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Content
• Introduction and Definition
A

• Advantage and Disadvantage

• SAR

• Classification
B

C

• Mechanism of action

• Therapeutic uses
• Pharmacokinetics
• Side effect
 Wide-spectrumβ-lactumbactericidal, chemical properties
being similar to the penicillins

 Cephamycins

: Streptomyces species or are synthetic
derivatives produced by substituting oxygen for sulfur
(methoxy group) in cephalosporin nucleus.

 Cephalosporium acremonium,

containing
common 7-aminocephalosporanic acid nucleus

the
Advantages
1. Non-toxic
2. ↓ risk of allergy.
3. More stable in
acidic medium
[less ring strain]
4. Higher
penicillinase
resistance.
5. Good activity ≠ Gve & G+ve

Disadvantage
1. Difficult to isolate
& purify [with
highly polar side
chain]
2. Lower potency
[less strained ring]
3. ↓ absorbed orally.
Mechanism of action:
Cephalosporins are bactericidal and have the
same mode of action as other beta-lactam
antibiotics (such as penicillin).
Cephalosporins disrupt the synthesis of
the peptidoglycan layer of bacterial cell walls.
 The peptidoglycan layer is important for cell
wall structural integrity.
These has been conventionally classified into four
generations. Based on Generation system
• This is based on chronological sequence of development,
but more importantly ,takes into consideration the overall
antibacterial spectrum as well as potency.
• First-generation cephalosporins are predominantly active
against Gram-positive bacteria, and successive generations
have increased activity against Gram-negative bacteria
(albeit often with reduced activity against Gram-positive
organisms).
First generation:
Developed in 1960, active against Gm+ weaker on Gm- orgnisms.
• Cephalothin: 1st cephalosporin used. (Parenteral)
active against: Streptococci, Staphylococci, gonococci,
meningococci, C.diptheriae and clostridia.
• Cephalexin: Orally active. commonly used.
(SPORIDEX)
• Cefadroxil: Excellent tissue penetration
(cefadrox)
Excreted unchanged in urine.
Dose adjustment in renal impaired patients.
• Cephazolin: Active against klebsiella and E.coli. (Parenteral)
Preferred parenteral 1st gen cephalosporin for
surgical prophylaxis ,
(ALCIZONE/ORIZOLIN)
Second generation:
• Cefuroxime: Resistant to Gm- beta lactamase (Parenteral)
Important use: meningitis caused by H. influenzae,

• Cefuroxime axetil: Ester of cefuroxime, effective oral
Uses: URTI, LRTI, UTI, skin and soft tissue infection
group B streptococci,salmonella, E.coli
(CEFTUM,ZOCEF)
Third generation
•
Broad-spectrum.
•
Active against Gm- enterobacteriacae.
•
Some are anti-pseudomal
•
Resistant to beta-lactamase.
Cefotaxim: (TAXIM/OMNATAX)

Prototype of third generation cephalosporin.

Widely distributed in body tissues and fluids, penetrates CSF best when
meninges are inflamed.
Uses: Aerobic Gm- bacteria infection, poor on anaerobes (B. fragilis),
Staphylococci and pseudomonas.
prominent indications: meningitis

11
Ceftriaxone:
• Longer duration of action. (MONOCEF/CEFERA)
• Good CSF penetration.
USES: Bacterial meningitis
Multi-Resistant typhoid fever
Complicated Uniary tract infection

Ceftazidime:
• Active against pseudomonas.
• Burn.

12

(CEFZID/TAZID)
Cefoperazone:
(CEFOMYCIN/NOVACIP)
• Strong anti-pseudomonal property.
• Cidal against S.typhi, B.fragilis.
• More susceptible to beta-lactamase.
USES: severe urinary, biliary, respiratory, skin-soft tissue infection,
meningitis and septicaemia.
Cefixime:

•
•

(ORIFIX/TAXIM-O/OMNATAX)

Orally active 3rd generation

Broad spectrum of action- enterobacteriaceae, H. influenzae, Strep
pyogenes. Not active against Staph and Pseudomonas .
Cefpodoxim proxetil.
(CEPODEM)
• Orally active 3rd generation
• Active against enterobacteriaceae and streptococci.
• Excellent outcome in RTI, UTI and soft-tissue infection.
Cefdinir:
(SEFDIN/ADCEF)
• Orally active
• 13 Excellent results in pneumonia,COPD,ENT & skin infections.
Fourth generation:
Cefepime:
(CEPIME/MEGAPIME)
• Highly resistant to beta-lactamase.
• Active against pseudomonas and Staph besides host of
organisms
Uses: Serious life-threatening hospital acquired pneumonia
Febrile neutropenia.
Bacterremia and septicaemia.
Cefpirome:
(CEFROM/CEFORTH)
• Treatment of serious and resistant hospital acquired
infections including septicaemia ,pneumonia.
• Covers some Gm+ organisms as well.
Cephalosporins are given parenterally and orally.
Extent of binding to plasma protein vary from one to another.
e.g. Cefazolin is 80% protein bound ( hence, long t1/2 )
Cephalexin is 10-15% protein bound
Relatively lipid insoluble ( like penicillins )
Hence,do not penetrate cells or the CNS, except for third
generations.
Mostly excreted unchanged by the kidney (glomerular &
tubular
secretion ), except, ceftazidime &
cefoperazone( glomerular)
Probenecid slows their elimination and prolong their half-live (
except Ceftazidime & cefoperazone)
Half-life 30-90 min; ceftriaxone 4-7 hr
1. Alternative to penicillin in allergic
patients
2. Upper respiratory tract infections
and otitis media
cefaclor
cefuroxime axetil
cefixime
cefprozil
3. Septicaemia caused by G- bacteria
( P.aeruginosae)
A penicillin(eg.Piperacillin/
Ticarcillin)
+aminoglycoside
OR
A cephalosporin(eg.
ceftazidime ) + AG
4. Urinary tract infections
Cefuroxime, Cefixime

.

5. Prophlaxis in surgery
Appendectomy ( bowel
anaerobes ) eg. Cefoxitin
Obstetrical &gynecological,
urological, orthopedic
procedures, etc
( S. aureus & S. epidermidis )
eg. Cefazoline

6. Meningitis- N. Meningitidis
Ceftriaxone
Cefotaxime( pref. in neonate)
1. Hypersensitivity reactions- most common
Anaphylaxis, bronchspasm, urticaria
Maculopapular rash- more common
2. Nephrotoxicity ; esp. cephradine
3. Thrombophlebitis ( i.v admin. )
4. Superinfections
5. Diarrhea-oral cephalosporins, cefoperazone,
ceftriaxone & moxalactam.
6. cefamandole, moxalactam & cefoperazone may cause:
a) bleeding disorders
b) Flushing, tachycardia, vomiting with alcohol intake
^ "cephalosporin" at Dorland's Medical Dictionary

^ "Cephalosporin spectrum of
resistance". Retrieved 1 July 2012.
^ Stork CM (2006). "Antibiotics, antifungals,
and antivirals". In Nelson LH,
M. Zaharna Clin. Chem. 2009

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Cephalosporins antibiotics

  • 1.
  • 2. Content • Introduction and Definition A • Advantage and Disadvantage • SAR • Classification B C • Mechanism of action • Therapeutic uses • Pharmacokinetics • Side effect
  • 3.  Wide-spectrumβ-lactumbactericidal, chemical properties being similar to the penicillins  Cephamycins : Streptomyces species or are synthetic derivatives produced by substituting oxygen for sulfur (methoxy group) in cephalosporin nucleus.  Cephalosporium acremonium, containing common 7-aminocephalosporanic acid nucleus the
  • 4. Advantages 1. Non-toxic 2. ↓ risk of allergy. 3. More stable in acidic medium [less ring strain] 4. Higher penicillinase resistance. 5. Good activity ≠ Gve & G+ve Disadvantage 1. Difficult to isolate & purify [with highly polar side chain] 2. Lower potency [less strained ring] 3. ↓ absorbed orally.
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  • 7. Mechanism of action: Cephalosporins are bactericidal and have the same mode of action as other beta-lactam antibiotics (such as penicillin). Cephalosporins disrupt the synthesis of the peptidoglycan layer of bacterial cell walls.  The peptidoglycan layer is important for cell wall structural integrity.
  • 8. These has been conventionally classified into four generations. Based on Generation system • This is based on chronological sequence of development, but more importantly ,takes into consideration the overall antibacterial spectrum as well as potency. • First-generation cephalosporins are predominantly active against Gram-positive bacteria, and successive generations have increased activity against Gram-negative bacteria (albeit often with reduced activity against Gram-positive organisms).
  • 9. First generation: Developed in 1960, active against Gm+ weaker on Gm- orgnisms. • Cephalothin: 1st cephalosporin used. (Parenteral) active against: Streptococci, Staphylococci, gonococci, meningococci, C.diptheriae and clostridia. • Cephalexin: Orally active. commonly used. (SPORIDEX) • Cefadroxil: Excellent tissue penetration (cefadrox) Excreted unchanged in urine. Dose adjustment in renal impaired patients. • Cephazolin: Active against klebsiella and E.coli. (Parenteral) Preferred parenteral 1st gen cephalosporin for surgical prophylaxis , (ALCIZONE/ORIZOLIN)
  • 10. Second generation: • Cefuroxime: Resistant to Gm- beta lactamase (Parenteral) Important use: meningitis caused by H. influenzae, • Cefuroxime axetil: Ester of cefuroxime, effective oral Uses: URTI, LRTI, UTI, skin and soft tissue infection group B streptococci,salmonella, E.coli (CEFTUM,ZOCEF)
  • 11. Third generation • Broad-spectrum. • Active against Gm- enterobacteriacae. • Some are anti-pseudomal • Resistant to beta-lactamase. Cefotaxim: (TAXIM/OMNATAX)  Prototype of third generation cephalosporin.  Widely distributed in body tissues and fluids, penetrates CSF best when meninges are inflamed. Uses: Aerobic Gm- bacteria infection, poor on anaerobes (B. fragilis), Staphylococci and pseudomonas. prominent indications: meningitis 11
  • 12. Ceftriaxone: • Longer duration of action. (MONOCEF/CEFERA) • Good CSF penetration. USES: Bacterial meningitis Multi-Resistant typhoid fever Complicated Uniary tract infection Ceftazidime: • Active against pseudomonas. • Burn. 12 (CEFZID/TAZID)
  • 13. Cefoperazone: (CEFOMYCIN/NOVACIP) • Strong anti-pseudomonal property. • Cidal against S.typhi, B.fragilis. • More susceptible to beta-lactamase. USES: severe urinary, biliary, respiratory, skin-soft tissue infection, meningitis and septicaemia. Cefixime: • • (ORIFIX/TAXIM-O/OMNATAX) Orally active 3rd generation Broad spectrum of action- enterobacteriaceae, H. influenzae, Strep pyogenes. Not active against Staph and Pseudomonas . Cefpodoxim proxetil. (CEPODEM) • Orally active 3rd generation • Active against enterobacteriaceae and streptococci. • Excellent outcome in RTI, UTI and soft-tissue infection. Cefdinir: (SEFDIN/ADCEF) • Orally active • 13 Excellent results in pneumonia,COPD,ENT & skin infections.
  • 14. Fourth generation: Cefepime: (CEPIME/MEGAPIME) • Highly resistant to beta-lactamase. • Active against pseudomonas and Staph besides host of organisms Uses: Serious life-threatening hospital acquired pneumonia Febrile neutropenia. Bacterremia and septicaemia. Cefpirome: (CEFROM/CEFORTH) • Treatment of serious and resistant hospital acquired infections including septicaemia ,pneumonia. • Covers some Gm+ organisms as well.
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  • 16. Cephalosporins are given parenterally and orally. Extent of binding to plasma protein vary from one to another. e.g. Cefazolin is 80% protein bound ( hence, long t1/2 ) Cephalexin is 10-15% protein bound Relatively lipid insoluble ( like penicillins ) Hence,do not penetrate cells or the CNS, except for third generations. Mostly excreted unchanged by the kidney (glomerular & tubular secretion ), except, ceftazidime & cefoperazone( glomerular) Probenecid slows their elimination and prolong their half-live ( except Ceftazidime & cefoperazone) Half-life 30-90 min; ceftriaxone 4-7 hr
  • 17. 1. Alternative to penicillin in allergic patients 2. Upper respiratory tract infections and otitis media cefaclor cefuroxime axetil cefixime cefprozil 3. Septicaemia caused by G- bacteria ( P.aeruginosae) A penicillin(eg.Piperacillin/ Ticarcillin) +aminoglycoside OR A cephalosporin(eg. ceftazidime ) + AG 4. Urinary tract infections Cefuroxime, Cefixime . 5. Prophlaxis in surgery Appendectomy ( bowel anaerobes ) eg. Cefoxitin Obstetrical &gynecological, urological, orthopedic procedures, etc ( S. aureus & S. epidermidis ) eg. Cefazoline 6. Meningitis- N. Meningitidis Ceftriaxone Cefotaxime( pref. in neonate)
  • 18. 1. Hypersensitivity reactions- most common Anaphylaxis, bronchspasm, urticaria Maculopapular rash- more common 2. Nephrotoxicity ; esp. cephradine 3. Thrombophlebitis ( i.v admin. ) 4. Superinfections 5. Diarrhea-oral cephalosporins, cefoperazone, ceftriaxone & moxalactam. 6. cefamandole, moxalactam & cefoperazone may cause: a) bleeding disorders b) Flushing, tachycardia, vomiting with alcohol intake
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  • 20. ^ "cephalosporin" at Dorland's Medical Dictionary ^ "Cephalosporin spectrum of resistance". Retrieved 1 July 2012. ^ Stork CM (2006). "Antibiotics, antifungals, and antivirals". In Nelson LH,
  • 21. M. Zaharna Clin. Chem. 2009