81 resultados para Automobiles -- Motors -- Exhaust gas


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The objective of this work was to combine the advantages of the dried blood spot (DBS) sampling process with the highly sensitive and selective negative-ion chemical ionization tandem mass spectrometry (NICI-MS-MS) to analyze for recent antidepressants including fluoxetine, norfluoxetine, reboxetine, and paroxetine from micro whole blood samples (i.e., 10 microL). Before analysis, DBS samples were punched out, and antidepressants were simultaneously extracted and derivatized in a single step by use of pentafluoropropionic acid anhydride and 0.02% triethylamine in butyl chloride for 30 min at 60 degrees C under ultrasonication. Derivatives were then separated on a gas chromatograph coupled with a triple-quadrupole mass spectrometer operating in negative selected reaction monitoring mode for a total run time of 5 min. To establish the validity of the method, trueness, precision, and selectivity were determined on the basis of the guidelines of the "Société Française des Sciences et des Techniques Pharmaceutiques" (SFSTP). The assay was found to be linear in the concentration ranges 1 to 500 ng mL(-1) for fluoxetine and norfluoxetine and 20 to 500 ng mL(-1) for reboxetine and paroxetine. Despite the small sampling volume, the limit of detection was estimated at 20 pg mL(-1) for all the analytes. The stability of DBS was also evaluated at -20 degrees C, 4 degrees C, 25 degrees C, and 40 degrees C for up to 30 days. Furthermore, the method was successfully applied to a pharmacokinetic investigation performed on a healthy volunteer after oral administration of a single 40-mg dose of fluoxetine. Thus, this validated DBS method combines an extractive-derivative single step with a fast and sensitive GC-NICI-MS-MS technique. Using microliter blood samples, this procedure offers a patient-friendly tool in many biomedical fields such as checking treatment adherence, therapeutic drug monitoring, toxicological analyses, or pharmacokinetic studies.

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A headspace-gas chromatography-tandem mass spectrometry (HS-GC-MS/MS) method for the trace measurement of perfluorocarbon compounds (PFCs) in blood was developed. Due to oxygen carrying capabilities of PFCs, application to doping and sports misuse is speculated. This study was therefore extended to perform validation methods for F-tert-butylcyclohexane (Oxycyte(®)), perfluoro(methyldecalin) (PFMD) and perfluorodecalin (PFD). The limit of detection of these compounds was established and found to be 1.2µg/mL blood for F-tert-butylcyclohexane, 4.9µg/mL blood for PFMD and 9.6µg/mL blood for PFD. The limit of quantification was assumed to be 12µg/mL blood (F-tert-butylcyclohexane), 48µg/mL blood (PFMD) and 96µg/mL blood (PFD). HS-GC-MS/MS technique allows detection from 1000 to 10,000 times lower than the estimated required dose to ensure a biological effect for the investigated PFCs. Thus, this technique could be used to identify a PFC misuse several hours, maybe days, after the injection or the sporting event. Clinical trials with those compounds are still required to evaluate the validation parameters with the calculated estimations.

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Very large molecular systems can be calculated with the so called CNDOL approximate Hamiltonians that have been developed by avoiding oversimplifications and only using a priori parameters and formulas from the simpler NDO methods. A new diagonal monoelectronic term named CNDOL/21 shows great consistency and easier SCF convergence when used together with an appropriate function for charge repulsion energies that is derived from traditional formulas. It is possible to obtain a priori molecular orbitals and electron excitation properties after the configuration interaction of single excited determinants with reliability, maintaining interpretative possibilities even being a simplified Hamiltonian. Tests with some unequivocal gas phase maxima of simple molecules (benzene, furfural, acetaldehyde, hexyl alcohol, methyl amine, 2,5 dimethyl 2,4 hexadiene, and ethyl sulfide) ratify the general quality of this approach in comparison with other methods. The calculation of large systems as porphine in gas phase and a model of the complete retinal binding pocket in rhodopsin with 622 basis functions on 280 atoms at the quantum mechanical level show reliability leading to a resulting first allowed transition in 483 nm, very similar to the known experimental value of 500 nm of "dark state." In this very important case, our model gives a central role in this excitation to a charge transfer from the neighboring Glu(-) counterion to the retinaldehyde polyene chain. Tests with gas phase maxima of some important molecules corroborate the reliability of CNDOL/2 Hamiltonians.

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Vaccination aims at generating memory immune responses able to protect individuals against pathogenic challenges over long periods of time. Subunit vaccine formulations based on safe, but poorly immunogenic, antigenic entities must be combined with adjuvant molecules to make them efficient against infections. We have previously shown that gas-filled microbubbles (MB) are potent antigen-delivery systems. This study compares the ability of various ovalbumin-associated MB (OVA-MB) formulations to induce antigen-specific memory immune responses and evaluates long-term protection toward bacterial infections. When initially testing dendritic cells reactivity to MB constituents, palmitic acid exhibited the highest degree of activation. Subcutaneous immunization of naïve wild-type mice with the OVA-MB formulation comprising the highest palmitic acid content and devoid of PEG2000 was found to trigger the more pronounced Th1-type response, as reflected by robust IFN-γ and IL-2 production. Both T cell and antibody responses persisted for at least 6 months after immunization. At that time, systemic infection with OVA-expressing Listeria monocytgenes was performed. Partial protection of vaccinated mice was demonstrated by reduction of the bacterial load in both the spleen and liver. We conclude that antigen-bound MB exhibit promising properties as a vaccine candidate ensuring prolonged maintenance of protective immunity.

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L'Europe centrale fait à la fois figure d'interface et de plateforme sur le continent européen dans des jeux politiques et économiques. L'adhésion à l'Union européenne est porteuse d'espoir en termes de développement de territoires encore marqués par près de 50 ans de régime socialiste. L'intégration de ces territoires à la mondialisation a été insufflée avant tout par des acteurs économiques privés, les firmes multinationales, dès le milieu des années 1990. Par leurs capacités d'investissements et leurs organisations en réseaux à l'échelle mondiale, ces firmes multinationales participent majoritairement à ce processus d'intégration qui repose donc avant tout sur des raisons opportunistes et rationnelles. Les firmes multinationales ont positionné ces territoires dans les activités les plus profitables à l'organisation de leur « chaîne globale de valeur » mondiale. On peut dès lors s'interroger sur l'ampleur et les formes d'intégrations à la mondialisation qu'apportent ces implantations d'entreprises multinationales en particulier pour les villes d'Europe centrale. Dans une approche d'analyse empirique multi-niveaux, la thèse replace les villes d'Europe centrale dans la compétition mondiale des firmes multinationales du secteur automobile qui a particulièrement participé à l'intégration de ces territoires dans des stratégies industrielles mondiales. A un niveau micro, nous analysons les stratégies des firmes automobiles par leurs réseaux d'organisation financière dans une approche à la fois gestionnaire et quantitative. A un niveau méso/macro, nous positionnons les villes d'Europe centrale dans les systèmes de villes européen et mondiaux, selon le rôle attribué dans les chaînes globales de valeur. À chaque étape de cette recherche, l'analyse prend en compte différentes échelles spatiales (urbaine, régionale, nationale, continentale) et plusieurs niveaux d'analyse (micro : les réseaux individuels d'entreprises, méso : les liens intra-urbains, macro : les attractivités interurbaines) afin de souligner les interactions multi échelles qui intègrent chaque espace considéré. Cela nous permet d'évaluer en particulier la place des relations de l'ex-UE15 avec l'Europe centrale dans le contexte des réseaux mondiaux. Les formes transnationales des réseaux des entreprises multinationales, se déployant dans un système de lieux identifiés (métropoles ou villes) sont replacées dans les logiques internationales d'accords bilatéraux, de réglementations régionales et de politiques d'attraction (comme fiscales) ou de soutien au développement (aides nationales ou européennes). L'approche empirique multi échelles, articule les différentes dimensions des stratégies de localisation des entreprises déployées dans leur approche du développement et de la stabilisation de leur chaine globale de valeur, avec les positions relatives des territoires et villes à différents niveaux d'intégration. Ainsi la thèse offre une vision originale de l'articulation des développements locaux des territoires face aux stratégies globales des entreprises.