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Antibiotics: Protein Synthesis, Nucleic Acid Synthesis and Metabolism

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Title: Antibiotics: Protein Synthesis, Nucleic Acid Synthesis and Metabolism

1
Antibiotics Protein Synthesis, Nucleic Acid
Synthesis and Metabolism
2
Principles and Definitions

Selectivity
Selectivty8 toxicity9
Therapeutic index
Toxic dose/ Effective dose
Categories of antibiotics
Bactericidal
Usually antibiotic of choice
Bacteriostatic
Duration of treatment sufficient for host defenses

3
Principles and Definitions

Antibiotic susceptibility testing (in vitro)
Minimum inhibitory concentration (MIC)
Lowest concentration that results in inhibition
of visible growth
Minimum bactericidal concentration (MBC)
Lowest concentration that kills 99.9 of the
original inoculum

4
Antibiotic Susceptibility Testing
5
Zone Diameter Standards for Disk Diffusion Tests
6
Principles and Definitions

Combination therapy
Prevent emergence of resistant strains
Temporary treatment until diagnosis is made
Antibiotic synergism
Penicillins and aminoglycosides
CAUTION Antibiotic antagonism
Penicillins and bacteriostatic antibiotics
Antibiotics vs chemotherapeutic agents vs
antimicrobials

7
Review of Initiation of Protein Synthesis
8
Review of Elongation of Protein Synthesis
9
Survey of Antibiotics
10
Protein Synthesis Inhibitors

Mostly bacteriostatic
Selectivity due to differences in prokaryotic and
eukaryotic ribosomes
Some toxicity - eukaryotic 70S ribosomes

11
Antimicrobials that Bind to the 30S Ribosomal
Subunit
12
Aminoglycosides (bactericidal)streptomycin,
kanamycin, gentamicin, tobramycin, amikacin,
netilmicin, neomycin (topical)

Mode of action - The aminoglycosides irreversibly
bind to the 16S ribosomal RNA and freeze the 30S
initiation complex (30S-mRNA-tRNA) so that no
further initiation can occur. They also slow
down protein synthesis that has already initiated
and induce misreading of the mRNA. By binding to
the 16 S r-RNA the aminoglycosides increase the
affinity of the A site for t-RNA regardless of
the anticodon specificity. May also destabilize
bacterial membranes.
Spectrum of Activity -Many gram-negative and some
gram-positive bacteria Not useful for anaerobic
(oxygen required for uptake of antibiotic) or
intracellular bacteria.
Resistance - Common
Synergy - The aminoglycosides synergize with
-lactam antibiotics. The -lactams inhibit cell
wall synthesis and thereby increase the
permeability of the aminoglycosides.

13
Tetracyclines (bacteriostatic)tetracycline,
minocycline and doxycycline

Mode of action - The tetracyclines reversibly
bind to the 30S ribosome and inhibit binding of
aminoacyl-t-RNA to the acceptor site on the 70S
ribosome.
Spectrum of activity - Broad spectrum Useful
against intracellular bacteria
Resistance - Common
Adverse effects - Destruction of normal
intestinal flora resulting in increased secondary
infections staining and impairment of the
structure of bone and teeth.

14
Spectinomycin (bacteriostatic)

Mode of action - Spectinomycin reversibly
interferes with m-RNA interaction with the 30S
ribosome. It is structurally similar to the
aminoglycosides but does not cause misreading of
mRNA.
Spectrum of activity - Used in the treatment of
penicillin-resistant Neisseria gonorrhoeae
Resistance - Rare in Neisseria gonorrhoeae

15
Antimicrobials that Bind to the 50S Ribosomal
Subunit
16
Chloramphenicol, Lincomycin, Clindamycin
(bacteriostatic)

Mode of action - These antimicrobials bind to the
50S ribosome and inhibit peptidyl transferase
activity.
Spectrum of activity - Chloramphenicol - Broad
range Lincomycin and clindamycin -
Restricted range
Resistance - Common
Adverse effects - Chloramphenicol is toxic (bone
marrow suppression) but is used in the treatment
of bacterial meningitis.

17
Macrolides (bacteriostatic)erythromycin,
clarithromycin, azithromycin, spiramycin

Mode of action - The macrolides inhibit
translocation.
Spectrum of activity - Gram-positive bacteria,
Mycoplasma, Legionella
Resistance - Common

18
Antimicrobials that Interfere with Elongation
Factors
Selectivity due to differences in prokaryotic and
eukaryotic elongation factors
19
Fusidic acid (bacteriostatic)

Mode of action - Fusidic acid binds to elongation
factor G (EF-G) and inhibits release of EF-G from
the EF-G/GDP complex.
Spectrum of activity - Gram-positive cocci

20
Inhibitors of Nucleic Acid Synthesis
21
Inhibitors of RNA Synthesis
Selectivity due to differences between
prokaryotic and eukaryotic RNA polymerase
22
Rifampin, Rifamycin, Rifampicin, Rifabutin
(bactericidal)

Mode of action - These antimicrobials bind to
DNA-dependent RNA polymerase and inhibit
initiation of mRNA synthesis.
Spectrum of activity - Wide spectrum but is used
most commonly in the treatment of tuberculosis
Resistance - Common
Combination therapy - Since resistance is
common, rifampin is usually used in combination
therapy.

23
Inhibitors of DNA Synthesis
Selectivity due to differences between
prokaryotic and eukaryotic enzymes
24
Quinolones (bactericidal)nalidixic acid,
ciprofloxacin, ofloxacin, norfloxacin,
levofloxacin, lomefloxacin, sparfloxacin

Mode of action - These antimicrobials bind to the
A subunit of DNA gyrase (topoisomerase) and
prevent supercoiling of DNA, thereby inhibiting
DNA synthesis.
Spectrum of activity - Gram-positive cocci and
urinary tract infections
Resistance - Common for nalidixic acid
developing for ciprofloxacin

25
Antimetabolite Antimicrobials
26
Inhibitors of Folic Acid Synthesis

Basis of Selectivity
Review of Folic Acid Metabolism

27
Sulfonamides, Sulfones (bacteriostatic)

Mode of action - These antimicrobials are
analogues of para-aminobenzoic acid and
competitively inhibit formation of dihydropteroic
acid.
Spectrum of activity - Broad range activity
against gram-positive and gram-negative bacteria
used primarily in urinary tract and Nocardia
infections.
Resistance - Common
Combination therapy - The sulfonamides are used
in combination with trimethoprim this
combination blocks two distinct steps in folic
acid metabolism and prevents the emergence of
resistant strains.

28
Trimethoprim, Methotrexate, Pyrimethamine
(bacteriostatic)

Mode of action - These antimicrobials binds to
dihydrofolate reductase and inhibit formation of
tetrahydrofolic acid.
Spectrum of activity - Broad range activity
against gram-positive and gram-negative bacteria
used primarily in urinary tract and Nocardia
infections.
Resistance - Common
Combination therapy - These antimicrobials are
used in combination with the sulfonamides this
combination blocks two distinct steps in folic
acid metabolism and prevents the emergence of
resistant strains.

29
Anti-Mycobacterial Antibiotics
30
Para-aminosalicylic acid (PSA) (bacteriostatic)

Mode of action - Similar to sulfonamides
Spectrum of activity - Specific for Mycobacterium
tuberculosis

31
Dapsone (bacteriostatic)

Mode of action - Similar to sulfonamides
Spectrum of activity - Used in treatment of
leprosy (Mycobacterium leprae)

32
Isoniazid (INH) (bacteriostatic )

Mode of action - Isoniazid inhibits synthesis of
mycolic acids.
Spectrum of activity - Used in treatment of
tuberculosis
Resistance - Has developed

33
Antimicrobial Drug ResistancePrinciples and
Definitions

Clinical resistance
Resistance can arise by mutation or by gene
transfer (e.g. acquisition of a plasmid)
Resistance provides a selective advantage
Resistance can result from single or multiple
steps
Cross resistance vs multiple resistance
Cross resistance -- Single mechanism-- closely
related antibiotics
Multiple resistance -- Multiple mechanisms --
unrelated antibiotics

34
Antimicrobial Drug ResistanceMechanisms