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Cephalosporins 1
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Cephalosporin antibiotics – derived from “cephalosporin C” – obtained from fungus Cephalosporium acremonium Cephalosporin nucleus Consists of dihydrothiazine ring fused to a β–lactam ring – 7-aminocephalosporanic acid 2
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7-aminocephalosporanic acid has been modified by addition of different side chains to create a whole family of cephalosporin antibiotics. these have been conventionally divided into 5 generations 3
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Mechanism of action All cephalosporins are bactericidal. MOA same as penicillin- Inhibit cell wall synthesis in a manner similar to penicillins Bind to different proteins than those which bind penicillin. PBP-1 &PBP-3 – This explains diffenece in spectrum, potency & lack of resistance. 4
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Inhibition of transpeptidation Imperfect cell wall Osmotic drive Activation of autolysin enzymes Lysis of bacteria BACTERICIDAL 5
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CLASSIFICATION Based on – antimicrobial spectrum – Chronological sequence of development – Divided into generations. 6
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First-generation agents Cephalexin (O) Cefadroxil (O) Cefazolin (i.m, i.v) Cefalothin (withdrawn) 7
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Exhibit good activity against gram-positive bacteria but modest activity against gram negative organisms. – Most gram-positive cocci – Strepto, – Pneumo, – Methicillin sens. Staph. are susceptible to first-generation cephalosporins Modest activity against E. coli, K. pneumoniae & Proteus mirabilis Most oral cavity anaerobes are sensitive. However, the Bacteroides fragilis group is resistant.Bacteroides fragilis 8
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Second-generation agents – Cefaclor (O) – Ceforanide – Cefuroxime acetil (O) – Cefuroxime (i.m, i.v) – Cefoprozil – Cefamandole (Banned) – Cefoxitin (Banned) – Cefotetan (Banned) 9
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Exhibit somewhat increased activity against gram negative organisms, – but much less active than third generation agents. Less active against gram positive cocci & bacilli compared to first gen. drugs. Use declined Clinically replaced by 3 rd & 4 th generation drugs. 10
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Third-generation agents Cefotaxime Ceftriaxone Cefdinir Cefibuten Cefpodoxime Ceftizoxime Ceftazidime Cefoperazone ( withdrawn ) 11
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Highly augmented activity against gram-negative organisms Less active than first generation agents against gram positive cocci & anaerobes. All are highly resistant to β-lactamases from gram negative bacteria. Some inhibit psuedomonas as well; ceftazidime, cefoperazone(withdrawn) 12
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Some members of this group have enhanced ability to cross the blood-brain barrier eg. Ceftriaxone and are effective in treating meningitis caused by pneumococci, meningococci, H. influenzae and susceptible gram negative rods. 13
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Fourth-generation agents Cefpirome P/E (im/iv) Cefepime P/E (iv) Cefozopran P/E 14
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Highly active against G –ve organisms Similar to third gen drugs for g +ve bacteria The fourth generation drugs comparable to third generation but more resistant to hydrolysis by β-lactamases. – Effective against bacterial infections resistant to earlier drugs 15
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Fifth-generation agents Ceftobiprole Ceftaroline Active against, g +ve cocci especially MRSA penicillin resistant S. pneumoniae and enterococci 16
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Resistance Impermeability to the antibiotic. – to reach its site of action Alteration in PBPs -antibiotics bind with low affinity Elaboration of β-lactamases; that can hydrolyze the β-lactam ring and inactivate the cephalosporin (most prevalent mech) 17
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Adverse reactions Pain after im injection Thrombophlebitis of injected vein. Diarrhoea more common with – oral Ceferadine – P/E Cefoperazone (Banned) 18
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Hypersensitivity reactions – Identical to penicillins, incidence is lower. – shared β-lactam structure – Allergic to penicillins- allergic to cephalosporins. CROSS- REACTIVITY. Rashes, frequent, anaphylaxis, angioedema, asthma, urticaria have also occurred. 19
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Cephalosporins potentially nephrotoxic drugs – Cephaloridine (withdrawn) RTN – Cephalothin (withdrawn) Acute tubular necrosis Serious bleeding – Cefoperazone(Banned), – Moxalactam(Banned). – Due to hypoprothrombinemia. 20
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Intolerance to alcohol Disulfiram like reaction – Cefamandole (Banned) – Cefotetan (Banned) – Moxalactam (Banned) – Cefoperazone (Banned) 21
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Therapeutic Uses Extensively used & therapeutically important antibiotics Effective therapeutic & prophylactic agents 22
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First Gen agents Excellent for skin & soft tissue infections Surgical prophylaxis first generation drugs are the preferred for prophylaxis in procedures in which skin flora are likely pathogens. 23
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Second Gen agents Displaced by third generation agents for Gram negative infections Oral-RTI (replaced by augmentin) 24
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Third Gen agents With/without aminoglycosides DOC- severe G -ve infections caused by Kleibsiella Enterobacter Proteus Providencia Serratia & haemophillus species. 25
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Ceftriaxone is the therapy of choice for all forms of Gonorrhea – 250 mg i.m as single dose i.v ceftriaxone for enteric fever Cefotaxime & ceftriaxone – Community aquired pneumonia 26
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Cefotaxime/ceftriaxone are used for initial treatment of meningitis because of their – antimicrobial activity, – good penetration into CSF – & record of clinical success They are DOC - Meningitis due to H. influenzae Sensitive S. pneumonae N. meningitidis G-ve enteric bacteria Ceftazidime + aminoglycosides – Psuedomonas meningitis DOC 27
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Fourth Generation Agents Same as third generation drugs Indicated for hospital acquired infections resistant to commonly used antibiotics 28
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Other β -lactam antibiotics 29
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Other β -lactam antibiotics Newer classes of β-lactam antibiotics are the Monobactams Carbapenems Carbacephems Important therapeutic agents with a β-lactam structure & are neither penicillins nor cephalosporins 30
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Monobactams Aztreonam Isolated from chromobacterium violaceum – Only monobactam currently in clinical use β - lactam ring, lacking the thiazolidine ring. - a monobactam 31
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Antimicrobial activity differs from those of other β - lactam antibiotics & more closely resembles that of an aminoglycoside Primarily affects : – Aerobic gram negative microorganisms – gram positive bacteria & anaerobic organisms are resistant Preferred-all sorts of gram negative infections in patients with renal impairment where aminoglycosides are to be avoided. 32
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Stable to most β-lactamases elaborated by gram negative bacteria. i.m / i.v Therapeutic conc. in CSF in the presence of inflammed meninges, Alternative to cephalosporins for therapy of meningitis caused by G-ve bacilli 33
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Carbapenems β-lactam antibiotic Broader spectrum of activity : than most other β- lactams. – gram-negative rods – gram-positive bacteria – and anaerobes. 34
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Carbapenems Imipenem Meropenem Ertapenem 35
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Imipenem Derived from compound produced by Streptomyces cattleya Mechanism same as penicillins Bactericidal Resistant to hydrolysis by β-lactamase Marketed in combination with cilastin – Inhibits degradation – by renal dipeptidase – Without cilastin renal dehydropeptidases inactivate the drug which results in low urinary tract concentrations. 36
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Adverse effects Nausea,vomiting Seizures Patients allergic to other β-lactam antibiotics may have hypersenstivity reactions when given imipenem 37
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Meropenem Therapeutic equivalence with imipenem Coadministration with cilastin not required Meropenem is less seizure producing compared to imipenem. 38
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Ertapenem Differs from imipenam & meropenem larger serum half life, OD. – Co-administration with cilastin not required – less seizure producing compared to imipenem. 39
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All are parenteral – i.v, im painful Imipenem 6 hrly Meropenam 8 hrly All are resistant to β – lactamases All bactericidal MOA same Patients allergic to other β-lactam antibiotics may have hypersenstivity reactions when given imipenem/carbapenems. 40
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Therapeutic uses Urinary tract infections Lower respiratory tract infections Intra-abdominal & gynaecological infections Skin, bone, joint, & soft tissue infections Especially cephalosporin/ penicillin resistant nosocomial bacteria. 41
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Carbacephems Loracarbef Synthetic β-lactam antibiotic Similar to cefaclor Antibacterial activity resembles II generation cephalosporins. 42
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THANK U 43
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