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Titlebook: Drug Safety Evaluation; Methods and Protocol Jean-Charles Gautier Book 2017Latest edition Springer Science+Business Media LLC 2017 immunohi

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978-1-4939-8406-0Springer Science+Business Media LLC 2017
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Nonclinical Development of Combination Drugsbination a detailed review of the nonclinical data available may suffice, particularly when the components have a history of coadministration at about the same dose and ratio as that of the proposed combination. For a marketed drug/NME combination, in addition to a review of the data for the markete
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Applications of Mass Spectrometry Imaging for Safety Evaluationvelopment phases. MSI allows to potentially address important questions in drug development such as “What is the localization of the drug and its metabolites in the tissues?”, “What is the pharmacological effect of the drug in this particular region of interest?”, or “Is the drug and its metabolites
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In Vivo Rat T-Lymphocyte , Assay: Detection and Expansion of Cells Deficient in the GPI-Anchored CD4nds of interest. Our methodology of combining phenotypic antibody labeling, magnetic enrichment, sorting, and single-cell clonal expansion can be used in genotoxicity/mutagenicity studies and in other general immunotoxicology research requiring identification, isolation, and expansion of extremely r
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NMR and MS Methods for Metabolomics drug development and molecular medicine are described in great detail, starting from sample preparation to determining the measurement details of all analytical platforms, and finally to discussing the corresponding specific steps of data analysis.
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Changing composition of paid workforcesbination a detailed review of the nonclinical data available may suffice, particularly when the components have a history of coadministration at about the same dose and ratio as that of the proposed combination. For a marketed drug/NME combination, in addition to a review of the data for the markete
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Practices and Orientations of CSCLvelopment phases. MSI allows to potentially address important questions in drug development such as “What is the localization of the drug and its metabolites in the tissues?”, “What is the pharmacological effect of the drug in this particular region of interest?”, or “Is the drug and its metabolites
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Designing Sociable CSCL Environmentsnds of interest. Our methodology of combining phenotypic antibody labeling, magnetic enrichment, sorting, and single-cell clonal expansion can be used in genotoxicity/mutagenicity studies and in other general immunotoxicology research requiring identification, isolation, and expansion of extremely r
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