Pharmacodynamics.doc
•Als PPTX, PDF herunterladen•
0 gefällt mir•470 views
What drugs do to the body
Empfohlen
Weitere ähnliche Inhalte
Was ist angesagt?
Was ist angesagt? (12)
Ähnlich wie Pharmacodynamics.doc
Ähnlich wie Pharmacodynamics.doc (20)
Mehr von Amna Medani
Mehr von Amna Medani (20)
Kürzlich hochgeladen
Kürzlich hochgeladen (20)
Pharmacodynamics.doc
- 1. PHARMACODYNAMICS Sites of drug action :- - Understanding of the depth of information of the drug action is necessary to achieve : - A suitable comparison of the relative benefits and risks of alternative drugs on selection . - A prediction of possible problems in a patient due to other disease processes or other drugs . - Drugs may have : - Non-specific generalized effect via response in organs with their highest concentrations ( volume of distribution ) .
- 2. - Specific-site effects via interactions of drugs with specific site (s) – one type of receptor families or more-i.e. selective drugs ( e.g.a β adrenceptive drug has high affinity for all β adrenergic receptors ) or non selective ( if it has affinity for all adrenergic receptors ) .It could also exhibit selectivity amongst the selected receptors ( β1adrenoceptors and not β2 adrenoceptors ) . - Specifity is reciprocal i.e. individual classes of drugs bind only to certain targets and individual targets recognize only certain classes of the drug . - Specifity may either be : - Biological ( receptor specifity e.g. ethanol causes smooth muscle contraction , but relaxation of vascular smooth muscles ; stimulation of gastric juice secretion , but not the salivary secretion ) . - Chemical due to the chemical of the chemical struture
- 3. DRUG SPECIFITY: I/ BIOLOGICAL ( RECEPTOR-SPECIFITY ): e.g. ETHANOL PRODUCES INHIBITORY EFFECT ON MOST CELLS AND TISSUES ( CONTRACTION OF SMOOTH MUSCLES , BUT RELAXATION OF THE VASCULAR SMOOTH MUSCLES AND STIMULATION OF GASTRIC SECRETION EXCEPT THE SALIVARY SECRETION.
- 4. II/CHEMICAL (STEREOSELECTIVITY) : e.g. HISTAMINE EFFECT BASED ON MARKED DIFFERENCE BETWEEN ENANTIOMERIC CHEMICAL STRUCTURE DUE TO PHARMACOLOGICAL ACTIVITY. TARGETS FOR DRUG ACTION : MOST DRUGS ARE EFFECTIVE BECAUSE
- 5. Drug antagonism : It is the complete or partial abolishment of a drug action in the presence of another drug . It is classified into : i/ Chemical antagonism :- This occurs when two substance combine in solution , so the effect of the active drug is lost ( e.g. inactivation of heavy metals by a chelating agent like dimercaprol which binds the metal ion tightly to form an inactive complex .
- 6. ii/ Pharmacokinetic antagonism :- This occurs when the antagonist effectively reduces the concentration of the active drug at its site of action by :- a/ Reducing the rate of absorption of the active drug from the GIT ( e.g. tetracycline and milk ). b/ Increasing the rate of metabolic degradation of the active drug ( e.g. reduction of the anticoagulant effect of warfarin by increasing its hepatic metabolism by phenobarbitone ) . c/ Increased renal excretion ( e.g. aspirin and sodium bicarbonate ) .
- 7. iii/ Competative Antagonism :- By receptor-blocking (e.g.for an agonist A and an antagonist B : PA = XA / (XA + KA ) = 1- PB ( here B is non surmountable ) . iv/ Non-competative antagonism :- This occurs when the antagonist blocks at some point of the chain that lead to the production of a response by the agonist ( e.g. verapamil and nifedipine prevent the flux of calcium ions through the cell membrane and hence block the contraction of smooth muscle produced by other drugs . This will reduce the slope of the agonist on the DRC .
- 8. v/ Physiological antagonism :- This occurs when the interaction of two drugs in the body tend to cancel each other ( e.g.noradrenaline rises arterial blood pressure by acting on the heart and peripheral circulation , while histamine lowers arterial blood pressure by causing vasodilation ) .It is not well demarcated from non-competitive antagonism .