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Adverse effects of drugs
Name: Sanjog Bam
Introduction
• It is harmful or seriously unpleasant effects at doses intended for
therapeutic effect and which call for reduction of doses or
withdrawal of the drug and or forecast hazard from future
administration.
• The term adverse drug reaction has been defined as ‘ any noxious
change which is suspected to be due to a drugs, occurs at doses
normally used in man, requires treatment or decreases in dose or
indicates caution in the future use of the same drug’.
(excludes trivial or expected side effects and poisonings or
overdose)
• WHO defination: “An adverse drug reaction is defined as” any
response to a drug that is noxious and unintended and that occurs
at doses used in human for prophylaxis, diagnosis or therapy”
• Adverse effects may develop promptly or only after prolonged
medication or even after stoppage of the drug.
• It is estimated that about 10-20%of hospitalized patient suffers
from adverse effects.
• Adverse effects have been classified in many ways. One
may divide them into:
Type A (predictable or augmented) reactions:
 These are based on the pharmacological properties of the drug.
 Means they are augmented but qualitatively normal response to the drug.
 Include side effects, toxic effects and consequences of drug withdrawal.
 More common (80%), dose related and mostly preventable and reversible.
 Bleeding due to anticoagulants, hypoglycemia due to insulin and sedation
due to antihistamines.
Type B (unpredictable or Bizarre) reactions:
 These are based on peculiarities of the patient and not on drug’s
known action; include allergy and idiosyncrasy.
 Less common, often non-dose related, generally more serious and
require withdrawal of the drug.
 Carry much higher risk of mortality.
 Agranulocytosis due to chloramphenicol, malignant-hyperthermia
due to halothane are examples
Severity of adverse affects:
• Minor reactions:
Minor reaction:
No need of therapy, antidote or prolongation of
hospitalization is required
Moderate reaction:
Requires change in drug therapy
Specific treatment or prolongs hospital stay by at least one
day
Severe reaction:
Potentially life-threatening, causes permanent damage or
requires intensive medical treatment.
Lethal reaction
Directly or indirectly contributes to death of the patient.
Pharmacovigilance
• According to WHO:”it is the science and activities relating to
the detection, assessment, understanding and prevention of
adverse effects or any other drug related problems”.
• The information generated by pharmacovigilance is useful in
educating doctors about ADRs and in the official regulation of
drug used.
• It has an important role in rational use medicines, as it provides
the basis for assessing safety of medicines.
Prevention of ADRs
ADRs can be minimized by observing the following practices:
i. Prescribe the minimum no. of drugs as required to
patients
ii. Avoid all inappropriate use of drugs in the context of
patient’s clinical condition.
iii. Use appropriate drug to right patient in right dose
iv. Elicit and take into consideration previous history of drug
reaction and allergic diseases; exercise caution.
v. Rule out possibility of drug interaction when more than
one drug is prescribed.
vi. Choose correct route of drug administration
vii. Carry out appropriate laboratory monitoring of drug level
in plasma
viii. Prescribe new drugs with caution.
Adverse drug effects may be categorized into
• Side effects :
These are unwanted but often unavoidable
pharmacodynamic effects that occur at therapeutical doses.
They can be predicted from the pharmacological profile of a
drug and are known to occur in a given percentage of drug
recipients.
Reduction in dose generally ameliorates the symptoms.
A side effects may be based on the same action as the
therapeutic effect,
Eg:
 atropine used in preanaesthetic medication for its
antisecretory action. The same action produces dryness of
mouth as a side effect.
 Acetazolamide acts as a diuretic by promoting
bicarbonate excretion. Acidosis occurs as a side effect due
to bicarbonate loss.
 Side effect may also based on a different facet of
action,
 eg promethazine produces sedation which is
unrelated to its anti-allergic action;
Estrogen cause nausea which is unrelated in their anti-
ovulatory action.
 An effect may be therapeutic in one context but
side effect in another context
Codiene used for cough produces constipation as a
side effect but latter is its therapeutic effect in
traveller’s diarrhoe.
Depression of AV conduction is the desired effect of
digoxin in atrial fibrillation, but the same may be
undesirable when it is used for CHF.
• Secondary effects:
These are indirect consequences of primary action of the
drugs, eg:
o Suppression of bacterial flora by tetracyclines paves the way for
superinfections.
o Corticosteriods weaken host defense mechanisms so that latent
tuberculosis gets activated.
• Toxic effects:
o These are the result of excessive pharmacological action of the
drug due to overdosage or prolonged use.
o Overdosage may be absolute(accidental, homicidal, suicidal) or
relative(i.e usual dose of gentamicin in presence of renal failure).
o The effects are predictable and dose related.
o They result from functional alteration (high dose of atropine
causing delirium) or drug induced tissue damaged (hepatic
necrosis from paracetamol overdosage.
o Toxicity may result from extension of the therapeutic eg; coma
by barbiturates, complete AV block by digoxin, bleeding due to
heparin.
• Another action may be responsible for toxicity
Eg: Morphine (analgesic) causes respiratory failure in
overdosage
Imipramine (antidepressant) overdosage causes cardiac
arrhythmia.
streptomycin( anti-tubercular) causes vestibular damage on
prolonged use.
 Intolerance:
– It is the appearance of characteristics toxic effects of a drug in
an individual at therapeutic doses.
– Intolerance means a low threshold to the normal
pharmacodynamic action of drug.
– Eg: single dose of triflupromazine induces muscular dystonias in
some individuals, specially children.
– Only few doses of carbamazepines may cause ataxia in some
people.
– One tablet of chloroquine may cause vomiting and abdominal
pain in an occasional patient.
• Idiosyncrasy:
it is genetically determined abnormal reactivity to
a chemical.
The drug interacts with some unique feature of
the individual , not found in majority of subjects,
and produces the uncharacteristic reaction.
Some idiosyncratic reaction are:
Barbiturates causes excitement and mental confusion
some individuals.
Quinine/quinidine causes cramps, diarrhoea,purpura,
asthma and vascular collapse in some patients.
Chloramphenicol produces nondose-related serious
aplastic anaemia in rare individuals.
• Drug allergy:
– it is an immunologically mediated reaction producing
stereotype symptoms which are unrelated to the
pharmacodynamic profile of the drug.
– Generally occurs even with much smaller doses and
have a different time course of onset and duration.
– This is also called drug hypersensitivity.
– Occurs only in a small proportion of the population
exposed to the drug.
– The drug or its metabolite acts as antigen or more
commonly hapten and produces antibodies/sensitized
lymphocytes.
– One drug can produce different types of allergic
reactions in different individuals, while widely
different drugs can produce the same reaction.
• Photosensitivity: Cutaneous reaction resulting
from drug induced sensitization of the skin to
UV radiation.
• The reactions are of two types:
a. Phototoxic :drug and its metabolites accumulates
in skin and bring phototoxic reaction. Eg:
tetracycline, thiazides, sulfonamides, nalidixic
acid etc
b. Photoallergic: drug or its metabolites induces a
cell mediated immune response which on
exposure to light.eg: sulfonylureas, chloroquine,
sulfonamides, chlorpromazine.
Teratogenicity
• It refers to capacity of a drug to cause foetal
abnormalities when administered to the pregnant
mother.
• Placental barrier unable to inhibit the passage of
some drugs
• Drugs can affect the foetus at 3 stages:
– Fertilization and implantation : conception to
implantation
– Organogenesis: 18- 55 days (most vulnerable)
– Growth and development: 56 days onwards eg:ACE
inhibitors can cause hypoplasia of organs, especially
lungs and NSAIDS may induce premature closure of
ductus arteriosus, methotrexate , warfarin,
thalidomide etc
Drug induced diseases
• Also called iatrogenic (physician induced)
diseases.
• Functional disturbances caused by drugs
which persist even after the offending drug
has been withdrawn and largely eliminated.
• Eg: peptic ulcer by salicylates and
corticosteroid, parkinson’s by phenothiazines
and other antipsychotics, hepatitis by
isoniazide.
pharmacodynamics
• What the drugs does to the body?
• Basic type of drug action can be broadly classifies as:
 Stimulants
 Depression
 Irritation
 Replacement
 Cytotoxic action
• Mechanism of drug action
The fundamental mechanism of drug action can be
distinguished into four categories.
I. Physical action
II. Chemical action
III. Through enzymes
IV. Through receptors
Drug –response relationship:
• When a drug is administered systemically, the dose response
relationship has two component:
i. Dose-plasma concentration relationship
ii. Plasma concentration –response relationship
• The first one is determined by pharmacokinetic
considerations and ordinarily descriptions of dose-response
relationship refers to the latter one.
• Generally, the intensity of response increase with increase in
dose and dose-response curve is a rectangular hyperbola
This is because drug receptor interaction obeys
law of mass action, accordingly-
E =Emax X [D]
KD [D]
Where E= observed effect at a dose[D] of the drug
Emax= maximal response
KD =dissociation constant of the drug- receptor complex
which is equal to the dose of drug at which half
maximal response is produced.
Advantages of plotting log dose-response curve
A wide range of drug doses can be easily displayed on a graph
Comparison between agonist and study of antagonists becomes easier.
• Drug potency= it refers to the amount of drug
needed to produce a certain response.
Relative potency is often more meaningful than
absolute potency.
Eg: if 10 mg of morphine= 100 mg of pethidine,
morphine is 10 times more potent than pethidine
• Drug efficacy: it refers to the maximal response
that can be elicited by the drug.
eg: morphine produces a degree of analgesia
not obtained with any dose of aspirin. Morphine
is more efficacious than aspirin.
COMBINED EFFECT OF DRUGS
• Synergism:
when the action of one drug is facilitated or increased by
the other, they are said to be synergism.
In a synergistic pair both the drugs can have action in the
same direction or given alone one may be inactive but still
enhance the action of the other when given together.
Synergism can be:
i. Additive : The effects of the two drugs are in the same
direction and simply add up.
Effect of drug A+B = effect of drug A + effect of drug B
ii. Supradditive(potentiation). The effect of combination
is greater than the individual effects of the
components:
effect of drug A+ B>effect of drug A + effect of drug B.
• Additive synergism:
• Supradditive synergism:
Aspirin + paracetamol As analgesic/antipyretic
Nitrous oxide + halothane As general anaesthetic
Amlodipine +atenolol As antihypertensive
Glibenclamide+ metformin As hypoglycaemia
Ephedrine + theophylline As bronchodilator
Acetylcholine + physostigmine Inhibition of break down
Levodopa + carbidopa/benserazide Inhibition of peripheral metabolism
Adrenaline + cocaine/desipramine Inhibition of neuronal uptake
Enalapril + hydrochlorothiazide
(anti-hypertensive)
Tackling two contributory factors
Sulfamethoxazole + trimethoprim Sequential blockade
ANTOGONISM:
• When one drug decreases or abolishes the action of
another, they are said to antagonistic.
• On the basis of mechanism ,antagonistic may be :
1. Physical antagonism:
 Based on the physical properties of drug.
 Eg: charcoal adsorbs alkaloids and can prevent their
absorption- used in alkaloid poisonings.
2. Chemical antagonism:
one chemical reacts with others forming inactive complex
products.
 KMn04 oxidizes alkaloids- used for gastric lavage in poisoning
 Tannins + alkaloids – insoluble alkaloidal tannate is formed.
 Chelating agents (BAL, EDTA,Cal. Disod. edetate) complex toxic
metals (As, Pb).
 Nitrates form methaemoglobin which reacts with cyanide
radical.
3. Physiological / functional antagonism:
the two drugs acts by the different receptor or way
but shows just opposite pharmacological action in
same physiological aspect.
Histamine and adrenaline in bronchus muscle and BP
Thiazides and triameterene in K+ exceretion.
Glucagon and insulin in blood sugar level.
4. Receptor antagonism:
one drug(antagonist) blocks the receptor action of
the other (agonist)
 Ach ----atropine
Morphine----naloxone
Diazepam----bicuculline
Therapeutic index
• The therapeutic index of a drug is the ratio of
the dose that produces toxicity to the dose
that produces a clinically desired or effective
response in a population of individuals.
• Therapeutic index= toxic dose/effective dose
• The therapeutic index is thus a measure of the
drug’s safety since a large value indicates that
there is a wide margin between doses that
are elective and doses that are toxic.

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ADVERSE EFFECTS OF DRUGS

  • 1. Adverse effects of drugs Name: Sanjog Bam
  • 2. Introduction • It is harmful or seriously unpleasant effects at doses intended for therapeutic effect and which call for reduction of doses or withdrawal of the drug and or forecast hazard from future administration. • The term adverse drug reaction has been defined as ‘ any noxious change which is suspected to be due to a drugs, occurs at doses normally used in man, requires treatment or decreases in dose or indicates caution in the future use of the same drug’. (excludes trivial or expected side effects and poisonings or overdose) • WHO defination: “An adverse drug reaction is defined as” any response to a drug that is noxious and unintended and that occurs at doses used in human for prophylaxis, diagnosis or therapy” • Adverse effects may develop promptly or only after prolonged medication or even after stoppage of the drug. • It is estimated that about 10-20%of hospitalized patient suffers from adverse effects.
  • 3. • Adverse effects have been classified in many ways. One may divide them into: Type A (predictable or augmented) reactions:  These are based on the pharmacological properties of the drug.  Means they are augmented but qualitatively normal response to the drug.  Include side effects, toxic effects and consequences of drug withdrawal.  More common (80%), dose related and mostly preventable and reversible.  Bleeding due to anticoagulants, hypoglycemia due to insulin and sedation due to antihistamines. Type B (unpredictable or Bizarre) reactions:  These are based on peculiarities of the patient and not on drug’s known action; include allergy and idiosyncrasy.  Less common, often non-dose related, generally more serious and require withdrawal of the drug.  Carry much higher risk of mortality.  Agranulocytosis due to chloramphenicol, malignant-hyperthermia due to halothane are examples
  • 4. Severity of adverse affects: • Minor reactions: Minor reaction: No need of therapy, antidote or prolongation of hospitalization is required Moderate reaction: Requires change in drug therapy Specific treatment or prolongs hospital stay by at least one day Severe reaction: Potentially life-threatening, causes permanent damage or requires intensive medical treatment. Lethal reaction Directly or indirectly contributes to death of the patient.
  • 5. Pharmacovigilance • According to WHO:”it is the science and activities relating to the detection, assessment, understanding and prevention of adverse effects or any other drug related problems”. • The information generated by pharmacovigilance is useful in educating doctors about ADRs and in the official regulation of drug used. • It has an important role in rational use medicines, as it provides the basis for assessing safety of medicines.
  • 6. Prevention of ADRs ADRs can be minimized by observing the following practices: i. Prescribe the minimum no. of drugs as required to patients ii. Avoid all inappropriate use of drugs in the context of patient’s clinical condition. iii. Use appropriate drug to right patient in right dose iv. Elicit and take into consideration previous history of drug reaction and allergic diseases; exercise caution. v. Rule out possibility of drug interaction when more than one drug is prescribed. vi. Choose correct route of drug administration vii. Carry out appropriate laboratory monitoring of drug level in plasma viii. Prescribe new drugs with caution.
  • 7. Adverse drug effects may be categorized into • Side effects : These are unwanted but often unavoidable pharmacodynamic effects that occur at therapeutical doses. They can be predicted from the pharmacological profile of a drug and are known to occur in a given percentage of drug recipients. Reduction in dose generally ameliorates the symptoms. A side effects may be based on the same action as the therapeutic effect, Eg:  atropine used in preanaesthetic medication for its antisecretory action. The same action produces dryness of mouth as a side effect.  Acetazolamide acts as a diuretic by promoting bicarbonate excretion. Acidosis occurs as a side effect due to bicarbonate loss.
  • 8.  Side effect may also based on a different facet of action,  eg promethazine produces sedation which is unrelated to its anti-allergic action; Estrogen cause nausea which is unrelated in their anti- ovulatory action.  An effect may be therapeutic in one context but side effect in another context Codiene used for cough produces constipation as a side effect but latter is its therapeutic effect in traveller’s diarrhoe. Depression of AV conduction is the desired effect of digoxin in atrial fibrillation, but the same may be undesirable when it is used for CHF.
  • 9. • Secondary effects: These are indirect consequences of primary action of the drugs, eg: o Suppression of bacterial flora by tetracyclines paves the way for superinfections. o Corticosteriods weaken host defense mechanisms so that latent tuberculosis gets activated. • Toxic effects: o These are the result of excessive pharmacological action of the drug due to overdosage or prolonged use. o Overdosage may be absolute(accidental, homicidal, suicidal) or relative(i.e usual dose of gentamicin in presence of renal failure). o The effects are predictable and dose related. o They result from functional alteration (high dose of atropine causing delirium) or drug induced tissue damaged (hepatic necrosis from paracetamol overdosage. o Toxicity may result from extension of the therapeutic eg; coma by barbiturates, complete AV block by digoxin, bleeding due to heparin.
  • 10. • Another action may be responsible for toxicity Eg: Morphine (analgesic) causes respiratory failure in overdosage Imipramine (antidepressant) overdosage causes cardiac arrhythmia. streptomycin( anti-tubercular) causes vestibular damage on prolonged use.  Intolerance: – It is the appearance of characteristics toxic effects of a drug in an individual at therapeutic doses. – Intolerance means a low threshold to the normal pharmacodynamic action of drug. – Eg: single dose of triflupromazine induces muscular dystonias in some individuals, specially children. – Only few doses of carbamazepines may cause ataxia in some people. – One tablet of chloroquine may cause vomiting and abdominal pain in an occasional patient.
  • 11. • Idiosyncrasy: it is genetically determined abnormal reactivity to a chemical. The drug interacts with some unique feature of the individual , not found in majority of subjects, and produces the uncharacteristic reaction. Some idiosyncratic reaction are: Barbiturates causes excitement and mental confusion some individuals. Quinine/quinidine causes cramps, diarrhoea,purpura, asthma and vascular collapse in some patients. Chloramphenicol produces nondose-related serious aplastic anaemia in rare individuals.
  • 12. • Drug allergy: – it is an immunologically mediated reaction producing stereotype symptoms which are unrelated to the pharmacodynamic profile of the drug. – Generally occurs even with much smaller doses and have a different time course of onset and duration. – This is also called drug hypersensitivity. – Occurs only in a small proportion of the population exposed to the drug. – The drug or its metabolite acts as antigen or more commonly hapten and produces antibodies/sensitized lymphocytes. – One drug can produce different types of allergic reactions in different individuals, while widely different drugs can produce the same reaction.
  • 13. • Photosensitivity: Cutaneous reaction resulting from drug induced sensitization of the skin to UV radiation. • The reactions are of two types: a. Phototoxic :drug and its metabolites accumulates in skin and bring phototoxic reaction. Eg: tetracycline, thiazides, sulfonamides, nalidixic acid etc b. Photoallergic: drug or its metabolites induces a cell mediated immune response which on exposure to light.eg: sulfonylureas, chloroquine, sulfonamides, chlorpromazine.
  • 14. Teratogenicity • It refers to capacity of a drug to cause foetal abnormalities when administered to the pregnant mother. • Placental barrier unable to inhibit the passage of some drugs • Drugs can affect the foetus at 3 stages: – Fertilization and implantation : conception to implantation – Organogenesis: 18- 55 days (most vulnerable) – Growth and development: 56 days onwards eg:ACE inhibitors can cause hypoplasia of organs, especially lungs and NSAIDS may induce premature closure of ductus arteriosus, methotrexate , warfarin, thalidomide etc
  • 15. Drug induced diseases • Also called iatrogenic (physician induced) diseases. • Functional disturbances caused by drugs which persist even after the offending drug has been withdrawn and largely eliminated. • Eg: peptic ulcer by salicylates and corticosteroid, parkinson’s by phenothiazines and other antipsychotics, hepatitis by isoniazide.
  • 16. pharmacodynamics • What the drugs does to the body? • Basic type of drug action can be broadly classifies as:  Stimulants  Depression  Irritation  Replacement  Cytotoxic action • Mechanism of drug action The fundamental mechanism of drug action can be distinguished into four categories. I. Physical action II. Chemical action III. Through enzymes IV. Through receptors
  • 17. Drug –response relationship: • When a drug is administered systemically, the dose response relationship has two component: i. Dose-plasma concentration relationship ii. Plasma concentration –response relationship • The first one is determined by pharmacokinetic considerations and ordinarily descriptions of dose-response relationship refers to the latter one. • Generally, the intensity of response increase with increase in dose and dose-response curve is a rectangular hyperbola This is because drug receptor interaction obeys law of mass action, accordingly- E =Emax X [D] KD [D] Where E= observed effect at a dose[D] of the drug Emax= maximal response KD =dissociation constant of the drug- receptor complex which is equal to the dose of drug at which half maximal response is produced.
  • 18. Advantages of plotting log dose-response curve A wide range of drug doses can be easily displayed on a graph Comparison between agonist and study of antagonists becomes easier.
  • 19. • Drug potency= it refers to the amount of drug needed to produce a certain response. Relative potency is often more meaningful than absolute potency. Eg: if 10 mg of morphine= 100 mg of pethidine, morphine is 10 times more potent than pethidine • Drug efficacy: it refers to the maximal response that can be elicited by the drug. eg: morphine produces a degree of analgesia not obtained with any dose of aspirin. Morphine is more efficacious than aspirin.
  • 20. COMBINED EFFECT OF DRUGS • Synergism: when the action of one drug is facilitated or increased by the other, they are said to be synergism. In a synergistic pair both the drugs can have action in the same direction or given alone one may be inactive but still enhance the action of the other when given together. Synergism can be: i. Additive : The effects of the two drugs are in the same direction and simply add up. Effect of drug A+B = effect of drug A + effect of drug B ii. Supradditive(potentiation). The effect of combination is greater than the individual effects of the components: effect of drug A+ B>effect of drug A + effect of drug B.
  • 21. • Additive synergism: • Supradditive synergism: Aspirin + paracetamol As analgesic/antipyretic Nitrous oxide + halothane As general anaesthetic Amlodipine +atenolol As antihypertensive Glibenclamide+ metformin As hypoglycaemia Ephedrine + theophylline As bronchodilator Acetylcholine + physostigmine Inhibition of break down Levodopa + carbidopa/benserazide Inhibition of peripheral metabolism Adrenaline + cocaine/desipramine Inhibition of neuronal uptake Enalapril + hydrochlorothiazide (anti-hypertensive) Tackling two contributory factors Sulfamethoxazole + trimethoprim Sequential blockade
  • 22. ANTOGONISM: • When one drug decreases or abolishes the action of another, they are said to antagonistic. • On the basis of mechanism ,antagonistic may be : 1. Physical antagonism:  Based on the physical properties of drug.  Eg: charcoal adsorbs alkaloids and can prevent their absorption- used in alkaloid poisonings. 2. Chemical antagonism: one chemical reacts with others forming inactive complex products.  KMn04 oxidizes alkaloids- used for gastric lavage in poisoning  Tannins + alkaloids – insoluble alkaloidal tannate is formed.  Chelating agents (BAL, EDTA,Cal. Disod. edetate) complex toxic metals (As, Pb).  Nitrates form methaemoglobin which reacts with cyanide radical.
  • 23. 3. Physiological / functional antagonism: the two drugs acts by the different receptor or way but shows just opposite pharmacological action in same physiological aspect. Histamine and adrenaline in bronchus muscle and BP Thiazides and triameterene in K+ exceretion. Glucagon and insulin in blood sugar level. 4. Receptor antagonism: one drug(antagonist) blocks the receptor action of the other (agonist)  Ach ----atropine Morphine----naloxone Diazepam----bicuculline
  • 24. Therapeutic index • The therapeutic index of a drug is the ratio of the dose that produces toxicity to the dose that produces a clinically desired or effective response in a population of individuals. • Therapeutic index= toxic dose/effective dose • The therapeutic index is thus a measure of the drug’s safety since a large value indicates that there is a wide margin between doses that are elective and doses that are toxic.