Post on 27-Nov-2014
Beta Lactam CompoundsMoises Jaime A. Jamila Jr., RPh University of Immaculate Conception MS Pharmacy class 24 July 2010
Beta Lactam CompoundsPenicillins y Cephalosporins y Monobactam y Carbapenems y Beta-lactamase inhibitorsy
- so named because of their unique fourmembered lactam ring
PENICILLINS
ChemistryA) B)
Thiazolidine ring Beta-lactam ring - carries secondary amino group
6-aminopenicillanic acid nucleus (A+B) - essential for the biologic activity of these compounds
beta-lactamase
Beta-lactam ring
penicilloic acid(no antibacterial activity)
3 Basic Groups:Penicillins y Antistaphylococcal Penicillinsy
Nafcilliny
Extended-Spectrum PenicillinsAmpicillin
Compounds stable to gastric acid:Penicillin V y Dicloxacillin y Amoxicilliny
Penicillin (Pen G)y
Greatest activity against:Gram (+) organisms Gram (-) cocci Non beta-lactamase producing anaerobes
y
Lesser activity against:Gram (-) rods
Antistaphylococcal Penicillins (Nafcillin) Nafcillin)resistant to staphylococcal betalactamases y Active against:-
Staphylococci Streptococciy
Not active against:Enterococci Anaerobic bacteria Gram (-) cocci and rods
ExtendedExtended-Spectrum Penicillins (Ampicillin and Antipseudomonal Penicillins) Penicillins)y
Possess the antibacterial spectrum of penicillins + an improved activity against gram (-) organisms Hydrolyzed by beta-lactamases
y
Penicillin Units and Formulations1 unit 1,600 units 1 M units = = = 0.6 mcg 1 mg 0.6 g
Penicillin Units and FormulationsMIC* salt : mcg/mL : Na+ or K+
Pen G K
: 1.7 mEq of K / M units (2.8 mEq/g) Nafcillin Na : 2.8 mEq/g Procaine and Benzathine salts- Provide repository forms for IM injections*minimum
inhibitory concentration
StabilityDry crystalline formstable for years at 4oC
Solutionstable for 24 hours at 20oC freshly prepared
Mechanism of Action-
Interferes with the transpeptidation reaction of bacterial cell wall synthesis
Resistance1. 2. 3. 4.
Inactivation of antibiotic by betalactamase Modification of transport PBPs* Impaired penetration of drug to target PBPs Efflux
*penicillin-binding protein(s)
1. Inactivation of antibiotic by betabetalactamasesy y
PenicillinsS. aureus, Haemophilus sp & E. coli
Penicillins and CephalosporinsP. Aeruginosa & Enterobacter Sp (AmpC -lactamases) ESBLs*
y
CarbapenemsMetallo -lactamases & carbapenemases*extended spectrum -lactamases
2. Modification of target PBPsy y
Methicillin-resistanceStaphylococci
Penicillin resistancePneumococci & Enterococci- Organisms produce PBPs that have low affinity for binding -lactam antibiotics, and consequently they are not inhibited except at high, often clinically unachievable drug concentrations.
3. Impaired penetration of drug to target PBPsy
G(-) species- Impermeable outer cell wall membrane w/c is absent in G(+) species - B-lactam antibiotics cross the outer membrane & enter G(-) organisms via outer membrane protein channels (porins) - B-lactamase: may hydrolyze drug faster than it enters the cell.
4. Effluxy
G(-) organisms- May produce an efflux pump (cytoplasmic and periplasmic protein components)
PHARMACOKINETICS
Absorptiony
Dicloxacillin, Ampicillin & Amoxicillin- Acid-stable - 500mg oral dose: 4-8 mcg/mL serum conc - Taken 1-2 hours before or after a meal (except amoxicillin)
Administrationy
IV is preferred to the IM route because of irritation and local pain from IM inj of large doses.
Distributiony
Polar
- intracellular conc are low than those found in extracellular fluids 1g Pen G IV: 20-50 mcg/mL serum conc Nafcillin : highly protein-bound Pen G & Ampicillin : less protein-bound
DistributionBenzathine and Procaine- Formulated to delay absorption
1.2 M u IM inj of Benzathine Penicillin : 0.02 mcg/mL serum conc 10 days : hemolytic streptococcal infection 600, 000 u IM inj of Procaine Penicillin : 1-2 mcg/mL serum conc for 12-24 hours
DistributionTissue Conc = Serum Conc Eye, Prostate & CNS: poor penetration Bacterial Meningitis18-24 M u daily dose of Penicillin will yield 15 mcg/mL serum conc, sufficient to kill strains of pneumococci & meningococci
Half - LifePenicillin - t : 30 minutes; 10 hours (renal failure) Ampicillin & Extended-Spectrum Penicillins - t : 1 hour
ExcretionRenal Excretion10% glomerular filtration 90% tubular secretion
Creatinine Clearance (Clcr )10 mL/min or less 1/4 to 1/3 of the normal dose
No dosage adjustment in renal failure: y NafcillinBiliary excretiony
Oxacillin, Dicloxacillin & CloxacillinBoth kidney & biliary excretion
Cockcroft and Gault equation(1976)Clcr (ml/min) = (140 - age ) x BW (kg) x *F ----------------------------------Serum creatinine (mg/dL) x 72
(140 - age ) x BW (kg) x *F ------------------------------------Serum creatinine (mmol/L) x 815 *F = (multiply by) 1 if male, and 0.85 if female
=
CLINICAL USE
Probenecid - Increases blood levels of Penicillin - Impairs renal tubular secretion of weak acids (B-lactam cmpds) - 0.5 g (10 mg/kg in children) q6o PO
Penicillin GDOC-
streptococci, meningococci, enterococci, penicillinsusceptible pneumococci, non-lactamase producing staphylococci,T. pallidum & other spirochetes, clostridium spp, actinomyces, & other G(+) rods & non B-lactamase producing G(-) anaerobic orgs.
Dose-
4-24 M u/day IV in 4-6 divided doses
Penicillin VOral form of penicillin y Indicated for minor infections y Poor bioavailability y QID dosing y Narrow antibacterial spectrumy
Benzathine Penicillin & Procaine Penicillin GIM inj yield low but prolonged drug levels. y Benzathine Penicillin-
1.2 M u IM q 3-4 wks B-hemolytic streptococcal pharyngitis 2.4 M u IM once a week for 1-3 wks (syphilis)
Methicillin, Methicillin, Nafcillin & Isoxazolyl Penicillins-
Resistant to staphylococcal B-lactamase
Systemic Staphylococcal Infections Oxacillin or Nafcillinx 8-12 g/day given by intermittent IV infusion of 1-2 g q4-6o (50100 mg/kg/day for chidren)
Oxacillin, Cloxacillin & Dicloxacillin (Isoxazolyl) 0.25-0.5 g orally q4-6o 15-25 mg/kg/day for children Acid-stable Given 1 hr before or after meals
Aminopenicillins, Aminopenicillins, Carboxypenicillins & Ureidopenicillins (ESPs)Enhanced ability to penetrate G(-) outer membrane y Inactivated by B-lactamasesy
Aminopenicillins (Amoxicillin & Ampicillin) Ampicillin)Both have identical spectrum of activity but amoxicillin is better absorbed orally. Amox 250-500mg TID = Ampi QID Tx: UTI, sinusitis, otitis, LRTI-
Ampicillineffective for shigellosis
B-lactamase Inhibitor CombinationAmpicillin, Amoxicillin, Ticarcillin (Carboxypenicillin) & Piperacillin (Ureidopenicillin) are available in combination with one of these B-lactamase inhibitors:Clavulanic acid Sulbactam Tazobactam - The addition of B-lactamase inhibitors extends the activity of these penicillins
CEPHALOSPORINS & CEPHAMYCINS
Cephalosporinsy
More stable than penicillins to many Blactamases; broader spectrum
Attachment of Various R1 & R2 groupsYielded drugs of good therapeutic activity and low toxicity. y Soluble in water y Relatively stable to pH y Relatively stable to temperature changesy
4 Generationsy
First Generation have better activity against G(+) organisms and the later Generations exhibit improve activity against G(-) aerobic organisms.
OTHER BETA-LACTAM BETADRUGS
MonobactamsMonocyclic B-lactam ring y Relatively resistant to B-lactamase and active against G(-) rods (pseudomonas & serratia) Aztreonamy Resembles aminoglycosides (spectrum of activity) - 1-2g IV q8o - t : 1-2 hrs; prolonged in renal failure - Penicillin allergic Px tolerate Aztreonam w/o reaction-
BetaBeta-lactamase inhibitors:Clavulanic Acid, Sulbactam & Tazobactam
Resembles B-lactam molecules; have weak antibacterial action. y Active against class A:ystaphylococci, H. influenzae, N. gonorrheae, salmonella, shigella, E. coli, & K. Pneumoniae
y
Not active against class C:enterobacter, citrobacter, serratia & pseudomonas (chromosomally encoded)
y
Inhibit Chromosomal B-lactamases:legionella, bacteroides and brahmanella
BetaBeta-lactamase inhibitorsAvailable in fixed combination w/ specific penicillins. y An inhibition will extend the spectrum of a penicillin provided that the inactivity of the penicillin is due to the destruction by Blactamases and that the inhibition is active against the B-lactamase producedy
Ampi+Sulbactam: active against S aureus & H influenzae but not against serratiay
Emperical therapy: aerobic & anaerobic infections (intra-abdominal infections)
Carbapenems(Imipenem, Meropenem & Ertapenem) Imipenem, Ertapenem) Imipeneminactivated by dehydropeptase in renal tubules Administered w/ cilastatin (renal dehydrogenase inhibitor) Penetrate CSF
Carbapenemsy
The B-lactam antibiotic of choice for the treatment of enterobacter infections. Dose: Imipenem: 0.25-0.5g IV q6-8o (t: 1 hr) Meropenem: 1g IV q8o Ertapenem: 1g q24o IV or IM (t: 4 hrs) : 1% lidocaine for IM
CarbapenemsADR: ImipenemN/V, diarrhea, skin rashes Excessive levels of imipenem in Px w/ RF may lead to seizures
OTHER INHIBITORS OF CELL WALL SYNTHESIS
Vancomyciny y y y
Produced by Streptococcus orientalis Active only against G(+) bacteria (staphylococcus) Poorly absorbed from the GIT Not removed by hemodialysis MOA:inhibit cell wall synthesis
Indication:Sepsis and endocarditis
Resistance:Due to modification of the D-ala-D-ala binding site, terminal D-ala is replaced by D-lactate
Vancomycin + Gentamiciny
Alternative regimen for Tx of enterococcal endocarditis (Px w/ serious penicillin allergy)
Vancomycin +Cefotaxime / Ceftriaxone / Rifampicin
Treatment of meningitis suspected or caused by highly penicillin-resistant strain of pneumococcus. Dose: A: 30mg/kg/d 2-3 div doses; 1g q12o P: 40mg/kg/d 3-4 div doses Renal Px: 1g every week PO: 0.125 0.25g q6o : Tx antibiotic-associated enterocolitis : vanco-resistant enterococci: metronidazole initial therapyy
VancomycinADR: Phlebitis at the site of inj, chills, fever Red man or red neck syndrome:infusion related flushing (caused by the release of H1 Prevented by prolonging infusion period to 1-2 hrs or by increasing the dosing interval.
TeicoplaninIM or IV y t: 45-70 hours; OD dosing y Similar to Vancomycin MOAy
FosfomycinMOA:Inhibits cytoplasmic enzyme enolpyruvate transferase (early stage of bacterial cell wall synthesis)
Resistance:Inadequate transport of drug into the cell.
Susceptibility test:Growth medium w/ glucose 6-phosphate.
Indication:Single 3g dose: Tx uncomplicated UTI in women. Safe in pregnancy. G(+) & G(-) t : 4 hours
Bacitraciny y y y
Obtained from Bacillus subtilis Nephrotoxic, limited to topical use; poorly absorbed Combined with polymyxin & neomycin Soln of 100-200 u/mL in saline: irrigation ( joints, wounds or pleural cavity) Inhibit cell wall formation by interfering w/ dephosphorylation in cycling of the lipid carrier that transfers peptidoglycan to the growing cell wall.
MOA:
Cycloseriney y y
Produced by Streptomyces orchidaceus Water soluble and very unstable to acid pH Inhibits G(+) & G(-), used almost exclusively to treat TB Structural analog of D-alanine & inhibits the incorporation of D-alanine
MOA: Dose:0.5-1g/d in 2-3 divided doses
ADR:Headache, tremors, acute psychosis & convulsions (dose: < 0.75 g/d)
G(+)
G(-) cocci / x
G(-) rods L x G
Entero -cocci
Staph
Strep
Anaerobic
BetaLactamase resistant
Penicillin Nafcillin Ampillin Monobactam Imipenem Meropenem Ertapenem Vancomycin Fosfomycin Cycloserine
/
x x / / x / x x / / / / / (methicillin & nafcillin-resistant bacteria) /
/ x / L
/
/ (pseudo & serratia) / (pseudomonas) G L
/ / / /
/ (exclusive for M. tuberculosis)
thank you
-moe