL set for these matrices in chickens by EMA. In conclusion, while the practical oral administration is discouraged at the population level, SC administration of TMC may be appropriate for geese, albeit impractical for flock therapy., (© 2024 John Wiley & Sons Ltd.)

Published
2024
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2. Engineering of the start condensation domain with improved N-decanoyl catalytic activity for daptomycin biosynthesis.

Author

Fan W, Hu L, Yang Y, Liu P, Feng Y, Gu RX, and Liu Q

Subjects
Bacterial Proteins metabolism, Bacterial Proteins genetics, Bacterial Proteins chemistry, Substrate Specificity, Anti-Bacterial Agents biosynthesis, Anti-Bacterial Agents chemistry, Anti-Bacterial Agents metabolism, Protein Domains, Daptomycin biosynthesis, Daptomycin chemistry, Protein Engineering methods, Molecular Docking Simulation, Molecular Dynamics Simulation
Abstract

Daptomycin, a lipopeptide comprising an N-decanoyl fatty acyl chain and a peptide core, is used clinically as an antimicrobial agent. The start condensation domain (dptC1) is an enzyme that catalyzes the lipoinitiation step of the daptomycin synthesis. In this study, we integrated enzymology, protein engineering, and computer simulation to study the substrate selectivity of the start condensation domain (dptC1) and to screen mutants with improved activity for decanoyl loading. Through molecular docking and computer simulation, the fatty acyl substrate channel and the protein-protein interaction interface of dptC1 are analyzed. Key residues at the protein-protein interface between dptC1 and the acyl carrier were mutated, and a single-point mutant showed more than three-folds improved catalytic efficiency of the target n-decanoyl substrate in comparing with the wild type. Moreover, molecular dynamics simulations suggested that mutants with increased catalytic activity may correlated with a more "open" and contracted substrate binding channel. Our work provides a new perspective for the elucidation of lipopeptide natural products biosynthesis, and also provides new resources to enrich its diversity and optimize the production of important components., (© 2024 Wiley‐VCH GmbH.)

Published
2024
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4. Spintronics : A Primer

Author

Jean-Philippe Ansermet and Jean-Philippe Ansermet

Subjects
Spintronics
Abstract

A sound understanding of magnetism, transport theory, spin relaxation mechanisms, and magnetization dynamics is necessary to engage in spintronics research. In this primer, special effort has been made to give straightforward explanations for these advanced concepts.This book will be a valuable resource for graduate students in spintronics and related fields. Concepts of magnetism such as exchange interaction, spin-orbit coupling, spin canting, and magnetic anisotropy are introduced. Spin-dependent transport is described using both thermodynamics and Boltzmann's equation, including Berry curvature corrections. Spin relaxation phenomenology is accounted for with master equations for quantum spin systems coupled to a bath. Magnetic resonance principles are applied to describe spin waves in ferromagnets, cavity-mode coupling in antiferromagnets, and coherence phenomena relevant to spin qubits applications.Key Features:• A pedagogical approach to foundational concepts in spintronics with simple models that can be calculated to enhance understanding.• Nineteen chapters, each beginning with a historical perspective and ending with an outlook on current research.• 1200 references, ranging from landmark papers to frontline publications.

Published
2024

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