Presentation is loading. Please wait.

Presentation is loading. Please wait.

By Amany Helmy Hasanin Assistant Professor of Clinical Pharmacology

Published byPeregrine Simmons Modified over 5 years ago

Similar presentations

Presentation on theme: "By Amany Helmy Hasanin Assistant Professor of Clinical Pharmacology"— Presentation transcript:

1 By Amany Helmy Hasanin Assistant Professor of Clinical Pharmacology
Pharmacodynamic-2 By Amany Helmy Hasanin Assistant Professor of Clinical Pharmacology

2 Student Activity Intrinsic activity is, a drug’s ability to elicit:
a) Strong receptor binding b) Weak receptor binding c) Response d) Excretion e) Distribution

3 Agonists A drug (chemical) that is able to alter the conformation of a receptor in such a way that it elicits a response in the system

4 Agonists Types Full Agonist Partial Agonist Inverse Agonist

5 Full Agonist Agonist binds to receptors to activate them
Agonist possess affinity and efficacy

6 Partial Agonist (Agonist-Antagonist) In presence of agonist
works as antagonist

7 Inverse Agonist Agonist Antagonist

8 Graded dose response curve
Emax 100% Response 50% ED50 Dose (Log) Graded dose response curve

9 Graded (quantitative) dose response curve
Drug A Drug B Emax 100% Response 50% ED50 ED50 Dose (Log)

10 Emax The maximal effect produced by the drug (= the maximum value of the dose-response curve) Efficacy

11 The dose that produces 50% of the maximum therapeutic effect
Effective dose fifty ED50 The dose that produces 50% of the maximum therapeutic effect

12 Slope The middle portion of the curve
(it reflects the effect of the drug produced by one unit of the dose)

13 Efficacy (Emax) Potency (ED50 and slope)
Data we can get from graded dose response curve Efficacy (Emax) Potency (ED50 and slope)

14 Graded (quantitative) dose response curve
Drug A Drug B Emax Response 50% ED50 ED50 Dose (Log)

15 Graded dose response curve
Drug A 100% Emax Drug B 100% Emax Response 50% 50% ED50 ED50 Dose (Log)

16 Antagonist binds to receptors prevents Affinity without efficacy
Agonist to bind Affinity without efficacy

17 Graded dose response curve
100% Response 50% ED50 Dose (Log) Graded dose response curve

18 Compete with agonists for the same recognition site of the receptors
Types of Receptor Antagonists Competitive Compete with agonists for the same recognition site of the receptors

19 competitive antagonist
Graded dose response curve Agonist+ competitive antagonist Agonist alone Emax Response 50% ED50 ED50 Dose (Log)

20 Types of Receptor Antagonists (Cont.)
Noncompetitive Prevent binding of the agonist or prevent activation of the receptor by the agonist

21 Non-competitive antagonist
Graded dose response curve Agonist alone Emax Agonist+ increasing doses of Non-competitive antagonist Response Dose (Log)

22 Is there any clinical application competitive and non competitive antagonist

23 Are there other types of antagonists
The action of a ligand can be reversed by non-receptor antagonists

24 Antagonist interact chemically with the agonist away from receptor
Chemical antagonist Antagonist interact chemically with the agonist away from receptor Negative charges on heparin are neutralized by positive charges on protamine sulfate (heparin antidote)

25 Physiological antagonist
Antagonist by acting on different receptors induce the opposite actions of the agonist

26 Histamine H receptors Epinephrine

27 Non-receptor Mediated Mechanisms
Drugs Acting on Enzymes Drugs Acting on Plasmatic Membranes Drugs Acting on the Genetic Apparatus Drugs Acting on Subcellular Structures Drugs Acting by Physical Means Drugs Acting by Chemical Action May affect permeability, carrier systems, transport processes or enzyme systems in the plasmatic membrane antifungal drugs increase permeability of fungal plasmatic membrane Drus acting on genetic apparatus Antibiotics (e.g. aminoglycosides, chloramphenicol & tetracyclines) inhibit bacterial protein synthesis Anticancer Drugs affect DNA synthesis or function Drugs acting on subcellular structures Mitochondria: salicylates uncouple oxidative phosphorylation Microtubules: Antimitotic agents

28 Drugs Acting on Enzymes

29 Drugs Acting on Plasmatic Membranes
Affect permeability, carrier systems, transport processes or enzyme systems in the plasmatic membrane

30 Drugs Acting on the Genetic Apparatus

31 Drugs Acting on Subcellular Structures
Mitochondria Microtubules

32 Drugs Acting by Physical Means
Demulcents (soothing): a substance that relieves irritation of the mucous membranes by forming a protective film, lozenges

33 Drugs Acting by Physical Means (Cont.)
Adsorbents: a substance that adsorbs another charcoal adsorbs gases and toxins in intestine

34 Drugs Acting by Physical Means (Cont.)
Lubricants: liquid paraffin is used in constipation Osmosis: osmotic diuretics e.g. Mannitol

35 Drugs Acting by Chemical Action
Antacids neutralize HCL in peptic ulcer Citrates interact with calcium to inhibit blood coagulation

36 Drugs Acting by Chemical Action (Cont.)
Protamine sulfate neutralizes heparin by its positive charges Heparin Protamine

37 Drugs Acting by Chemical Action (Cont.)
Chelation Desferroxamin (multiple blood transfusion)

38 At the end I am expecting from you to be able to
Compare efficacy and potency of two drugs Identify and compare between different types of agonist Specify and compare between different types of antagonist

39

Download ppt "By Amany Helmy Hasanin Assistant Professor of Clinical Pharmacology"

Similar presentations

Introduction to Pharmacology

Introduction to Pharmacology
LAKSHMAN KARALLIEDDE OCTOBER 2011

LAKSHMAN KARALLIEDDE OCTOBER 2011
Drug Chemistry and Toxicology CHE 618 Alexander Nazarenko.

Drug Chemistry and Toxicology CHE 618 Alexander Nazarenko.
DRUG-RECEPTOR INTERACTIONS

DRUG-RECEPTOR INTERACTIONS
QUANTITATIVE ASPECTS OF DRUG ACTION

QUANTITATIVE ASPECTS OF DRUG ACTION
QUANTITATIVE ASPECTS OF DRUG ACTION ilo s By the end of this lecture you will be able to :  Recognize different dose response curves  Classify different.

QUANTITATIVE ASPECTS OF DRUG ACTION ilo s By the end of this lecture you will be able to :  Recognize different dose response curves  Classify different.
Nomenclature: Every drug has three names: 1) Chemical Name:  The drug is named according to its chemical structure. 2) Generic name (common name): 

Nomenclature: Every drug has three names: 1) Chemical Name:  The drug is named according to its chemical structure. 2) Generic name (common name): 
Drug ? RESPONSE altering their biochemical &/or biophysical activity  Depress  Activate  Replace  Irritate  Destroy PHARMACODYNAMICS  Absorb 

Drug ? RESPONSE altering their biochemical &/or biophysical activity  Depress  Activate  Replace  Irritate  Destroy PHARMACODYNAMICS  Absorb 
PHL 211 Pharmacology Fifth Lecture By Abdelkader Ashour, Ph.D. Phone: 4677212 Email: aeashour@ksu.edu.sa.

PHL 211 Pharmacology Fifth Lecture By Abdelkader Ashour, Ph.D. Phone:
Pharmacology-1 PHL 313 Fourth Lecture By Abdelkader Ashour, Ph.D. Phone: 4677212

Pharmacology-1 PHL 313 Fourth Lecture By Abdelkader Ashour, Ph.D. Phone:
Drug-Receptor Interactions Pharmacodynamics

Drug-Receptor Interactions Pharmacodynamics
RESPONSE To alter their biochemical &/or biophysical activity  Depress  Activate  Replace  Irritate  Destroy PHARMACODYNAMICS  Absorb  Distribute.

RESPONSE To alter their biochemical &/or biophysical activity  Depress  Activate  Replace  Irritate  Destroy PHARMACODYNAMICS  Absorb  Distribute.
RESPONSE To alter their biochemical &/or biophysical activity  Depress  Activate  Replace  Irritate  Destroy PHARMACODYNAMICS  Absorb  Distribute.

RESPONSE To alter their biochemical &/or biophysical activity  Depress  Activate  Replace  Irritate  Destroy PHARMACODYNAMICS  Absorb  Distribute.
Principles of Pharmacology: Pharmacodynamics

Principles of Pharmacology: Pharmacodynamics
Principles of Pharmacology: Pharmacodynamics

Principles of Pharmacology: Pharmacodynamics
PHC 222 Part(I) Dr. Huda Al Salem Lecture (7). Factors that affect the efficacy 2- Concentration-Response Curves: Agonist Antagonist Partial agonist Desensetization.

PHC 222 Part(I) Dr. Huda Al Salem Lecture (7). Factors that affect the efficacy 2- Concentration-Response Curves: Agonist Antagonist Partial agonist Desensetization.
Lecture 6 II. Non-receptor Mechanisms. Direct Physical blocking of channel local anesthetic & amiloride Modulator Bind to the channel protein itself Ca.

Lecture 6 II. Non-receptor Mechanisms. Direct Physical blocking of channel local anesthetic & amiloride Modulator Bind to the channel protein itself Ca.
Pharmacology UG-Course Touqeer Ahmed PhD 19 th February, 2015 Atta-ur-Rahman School of Applied Biosciences National University of Sciences and Technology.

Pharmacology UG-Course Touqeer Ahmed PhD 19 th February, 2015 Atta-ur-Rahman School of Applied Biosciences National University of Sciences and Technology.
Types of antagonists. Antagonists, Overview  Definition “An antagonist is a substance that does not provoke a biological response itself, but blocks.

Types of antagonists. Antagonists, Overview  Definition “An antagonist is a substance that does not provoke a biological response itself, but blocks.
BASIC PHARMACOLOGY 2 SAMUEL AGUAZIM(MD).

BASIC PHARMACOLOGY 2 SAMUEL AGUAZIM(MD).

Similar presentations

Ads by Google