1. 1 Infectious Diseases�Antimicrobial, antibacterial therapy��Prof. Elisabeth Nagy �Institute of Clinical Microbiology, �University of Szeged
Antibiotic selection in different infectious diseases.
6. November 2007
2. 2 Why is the antimicrobial therapy different from therapy with other drugs? Every specialist in medicine use antibiotics
The consequences of the inappropriate antibiotic usage is not seen immediately
Many patients with infectious diseases can recover without antibiotics
Empirical – calculated antibiotic selection
Antibiotic therapy guided by in vitro antibiotic resistance determination
Laboratory methods to help antibiotic selection
3. 3 Selection of antibiotics for therapy The selection of the antibiotic should depend on
the place of the infection
the severity of the infection, the general condition of the patient
the causative agent
the local or regional resistance situation
It should be considered the changing spectra of the causative agents
Antibiotics should be used only if bacterial infection has been proven or assumed
If we give antibiotics, the antibiotic and its doses should be clinical efficacious (”hit and run”).
4. 4 Motto Louis Pasteur: Ce sont les microbes qui auront le dernier mot.
5. 5 It will not be discussed: Antiviral therapy and prophylaxis
Antiparasitic therapy and prophylaxis
Antibacterial prophylaxis
6. 6 We will discuss: The main classes of antibiotics and their most important characteristics
Antibiotic selection in the most important clinical settings (pathogen specific antibiotic selection)
Antifungal therapy in systemic fungal infections
Laboratory methods to help antibiotic selection
7. 7 Beta-lactam antibiotics The largest group of antibiotics
The main features of their antibiotic activity:
Slow bactericidal effect, they can have effect on multiplying bacteria
Above a given concentration the killing effect can not be increased
They have no post-antibiotic effect
There is an inoculum's effect (e.g. beta-lactamase producing staphylococci)
During therapy the serum concentration of the beta-lactam antibiotics should be kept above the MIC of the pathogen (it should be given in long infusion)
8. 8 Beta-lactam antibiotics Main groups:
Penicillines (phenoxymethilpenicillin, benzylpenicillin, ampicillin, amoxicillin flucoloxacillin, methicillin)
Cephalosporins (I., II., III., IV. generation)
Cephamycins
Oxacephems
Carbapenems
Monobactams
Beta-lactam/beta-lactamase inhibitor combinations
9. 9 Beta-lactam antibiotics Their activity:
In the bacterial cell they bind to the penicillin binding proteins (target molecules) and inhibit the cell wall production
Resistance mechanisms against beta-lactam antibiotics:
Production of beta-lactamases (>100 different enzymes). The genes coding the different enzymes can be found on plasmid, on the chromosome, or on transposons
Mutation of the penicillin binding proteins (MRSA)
Changes in the cell wall permeability
(Changes in the efflux pump)
10. 10 Aminoglycosids The classical aminoglycosids:
Streptomycin (anti -uberculotic activity)
Neomycin (only locally)
Kanamycin (is not used because toxicity)
Spectinomycin (N. gonorrhoeae)
The modern aminoglycosids:
Gentamicin
Tobramycin
Netilmicin
Amikacin
(Sisomicin, dibecamicin)
11. 11 Aminoglycosides Their activity:
Bactericidal antibiotics
They are toxic (oto- and nephrotoxicity)
In the case of frequent administration they cumulate
They inhibit the protein synthesis (binding to the 30s ribosomal protein they inhibit the activity of the mRNS)
They have an expressed post-antibiotic activity
They can be combined with the beta-lactam antibiotics (synergistic effect)
The antibacterial effect is concentration dependent (daily one dose - high peek concentration)
12. 12
13. 13 Aminoglycosides Their activity:
Bactericidal antibiotics
They are toxic (oto- and nephrotoxicity)
In the case of frequent administration they cumulate
They inhibit the protein synthesis (binding to the 30s ribosomal protein they inhibit the activity of the mRNS)
They have an expressed post-antibiotic activity
They can be combined with the beta-lactam antibiotics( synergistic effect)
The antibacterial effect is concentration dependent (daily one dose - high peek concentration)
14. 14
15. 15 Aminoglycosides Their activity:
Bactericidal antibiotics
They are toxic (oto- and nephrotoxicity)
In the case of frequent administration they cumulate
They inhibit the protein synthesis (binding to the 30s ribosomal protein they inhibit the activity of the mRNS)
They have an expressed post-antibiotic activity
They can be combined with the beta-lactam antibiotics (synergistic effect)
The antibacterial effect is concentration dependent (daily one dose - high peek concentration)
16. 16 Aminoglycosides Resistance mechanisms:
Changes of the target (mutation of the ribosomal proteins)
Changes in the permeability of the cell wall (due mutation the active transport of the AGs will be inhibited)
Aminoglycoside modifying enzymes (12) (coded on plasmids)
6 modify gentamicin
6 modify tobramycin
4 modify netimicin
2 modify amikacin
Active efflux pump function
17. 17 Quinolones - fluoroquinolones They have been in the clinical practice since
Quinolones are active against Enterobacteriaceae
Fluoroquinolones - have a broader spectrum, especially the 3rd and 4th generation compounds
They are bactericidal antibiotics, their activity is dependent from
concentration (we had to reach the effective bactericidal activity)
AND
time dependent (to prevent resistance due to mutation)
18. 18
19. 19 Quinolones and fluoroquinolones I. Quinolones : nalidixic acid
non complicated urinary tract infection
oxolinic acid
Fluoroquinolones:
1st gen.: norfloxacine UTI and enteric infections
2nd gen.: pefloxacine as above + chronic ART and LRT ofloxacine infections, HAP, biliary tract inf.,
ciprofloxacine Go., bon and soft tissue inf.
20. 20 Quinolones and fluoroquinolones II. Fluoroquinolones:
3rd gen.: sparfloxacin CAP, HAP, BAE
grepafloxacin intra-abdominal, biliary inf.
levofloxacin UTI, pelvic inf., better effect on Gram-positive bacteria
4th gen.: clinafloxacin
(trovafloxacin) + anti-anaerobic effect
moxifloxacin
CAP= community aquiered pneumonia
NAP nosocomial aquiered pneumonia
BAE Bronchitis acut exacerbatioCAP= community aquiered pneumonia
NAP nosocomial aquiered pneumonia
BAE Bronchitis acut exacerbatio
21. 21 Activity of quinolones - fluoroquinolones They inhibit the DNA synthesis by inhibiting different enzymes bactericidal effect
topoisomerase II (gyrase A, B) Gram-negative bacteria
topoisomerase IV parC Gram-positive bacteria
As a consequence :
the double strand structure of the DNA can not be formed
the DNA can not have a place in the cell
the single stranded DNA will be split by the endonucleases outside the cell
22. 22 Development of resistance against the fluoroquinolones Due to mutation of chromosomal genes
target mutation
gyrA, gyrB (Gram-negative bacteria)
parC, parE (Gram-positive bacteria)
gene mutations responsible for active efflux pump function
It has been proved in P. aeruginosa (?15), S. pneumoniae, B. fragilis
Mutations of genes responsible for the permeability of the cell wall
Plasmid coded resistance has been described
23. 23 Macrolides (azalides) Activity:
bacteriostatic drugs (in high concentration and in the case of low inoculum they can be bactericidal)
Narrow spectrum - „broad spectrum”
Mechanism of the effect:
Inhibition of the protein synthesis (they bind to the 50s subunit of the 70s ribosome)
Their activity is time dependent, above of certain concentration their activity can not be increased
They have a long postantibiotic effect
24. 24 Macrolides (azalides) The classical drugs: erythromycin, oleandomycin
Half time: 1,2 h
Because of wrong absorption sub-therapeutic level
Motilin like effect - diarrhoea
New compounds:
Better pharmacokinetics (high tissue concentration!!!)
No motilin like effect
Cross-resistance with the older substances
Half life: josamycin (Wilprafen) 1,5 h
clarythromycin (Klacid) 3-5 h
roxithromycin (Rulid) 8-12 h
azithromycin 11-14 h
25. 25 Macrolides are the drug of choice CAP (atypical pneumonia)
Mycoplasma pneumoniae,
Chlamydia pneumoniae,
Legionella pneumophila
STDs, pelvic infections
Chlamydia trachomatis
Haemophylus ducreyi
Ureaplasma urealyticum
Gastrointestinal infection
Campylobacter spp/ Helicobacter pylori
Other infections
Corynebacterium diphteriae diminish carrier status
Borelliosis (Lyme-disease)
Mild skin and soft tissue infections
26. 26 Resistance to macrolides Decreased permeability (due to mutation)
Production of macrolide splitting enzymes
Decreased binding to the receptor (due to mutation)
Active efflux
The different resistance mechanisms means cross resistance to the different macrolides
27. 27 Lincosamides Lincomycin, clindamycin (Dalacin C)
They are active against:- Gram-positive bacteria
- anaerobes
Excellent penetration to the bones and soft tissue
They can be used in case of:
Aspiration pneumonia
Osteomyelitis
In myonecrosis cased by S. pyogenes (in combination with penicillin)
Diabetic foot ulcer
Bacterial vaginosis as an alternative therapy
Resistance mechanisms are the same as in macrolides
28. 28 Tetracyclines The oldest „broad spectrum” antibiotic
They are bacteriostatic, they inhibit the protein synthesis of bacteria by binding to the 30s subunit of the ribosome
The resistance is spreading very quickly among different bacteria ( the gene can be found on transposons)
Active efflux
Mutation at the site of the binding of the antibiotic
Different derivatives:
Older derivatives: oxytetracyclin, chlortetracyclin
Newer derivatives: doxycyclin, minocyclin
Tygecyclin (introduced recently in clinical practice)
29. 29 Other antibiotics: Chloramphenicol:
Broad spectrum, bacteriostatic
Inhibit the protein synthesis
Toxic (potentially fatal aplastic anaemia)
It can be used in special cases:
Sever, life threatening mixed infections (aerobic + anaerobic)
In meningitis caused by ampicillin resistant H. influenzae
Brain abscess (good penetration through the inflamed menings)
Severe Salmonella thyphi infection
30. 30 Other antibiotics: Vancomycin / teicoplanin:
Bactericidal activity, they inhibit the cell wall synthesis, damage the cytoplasma membrane and inhibit the RNA synthesis
High molecular weight glycopeptides
They act only on Gram-positive bacteria including:
MRSA. MRSE, Enterococcus spp, Corynebacterium JK, D2, Clostridium difficile
No cross resistance with beta-lactam antibiotics
Synergistic effet with combination of aminoglycosides
Resistance appeared in the 1980s (the genes can be found on the chromosome or on plasmids) (vanA, B, C):
Enterococci, staphylococci
31. 31 Other antibiotics: Nitroimidazoles: metronidazole, tinidazole
Bacteriocidal antibiotics their metabolites damage the bacterial DNA
Antiparasitic drug
They act on Gram-negative anaerobes,
And on some Gram-positive anaerobes (C. difficile)
Resistance is rare (Bacteroides spp)
Genes which can be found on the chromosome and on plasmids are responsible for the resistance (nimA, B, C, D, E)
32. 32 Other antibiotics: Sulphonamidok, trimetoprim
(co-trimoxazol: TMP/SMX 1:20 combination has a
synergistic effect)
Mupirocin (elimination of carriage of S. aureus, MRSA)
Fosfomycin (uncomplicated UTI)
Rifampicin (in combination against Gram-positive bacteria)
Nitrofurantoin (UTI)
Polymyxinek (Colistin) (against pan-resistant pseudomonas inf.)
33. 33 Infectious diseases
possible pathogens
selection of antibiotics
34. 34 Upper respiratory tract infections�tonsillo-pharyngitis Viruses (80-85%) do not give antibiotics !!
S. pyogenes (+ C and G ) penicillin G, (1.,2.g cephalos.) macrolides
S. aureus methicillin, (2.g cephalos.), amoxi/clav
H. influenzae ampicillin (2., 3.g cephalos.)
Vincent angina (anaerobes) amoxi/clav, amp/sulb, clindamycin
C. diphtheriae penicillin G, erythromycin (antitoxin)
Y. enterocolitica 2.g. cephalosporins
M. pneumoniae macrolides
(N. meningitidis)* penicillines, macrolides
in case of carrige rifampicin/cipro, ceftriaxon
Sarjadzó gomba* nystatin (locally)
carrige or sign of systemic infection? Penicillin g esetében 7 nap cepahlosporinok esetében 5 napPenicillin g esetében 7 nap cepahlosporinok esetében 5 nap
35. 35 Upper respiratory tract infections�acute sinusitis Dominating flora:
H. influenzae (b or other serotype) ? 25% ?
S. pneumoniae 35%
M. catarrhalis 20% (100%-beta-lactamase producers)
Rare pathogens:
Other streptococci
S. aureus
Pseudomonas spp
Enterobacteriaceae
viruses (rhinovirus, influenza, parainfluenza)
(anaerobes)
Therapy: ampicillin/amoxicillin, 2., 3. g cephalosporins, beta-lactam/beta-lactamase inhibitor combination, macrolides
36. 36 Upper respiratory tract infections�chronic sinusitis Most frequently isolated bacteria:
a-hemolytic streptococci Bacteroides sp
H. influenzae Porphyromonas sp
S. aureus Fusobacterium sp
S. pneumoniae Peptostreptococcus sp
M. catarrhalis Peptococcus sp
Pseudomonasok V. parvula
Klebsiella spp Propionibacterium sp
Proteus spp
Therapy: antibiotic with an activity against aerobic and anaerobic bacteria (amoxi/clav, combination therapy)
Indirect pathogenesity
37. 37 Upper respiratory tract infections�acut otitis media (AOM) Most frequent pathogens:
S. pneumoniae
H. influenzae
M. catarrhalis
(S. aureus (<2%))
(M. pneumoniae)
viruses (RSV, influenza, adeno)
Therapy:
ampicillin/amoxicillin, amoxi/clav, cefaclor, cefuroxim, cefprozil, (pulmonary fluoroquinolones)
38. 38 Pneumonia�Community acquired pneumonia (CAP) Most frequent pathogens in different age groups:
Age group Pathogens
New born S. agalactiae
C. trachomatis
Infants S. pneumoniae
H. influenzae b
Young adult M. pneumoniae
H. influenzae
S. aureus
Elderly S. pneumoniae
Legionella
In any age group viruses
39. 39 Pneumoniák�Community acquired pneumonia (CAP) Distribution of pathogens according to underlying disease
Undelaying disease Possible pathogen
COPD S. penumoniae, H. influenzae, Gram- negative rods
CF P. aeruginosa, S. aureus
HIV P. carinii, atypical mycobacteria
Alcoholism S. pneumoniae, H. influenzae, K. pneumoniae
Diabetes mellitus S. aureus, mucormycosis
40. 40 Pneumonia�Therapy of the community acquired pneumonia (CAP) - Beta-lactam (amoxicillin vagy amoxi/clav. or ceftriaxon) +/- macrolide
- New pulmonary fluoroquinolones (moxifloxacin, levofloxacin)
- In the case of virus pneumonia antibiotic should be given only as a adjuvant therapy to patients with underlying disease or extreme age
41. 41 Other pneumonia cases� Hospital acquired pneumonia (HAP):
antibiotic should be given according the antibiogram
Aspiration pneumonia:
anaerobes can always be involved
clindamycin,
beta-lactam - beta-lactamase inhibitor combination
in severe case carbapenems
(cefoxitin / aminoglycoside combination)
42. 42 Acut bronchitis virus infection antibiotic should not be given !!
M. pneumoniae macrolide, doxycyclin
C. pneumoniae macrolide, doxycyclin
S. pneumoniae
H. influenzae not always need the antibiotic therapy
M. catarrhalis (if yes: pulmonary quinolones moxifloxacin, levofloxacin or amoxi/clav)
43. 43 Chronic bronchitis with acute exacerbation (CBAE) Pathogens: H. influenzae
S. pneumoniae
M. catarrhalis
in rare cases M. pneumoniae
Therapy: Amoxi/clav
new macrolides (azithromycin)
doxycyclin
pulmonary fluoroquinolones
44. 44 Gastrointestinal diseases Virus infections:
rotavirus in infants and young children)
adeno, astro, noro, calici virus, etc.
Administration of antibiotics is not recommended !!
Bacterial infections:
Salmonella sp (fluoroquinolones)
Shigella (ampicillin, chloramphenicol)
Campylobacter (macrolides)
Y. eneterocolitica (if needed according to antibiogram)
Vibrio cholerae (tetracyclin)
E. coli
S. aureus
C. difficile (vacomycin ??? metronidazole)
Administration of antibiotics is recommended only in sever cases
45. 45 Urinary tract infections Non-complicated UTI: administration of antibiotics p.o. for 3-5 days
Sulphametoxasol-trimetoprim
Trimetoprim 3 days
Fluoroquinolones (1st and 2nd generation)
Beta-lactam antibiotikums
ampicillin (resistance problems)
amoxicillin (resistance problems)
Augmentin (amoxicillin/clavulánsav) 5 days
Unasyn (ampicillin/sulbactam)
(cephalexin)
(cefaclor)
One day therapy is not recommended any more!!!
46. 46 UTI (cont.) Non-complicated pyelonephritis
Antibiotics should be given parenteral and afterwards p.o. at least for 7-10 days:
beta-lactam (2nd gen. cephalosporins, Augmentin, Unasyn)
aminoglycosides (gentamycin, tobramycin)
After 2 weeks of treatment urine cultuer should be carried out
Complicated UTIs
Antibiotics should be given parenteral afterwards p.o. for 2-6 weeks (hospitalisation is needed at the beginning of the therapy)
Antibiotics should be given according to antibiogram!!
Asymptomatic bacteruria – no need of treatment only if the patient is pregnant.
47. 47 Anaerobic infections Frequently mixed infection caused by aerobic and anaerobic bacteria:
Aminoglycosid + clindamycin /(cefoxitin) /metronidazol
Carbapenems
Amoxicillin/clavulánsav, piperacillin /tazobactam
Aminoglycosides are not active against anaerobes
Only the 4th gen. Fluoroquinolones have anti-anaerobic effect (clinafloxacin, moxifloxacin)
48. 48 Meningitis Age group Frequent pathogen Other pathogens
New born Streptococcus B S. pneumoniae
E. coli H. influenzae
Listeria spp S. aureus
Enterobacteriaceae
1-3 month Streptococcus B E. coli
S. pneumoniae Salmonella spp
H. influenzae
Listeria spp
3 month-5 years S. pneumoniae S. pyogenes
H. influenzae Salmonella spp
N. meningitidis
>5 years S. pneumoniae S. pyogenes
N. meningitidis S. aureus
49. 49 Meningitis Empiric therapy:
In new born: ceftriaxon/cefotaxim + ampicillin
>1 month – 50 years: ceftriaxon/cefotaxim +vancomycin
>50 years: (ampicillin) + ceftriaxon/cefotaxim + vancomycin, meropenem
Surgery /trauma: ceftazidim + vancomycin, meropenem
According to the culture results the empiric therapy should be changed
50. 50 Problematic bacterial strains according to antibiotic resistance Nosocomial multiresistant strains:
MRSA
MRS cagulase-negative
Acinetobacter baumani
Pseudomonas aeruginosa
Enterococcus faecalis/faecium
Enterobacter cloaceae
Other problematic strains:
- penicillin resistant S. pneumoniae
- erythromycin resistant S. pyogenes,
S. pneumoniae
- fluoroquinolone resistant Gram-
negative bacteria
- imipenem resistant pseudomonas, B. fragilis
- ESBL producing Gram-negative
strains
- metronidazol resistant Bacteroides
- multi-resistant Mycobacterium
- etc.
51. 51 Therapy of the systemic fungal infections Special patients population
Difficulties in the laboratory diagnosis
Most frequent pathogenic fungi
52. 52 Special patient population in risk �(systemic fungal infections) Broad spectrum antibiotic therapy
Aggressive tumour chemotherapy
immunosuppressive therapy
immundefficient status for any reason
invasive procedures
intra-abdominal surgery
long-term parenteral nourishing
intra-venous and intra-arterial catheters
53. 53 Difficulties in the laboratory diagnosis� (systemic fungal infections) The physician should think on it
The culture of fungi form the blood in sepsis caused by fungi is successful only in <50%
To detect the antigen from the blood is not sensitive enough
Molecular genetic methods (PCR) can prove the presence of fungi in genus or species level but can not recover resistance
The growth rate is slow
Standardisation of the resistance determination is difficult
54. 54 Fugi causing systemic infections Candida albicans
Other Candida spp
Aspergillus spp
Fusarium spp
Malassezia spp
Trichosporon spp
Cryptococcus neoformans
Blastoschizomyces capitatum
Hansenula anomala
Etc.
55. 55 Antifungal drugs used in systemic fungal infection I.
56. 56
57. 57 Antifungal drugs used in systemic fungal infection New antifungal drugs are developed they are under clinical investigation (terbinafin, other echinocandins, sordarins, chitin synthetase inhibitors, topoisomerase inhibitors)
Antifungal drugs such as antibacterial drugs can be used in combination to increase activity
58. 58 Laboratory methods Disc diffusion method (semi-quantitative S, IM, R)
MIC = minimal inhibitory concentration (”break-point”)
Antibiotic serum level determination (vancomycin, aminoglycosides)
Determination of bactericidal activity in the blood (in case of treatment of endocarditis)
Investigation the effect of antibiotic combinations
What can we do with the pan-resistant isolates?
59. 59
60. 60 Method for detection ESBL production (extended spectrum beta-lactamase)
61. 61 Multiresistant isolates in the clinical practice Citrobacter freundii isolated for the blood culture of a septic patient
(only doxycyclin susceptibility)
62. 62
63. 63 Strategies how to use antibiotic in severly ill patient The starting antibiotic should have the optimal effect. If the conditions of the patient is improving the antibiotic can be changed (”streamlining”, ”step down” therapy)
In sever infection such as bacterial sepsis the therapy used in the 24-48 hours will decide the future of the patient and the rate of the lethality!!
64. 64 Erroneous beliefs in connection with the antibiotic therapy The broadest spectrum antibiotic is always the best.
The infectious diseases should be treated immediately (we have no time to take samples).
The improvement or deterioration of the patient’s condition after introduction of an antibiotic therapy is the sign of the efficacy or ineffectiveness of the selected antibiotic.
More sever infection needs more broader spectrum antibiotic treatment.
The more sever is the infection the more recently developed antibiotic should be used.
The combination of 2 or more antibiotics is more effective than a properly selected single one.
The antibiotic which I use will not select antibiotic resistance
65. 65 - SANFORD GUIDE 37th edition (2007)
Guide to antimicrobial therapy (ISBN 930808-04-6)
Actual national guide lines (evidence based)
International guidelines (UK, USA, Canada)
Guide lines of the pharmaceutical companies
