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The main objectives of produgs are as follow: Improvement of lipophilicity Enhancement of water solubility Increased metabolic stability Improvement of taste site – specific drug delivery prodrugs • Prepared from a drug & a carrier site of transporting the drug from the site of application selectively to the target cells. e.g. Brain specific targeting of a hydrophilic drug + Lipophilic carrier (a dihydropyridine) Result in a lipophilic prodrug • Inside the brain The lipophilic carrier is converted enzymatically To a highly hydrophilic charged species which is locked in the brain and then hydrolyzed back to the drug and N-methyl nicotinic acid is eliminated from the brain. The dihydropyridine/pyridinium redox chemical delivery system CDS XH group on the drug is an amine, hydroxyl or carboxyl. Lipophilic prodrug N-methyl nicotinic acid Interference with transport characteristics • The introduction of a hydrophilic disposable moiety into the drug prevent its absorption from the gastrointestinal tract. e.g. Decreased toxicity and adverse reaction • The presence of the thiol group in Captopril is considered as one of the responsible factors for the adverse reaction of these drugs. • The masking of the SH group, which in vivo regenerates this group, results in less toxic and probably longer acting drug . Increased duration of action • Bitolterol is a prodrug form of colterol in which the catechol hydroxyl groups have been converted to 4-methylbenzoic(p-toloyl) acid esters, providing increased lipid solubility and prolonged duration of action. Bronchodilator Activity • Furthermore, the prodrug is preferentially distributed in lung tissues rather than the plasma or heart so that the bronchodilator effect, following subsequent biotransformation of the prodrug, is not associated with undesirable cardiovascular effect, and is slow and prolonged.