Title: AMINOGLYCOSIDES
1AMINOGLYCOSIDES
- The different members of this group share many
properties in common.
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3AMINOGLYCOSIDES
- Streptomycin
- Gentamicin
- Tobramycin
- Amikacin
- Netilmicin
- Kanamycin
- Neomycin
4AMINOGLYCOSIDES
- Amino sugars linked through glycosidic bonds.
- Polycations This is in part responsible for many
of their shared pharmacokinetic properties
5ANTIBACTERIAL ACTIVITY
- Primarily active against aerobic gram negative
bacteria. - Active against many staphylococci and certain
Mycobacteria. - Anaerobic bacteria are not susceptible.
6SENSITIVITY AND RESISTANCE
7AMINOGLYCOSIDE TRANSPORT
- Transport across the cell membrane is by active
transport. - Antimicrobial activity is reduced in an anaerobic
environment and at low pH.
8RESISTANCE
- Cross-resistance occurs to varying degrees with
the different aminoglycosides. - Amikaciin
9ABSORPTION AND DISTRIBUTION
- Oral bioavailability is low.
- Once daily dosing (postantibiotic effect).
- Distribution into most body tissues including the
CNS is low.
10EXCRETION
- Rapidly and almost entirely excreted by
glomerular filtration (proportional to creatinine
clearance). - Accumulation occurs with impaired renal function.
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13PHARMACOKINETICS
- Monitor the serum concns of the drugs (T.I. is
close to 1).
14THERAPEUTIC USES
- Severe , complicated infections.
- Often combined with ß-lactams.
15STREPTOMYCIN
- Bacterial endocarditis (combined with a
penicillin or vancomycin). - Tuberculosis.
16Gentamicin, Tobramycin, Netilmicin and Amikacin
- Similar in clinical indications and range of
activity. - Gentamicin is often preferred but resistance may
limit its use.
17THERAPEUTIC USES
- Serious gram negative infections especially those
due to Pseudomonas, Enterobacter, Klebsiella,
Serratia etc. - UTIs, bacteremia, meningitis, infected burns,
pneumonia, osteomyelitis, ear infections etc.
18THERAPEUTIC USES
- Severe Pseudomonas infections are best treated
with one of these 4 AGs plus an antipseudomonal
penicillin or cephalosporin. - Gentamicin combined with a penicillin is often
used to treat bacterial endocarditis.
19THERAPEUTIC USES
- Tobramycin is often used in pseudomonal
infections. - Amikacin is used as the preferred agent in
hospitals. - Netilmicin- may be useful in resistant
infections.
20DRUG INTERACTIONS
- Antipseudomonal penicillins inactivate
aminoglycosides. - Ethacrynic acid and other loop diuretics.
- Nephrotoxic agents.
- Neuromuscular blocking agents.
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22SHARED PROPERTIES OF THE AMINOGLYCOSIDES
Inhibit protein synthesis by binding to the 30S ribosomal subunit
Pharmacokinetics-Poorly absorbed from the GI tract, Dont get into the CNS very well, Rapidly excreted by kidney
Toxicity-Ototoxicity, Nephrotoxicity, Neuromuscular blockade
23 THERAPEUTIC USES OF THE AMINOGLYCOSIDES
Streptomycin T.B., Endocarditis
Gentamicin Endocarditis, gram negative infections, Pseudomonas
Tobramycin Gram negative infections, Pseudomonas
Amikacin Reserve drug for gram negative- infections
24Wheel of Bugs
Gram-negative
H. influenzae
Neissseria spp
E. Coli (coliforms)
Bacteroides spp
P. aeruginosa
Anaerobic
Clostridium spp
S. aureus
Streptococcus spp
Enterococcus spp
Gram-positive
25MECHANISM OF ACTION
- Bactericidal.
- They inhibit protein synthesis by binding
irreversibly to the 30S ribosomal subunit.
26A
50S
Nascent polypeptide chain
Transferase site
aa
mRNA
template
P
AGs
30S
Mechanism of action of Aminoglycosides
27Mature protein
Blocks initiation
Growing polypeptide
50S
Premature termination
5
3
Wrong amino acid is incorporated
30S
5
mRNA translation
aminoglycoside
Effects of Aminoglycosides
28 Aminoglycosides on Protein Synthesis
Mature Protein
Growing Polypeptide
50S
AUG
3
5
30S
mRNA translation
Amino Glycoside
29MECHANISM OF ACTION
- Exact mechanism of cell death is unknown.
- Postantibiotic effect.
30RESISTANCE
- Alterations in ribosomal proteins.
- Decreased permeability to the antibiotic.
- Induction of bacterial enzymes that inactivate
these drugs.
31RESISTANCE
- Alterations in ribosomal proteins.
- Decreased permeability to the antibiotic.
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33TOXICITY
- Ototoxicity (Vestibular and Auditory).
- Nephrotoxicity.
- Neuromuscular Blockade.
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35OTOTOXICITY
- The most serious toxic effect (uncommon,
irreversible and cumulative). - Caused by all the aminoglycosides
36OTOTOXICITY
- Both auditory and vestibular dysfunction can
occur. - Results from destruction of sensory hair cells.
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38OTOTOXICITY
- Several factors increase the risk.
- Careful monitoring is important.
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41NEPHROTOXICITY
- Aminoglycosides accumulate in the renal cortex
(mainly proximal tubules). - Several factors may increase the risk.
- Reversible and usually mild.
- Reduced excretion can lead to ototoxicity.
42NEPHROTOXICITY
- Several factors may increase the risk.
- Reversible and usually mild.
- Reduced excretion can lead to ototoxicity.
43NEUROMUSCULAR BLOCKADE
- Rare but potentially serious.
- Occurs at high concentrations of aminoglycosides
or in patients with an underlying risk factor. - Acute neuromuscular blockade, respiratory
paralysis and death can occur.
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45NEUROMUSCULAR BLOCKADE
- Results from decreased ACH release and decreased
postsynaptic sensitivity. - Treated with supportive measures and calcium (or
neostigmine).