Antimicrobial agents Mechanisms of action: selective toxicity interference with the cell wall block of bact. cell metabolism nucleic acid synthesis inhibition proteosynthesis inhibition
Antimicrobial agents PharmDr. Ondej Zendulka, Ph.D.
Antimicrobial agents difference antibiotics-chemotherapeutics
classification: chem. structure mechanism of action extent of
effect antibacterial spectrum Antimicrobial agents Mechanisms of
action: selective toxicity interference with the cell wall block of
bact. cell metabolism nucleic acid synthesis inhibition
proteosynthesis inhibition Bacterial cell wall Antimicrobial agents
Bacterial cell wall Antimicrobial agents Bacterial cell wall
Antimicrobial agents selective toxicity antimicrobial spectrum MIC,
MBC, MAC postantibiotic effect resistance Terminology Mechanisms of
resistance: decrease of ATBs intracelullar conc. inactivation of
ATB modification of ATBs target site Antimicrobial agents
Resistance = ability of microbial cells to withstand the effect of
ATB absolute relative coupled cross Antimicrobial agents primary
secondary Combinations of ATBs: spectrum widening resistance
development restriction decrease in AE incidence increase in
effectivity effects: synergistic, additive, indifferent,
antagonistic Antimicrobial agents Which ATB? empirical x bacterial
sensitivity pharmacokinetics Antibiotic policy in CR prophylactic
administration of ATBs Antimicrobial agents Antibiotics -lactams
amphenicols tetracyclines macrolides azalides streptogramines
ketolides oxazolidinones lincosamides aminoglycosides glycopeptides
miscellaneous ATBs local ATBs sulphonamides quinolones imidazoles
Antimicrobial agents -lactams penicillins cephalosporins
cephamycins monobactams carbapenems + inhibitors of -lactamases
Penicillins MofA: binding to PBP, inhibition of transpeptidases,
autolysis => bactericidal Penicillins produced by Penicillium
mould resistance : -lactamases modification of PBP cell wall
penetration block low toxicity, AE hypersensitivity Narrow spectrum
penicillines Benzylpenicillin (Penicillin G) for parenteral use
only destroyed by -lactamases spectrum: Streptococc., Meningococc.
and gonococc. crystalic, procain or benzathin salt
Fenoxymethylpenicillin (Penicillin V) for peroral administration
Penamecillin ester of penicilline G for peroral use Narrow spectrum
penicillines Penicillines stable against lactamases efective only
against Staphylococc. and Streptococc. oxacillin, cloxacillin,
flucloxacillin, dicloxacillin 4-6h 0,5-1g p.o. or parent. Narrow
spectrum penicillines Wide spectrum penicillines Aminopenicillins
wider spectrum - Haemophilus influenzae lower efficacy against
-hemolytic streptoc. combination with inhibitors of lactamases
ampicillin (becampicillin, pivampicillin), amoxycillin
Carboxypenicillins effective against Pseudomonas aeruginosa
nonstable in stomach combination with lactamases inhibitors
ticarcillin, carbenicillin Wide spectrum penicillines
Ureidopenicillins widest spectrum, pseudomonades, klebsiellas not
stable in acid environment combined with lactamases inhibitors
piperacillin, azlocillin, mezlocillin Wide spectrum penicillines
Inhibitors of -lactamases usually without own antimicrobial
properties clavulanic acid, sulbactam, tazobactam coamoxicillin
(clavulanic ac.) cotikarcillin (clavulanic ac.) coampicillin
(sulbactam) sultamicillin (sulbactam) copiperacillin (tazobactam)
Cephalosporins MofA: the same as in penicillins produced by
Cephalosporinum Spectrum: differs between generations NOT
EFFECTIVE: Campylobacter jejuni Legionella pneumophilla Clostridium
difficile Enterococcus fecalis mycoplasmas, mycobacterias,
chlamydias Cephalosporins Cephalosporins I. generation high
efficacy against G+ (streptoc., staphyloc.) from G- against E.
coli, K. pneumoniae, H. influenza partially stable against
lactamases crossed resistance with penicillines cefazolin,
cefalotin, cefapirin parenteral cefalexin, cefadroxil - peroral
high efficacy against G+ (streptoc., staphyloc.), enteroc. from G-
like I. gen, Shigella, Enterobacter mainly against respeiratory
infections cefuroxim, cefamandol parenteral cefuroxim-axetil,
cefaclor, cefprosil, cefpodoxim-proxetil - peroral Cephalosporins
II. generation high efficacy against G+ but lower on staphyloc. G-
sensitive including Pseudomonas more resistant to lactamases than
I. And II. gen. cefotaxim, ceftriaxon, cefmenoxim, ceftazidim,
cefoperazon, cocefoperazon, cefsulodin parenteral cefixim,
ceftibuten, cefetamet-pivoxil - peroral Cephalosporins III.
generation wide spectrum, high efficacy serious infections
cefpirom, cefepim Cephamycins good results against anaerobes
cefoxitin Cephalosporins IV. generation Monobactams bactericidal G-
aerobes -lactamases resistant aztreonam, carumonam wide spectrum
imipenem, meropenem Carbapenems Amphenicols Mof A.: proteosynthesis
inhibition 50S subunit Spectrum: majority of G + i G -, anaerobes,
ricketsias, chlamydias, mycoplasmas per os or parenterally
interferention with metabolism of other drugs reversible or
irreversible myelosuppresion, contraindicated in newborns
chloramphenicol, thiamphenicol Tetracyclines M ofA :
proteosynthesis inhibition- 30S subunit Spe c trum: most of G + i G
-, chlamydi as, my c opla s ma s parenterally or per os crossed
resistance deposition into bones and cartilages = discoloration,
contraindicated in pregnant women and childrens (to 8 yrs) doxycy c
lin e, minocy c lin e Macrolides MofA: proteosynthesis inhibition,
50S subunit Spectrum: majority of G + i G -, chlamydias,
mycoplasmas bacteriostatic eff. alternative for penicillines
crossed resistance GIT intoleration, metabolism via CYP 450 3A
erythromycin, spiramycin, josamycin, roxithromycin, clarithromycin,
dirithromycin Azalides MofA: like macrolides Spectrum: like
erytromycin bacteriostatic eff. resistance crossed with
erythromycin GIT intolerance, metabolization via CYP 450A3
azithromycin ATBs related to macrolides Streptogramins
quinupristin, dalfopristin parenterally, multiresistant G+ cocci
Ketolides telithromycin does not inhibit CYP450 Oxazolidinones
linezolid against resistant strains Lincosamides MofA.:
proteosynthesis inhibition 50S subunit Spectrum: G+ cocc. and
bacill., G- cocc. AE: GIT, pseudomembraneous colitis clindamycin,
lincomycin Aminoglycosides MofA: proteosynthesis inhibition,
binding to different ribosomal sites Spectrum: G -, staphylococcus,
brucellias slow developing resistance only parenterally
postantibiotic effect nephro-, oto-, neurotoxicity streptomycin,
sisomicin, tobramycin, netilmicin, amikacin, isepamicin
Glycopeptides Mof A: inhibition of cell wall synthesis Spectrum:
only G + slow developing resistance not absorbed from GIT nephro-,
ototoxicity, release of histamine vancomycin, teicoplanin
Miscellaneous ATBs Fusidic acid MofA: inhibition of cell waal
proteins synthesis Spectrum: penicillin resistant staphyloc. fast
resistance => combinations Rifampicin MofA.: inhibition of
bacterial DNA-dependent RNA-polymerases Spectrum: Staphylococc.,
Haemophilus, neisserias, mycoplasmas colours urine and salivas,
induces CYP450 Rifaximin rifampicin derivative Phosphomycin MofA.:
inhibition of peptidoglycane synthesis Spectrum: Staphylococc. and
Enterococc. synergistic with cephalosporines and aminoglycosides
Miscellaneous ATBs Polymyxin B, colistin (polymixin E) polypeptides
high system toxicity => locally nephrotoxicity, neurotoxicity
Spectinomycin MofA.: proteosynthesis inhibition Spectrum: Neiseria
gonorrhoae therapy of gonorrhea Miscellaneous ATBs ATBs for local
use Neomycin aminoglycoside in combination with bacitracin
(Framykoin) Bacitracin polypeptide low resistance and allergy
Mupirocin inhibition of proteosynthesis skin infections therapy
Chemotherapeutics Sulphonamides Trimethoprim Quinolones
Metronidazole Nitrofurantoin Sulphonamides one of the oldest basic
structure sulfanilamide small therapeutic importance MofA:
competitive inhibition of bacterial cell metabolism on the level of
folic acid bacteriostatic effect spectrum: streptococcus,
haemophillus, nocardia, actinomycets, chlamydia, Toxoplasma gondi,
Neisseria meningitidis today therapy of urinary tract infections
and in the combination with trimethoprim strong binding to
plasmatic proteins = drug interactions AE: skin phototoxicity,
Stevens-Johns syndrome; myelotoxicity; haemolytic anaemia; allergic
reaction; crystalluria Sulphonamides Sulfisoxazole short acting,
fast absorption and elimination protein binding up to 92% urinary
infections Sulfathiazole for topicall administration
Sulfamethoxazole in combination with trimethoprim - cotrimoxazole
protein binding 70% Sulfasalazine poor absorption from GIT = local
effect in the intestine, ulcerative colitis Sulphonamides
Trimethoprim blocks dihydrofolate reductase (50 000x more selective
to bacterial enzyme) synergistic effect with sulphonamides high
levels in prostate and vaginal mucus (lower pH) CYP metabolism
urine (low pH = faster elimination) combination: trimethoprim a
sulfamethoxazole = co-trimoxazole 1:5: Triprim, Biseptol
Kotrimoxazol, Sumetrolin I: respiratory infections, prevention and
therapy of pneumonia, urinary infections Quinolones MofA:
inhibition of DNA gyrase - nucleic acid synthesis inhibition
(topoisomerase II) bactericidal spectrum: older molecules mainly
G-; modern drugs wide spectrum high F after p.o. administration,
good distribution except CNS, excreted into urine AE: 2-8% nemocnch
GIT problems, cephalgia, sleeping disorders skin symptoms risk of
tendons rupture I: urinary tract infections prostatitits bone and
joint infections skin infections prophylaxis in neutropenic
patients CI: children, breastfeeding, pregnancy Quinolones
Quinolones for the therapy of urinary infections poor tissue
distribution, excreted unchanged oxoline and nalidixic acid
norfloxacine partial systemic effect, therapy of gonorrhea high
rate of mild adverse effects (GIT) Quinolones Quinolones for
therapy of systemic infections- Fluoroquinolones ciprofloxacin,
ofloxacin, lomefloxacin, pefloxacin. good tissue distribution
therapy of respiratory, skin, GIT and other severe infections
sparfloxacin, trovafloxacin, rufloxacin, grepafloxacin bile
elimination life-threatening infections caused by multiresistant
strains AE: often, mild, GIT, artralgia, cartilage disruption
Quinolones Imidazoles MofA: inhibition of DNA replication spectrum:
anaerobes and protozoa : Bacteroides, Clostrididum, Giardia
Metronidazole metabolized in liver and excreted into urine AE:
metallic taste nausea, vommiting, diarrhoea CNS (cephalgia, sleping
disorders, depression) disulfiram reaction Ornidazole Tinidazole
antiparasitic agent Others Nitrofurantoin MofA: interferes with
bacterial DNA spectrum: E.coli, Klebsiella, Enterobacter,
enterococci, staphylococci administered orally effective levels in
urine, alkaline pH decreases the efficacy AE: often GIT irritation,
polyneuropathy, myelotoxicity, chronic hepatitis, pulmonary
disorders I: therapy and prophylaxy of urinary tract infections
Furantoin, Nitrofurantoin
