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TOXICITY OF AMINOGLYCOSIDE ANTIBIOTICS
INTRODUCTION
• Group of natural and semisynthetic antibiotics.
• Amino sugar + aminocyclitol via glycoside bond.
• Streptomycin – 1st discovered – 1944 – Waksman &
  co-workers from Streptomyces griseus ( actinobacterium )
• Amikacin – 1st semi synthetic – from Kanamycin
• Bactericidal drug – Inhibit protein synthesis –
  Formation of aberrant proteins – streptomycin (bind
  with 30S subunit) – others (bind with 50S subunit) –
  Bacteria more permeable – leakage – cell death
• Excellent water solubility – Poor lipid soluble.
• Nephrotoxicity – due to increased no: of amino groups
     Eg :- Neomycin – 6 amino group – more toxic
           Streptomycin – 3 amino group – less toxic
• They are not absorbed from the gut. So I/m or I/v

• Uses : Local & Systemic infection – Mainly Gram –ve

• In Vet practice, Neomycin – toxic – so topical only

               Gentamicin – Broad spectrum antibiotic
I. NEPHROTOXICITY
• Excessive accumulation in PCT cells ( 40 – 50 times
  than in blood )
• Basic polycation, attract to membrane phospholipids
• High Phosphatidyl inositol content – PCT &
  Cochlea
• Pinocytosis – sequestrate in lysosomes –interact with
  organelles - cell death – cell necrosis
• Inhibit phospholipidases, ATPases - reduced PG
  synthesis – direct effect on GFR.
• Toxicity reversible initially- renewable PCT cells
• Manifestations : Enzymes of brush border in
  urine, proteinuria, casts, low GFR etc..
• Reduced antibiotic clearance – lead to ototoxicity
• Later stages - polyuria – loss of response to ADH
• Neomycin – 6 amino group – more toxic
  DihydroStreptomycin – 3 amino group – less toxic
II. OTOTOXICITY
• Both Vestibular & auditory dysfunction
• Accumulate in perilymph & endolymph
• Ototoxicity – irreversible – Non renewable cells
• Cochlear damage – Hearing loss (high frequency
  sound first) – loss of hair cells in Organ of Corti
• Vestibular damage – Affect balance of body –
  Nystagmus, incoordination, vertigo, head
  tilt, ataxia, loss of righting reflex etc...
• Vestibulotoxicity – Streptomycin > Gentamicin
• Ototoxicity – Neomycin > Kanamycin & Amikacin
• Cats are more susceptible than dogs.
• Renal dysfunction increase ototoxicity
III NEUROMUSCULAR BLOCKAGE
• Interfere Acetyl Choline release from motor nerve
  ending – antagonism of Calcium ( exocytosis )
• Decrease sensitivity of post synaptic membrane
• Toxicity only when administer along with
  neuromuscular blocking agent & general anesthetic
• Muscular weakness, apnea, respiratory arrest
• Neomycin & Streptomycin high side effect
IV OTHER EFFECTS
• Less allergic reactions
• Peripheral neuritis & optic nerve damage
• Intestinal malabsorption syndrome
• Diarrhea, Flattening of intestinal villi etc…
DRUG INTERACTIONS

• Loop diuretics or Osmotic diuretics => Enhanced
  nephrotoxicity & ototoxicity

• Inhalant anesthetics or neuromuscular blocking
  agents => respiratory paralysis
• Halothane => Cardiovascular depression
• Cephalosporin => additive nephrotoxicity
• Carbenicillin or Ticarcillin => inactivate
CONTRAINDICATIONS & PRECAUTIONS

• In hypersensitive animals, Animals with renal
  diseases, Neonatal & Geriatrics - dose rate
  reduced & treatment interval increased.
• Not recommended in pregnants – adverse effect
  on foetus
TREATMENT
• Infusion of neurotropic factor , neurotropin 3 (NT-3)
  in membraneous labrynth
• Dialysis
• Administration of carbenicillin or ticarcillin (12-
  20g/day) to complex with aminoglycosides
• Ca salts or neostigmine given I/v, to treat
  neuromuscular blockage
• Avoiding concurrent use of nephrotoxic drugs
Toxicity of aminoglycoside antibiotics

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Toxicity of aminoglycoside antibiotics

  • 2. INTRODUCTION • Group of natural and semisynthetic antibiotics. • Amino sugar + aminocyclitol via glycoside bond. • Streptomycin – 1st discovered – 1944 – Waksman & co-workers from Streptomyces griseus ( actinobacterium ) • Amikacin – 1st semi synthetic – from Kanamycin • Bactericidal drug – Inhibit protein synthesis – Formation of aberrant proteins – streptomycin (bind with 30S subunit) – others (bind with 50S subunit) – Bacteria more permeable – leakage – cell death
  • 3. • Excellent water solubility – Poor lipid soluble. • Nephrotoxicity – due to increased no: of amino groups Eg :- Neomycin – 6 amino group – more toxic Streptomycin – 3 amino group – less toxic • They are not absorbed from the gut. So I/m or I/v • Uses : Local & Systemic infection – Mainly Gram –ve • In Vet practice, Neomycin – toxic – so topical only Gentamicin – Broad spectrum antibiotic
  • 4. I. NEPHROTOXICITY • Excessive accumulation in PCT cells ( 40 – 50 times than in blood ) • Basic polycation, attract to membrane phospholipids • High Phosphatidyl inositol content – PCT & Cochlea • Pinocytosis – sequestrate in lysosomes –interact with organelles - cell death – cell necrosis • Inhibit phospholipidases, ATPases - reduced PG synthesis – direct effect on GFR.
  • 5. • Toxicity reversible initially- renewable PCT cells • Manifestations : Enzymes of brush border in urine, proteinuria, casts, low GFR etc.. • Reduced antibiotic clearance – lead to ototoxicity • Later stages - polyuria – loss of response to ADH • Neomycin – 6 amino group – more toxic DihydroStreptomycin – 3 amino group – less toxic
  • 6. II. OTOTOXICITY • Both Vestibular & auditory dysfunction • Accumulate in perilymph & endolymph • Ototoxicity – irreversible – Non renewable cells • Cochlear damage – Hearing loss (high frequency sound first) – loss of hair cells in Organ of Corti • Vestibular damage – Affect balance of body – Nystagmus, incoordination, vertigo, head tilt, ataxia, loss of righting reflex etc...
  • 7. • Vestibulotoxicity – Streptomycin > Gentamicin • Ototoxicity – Neomycin > Kanamycin & Amikacin • Cats are more susceptible than dogs. • Renal dysfunction increase ototoxicity
  • 8. III NEUROMUSCULAR BLOCKAGE • Interfere Acetyl Choline release from motor nerve ending – antagonism of Calcium ( exocytosis ) • Decrease sensitivity of post synaptic membrane • Toxicity only when administer along with neuromuscular blocking agent & general anesthetic • Muscular weakness, apnea, respiratory arrest • Neomycin & Streptomycin high side effect
  • 9. IV OTHER EFFECTS • Less allergic reactions • Peripheral neuritis & optic nerve damage • Intestinal malabsorption syndrome • Diarrhea, Flattening of intestinal villi etc…
  • 10. DRUG INTERACTIONS • Loop diuretics or Osmotic diuretics => Enhanced nephrotoxicity & ototoxicity • Inhalant anesthetics or neuromuscular blocking agents => respiratory paralysis • Halothane => Cardiovascular depression • Cephalosporin => additive nephrotoxicity • Carbenicillin or Ticarcillin => inactivate
  • 11. CONTRAINDICATIONS & PRECAUTIONS • In hypersensitive animals, Animals with renal diseases, Neonatal & Geriatrics - dose rate reduced & treatment interval increased. • Not recommended in pregnants – adverse effect on foetus
  • 12. TREATMENT • Infusion of neurotropic factor , neurotropin 3 (NT-3) in membraneous labrynth • Dialysis • Administration of carbenicillin or ticarcillin (12- 20g/day) to complex with aminoglycosides • Ca salts or neostigmine given I/v, to treat neuromuscular blockage • Avoiding concurrent use of nephrotoxic drugs