Search results for "reparations"

showing 10 items of 367 documents

Chemistry and biology of new marine alkaloids from the indole and annelated indole series.

2003

Chemistry and biology of marine natural products from the indole and annelated indole series have become an attractive research field for development of new pharmacological lead substances. In the past years some of the isolated natural organic compounds were synthesized by chemists and evaluated with great enthusiasm to find new lead natural compounds against different diseases. In this review the latest results for new compounds including isolation, biological evaluation, synthetic pathways and some retrosynthetic analyses are summarized.

PharmacologyIndole testIndolesChemistryOrganic ChemistryAntineoplastic AgentsMarine BiologyMarine Biology (journal)BiochemistryChemical synthesisBiological FactorsStructure-Activity RelationshipAlkaloidsAnti-Infective AgentsPharmaceutical PreparationsDrug DiscoveryMolecular MedicineOrganic chemistryAnimalsBiological evaluationCurrent medicinal chemistry
researchProduct

Quantitative in vivo microdialysis in pharmacokinetic studies: some reminders.

2005

This paper reviews the empirical methods of quantitative microdialysis that have been used to interpret the results obtained from pharmacokinetic studies. The concept of extraction efficiency or recovery and the properties of recovery in vivo (variation with flow rate, time dependency and influence of the mode of administration) are considered. The most frequently used methods for determining recovery in vivo are described and evaluated in the light of recent theoretical studies. Specifically, we review the variation of flow rate method, the very slow flow method, the no net flux method and the delivery and retrodialysis methods. Special emphasis is placed on the description of each method,…

PharmacologyMicrodialysisChemistryMicrodialysisClinical BiochemistryPharmacologySlow FlowPharmacokineticsPharmaceutical PreparationsIn vivoNo net fluxAnimalsHumansTime dependencyPharmacokineticsBiomedical engineeringCurrent drug metabolism
researchProduct

Nonsense codons suppression. An acute toxicity study of three optimized TRIDs in murine model, safety and tolerability evaluation.

2022

Stop mutations cause 11% of the genetic diseases, due to the introduction of a premature termination codon (PTC) in the mRNA, followed by the production of a truncated protein. A promising therapeutic approach is the suppression therapy by Translational Readthrough Inducing Drugs (TRIDs), restoring the expression of the protein. Recently, three new TRIDs (NV848, NV914, NV930) have been proposed, and validated by several in vitro assays, for the rescue of the CFTR protein, involved in Cystic Fibrosis disease. In this work, an acute toxicological study for the three TRIDs was conducted in vivo on mice, according to the OECD No.420 guidelines. Animals were divided into groups and treated with …

PharmacologyNonsense mutationCystic Fibrosis Transmembrane Conductance RegulatorGeneral MedicineOxadiazoleMiceDisease Models AnimalPremature termination codon (PTC)Pharmaceutical PreparationsCodon NonsenseProtein BiosynthesisAnimalsToxicity studyTranslational readthrough inducing drugs(TRIDs)Biomedicinepharmacotherapy = Biomedecinepharmacotherapie
researchProduct

Investigation of various shellac grades: additional analysis for identity.

2009

Background: A number of different grades of shellac are commercially available and most of them are known only as generic shellac and are not further differentiated. The investigated grades of shellac in this study are based on different insect strains, host trees, refining methods, and products from different suppliers. Method: The Gardner/Iodine color values of alcoholic and aqueous solutions of the various shellac grades were measured. Glass transition temperatures and pKa-values were determined. To assess chemical differences in the tested shellac grades, MALDI-TOF analysis was performed. Results: Differences were found in color, TG, and pKa-values and in the mass spectra by MALDI-TOF a…

PharmacologyQuality ControlInsectaChemistryOrganic ChemistryPharmaceutical ScienceMineralogyColorExcipientsPharmaceutical technologyvisual_artDelayed-Action PreparationsSpectrometry Mass Matrix-Assisted Laser Desorption-IonizationDrug DiscoveryShellacvisual_art.visual_art_mediumAnimalsTransition TemperatureFood scienceControl parametersResins PlantDrug development and industrial pharmacy
researchProduct

A topological sub-structural approach for predicting human intestinal absorption of drugs.

2004

The human intestinal absorption (HIA) of drugs was studied using a topological sub-structural approach (TOPS-MODE). The drugs were divided into three classes according to reported cutoff values for HIA. "Poor" absorption was defined as HIAor =30%, "high" absorption as HIAor =80%, whereas "moderate" absorption was defined between these two values (30%HIA79%). Two linear discriminant analyses were carried out on a training set of 82 compounds. The percentages of correct classification, for both models, were 89.02%. The predictive power of the models were validated by three test: a leave-one-out cross validation procedure (88.9% and 87.9%), an external prediction set of 127 drugs (92.9% and 80…

PharmacologyQuantitative structure–activity relationshipChemistryOrganic ChemistryBiological AvailabilityQuantitative Structure-Activity RelationshipGeneral MedicineModels TheoreticalLinear discriminant analysisTopologyCross-validationIntestinal absorptionBioavailabilityIntestinal AbsorptionPharmaceutical PreparationsTest setDrug DiscoveryHuman intestinal absorptionCutoffHumansIntestinal MucosaEuropean journal of medicinal chemistry
researchProduct

Multivariate equivalence tests for use in pharmaceutical development.

2014

Statistical equivalence analyses are well-established parts of many studies in the biomedical sciences. Also in pharmaceutical development and manufacturing equivalence testing methods are required in order to statistically establish similarities between machines, process components, or complete processes. This article presents a choice of multivariate equivalence testing procedures for normally distributed data as generalizations of existing univariate methods. In all derived methods, variability is interpreted as nuisance parameter. The use of the proposed methods in pharmaceutical development is demonstrated with a comparative analysis of dissolution profiles.

PharmacologyStatistics and ProbabilityMultivariate statisticsMahalanobis distanceEquivalence testingDrug Industrybusiness.industryUnivariateNormal DistributionMachine learningcomputer.software_genreDelta methodPharmaceutical PreparationsSolubilityResearch DesignData Interpretation StatisticalMultivariate AnalysisEconometricsNuisance parameterPharmacology (medical)Artificial intelligencebusinesscomputerEquivalence (measure theory)MathematicsJournal of biopharmaceutical statistics
researchProduct

Introduction to molecular topology: basic concepts and application to drug design.

2012

In this review it is dealt the use of molecular topology (MT) in the selection and design of new drugs. After an introduction of the actual methods used for drug design, the basic concepts of MT are defined, including examples of calculation of topological indices, which are numerical descriptors of molecular structures. The goal is making this calculation familiar to the potential students and allowing a straightforward comprehension of the topic. Finally, the achievements obtained in this field are detailed, so that the reader can figure out the great interest of this approach.

PharmacologyTheoretical computer scienceMolecular Structurebusiness.industryComputer scienceQuantitative Structure-Activity RelationshipGeneral Medicinecomputer.software_genreField (computer science)ComprehensionPharmaceutical PreparationsDrug DesignDrug DiscoveryNumerical descriptorsSelection (linguistics)Molecular MedicineComputer Aided DesignAnimalsComputer-Aided DesignHumansArtificial intelligenceMolecular topologybusinesscomputerCurrent computer-aided drug design
researchProduct

Strategies and Molecular Probes to Investigate the Role of Cytochrome P450 in Drug Metabolism

2003

Drug metabolism is the major determinant of drug clearance and, because of polymorphic or inducible expression of drug-metabolising cytochrome P450s (CYPs), is the factor most frequently responsible for interindividual differences in pharmacokinetics. A number of well characterised CYP substrates and inhibitors have been identified that allow precise measurements of individual CYP isoforms. Their use, alone or in combination, facilitates the phenotype characterisation of hepatocytes in vitro and in vivo. Two procedures are used for in vitro investigation of the metabolic profile of a drug: incubation with microsomes and incubation with metabolically competent cells. The major limitation of …

PharmacologybiologyCytochrome P450In Vitro TechniquesIsozymeIn vitroRatsCytochrome P-450 Enzyme SystemPharmaceutical PreparationsBiochemistryIn vivoMolecular Probesbiology.proteinMicrosomeAnimalsCytochrome P-450 Enzyme InhibitorsHumansDrug InteractionsPharmacology (medical)Enzyme InhibitorsEnzyme inducerAntibodies BlockingCytochrome P-450 Enzyme InhibitorsDrug metabolismClinical Pharmacokinetics
researchProduct

Bioequivalence of oral products and the biopharmaceutics classification system: science, regulation, and public policy.

2011

The demonstration of bioequivalence (BE) is an essential requirement for ensuring that patients receive a product that performs as indicated by the label. The BE standard for a particular product is set by its innovator, and this standard must subsequently be matched by generic drug products. The Biopharmaceutics Classification System (BCS) sets a scientific basis for an improved BE standard for immediate-release solid oral dosage forms. In this paper, we discuss BE and the BCS, as well as the issues that are currently relevant to BE as a pharmaceutical product standard.

Pharmacologybusiness.industryBiopharmaceuticsPublic policyAdministration OralBioequivalencePharmacologyBiopharmaceutics Classification SystemhumanitiesArticleBiopharmaceuticsPolicyRisk analysis (engineering)Pharmaceutical PreparationsTherapeutic EquivalencyInnovatorGeneric drugMedicineDrugs GenericHumansPharmacology (medical)Product (category theory)Product standardbusinessClinical pharmacology and therapeutics
researchProduct

The Prediction of Human Intestinal Absorption Based on the Molecular Structure

2014

Human Intestinal Absorption (HIA) has been modeled many times by using classification models. However, regression models are scarce. Here, Artificial Neural Networks (ANNs) are implemented for this purpose. A dataset of structurally diverse chemicals with their respective experimental HIA were used to design robust, true predictive and widespread applicable ANN models. An input variables pool was made up of structural invariants calculated by using either Dragon or our software Desmol 1. The selection of best variables was performed following three steps using the entire dataset of molecules. Firstly, variables poorly correlated with the experimental data were eliminated. Secondly, input va…

Pharmacologyeducation.field_of_studyMolecular StructureArtificial neural networkComputer sciencebusiness.industryClinical BiochemistryPopulationReproducibility of ResultsPattern recognitionFeature selectionRegression analysisModels TheoreticalBackpropagationIntestinal absorptionIntestinal AbsorptionPharmaceutical PreparationsResamplingTest setHumansNeural Networks ComputerArtificial intelligenceeducationbusinessCurrent Drug Metabolism
researchProduct