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Excretion of Drugs
By the end of this lecture, students should be able
to
 Identify main and minor routes of Excretion including
renal elimination and biliary excretion
 Describe enterohepatic circulation and its
consequences on duration of drugs.
 Describe some pharmacokinetics terms including
clearance of drugs.
 Biological half-life (t ½), multiple dosing, steady state
levels, maintenance dose and Loading dose.
Routes of Excretion
Main Routes of Excretion
 Renal Excretion
 Biliary Excretion
Minor Routes of Excretion.
 Exhaled air (Exhalation)
 Salivary
 Sweat
 Milk
 Tears
Renal Excretion
Structure of kidney
The structure unit of kidney is nephron
That consists of :
 Glomerulus
 Proximal convoluted tubules
 Loop of Henle
 Distal convoluted tubules
 Collecting ducts
Kidney
Renal Excretion includes
 Glomerular filtration.
 Passive tubular reabsorption.
 Active tubular secretion.
Polar drug= water soluble
Non polar drug = lipid soluble
Glomerular filtration (GFR):
 Depends upon renal blood flow (600 ml/min)
 GFR 20% of renal blood flow = 125 ml/min.
 Glomerular filtration occurs to
 Low molecular weight drugs
 Only free drugs (unbound to plasma proteins)
are filtered.
Active Tubular Secretion:
 occurs mainly in proximal tubules; increases
drug concentration in lumen
 organic anionic and cationic transporters
mediate active secretion of anioinc and
cationic drugs.
 can transport drugs against concentration
gradients.
 Penicillin is an example of actively secreted
drug.
System for Acidic drugs.
 Salicylates
 Sulphonamides
 Penicillin
Transport of acidic drugs is blocked by
probenecid
System for Basic drugs
 Morphine
 Atropine
 Quinine
 Neostigmine
Passive Tubular Re-absorption
 In distal convoluted tubules & collecting ducts.
 Passive diffusion of unionized, lipophilic drugs
 Lipophilic drugs can be reabsorbed back into
blood circulation and excretion in urine will be
low.
 Ionized drugs are poorly reabsorbed & so
urinary excretion will be high.
Urinary pH trapping (Ion trapping)
 Changing pH of urine by chemicals can inhibit or
enhance the tubular drug reabsorption back into
blood.
 Ion trapping is used to enhance renal clearance
of drugs during toxicity.
 Urine is normally slightly acidic and favors
excretion of basic drugs.
Urinary pH trapping (Ion trapping)
 Acidification of urine using ammonium chloride
(NH4Cl) increases excretion of basic drugs as
amphetamine.
 Alkalization of urine using sodium bicarbonate
NaHCO3 increases excretion of acidic drugs as
aspirin.
Renal Excretion
Drugs excreted mainly by the kidney include:
 Aminoglycosides antibiotics (as gentamycin)
 Penicillin
 Lithium
These drugs are should be prescribed carefully
in
 patients with renal disease.
 Elderly people
Biliary Excretion
 Occurs to few drugs that are excreted into feces.
 Such drugs are secreted from the liver into bile
by active transporters, then into duodenum.
 Some drugs undergo enterohepatic circulation
back into systemic blood circulation.
Enterohepatic circulation
 Drugs excreted in the bile in the form of
glucouronides will be hydrolyzed in intestine
by bacterial flora liberating free drugs that
can be reabsorbed back into blood if lipid
soluble.
 This prolongs the duration of action of drugs
e.g. digoxin, morphine, thyroxine.
Plasma half-life (t ½)
 is the time required for the plasma
concentration of a drug to fall to half.
 Is a measure of duration of action.
 Determine the dosing interval
Drugs of short plasma half life
 Penicillin, tubocurarine.
Drugs of long plasma half life
 Digoxin, thyroxine, arsenic.
Factors that may increase half-life (t ½ )
Decreased metabolism
 Liver disease.
 Microsomal inhibitors.
Decreased clearance
 Renal disease.
 Congestive heart failure.
High binding of drugs
 Plasma proteins.
 Tissue binding.
Enterohepatic recycling
Loading dose
 is the large initial dose that is given to achieve
rapid therapeutic plasma level.
 After administration of the drug, the plasma
concentration decreases due to distribution of
drug to other tissues.
 These doses balances the drug distribution.
Maintenance doses
 are the doses required to maintain the
therapeutic level of the drug constant or the
steady state of the drug.
 These doses balance the amount of drug lost
during metabolism and clearance.
 The patient needs to take regular doses of a
drug such as amoxicillin ( 500 mg) 8 hourly to
maintain the therapeutic level.
Steady state levels.
 A state at which the therapeutic plasma
concentration of the drug remains constant with
the therapeutic window (the range between
effective and toxic levels of drugs).
 rate of drug administration = rate of drug
elimination
Therapeutic window
Steady state levels
Steady state of a drug
Summary
 Polar drugs are readily excreted and poorly
reabsorbed.
 Lipid soluble drugs are reabsorbed back and
excretion will be low
 Acidic drugs are best excreted in alkaline urine
(sodium bicarbonate).
 Basic drugs are best excreted in acidic urine
(ammonium chloride).
 Enterohepatic circulation prolongs half life of the
drug.
Questions?

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Pharmacokinetics.ppt

  • 1. Excretion of Drugs By the end of this lecture, students should be able to  Identify main and minor routes of Excretion including renal elimination and biliary excretion  Describe enterohepatic circulation and its consequences on duration of drugs.  Describe some pharmacokinetics terms including clearance of drugs.  Biological half-life (t ½), multiple dosing, steady state levels, maintenance dose and Loading dose.
  • 2. Routes of Excretion Main Routes of Excretion  Renal Excretion  Biliary Excretion Minor Routes of Excretion.  Exhaled air (Exhalation)  Salivary  Sweat  Milk  Tears
  • 3. Renal Excretion Structure of kidney The structure unit of kidney is nephron That consists of :  Glomerulus  Proximal convoluted tubules  Loop of Henle  Distal convoluted tubules  Collecting ducts
  • 5. Renal Excretion includes  Glomerular filtration.  Passive tubular reabsorption.  Active tubular secretion.
  • 6.
  • 7. Polar drug= water soluble Non polar drug = lipid soluble
  • 8. Glomerular filtration (GFR):  Depends upon renal blood flow (600 ml/min)  GFR 20% of renal blood flow = 125 ml/min.  Glomerular filtration occurs to  Low molecular weight drugs  Only free drugs (unbound to plasma proteins) are filtered.
  • 9. Active Tubular Secretion:  occurs mainly in proximal tubules; increases drug concentration in lumen  organic anionic and cationic transporters mediate active secretion of anioinc and cationic drugs.  can transport drugs against concentration gradients.  Penicillin is an example of actively secreted drug.
  • 10. System for Acidic drugs.  Salicylates  Sulphonamides  Penicillin Transport of acidic drugs is blocked by probenecid System for Basic drugs  Morphine  Atropine  Quinine  Neostigmine
  • 11. Passive Tubular Re-absorption  In distal convoluted tubules & collecting ducts.  Passive diffusion of unionized, lipophilic drugs  Lipophilic drugs can be reabsorbed back into blood circulation and excretion in urine will be low.  Ionized drugs are poorly reabsorbed & so urinary excretion will be high.
  • 12. Urinary pH trapping (Ion trapping)  Changing pH of urine by chemicals can inhibit or enhance the tubular drug reabsorption back into blood.  Ion trapping is used to enhance renal clearance of drugs during toxicity.  Urine is normally slightly acidic and favors excretion of basic drugs.
  • 13. Urinary pH trapping (Ion trapping)  Acidification of urine using ammonium chloride (NH4Cl) increases excretion of basic drugs as amphetamine.  Alkalization of urine using sodium bicarbonate NaHCO3 increases excretion of acidic drugs as aspirin.
  • 14. Renal Excretion Drugs excreted mainly by the kidney include:  Aminoglycosides antibiotics (as gentamycin)  Penicillin  Lithium These drugs are should be prescribed carefully in  patients with renal disease.  Elderly people
  • 15. Biliary Excretion  Occurs to few drugs that are excreted into feces.  Such drugs are secreted from the liver into bile by active transporters, then into duodenum.  Some drugs undergo enterohepatic circulation back into systemic blood circulation.
  • 16. Enterohepatic circulation  Drugs excreted in the bile in the form of glucouronides will be hydrolyzed in intestine by bacterial flora liberating free drugs that can be reabsorbed back into blood if lipid soluble.  This prolongs the duration of action of drugs e.g. digoxin, morphine, thyroxine.
  • 17.
  • 18. Plasma half-life (t ½)  is the time required for the plasma concentration of a drug to fall to half.  Is a measure of duration of action.  Determine the dosing interval Drugs of short plasma half life  Penicillin, tubocurarine. Drugs of long plasma half life  Digoxin, thyroxine, arsenic.
  • 19. Factors that may increase half-life (t ½ ) Decreased metabolism  Liver disease.  Microsomal inhibitors. Decreased clearance  Renal disease.  Congestive heart failure. High binding of drugs  Plasma proteins.  Tissue binding. Enterohepatic recycling
  • 20. Loading dose  is the large initial dose that is given to achieve rapid therapeutic plasma level.  After administration of the drug, the plasma concentration decreases due to distribution of drug to other tissues.  These doses balances the drug distribution.
  • 21. Maintenance doses  are the doses required to maintain the therapeutic level of the drug constant or the steady state of the drug.  These doses balance the amount of drug lost during metabolism and clearance.  The patient needs to take regular doses of a drug such as amoxicillin ( 500 mg) 8 hourly to maintain the therapeutic level.
  • 22. Steady state levels.  A state at which the therapeutic plasma concentration of the drug remains constant with the therapeutic window (the range between effective and toxic levels of drugs).  rate of drug administration = rate of drug elimination
  • 25. Steady state of a drug
  • 26. Summary  Polar drugs are readily excreted and poorly reabsorbed.  Lipid soluble drugs are reabsorbed back and excretion will be low  Acidic drugs are best excreted in alkaline urine (sodium bicarbonate).  Basic drugs are best excreted in acidic urine (ammonium chloride).  Enterohepatic circulation prolongs half life of the drug.