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Structure-activity relationship requiring metabolic activation

The third step is to optimize the lead molecule through iterative chemical synthesis and biological testing, aiming to obtain molecules with the required potency (typically nanomolar), selectivity, bioavailability, and DMPK (drug metabolism and pharmacokinetics) properties. This step usually requires considerable time and resources usually the synthesis of hundreds of compounds is needed to deduce a robust SAR (structure-activity relationship). Such resources can be considerably reduced and the... [Pg.14]

However, the acctimulated Information on azadirachtin, while promising, is presently much less than that needed for insecticidal product commercialization (41). The mode of action, structure-activity relationships (SAR s), formulation, and metabolism of azadirachtin are not yet well understood. Furthermore, formulation studies are required prior to product development and commercialization. Consequently, further investigations are needed before the full potential of azadirachtin as an insect control agent or insecticide can be realized. [Pg.405]

The discovery of Zanamivir as a potent and selective inhibitor of influenza virus sialidase prompted several researchers to investigate the synthesis and structure-activity relationship studies of Neu5Ac2en-based compounds as potential sialidase inhibitors. Exploration of these SAR studies were undertaken to optimize inhibitory activity and to improve the physicochemical properties of the sialic acid-based influenza virus sialidase inhibitor. A few in vitro assays are commonly employed to measure the effectiveness of influenza virus sialidase inhibitors. The first involves a fluorometric assay that measures release of a synthetic fluorophore following its cleavage from Neu5Ac by sialidase. Dye-uptake assay, such as the Neutral Red uptake assay, measures the uptake of a vital stain, Neutral Red in cell culture. The process requires intact membranes and active metabolism in the cell, and is expressed as percent protective rate against virus infection. The plaque-reduction assay is used to measure sialidase inhibition indirectly in cell culture, and provides some measure of the inhibitor s effect on the viability of the influenza virus. In vitro and in vivo systems for analysis of inhibitors of influenza virus enzymes have been reviewed.71... [Pg.304]


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Metabolic Structuring

Metabolic activation

Metabolism activation

Metabolism active

Metabolism structure

Metabolism/metabolic activity

Structural requirements

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