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Dr. D. K. Brahma
Associate Professor
Department of Pharmacology
NEIGRIHMS, Shillong
Factors Modifying Drug Action
Introduction
• Responses variation to a Drug – (1) person to person; and (2) also same
person on different occasions
• Individuals differ in pharmacokinetic handling of drugs – varying
plasma/target site conc. – Metabolized drug Vs excreted unchanged
drugs – Propranolol and Atenolol
• Variation in number or state of receptors, coupling proteins or other
components of response effectuation
• Variations in hormonal/neurogenic tone or concentrations – atropine,
propranolol, captopril
• Categories of factors: Genetic and Nongenetic including
environmental, circumstantial and personal variables
• Factors modify drug action
– Quantitatively – action increased or decreased
– Qualitatively: Altered response – allergic reaction or idiosyncrasy
1. Body Size
Influences the conc. of the drug attained at the site of action –
obese/lean/children – Body weight (BW) and Body Surface area
(BSA)
 Individual dose = x average adult dose
Individual dose = x average adult dose
BSA can be calculated by Dubois Formula
BSA (m2
) = BW (kg)0.425
x Height (cm)0.725
X 0.007184
BW (kg)
70
BSA (m2
)
1.7
Example – 40 kg / 70 x 500 mg
2000 /7 == 285 mg
2. Age
• Young`s formula
• Child dose = x adult dose
• Dilling`s formula
• Child dose = x adult dose
• Note: Infants & children are not small adults – physiological differences
– Low g.f.r and tubular transport – Gentamicin and Penicillin
– Low hepatic drug metabolizing systems in newborns – gray baby syndrome
– Blood brain barrier (BBB) is more permeable - Kernicterus
– Absorption of drugs altered – lower gastric acidity ad slow intestinal transit
– Faster transdermal absorption and faster rectal absorption - Diazepam
– After 1 (one) year faster metabolism than adults – phenytoin, carbamazepine
– Caution – Corticosteroids, androgens, tetracyclines …. Elderly ????
Age
Age + 12
Age
20
Example : (8 years / 8 years + 12) x 500 mg
- (8 x 500) / (8 + 12) = 200 mg
3. Sex
 Females have smaller body size – required doses are
lower
 Digoxin in Maintenance therapy of heart failure –
mortality higher
 Beta blockers, methyldopa, diuretics – sexual function
interference in males
 Gynaecomastia – Metoclopramide, chlorpromazine,
ketoconazole etc.
 Pregnancy – particularly 3rd
trimester
4. Species and Race
Species variation in drugs responses do exist
Some strains of rabbits – resistant to atropine
Rat and mice are resistant to digitalis
Race – racial differences have been observed
Blacks require higher doses of atropine and ephedrine, while
Mongols require lower doses
Africans – beta blockers are less effective
SMON – Japan but not among Indians
5. Genetics
Determinants of drug responses – transporter, enzymes, ion
channels, receptors and couplers – controlled genetically –
Individual variation of responses
Pharmacogenetics: Use of genetic information to guide the choice
of drug and dose on an individual basis – to identify individuals
who are either more likely or less likely respond to a drug
so far genetic abnormalities have been identified
Personalized medicine goal yet to achieve
G-6PD deficiency – Primaquine, chlroquin, quinine, dapsone, aspirin
Malignant hypothermia with halothane etc.
Low variants of CYP2C9 – Warfarin bleeding; Isoniazid - acetylators
6. Route of administration
Route determines the speed and intensity of drug response –
Parenteral for speedy action
A drug may have different actions via different routes –
Magnesium sulfate
7. Environmental factors
Drug metabolism may get induced – exposure to insecticides,
carcinogens, tobacco smoke and charcoal broiled meat etc.
Food interferes absorption of some drugs while enhances some
drugs – ampicillin gets reduced griseofulvin gets enhanced
Hypnotics taken at night
8. Psychological factors
Efficacy of a drug can be affected by patient`s beliefs, attitudes and
expectations – particularly CNS drugs – more GA in nervous and
anxious patients – alcohol and performance
Placebo: An inert substance which is given in the garb of
medicine. Works by psychodynamic effects (not
pharmacodynamics) – sometimes responses equivalent to active
drugs
Placebo reactors
Induce psychological responses – release of endorphins in brain
Uses – Control device in clinical trials and to treat a patient
Lactose tablet/capsules or water injections etc.
Nocebo: Negative psychodynamic effects of drugs
9. Pathological states
Diseases can influence drug disposition – GIT diseases, Liver diseases,
Kidney diseases, Congestive heart failure and Thyroid etc.
GIT: Coeliac diseases – amoxicillin absorption decreased while
Cephalexin and cotrimoxazole increased; Achlorohydria – Reduced
aspirin absorption – NSAIDs aggravate peptic ulcer
Liver diseases: Liver disease (cirrhosis) influence drug action
Increased bioavailability of drugs with high first pass metabolism
Serum albumin reduced – protein bound drugs like Warfarin – more free
drug
Metabolism and elimination of drugs may be reduced – Doses should be
reduced – Morphine, Propranolol, lignocaine etc.
Prodrugs are less effective (becampicillin)
9. Pathological states – contd.
Kidney diseases: Pharmacokinetics of many drugs are affected
Clearance of drugs in unchanged form (aminoglycosides, digoxin,
phenobarbitone) reduced – parallel to CLcr - loading dose not altered – dose
should be reduced
Plasma protein, albumin reduced – binding of acidic drugs affected
Permeability of BBB increased – Opiates etc. more CNS depression
Drugs acting via kidney mechanism – become ineffective – Thiazides and
urinary antiseptics
CCF: (1) Alter drug kinetics by decreased absorption (Thiazide), (2)
modifying Volume of distribution Lignocaine), (3) retarding the
elimination (lignocaine)- decreased perfusion and congestion of liver;
reduced g.f.r, increased tubular reabsorption – doses need reduction
Contd.
Thyroid diseases: Hypothyroid states – sensitive to
digoxin, morphine and CNS depressants;
Hyperthyroid states – resistant to inotropic action –
prone to cause arrhythmia by digoxin
10. Presence of other drugs: Drug interactions –
Pharmacokinetic and Pharmacodynamic
11. Cumulation: If Rate of administration > Rate of
elimination – cumulataion. Slowly eliminating drugs
are prone – Prolonged use of Chloroquine
12. Tolerance
Requirement of higher dose of a drug to produce a given response –
refractoriness – sulfonylureas in type 2 diabetes and beta-2 agonists in
bronchial asthma - adaptive biological phenomena
Natural: Species/individual inherently less sensitive – Rabbits to atropine and
Blacks to beta – blockers
Acquired: Repeated use of a drug in an individual who was initially responsive
become non-responsive (tolerant) – CNS depressants
 Due to uninterrupted presence of drug in the body – no tolerance to cocaine and atropine
 Tolerance may develop to one action of the drug – but not to other action – Chlorpromazine,
phenobarbitone, Morphine
Cross tolerance: Tolerance to pharmacologically related drugs – alcoholics to
barbiturates and GA; Morphine and Pethidine
Contd.
Tolerance Mechanism:
Pharmacokinetic/drug disposition tolerance – effective concentration of the
drug at the site of action is decreased – due to enhancement of elimination
on chronic use – Barbiturates and Carbamazepine induce own metabolism
Pharmacodynamic tolerance: lesser drug action – cells of target organs
become less responsive – Morphine, Barbiturates, Nitrates etc. …. Down
regulation/desensitization of receptors
Tachyphylaxis (Tachy – fast’ phylaxis – protection): Rapid
development of tolerance when a drug is repeated in quick
succession – reduction of responses
Usually with indirectly acting drugs – Ephedrine, tyramine, nicotine etc.
Also down regulation of receptors
Summary
Remember the different factors modifying drug actions
Remember: Young`s formula, Placebo, Cumulation,
Tolerance, cross tolerance and Tachyphylaxis
Drug use in children, elderly, pregnancy and different
pathological states will be discussed individually
Thank you/Khublei shibun

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Factors Modifying Drug Action

  • 1. Dr. D. K. Brahma Associate Professor Department of Pharmacology NEIGRIHMS, Shillong Factors Modifying Drug Action
  • 2. Introduction • Responses variation to a Drug – (1) person to person; and (2) also same person on different occasions • Individuals differ in pharmacokinetic handling of drugs – varying plasma/target site conc. – Metabolized drug Vs excreted unchanged drugs – Propranolol and Atenolol • Variation in number or state of receptors, coupling proteins or other components of response effectuation • Variations in hormonal/neurogenic tone or concentrations – atropine, propranolol, captopril • Categories of factors: Genetic and Nongenetic including environmental, circumstantial and personal variables • Factors modify drug action – Quantitatively – action increased or decreased – Qualitatively: Altered response – allergic reaction or idiosyncrasy
  • 3. 1. Body Size Influences the conc. of the drug attained at the site of action – obese/lean/children – Body weight (BW) and Body Surface area (BSA)  Individual dose = x average adult dose Individual dose = x average adult dose BSA can be calculated by Dubois Formula BSA (m2 ) = BW (kg)0.425 x Height (cm)0.725 X 0.007184 BW (kg) 70 BSA (m2 ) 1.7 Example – 40 kg / 70 x 500 mg 2000 /7 == 285 mg
  • 4. 2. Age • Young`s formula • Child dose = x adult dose • Dilling`s formula • Child dose = x adult dose • Note: Infants & children are not small adults – physiological differences – Low g.f.r and tubular transport – Gentamicin and Penicillin – Low hepatic drug metabolizing systems in newborns – gray baby syndrome – Blood brain barrier (BBB) is more permeable - Kernicterus – Absorption of drugs altered – lower gastric acidity ad slow intestinal transit – Faster transdermal absorption and faster rectal absorption - Diazepam – After 1 (one) year faster metabolism than adults – phenytoin, carbamazepine – Caution – Corticosteroids, androgens, tetracyclines …. Elderly ???? Age Age + 12 Age 20 Example : (8 years / 8 years + 12) x 500 mg - (8 x 500) / (8 + 12) = 200 mg
  • 5. 3. Sex  Females have smaller body size – required doses are lower  Digoxin in Maintenance therapy of heart failure – mortality higher  Beta blockers, methyldopa, diuretics – sexual function interference in males  Gynaecomastia – Metoclopramide, chlorpromazine, ketoconazole etc.  Pregnancy – particularly 3rd trimester
  • 6. 4. Species and Race Species variation in drugs responses do exist Some strains of rabbits – resistant to atropine Rat and mice are resistant to digitalis Race – racial differences have been observed Blacks require higher doses of atropine and ephedrine, while Mongols require lower doses Africans – beta blockers are less effective SMON – Japan but not among Indians
  • 7. 5. Genetics Determinants of drug responses – transporter, enzymes, ion channels, receptors and couplers – controlled genetically – Individual variation of responses Pharmacogenetics: Use of genetic information to guide the choice of drug and dose on an individual basis – to identify individuals who are either more likely or less likely respond to a drug so far genetic abnormalities have been identified Personalized medicine goal yet to achieve G-6PD deficiency – Primaquine, chlroquin, quinine, dapsone, aspirin Malignant hypothermia with halothane etc. Low variants of CYP2C9 – Warfarin bleeding; Isoniazid - acetylators
  • 8. 6. Route of administration Route determines the speed and intensity of drug response – Parenteral for speedy action A drug may have different actions via different routes – Magnesium sulfate 7. Environmental factors Drug metabolism may get induced – exposure to insecticides, carcinogens, tobacco smoke and charcoal broiled meat etc. Food interferes absorption of some drugs while enhances some drugs – ampicillin gets reduced griseofulvin gets enhanced Hypnotics taken at night
  • 9. 8. Psychological factors Efficacy of a drug can be affected by patient`s beliefs, attitudes and expectations – particularly CNS drugs – more GA in nervous and anxious patients – alcohol and performance Placebo: An inert substance which is given in the garb of medicine. Works by psychodynamic effects (not pharmacodynamics) – sometimes responses equivalent to active drugs Placebo reactors Induce psychological responses – release of endorphins in brain Uses – Control device in clinical trials and to treat a patient Lactose tablet/capsules or water injections etc. Nocebo: Negative psychodynamic effects of drugs
  • 10. 9. Pathological states Diseases can influence drug disposition – GIT diseases, Liver diseases, Kidney diseases, Congestive heart failure and Thyroid etc. GIT: Coeliac diseases – amoxicillin absorption decreased while Cephalexin and cotrimoxazole increased; Achlorohydria – Reduced aspirin absorption – NSAIDs aggravate peptic ulcer Liver diseases: Liver disease (cirrhosis) influence drug action Increased bioavailability of drugs with high first pass metabolism Serum albumin reduced – protein bound drugs like Warfarin – more free drug Metabolism and elimination of drugs may be reduced – Doses should be reduced – Morphine, Propranolol, lignocaine etc. Prodrugs are less effective (becampicillin)
  • 11. 9. Pathological states – contd. Kidney diseases: Pharmacokinetics of many drugs are affected Clearance of drugs in unchanged form (aminoglycosides, digoxin, phenobarbitone) reduced – parallel to CLcr - loading dose not altered – dose should be reduced Plasma protein, albumin reduced – binding of acidic drugs affected Permeability of BBB increased – Opiates etc. more CNS depression Drugs acting via kidney mechanism – become ineffective – Thiazides and urinary antiseptics CCF: (1) Alter drug kinetics by decreased absorption (Thiazide), (2) modifying Volume of distribution Lignocaine), (3) retarding the elimination (lignocaine)- decreased perfusion and congestion of liver; reduced g.f.r, increased tubular reabsorption – doses need reduction
  • 12. Contd. Thyroid diseases: Hypothyroid states – sensitive to digoxin, morphine and CNS depressants; Hyperthyroid states – resistant to inotropic action – prone to cause arrhythmia by digoxin 10. Presence of other drugs: Drug interactions – Pharmacokinetic and Pharmacodynamic 11. Cumulation: If Rate of administration > Rate of elimination – cumulataion. Slowly eliminating drugs are prone – Prolonged use of Chloroquine
  • 13. 12. Tolerance Requirement of higher dose of a drug to produce a given response – refractoriness – sulfonylureas in type 2 diabetes and beta-2 agonists in bronchial asthma - adaptive biological phenomena Natural: Species/individual inherently less sensitive – Rabbits to atropine and Blacks to beta – blockers Acquired: Repeated use of a drug in an individual who was initially responsive become non-responsive (tolerant) – CNS depressants  Due to uninterrupted presence of drug in the body – no tolerance to cocaine and atropine  Tolerance may develop to one action of the drug – but not to other action – Chlorpromazine, phenobarbitone, Morphine Cross tolerance: Tolerance to pharmacologically related drugs – alcoholics to barbiturates and GA; Morphine and Pethidine
  • 14. Contd. Tolerance Mechanism: Pharmacokinetic/drug disposition tolerance – effective concentration of the drug at the site of action is decreased – due to enhancement of elimination on chronic use – Barbiturates and Carbamazepine induce own metabolism Pharmacodynamic tolerance: lesser drug action – cells of target organs become less responsive – Morphine, Barbiturates, Nitrates etc. …. Down regulation/desensitization of receptors Tachyphylaxis (Tachy – fast’ phylaxis – protection): Rapid development of tolerance when a drug is repeated in quick succession – reduction of responses Usually with indirectly acting drugs – Ephedrine, tyramine, nicotine etc. Also down regulation of receptors
  • 15. Summary Remember the different factors modifying drug actions Remember: Young`s formula, Placebo, Cumulation, Tolerance, cross tolerance and Tachyphylaxis Drug use in children, elderly, pregnancy and different pathological states will be discussed individually