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Drug Excretion
Dr Naser Ashraf Tadvi
Associate Professor
Drug elimination
Metabolism
(Biotransformation)
Excretion+
Biotransformation
• “ Chemical alteration of the
drug in the body.”
Converts non polar
(lipid soluble)
substances
In to polar (lipid
insoluble)
substance
No reabsorption in
renal tubules
Excretion in urine
Excretion
• Excretion is the passage out of
systemically administered drugs.
• Removal of the drug and its metabolite
from body is known as drug excretion
Routes of drug excretion
Major
• Renal
• Biliary
• Fecal
• Alveolar
Minor
• Skin
• Saliva
• Sweat
• Hair
• Milk
KIDNEY
• Most common for majority of the drugs.
• Excretes water soluble substances.
• Renal excretion determined by 3 processes:
– Glomerular filtration
– Tubular reabsorption
– Tubular secretion
• NET RENAL EXCRETION = (Glomerular filtration +
Tubular secretion ) – (tubular reabsorption )
Glomerular Filtration
• Glomerular capillaries have large pores.
• All FREE drugs (lipid soluble or insoluble) are filtered
through it.
• Glomerular filtration depend upon …
• Molecular size
• Plasma protein binding
• Renal blood flow.
• Normal GFR is 120 ml/min
Tubular reabsorption
• Occurs by passive diffusion and depends on
– Lipid solubility
– pKa of drug
– pH of urine
• pH of urine
– pH of urine is Acidic so generally weakly acidic drugs have
more chance of reabsorption
– Sodium bicarbonate used in Salicylate and barbiturate
poisoning to alkalinize urine
– Ascorbic acid can be used to ↑ excretion of Morphine
Tubular secretion
• Energy requiring carrier mediated active
transport
– OAT and OCT at proximal tubules.
– P-gp and MRP2 are located in the luminal
membrane of proximal tubular cells.
– ORGANIC ACID TRANSPORT (OAT) :
• Penicillin, probenecid, uric acid, salicylates,
indomethacin
– ORGANIC BASE TRANSPORT (OCT) :
• Morphine, quinidine, Procaine, Thiazides, furosemide
Drug interactions due to competition of
tubular secretion
• Probenecid
– Organic acid which has high affinity for the tubular OATP.
– Blocks the active transport of both penicillin and uric acid.
• Aspirin ↓ tubular secretion of methotrexate
• Quinidine inhibits p-glycoprotein and ↓ renal
and biliary clearance of digoxin
Penicillin is
exogenous
substance
Primarily undergoes
tubular secretion
so excreted
Probenecid
prevents this
RETAINED IN THE
BODY.
Uric acid is
endogenous
substance
Primarily undergoes
tubular reabsorption
so retained
Probenecid
prevents this
EXCRETED FROM THE
BODY.
Renal Elimination can enhanced by..
• Diuretics which increases the urine flow.
• Adjusting the pH of urine. How ?
Biliary excretion and enterohepatic
circulation
• Liver cells also transport various drugs and
endogenous substances like bilirubin from
plasma to bile using OATP and OCT
• Relatively larger Mol. weight drugs > 300
eliminated in bile
• Most of free drug in gut, including which is
released by deconjugation of glucuronides by
enteric bacteria are reabsorbed by Entero
hepatic circulation
Enterohepatic circulation
Enterohepatic
circulation
Drug enters
intestine
Absorbed in
portal blood
Reaches
liver
Taken by
hepatocytes
Excreted in
bile
Major fraction
gets excreted
Minor
fraction
reenters
circulation
So
increase
in
bioavailab
ility
Drugs undergoing enterohepatic
circulation
• Ampicillin
• Rifampicin
• Estrogen
• Morphine
• Doxycycline
• Cefoperazone
Faecal excretion
• Orally administered drugs that are
unabsorbed → excreted in feces
• Example
– streptomycin, neomycin, cholestyramine.
• Some drugs are expelled in expired air.
• Volatile General anaesthetics
• Alcohol
• Paraldehyde It is important from
medico legal
perspective because
presence of alcohol in
breath stamps that a
person has jumped
legal boundary !!!
Only 5 % of alcohol is
excreted in expired air. So
not important from
pharmacological or medical
point of view.
Entry through
inspiration
Exit through
expiration !!!
Alveolar excretion
Skin, Sweat, Saliva, Hair
• Skin:
o Arsenic and heavy metals like mercury gets
excreted in skin.
o Griseofulvin secreted through keratin precursor
cells
• Hair follicles: Arsenic, iodides, mercury salts
• Saliva: Iodine, potassium iodide, lithium,
phenytoin
• Sweat: Rifampicin, Amines, urea derivatives
Milk
• Most drugs enter breast milk by passive diffusion
• More lipid soluble and less protein bound drugs are
better concentrated in milk.
• “Basic drugs”are more concentrated in it as pH of
milk is acidic 6.8 -7.0
Drug
administered to
mother
Enters breast
milk
Reaches breast
feeding infant
May produce
effect on infant
Drugs in lactation
• Total amount of drug reaching infant through
milk is small and majority drugs have no
significant effect on infant.
• In infants → slower elimination → cumulation
may occur when baby receives it with frequent
breast feeding.
• Drugs should be administered only when
indicated and safe drugs should be used
• Safe drugs: Antacids, iron salts, paracetamol,
insulin, salbutamol , cephalosporin
Examples of drugs contraindicated in
lactation
• Radioactive iodine administered to mother →
reach the infant in breast milk → fetal goitre.
• Avoid chloramphenicol, tetracycline,
sulfonamides.
• Ergotamine → may cause ergotism.
• Chloroquine for rheumatoid arthritis → retinal
damage in infant.
• Cytotoxic drugs are absolutely contraindicated.
• If a drug is acidic in nature
• If a drug is alkaline in nature
• Some drugs are excreted unchanged in urine….so
in case of renal failure…
• Drugs, metabolites and toxins are excreted in the
urine →
How excretion pattern affects the therapeutic
effect…….
Its excretion can be
enhanced by
alkalinizing it.
Its excretion can be
enhanced by
acidifying it.
It is accumulated in
the body and
produces ADR.
So frequently
produces
nephrotoxicity
Drug excretion new

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Drug excretion new

  • 1. Drug Excretion Dr Naser Ashraf Tadvi Associate Professor
  • 3. Biotransformation • “ Chemical alteration of the drug in the body.” Converts non polar (lipid soluble) substances In to polar (lipid insoluble) substance No reabsorption in renal tubules Excretion in urine
  • 4. Excretion • Excretion is the passage out of systemically administered drugs. • Removal of the drug and its metabolite from body is known as drug excretion
  • 5. Routes of drug excretion Major • Renal • Biliary • Fecal • Alveolar Minor • Skin • Saliva • Sweat • Hair • Milk
  • 6. KIDNEY • Most common for majority of the drugs. • Excretes water soluble substances. • Renal excretion determined by 3 processes: – Glomerular filtration – Tubular reabsorption – Tubular secretion • NET RENAL EXCRETION = (Glomerular filtration + Tubular secretion ) – (tubular reabsorption )
  • 7. Glomerular Filtration • Glomerular capillaries have large pores. • All FREE drugs (lipid soluble or insoluble) are filtered through it. • Glomerular filtration depend upon … • Molecular size • Plasma protein binding • Renal blood flow. • Normal GFR is 120 ml/min
  • 8. Tubular reabsorption • Occurs by passive diffusion and depends on – Lipid solubility – pKa of drug – pH of urine • pH of urine – pH of urine is Acidic so generally weakly acidic drugs have more chance of reabsorption – Sodium bicarbonate used in Salicylate and barbiturate poisoning to alkalinize urine – Ascorbic acid can be used to ↑ excretion of Morphine
  • 9. Tubular secretion • Energy requiring carrier mediated active transport – OAT and OCT at proximal tubules. – P-gp and MRP2 are located in the luminal membrane of proximal tubular cells. – ORGANIC ACID TRANSPORT (OAT) : • Penicillin, probenecid, uric acid, salicylates, indomethacin – ORGANIC BASE TRANSPORT (OCT) : • Morphine, quinidine, Procaine, Thiazides, furosemide
  • 10. Drug interactions due to competition of tubular secretion • Probenecid – Organic acid which has high affinity for the tubular OATP. – Blocks the active transport of both penicillin and uric acid. • Aspirin ↓ tubular secretion of methotrexate • Quinidine inhibits p-glycoprotein and ↓ renal and biliary clearance of digoxin
  • 11. Penicillin is exogenous substance Primarily undergoes tubular secretion so excreted Probenecid prevents this RETAINED IN THE BODY. Uric acid is endogenous substance Primarily undergoes tubular reabsorption so retained Probenecid prevents this EXCRETED FROM THE BODY.
  • 12. Renal Elimination can enhanced by.. • Diuretics which increases the urine flow. • Adjusting the pH of urine. How ?
  • 13. Biliary excretion and enterohepatic circulation • Liver cells also transport various drugs and endogenous substances like bilirubin from plasma to bile using OATP and OCT • Relatively larger Mol. weight drugs > 300 eliminated in bile • Most of free drug in gut, including which is released by deconjugation of glucuronides by enteric bacteria are reabsorbed by Entero hepatic circulation
  • 14. Enterohepatic circulation Enterohepatic circulation Drug enters intestine Absorbed in portal blood Reaches liver Taken by hepatocytes Excreted in bile Major fraction gets excreted Minor fraction reenters circulation So increase in bioavailab ility
  • 15. Drugs undergoing enterohepatic circulation • Ampicillin • Rifampicin • Estrogen • Morphine • Doxycycline • Cefoperazone
  • 16. Faecal excretion • Orally administered drugs that are unabsorbed → excreted in feces • Example – streptomycin, neomycin, cholestyramine.
  • 17. • Some drugs are expelled in expired air. • Volatile General anaesthetics • Alcohol • Paraldehyde It is important from medico legal perspective because presence of alcohol in breath stamps that a person has jumped legal boundary !!! Only 5 % of alcohol is excreted in expired air. So not important from pharmacological or medical point of view. Entry through inspiration Exit through expiration !!! Alveolar excretion
  • 18. Skin, Sweat, Saliva, Hair • Skin: o Arsenic and heavy metals like mercury gets excreted in skin. o Griseofulvin secreted through keratin precursor cells • Hair follicles: Arsenic, iodides, mercury salts • Saliva: Iodine, potassium iodide, lithium, phenytoin • Sweat: Rifampicin, Amines, urea derivatives
  • 19. Milk • Most drugs enter breast milk by passive diffusion • More lipid soluble and less protein bound drugs are better concentrated in milk. • “Basic drugs”are more concentrated in it as pH of milk is acidic 6.8 -7.0 Drug administered to mother Enters breast milk Reaches breast feeding infant May produce effect on infant
  • 20. Drugs in lactation • Total amount of drug reaching infant through milk is small and majority drugs have no significant effect on infant. • In infants → slower elimination → cumulation may occur when baby receives it with frequent breast feeding. • Drugs should be administered only when indicated and safe drugs should be used • Safe drugs: Antacids, iron salts, paracetamol, insulin, salbutamol , cephalosporin
  • 21. Examples of drugs contraindicated in lactation • Radioactive iodine administered to mother → reach the infant in breast milk → fetal goitre. • Avoid chloramphenicol, tetracycline, sulfonamides. • Ergotamine → may cause ergotism. • Chloroquine for rheumatoid arthritis → retinal damage in infant. • Cytotoxic drugs are absolutely contraindicated.
  • 22. • If a drug is acidic in nature • If a drug is alkaline in nature • Some drugs are excreted unchanged in urine….so in case of renal failure… • Drugs, metabolites and toxins are excreted in the urine → How excretion pattern affects the therapeutic effect……. Its excretion can be enhanced by alkalinizing it. Its excretion can be enhanced by acidifying it. It is accumulated in the body and produces ADR. So frequently produces nephrotoxicity