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ISHIK UNIVERSITY FACULTY OF DENTISTRY

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Presentation on theme: "ISHIK UNIVERSITY FACULTY OF DENTISTRY"— Presentation transcript:

1 ISHIK UNIVERSITY FACULTY OF DENTISTRY
Pharmacology Dr. Esra Tariq Bayrakdar Pharmacist (M.Sc.)

2 Drug Receptors The drug receptors are macromolecular sites which are situated on the surface or inside the effector cells with which specific agonist combines to produce its response. Antagonist prevents the action of an agonist on a receptor, but does not have any effect of its own

3 Drug-receptor interaction
Each drug requires a target within the body called a receptor. Binding of drugs to receptor is: Reversible : Effect for short time (reversible bonding forces)…most drugs Irreversible: Effect is prolonged (Covalent bonding forces) : aspirin cause irreversible inhibition of PG synthesis.

4 Drugs act by antagonize or inhibit:
Cell surface Receptors Ion Channels Enzyme Inhibition Transport Inhibitors Nuclear Receptors

5 1)Action of a receptor : A spesific macromolecule, usually a protein to which a specific group of drugs or naturally occurring subtances (neurotransmitters or hormones) can bind. The biochemical evets that result from a dru- receptor interaction and which produce effect, are complex. The binding of drug to receptor result formation of : Drug-Receptor Complex…Then the effect. Drug + Receptor  Drug-receptor complex  effect

6 Types and subtypes of receptors
Main Actions of Naturale agonist Agonist Drug Antagonist Drug Adrenoceptor α1 α2 β1 β2 Vasoconstruction Hypotension Sedation Increase HR Bronchodilation Noradrenaline Clonidine Dopamine Salbutamol Prazosin Atenolol Cholinergic Muscarinic Heart rate Atropine Histamine H1 H2 Bronchoconstruction Increase gastric acidity Chlorpheniramine Ranitidine Are Drugs That Anatgonize Cell Surface Receptors Clinically Useful? Angiotensin receptor blockers (losartan, valsartan) for high blood pressure, HF Beta-adrenoceptor Blockers (propranolol, Atenolol) for angina, MI, HF, HBP

7 Functions of a receptor may be briefly summarized as follows:
Receptors largely determine the quantitative relations between dose or concentration of drug and pharmacologic effects. Receptors are responsible for selectivity of drug action. Receptors mediate the actions of both pharmacologic agonists and antagonists.

8 2) Action on an enzyme Enzymes, like receptors; are protein macromolecules which subtrates interact to produce activation or inhibition Examples: Enalapril (inhibits ACE-Anti-HTN) 3) Transport Inhibitors: Sodium pump inhibitors . Such as: Digoxin inhibits the membrane bound Na+/K+ATPase (Used in HF) Diuretics (Loop DU) inhibit the Na+/Cl- co- tranporter in the kidney

9 4) Actions on membrane ion channels
The conduction of impulses in nerve tissues and electromechanical coupling in muscle depend on the movement of ions particularly sodium, calcium, and potassium, through membrane channels. Several groups of drugs interfere with these processes: Antiarrythmic drugs (Quanidine: Na Channel blockers) Local anesthetics as (Lidocaine: Sodium channel Blocker) Anti-HTN: amlodipine (Ca channel blockers) Oral Anti-DM: Sulphonylureas block ATP-sensitive potassium channels in pancreatic B-cells

10 5) Drugs work by antagonizing Nuclear receptors:
Lipid soluble ligand can easily diffuse across cell membrane and move to the nucleus of the cell where it binds to nuclear receptors (DNA) and then activate the transcription of spesific gene. Estrogen receptor antagonists for the prevention and treatment of breast canser (Tamoxifen)

11 Agonists: Drugs that binds to receptor and stimulates or activates the receptor to produce an effect (salbutamol at beta-1 receptor). Antagonists are drug that binds to receptors and prevents the action of an agonist but does not have any effect itself (losartan at the angiotensin II receptor) Have only the affinity but no intrinsic activity.

12 Drug Tolerance is seen when the same dose of drug given repeatedly loses its effect or when greater doses are required to obtain previous effect. Eg. Tolerance of Glyceryl trinitrate occurs in treatment of angina pectoris when given repeatedly so a drug free time of 8-12 h is advised.

13 Up-Regulation : Continouse or repeated exposure to antagonists initially can increase the receptors and with chronic exposure to antagonist, the number of receptors on cell membrane surface increase. Eg. Β-blockers (propranolol) should not be stopped promptly in people with ischemic heart disease (IHD) because it presipitates unstable angina or mycardial infarction ( avoid sudden withdrawal)

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15 Combined effect of drugs
SYNERGISM When two drugs are given simultaneously, and the action of one drug is increased by the other, they are treated as synergistic. In the synergism, the drugs can have action in the same direction or when given alone, one may be inactive. Synergism can be additive or supradditive in nature.

16 Drug Antagonism COMPETITIVE ANTAGONISM
In competitive antagonism, the antagonist binds with the same receptor as agonist. If the log dose response curve with agonist is obtained in the presence of antagonist, it will be found that antagonist has no effect of its own and there is parallel rightward shift in the dose response curve of agonist with no change in shape, slope or maximum response. Eg. Acetylcholine (as agonist) – atropine (as antagonist).

17 NON-COMPETITIVE ANTAGONISM
Antagonist binds to another site or receptor. The antagonist is not displaced by a high concentration of the agonist on the same receptor and the dose- response curve is flattened and its slope and maximum response will be decreased. Eg. Noradrenaline--- Phenoxybenzamine


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