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ANTIBIOTICS
Antibiotics are obtained from
Fungi
penicillins,cephalosporin,griseofulvin
Bacteria
polymyxin B,Tyrothricin
colistin,aztreonam,bacitracin
Actinomycetes
aminoglycosides,macrolides,tetracyclines
polyenes,chloramphenicol
CLASSIFICATION-
A) Chemical structure
Β-lactam antibiotics-
penicillins,cephalosporins,monobactams,carbapenems
Tetracyclins
Oxytetracycline,doxytetracycline
Nitrobenzene derivative- chloramphenicol
Aminoglycosides
Streptomycin,gentamycin,amikacin,neomycin
Macrolide antibiotics
Erythromycin,clarithromycin,azithromycin
Glycopeptide antibiotics
Vancomycin,teicoplanin
Lincosamide antibiotics
Lincomycin,clindamycin
Oxazolidinone- linezolid
Polypeptide antibiotics
Polymyxin-B, colistin,bacitracin
Polyene antibiotics
Nystatin,amphotericin-B
B. Mechanism of action
1. Inhibit cell wall synthesis
penicillins,cephalosporins,cycloserines
vancomycin,bacitracin
2. Causes leakage from cell wall membrane
Polypeptide-polymyxins,colistin,bacitracin
Polyenes- amphotericin B,nystatin
3. Inhibit protein syntheis
tetracyclins,chloramphenicol,erythromycin,
clindamycin
4. Cause misreading of m-RNA code and affect
permeability
Aminoglycosides-streptomycin,gentamycin
SPECTRUM OF ACTIVITY
Narrow spectrum
penicillin G
streptomycin
erythromycin
Broad spectrum
tetracyclines
chloramphenicol
PENICILLINS
First antibiotic to be used clinically in 1941
Originally obtained from fungus
Penicillium notatum
Present source is a high yeilding mutant of
P. chrysogenum
CHEMISTRY AND PROPERTIES
1- Thiazolidine ring
2- β-lactam ring
CH C
CH3
CH3
CH
S
C NH
COOHC N
O
O
R
12
Benzyl side chain
PENICILLINS
Amide linkage
MECHANISM OF ACTION
- Inhibit transpeptidase so that cross linking
does not take place
-When bacteria divide in presence of β-lactam
antibiotics –cell wall deficient(CWD) forms are
produced
-because the interior of the bacterium is
hyperosmotic ,the CWD forms swell & burst
bacterial lysis
Lytic effect of these antibiotics may also be due to
derepression of some bacterial autolysins which
normally function during cell division
Penicillin G
Spectrum- narrow
active only against gram +ve bacteria
Cocci: Streptococci,Pneumococci
gram –ve cocci- Neisseria gonorrhoeae
N.meningitidis
Bacilli: gram +ve - Corynebacterium. Dephtheriae
clostridia tetani
garm –ve- Actinomyces israelii
BACTERIAL RESISTANCE
Many bacteria are inherently insensitive to PnG
Because in them the target enzyme & PBPs are located
deeper under lipoprotein barrier wher PnG is unable to
penetrate
Production of penicillinase
it is a narrow spectrum β-lactamase which opens the
β-lactam ring and inactivates PnG.
Some bacteria become Penicillin tolerant –their target
Enzymes are altered to have low affinity for penicillin
Gram –ve bacteria have porin channels located in their
outer membrane.some gram –ve bacteria become resistant
By loss or alteration of porin channels.
PHARMACOKINETICS
A-
PnG is acid labile-destroyed by gastric acid
absorption from i.m route is rapid & complete
D –
Reaches most of the body fluids
Penetration in CSF is poor
M-
Little metabolised because of rapid excretion
E-
Very rapid renal excretion
ADVERSE EFFECTS
Local irritancy and direct toxicity
pain at i.m injection site
nausea on oral ingestion
Larger dose injected i.v –
Mental confusion
Muscular twitching
convulsions,coma.
Hypersensitivity
rash,itching & fever
USES
1.Streptococcal infections
2. Pneumococcal infections
3.Meningococcal infections
4.Gonorrhoea
5.Syphilis
6. Diphtheria
7.Tetanus
8.Drug of choice for rare infections like
anthrax,rat bite fever,trench mouth
SEMISYNTHETIC PENICILLINS
Shortcomings of PnG
-Poor oral efficacy
-Suseptibility to penicillinase
-Narrow spectrum of activity
-Hypersensitivity reactions
CLASSIFICATION
1.Acid resistant alternative to PnG
phenoxymethyl penicillin(Penicillin V)
2.Penicillinase-resistant penicillins
methicillin,cloxacillin
3.Extended spectrum penicillins
a) aminopenicillins: ampicillin.bacampicillin,amoxicillin
b) carboxypenicillins: carbenicillin,ticarcillin
c) ureidopenicillins: piperacillin,mezlocillin
β-lactamase inhibitors
Clavulanic acid,sulbactum,tazobactum
1.Acid resistant alternative to PnG
-acid stable
-oral absorption better
-antibacterial spectrum identical to PnG
-but it is1/5 as active against Neisseria
2.Penicillinase-resistant penicillins
-these have side chains that protect the β-lactam
ring from attack by staphylococcal penicillinase
Methecillin-
penicillinase resistant but not acid resistant
Cloxacillin-
Highly penicillinase resistant as well as acid resistant
3. Extended spectrum penicillins
Effective against gram-ve bacilli
1.Aminopenicillins
-These have amino group in side chain
-prodrugs
-none is resistant to penicillinase
AMPICILLIN
Uses
-UTI
-RTI
-Meningitis
-Gonorrhoea
BACAMPICILLIN
Ester prodrug of ampicillin
Completely absorbed from g.i.t
AMOXICILLIN
Close congener of ampicillin
Not a prodrug
Oral absorption is better
2. CARBOXYPENICILLINS
-active against pseudomonas aeruginosa & proteus
- Carbenicillin is neither penicillinase resistant nor
acid resistant
-inactive orally
3.UREDOPENICILLINS
Piperacillin
-8 times more active than carbenicillin
-used mainly in immunocompromised patients
having serious gram-ve infections
BETA-LACTAMASE INHIBITORS
Clavulanic acid
Obtained from streptomyces clavuligerus
Has β lactam ring but no antibacterial activity

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Antibiotics basic

  • 1. ANTIBIOTICS Antibiotics are obtained from Fungi penicillins,cephalosporin,griseofulvin Bacteria polymyxin B,Tyrothricin colistin,aztreonam,bacitracin Actinomycetes aminoglycosides,macrolides,tetracyclines polyenes,chloramphenicol
  • 2. CLASSIFICATION- A) Chemical structure Β-lactam antibiotics- penicillins,cephalosporins,monobactams,carbapenems Tetracyclins Oxytetracycline,doxytetracycline Nitrobenzene derivative- chloramphenicol Aminoglycosides Streptomycin,gentamycin,amikacin,neomycin
  • 4. Polypeptide antibiotics Polymyxin-B, colistin,bacitracin Polyene antibiotics Nystatin,amphotericin-B B. Mechanism of action 1. Inhibit cell wall synthesis penicillins,cephalosporins,cycloserines vancomycin,bacitracin
  • 5. 2. Causes leakage from cell wall membrane Polypeptide-polymyxins,colistin,bacitracin Polyenes- amphotericin B,nystatin 3. Inhibit protein syntheis tetracyclins,chloramphenicol,erythromycin, clindamycin 4. Cause misreading of m-RNA code and affect permeability Aminoglycosides-streptomycin,gentamycin
  • 6. SPECTRUM OF ACTIVITY Narrow spectrum penicillin G streptomycin erythromycin Broad spectrum tetracyclines chloramphenicol
  • 7. PENICILLINS First antibiotic to be used clinically in 1941 Originally obtained from fungus Penicillium notatum Present source is a high yeilding mutant of P. chrysogenum
  • 8. CHEMISTRY AND PROPERTIES 1- Thiazolidine ring 2- β-lactam ring CH C CH3 CH3 CH S C NH COOHC N O O R 12 Benzyl side chain PENICILLINS Amide linkage
  • 9. MECHANISM OF ACTION - Inhibit transpeptidase so that cross linking does not take place -When bacteria divide in presence of β-lactam antibiotics –cell wall deficient(CWD) forms are produced -because the interior of the bacterium is hyperosmotic ,the CWD forms swell & burst bacterial lysis
  • 10. Lytic effect of these antibiotics may also be due to derepression of some bacterial autolysins which normally function during cell division Penicillin G Spectrum- narrow active only against gram +ve bacteria Cocci: Streptococci,Pneumococci gram –ve cocci- Neisseria gonorrhoeae N.meningitidis
  • 11. Bacilli: gram +ve - Corynebacterium. Dephtheriae clostridia tetani garm –ve- Actinomyces israelii BACTERIAL RESISTANCE Many bacteria are inherently insensitive to PnG Because in them the target enzyme & PBPs are located deeper under lipoprotein barrier wher PnG is unable to penetrate
  • 12. Production of penicillinase it is a narrow spectrum β-lactamase which opens the β-lactam ring and inactivates PnG. Some bacteria become Penicillin tolerant –their target Enzymes are altered to have low affinity for penicillin Gram –ve bacteria have porin channels located in their outer membrane.some gram –ve bacteria become resistant By loss or alteration of porin channels.
  • 13. PHARMACOKINETICS A- PnG is acid labile-destroyed by gastric acid absorption from i.m route is rapid & complete D – Reaches most of the body fluids Penetration in CSF is poor M- Little metabolised because of rapid excretion E- Very rapid renal excretion
  • 14. ADVERSE EFFECTS Local irritancy and direct toxicity pain at i.m injection site nausea on oral ingestion Larger dose injected i.v – Mental confusion Muscular twitching convulsions,coma. Hypersensitivity rash,itching & fever
  • 15. USES 1.Streptococcal infections 2. Pneumococcal infections 3.Meningococcal infections 4.Gonorrhoea 5.Syphilis 6. Diphtheria 7.Tetanus
  • 16. 8.Drug of choice for rare infections like anthrax,rat bite fever,trench mouth SEMISYNTHETIC PENICILLINS Shortcomings of PnG -Poor oral efficacy -Suseptibility to penicillinase -Narrow spectrum of activity -Hypersensitivity reactions
  • 17. CLASSIFICATION 1.Acid resistant alternative to PnG phenoxymethyl penicillin(Penicillin V) 2.Penicillinase-resistant penicillins methicillin,cloxacillin 3.Extended spectrum penicillins a) aminopenicillins: ampicillin.bacampicillin,amoxicillin b) carboxypenicillins: carbenicillin,ticarcillin c) ureidopenicillins: piperacillin,mezlocillin β-lactamase inhibitors Clavulanic acid,sulbactum,tazobactum
  • 18. 1.Acid resistant alternative to PnG -acid stable -oral absorption better -antibacterial spectrum identical to PnG -but it is1/5 as active against Neisseria 2.Penicillinase-resistant penicillins -these have side chains that protect the β-lactam ring from attack by staphylococcal penicillinase Methecillin- penicillinase resistant but not acid resistant
  • 19. Cloxacillin- Highly penicillinase resistant as well as acid resistant 3. Extended spectrum penicillins Effective against gram-ve bacilli 1.Aminopenicillins -These have amino group in side chain -prodrugs -none is resistant to penicillinase
  • 20. AMPICILLIN Uses -UTI -RTI -Meningitis -Gonorrhoea BACAMPICILLIN Ester prodrug of ampicillin Completely absorbed from g.i.t AMOXICILLIN Close congener of ampicillin Not a prodrug Oral absorption is better
  • 21. 2. CARBOXYPENICILLINS -active against pseudomonas aeruginosa & proteus - Carbenicillin is neither penicillinase resistant nor acid resistant -inactive orally 3.UREDOPENICILLINS Piperacillin -8 times more active than carbenicillin -used mainly in immunocompromised patients having serious gram-ve infections
  • 22. BETA-LACTAMASE INHIBITORS Clavulanic acid Obtained from streptomyces clavuligerus Has β lactam ring but no antibacterial activity