Review of Antimicrobial Agents Part I

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Review of Antimicrobial Agents Part I

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Review of Antimicrobial Agents Part I Siriluck Anunnatsiri, MD, MCTM, MPH Infectious Diseases & Tropical Medicine Department of Medicine Khon Kaen University – PowerPoint PPT presentation

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Title: Review of Antimicrobial Agents Part I

1
Review of Antimicrobial AgentsPart I

Siriluck Anunnatsiri, MD, MCTM, MPH
Infectious Diseases Tropical Medicine
Department of Medicine
Khon Kaen University

2
Classification of Antimicrobial Agents

?-lactam antibiotics
Penicillins, Cephalosporins, Carbapenems,
Monobactams, ?-lactam/?-lactamases inhibitors
Aminoglycosides
Macrolides
Ketolides Telithromycin, Dirithromycin
Lincosamides Lincomycin, Clindamycin
Quinolones
Chloramphenicol

3
Classification of Antimicrobial Agents

Tetracyclines, Tigecycline
Sulfamethoxazole/Trimethoprim (SMX/TMP)
Glycopeptides Vancomycin, Teicoplanin
Oxazolidinones Linezolid
Fosfomycin
Fusidic acid
Polymyxins Polymyxin B, Colistin
Metronidazole

4
Classification of Antimicrobial Agents

Lipopeptide Daptomycin
Streptogramins Quinupristin-Dalfopristin

?-lactam antibiotics
Aminoglycosides
Glycopeptides
5
Antimicrobial Properties

Structure
Spectrum
Mechanisms of action
Mechanism of resistance

Pharmacokinetic
Absorption
Distribution
Metabolism
Elimination
Pharmacodynamic
Drug interaction
Side effect

6
Beta-lactams Antibiotic Basic Structure
Aminoacyl
Thiazolidine ring
Dihydrothiazine ring
Hydroxyethyl
7
Beta-lactams Antibiotic General Properties

Inhibit cell wall synthesis
Bactericidal effect
Time-dependent bactericidal action
Inoculum effect on antimicrobial activity is more
prominent
In GNB - No or short PAE for most ?-lactam
Share ?-lactam class allergic reaction except
monobactams

8
PD Parameters affecting Antibiotic Potency
AUC/MIC gt125 for GNB gt25-50 for GPC Cmax/MIC gt10
gt 40-50 of dosing interval
9
Inoculum Effect

The effect of inoculum size on antimicrobial
activity
Dense population can be less susceptible to
?-lactams
Failure to express receptor (PBP)
High concentration of ?-lactamases
Trend to presence of resistant subpopulation

10
Postantibitic Effect

A persistent suppression of growth after levels
have fallen below the MIC

11
Bacterial Cell Wall Synthesis
Hiramatsu K. Lancet Infect Dis 2001 1 147-155
12
Bacterial Cell Wall Synthesis
(Transpeptidase)
Hiramatsu K. Lancet Infect Dis 2001 1 147-155
13
Beta-lactams Antibiotic Mechanism of Action
Hiramatsu K. Lancet Infect Dis 2001 1 147-155
14
Beta-lactams Antibiotic Mechanism of Resistance

?-lactamases destruction of antibiotic
Failure of antibiotic to penetrate the outer
membrane of gram-negative to reach PBP target
Efflux of antibiotic across the outer membrane of
gram-negative
Low-affinity binding of antibiotic to PBP target

15
Beta-lactams Antibiotic Adverse Reactions

Hypersensitivity 3 to 10
Irritability, jerking, confusion, seizures
especially with high dose penicillins and
imipenem
Leukopenia, neutropenia, thrombocytopenia
therapy gt 2 weeks
Interstitial nephritis
Cephalosporin-specific cefamandole, cefotetan,
cefmetazole, cefoperazone, moxalactam
Hypoprothrombinemia - due to reduction in vitamin
K-producing bacteria in GI tract

16
Penicillins Classification

Natural penicillins
Penicillin V, Penicillin G
Aminopenicillins
Ampicillin, Amoxicillin
Penicillinase-resistant penicillins
Cloxacillin, Dicloxacillin, Nafcillin,
Methicillin
Carboxypenicillins
Carbenicillin, Ticarcillin
Ureidopenicillin
Piperacillin, Azlocillin, Mezlocillin

17
Natural Penicillins Spectrum of Activity

Gram-positive Gram-negative
S. pneumoniae Neisseria meningitidis
Streptococcus sp.
Enterococcus sp. Anaerobes
C. diphtheriae Above the diaphragm
B. anthracis Clostridium perfringens
L. monocytogenes
Other
Treponema pallidum
Leptospira sp.

18
Penicillinase-Resistant Penicillins Spectrum

Gram-positive
MSSA
MSSE
Streptococcus sp.

19
Aminopenicillins Spectrum of Activity

Gram-positive Gram-negative
Streptococcus sp. Proteus mirabilis
Enterococcus sp. Salmonella sp.
L. monocytogenes Shigella
C. diphtheriae some E. coli
H. influenzae
N. meningitidis
Anaerobes
Above the diaphragm
Clostridium perfringens

20
Carboxypenicillins Spectrum of Activity

Gram-positive Gram-negative
Streptococcus sp. Proteus mirabilis
C. diphtheriae Salmonella sp.
Shigella
E. coli
H. influenzae
Neisseria sp.
Anaerobes Enterobacter sp.
Fairly good activity P. aeruginosa
Citrobacter sp.
Serratia sp.

21
Ureidopenicillins Spectrum of Activity

Gram-positive Gram-negative
Streptococcus sp. Proteus mirabilis
Enterococcus sp. Salmonella sp.
L. monocytogenes Shigella
E. coli
Klebsiella sp.
H. influenzae
Neisseria sp.
Anaerobes Enterobacter sp.
Fairly good activity P. aeruginosa
S. marcescens

22
Penicillins Pharmacology

Administration Oral, IV, IM
Varying oral absorption
40 for Ampicillin ? 75 for Amoxicillin
Varying protein binding
17 for aminopenicillin ? 97 for dicloxacillin
More free drugs in the presence of probenecid
Mainly excrete via renal tubular cells, which can
be blocked by probenecid.

23
Penicillins Pharmacology

Dose adjustment is needed when CCr lt 10-20
ml/min, on hemodialysis or CVVH
Biliary excretion is important only for nafcillin
and antipseudomonal penicillins.
Well distributed to most tissues, high
concentration in urine and bile
Relatively insoluble in lipid and penetrate cells
relatively poorly

24
Cephalosporins Classification
1st Generation 2nd Generation Cephamycins 3rd Generation 4th Generation
Cefazolin Cefamandole Cefmetazole Ceftriaxone Cefepime
Cephalothin Cefonicid Cefotetan Cefotaxime Cefpirome
Cephapirin Cefmetazole Cefoxitin Ceftazidime
Cephradine Cefotetan Cefoperazone
Cefadroxil Cefoxitin Ceftizoxime
Cephalexin Cefuroxime Cefsulodin
Cefprozil Moxalactam
Loracarbef Cefdinir
Cefaclor Cefditoren
Cefixime
Ceftibuten
Cefpodoxime
25
1st Generation Cephalosporins SpectrumBest
activity against gram-positive aerobes, with
limited activity against a few gram-negative
aerobesGram-positive Gram-negativeMSSA
EnterobacteriaceaeStreptococcus sp.

2nd Generation Cephalosporins/Cephamycins
Spectrum
More active against gram-negative aerobes
Cephamycin group has activity against
gram-negative anaerobes including Bacteroides
fragilis

26
3rd Generation Cephalosporins Spectrum

Increase potency against gram-negative aerobes
Ceftriaxone and cefotaxime have the best activity
against MSSA and Streptococcus sp.
Ceftazidime, moxalactam, cefixime, and ceftibuten
have less activity against MSSA
Ceftazidime, cefoperazone, and cefsulodin have
activity against P. aeruginosa.

27
4th Generation Cephalosporins Spectrum

Extended spectrum of activity
gram-positives similar to ceftriaxone
gram-negatives Enterobacteriaceae including
cephalosporinase-producer, P. aeruginosa.
Stability against ?-lactamases poor inducer of
extended-spectrum ? -lactamases

28
Cephalosporins Pharmacology

Polar, water-soluble compounds
Administration IM, IV, oral, intraperitoneum
High oral bioavailability
Varying protein binding 10 -gt 98
Largely confined to extracellular compartment,
relatively poor intracellular concentration
Good CNS penetration Only 3rd 4th gen.
cephalosporins
Almost excrete via renal tubular secretion,
except ceftriaxone and cefoperazone are largely
eliminated via biliary route

29
Carbapenems

Imipenem
N-formimidoyl derivative of thienamycin
Need to combine with cilastatin to prevent renal
dehydropeptidase I hydrolysis and nephrotoxic
effect
Meropenem, Ertapenem
?-1-methyl, 2-thio pyrrolidinyl derivative of
thienamycin

30
Carbapenems Spectrum of Activity

Most broad spectrum of activity of all
antimicrobials
Have activity against gram-positive and
gram-negative aerobes, anaerobes, Nocardia sp.,
rapid-growing mycobacteria
Bacteria not covered by carbapenems include MRSA,
MRSE, E. faecium, C. difficile, S. maltophilia,
B. cepacia
Ertapenem not active against P. aeruginosa and
Acinetobacter sp.

31
Carbapenems Pharmacology

Absorbed poorly after oral ingestion
T1/2
Imipenem, Meropenem 1 hr
Ertapenem 4 hr
Well distributed to body compartment and
penetrate well into the most tissues
Excrete via renal, dosage adjustment is required
in patient with impaired renal function.
Need supplement dose in patient performing CVVH,
hemodialysis

32
?-Lactam/?-Lactamase Inhibitor

Ampicillin/sulbactam (A/S)
Amoxicillin/clavulanate (A/C)
Ticarcillin/clavulanate (T/C)
Piperacillin/tazobactam (P/T)
Cefoperazone/sulbactam (C/S)

33
?-Lactam/?-Lactamase Inhibitor Spectrum

Maintain spectrum of ?-Lactams but enhance
activity against ?-Lactamase (Ambler class A)
producing organisms
Activity against MSSA, Streptococcus sp.,
Enterococcus sp. (Except C/S), ?-Lactamase
producing Enterobactericeae, P. aeruginosa (Only
P/T, C/S), Anaerobes.

34
?-Lactam/?-Lactamase Inhibitor Pharmacology

Clavulanate, Sulbactam Moderately well absorbed
Good tissue distribution
Penetration into inflamed meninges
Clavulanate, Sulbactam Poor
Tazobactam Good in animal model
Excretion
Clavulanate Lung, feces, urine
Sulbactam, Tazobactam - Urine

35
Monobactams

Aztreonam
Bind primarily to PBP 3 in Enterobacteriaceae,
P. aeruginosa, and other gram-negative aerobes
No activity against gram-positive or anaerobic
bacteria
Low incidence of drug hypersensitivity no
cross-reaction with other ?-Lactams
Weak ?-Lactamase inducer

36
Aminoglycosides Basic Chemical Structure
Aminocyclitol Ring
37
Aminoglycosides Classification
Family Member
Streptidine aminocyclitol ring Streptidine aminocyclitol ring
Streptomycin Streptomycin
Spectinomycin
2-deoxystreptamine aminocyclitol ring 2-deoxystreptamine aminocyclitol ring
Kanamycin Kanamycin, Amikacin, Tobramycin, Dibekacin
Gentamicin Gentamicin, Netilmicin, Sisomicin, Isepamicin
Neomycin Neomycin, Paromomycin
38
Aminoglycosides Mechanism of Action
39
Aminoglycosides Mechanism of Resistance
Adenyltransferase
Acetyltransferases
Phosphotransferases
40
Aminoglycosides Spectrum of Activity

Gram-Negative Aerobes
Enterobacteriaceae, P. aeruginosa, Acinetobacter
sp.- Kanamycin Gentamicin groups
F. tularensis, Brucella sp., Y. pestis -
Streptomycin, gentamicin
N. gonorrhoeae - Spectinomycin
Mycobacteria
M. tuberculosis Streptomycin, kanamycin,
amikacin
Non-tuberculous Amikacin, streptomycin

41
Aminoglycosides Spectrum of Activity

Gram-Positive Aerobes (In vitro synergy)
S. aureus, S. epidermidis, viridans
streptococci, Enterococcus sp.
Nocardia sp. - Amikacin
E. histolytica, C. parvum - Paromomycin

42
Aminoglycosides Pharmacology

Bactericidal effect
Concentration dependent killing
Little influence by inoculum effect
Presence of PAE effect
Administration IV, IM, intrathecal,
intraperitoneum, inhale, oral (neomycin,
paromomycin), topical
Low level of protein binding (10), high water
solubility, lipid insolubility

43
Aminoglycosides Pharmacology

99 of drug is excreted unchanged by glomerular
filtration
5 of excreted drug is reabsorbed at renal
proximal tubule

44
Once-Daily Aminoglycosides

Equal efficacy compared to multiple-dose
administration
May lower but not eliminate risk of drug-induced
nephrotoxicity and ototoxicity
Simple, less time consuming, and more cost
effective
Does not worsen neuromuscular function in
critically ill ventilated patients
Probably should not be used in enterococcal
endocarditis
Need further study in pregnancy, cystic fibrosis,
GNB meningitis, endocarditis, and osteomyelitis

45
Aminoglycosides Adverse Effects

Neuromuscular blockage
Nephrotoxicity
Reversible if detection early
Risk factors prolonged trough level, volume
depletion, hypotension, underlying renal
dysfunction, elderly, other nephrotoxins
Ototoxicity
Cumulative dose
8th cranial nerve damage - irreversible
Vestibular toxicity dizziness, vertigo, ataxia
Auditory toxicity tinnitus, decreased hearing
(high frequency)

46
Glycopeptides

Vancomycin
Teicoplanin

47
Glycopeptides Mechanism of Action
Hiramatsu K. Lancet Infect Dis 2001 1 147-155
48
Glycopeptides Mechanism of Resistance in S.
aureus
Hiramatsu K. Lancet Infect Dis 2001 1 147-155
49
Glycopeptide-resistant S. aureus
NCCLS NCCLS NCCLS BSAC BSAC
S I R S R
Vancomycin lt4 8-16 gt32 lt4 gt8
Teicoplanin lt8 16 gt32 lt4 gt8
NCCLS The National Committee for Clinical
Laboratory Studies BSAC The British Society for
Antimicrobial Chemotherapy
50
Glycopeptide-resistant S. aureus

Recommend using MIC determination for
confirmation of VISA, GISA, or VRSA isolates
Heteroresistance phenomenon Hetero-VRSA
Only a subpopulation of S. aureus can grow on
vancomycin-containing agar (gt8 ?g/ml)
Precursor of VISA/VRSA isolates
Population analysis is needed to identify
hetero-VRSA

51
Glycopeptide-resistant Enterococci
Stain Characteristics Acquired resistance level, Type Acquired resistance level, Type Acquired resistance level, Type Acquired resistance level, Type Acquired resistance level, Type Intrinsic resistance, low level, Type VanC1, C2, C3
Stain Characteristics High, VanA Variable, VanB Moderate, VanD Low Low Intrinsic resistance, low level, Type VanC1, C2, C3
Stain Characteristics High, VanA Variable, VanB Moderate, VanD VanG VanE Intrinsic resistance, low level, Type VanC1, C2, C3
MIC, mg/L
Vancomycin 64-100 4-1000 64-128 16 8-32 2-32
Teicoplanin 16-512 0.5-1 4-64 0.5 0.5 0.5-1
Modified Target D-Ala-D-Lac D-Ala- D-Lac D-Ala- D-Lac D-Ala-D-Ser D-Ala-D-Ser D-Ala- D-Ser
Courvalin P. Clin Infect Dis 2006 42 S25-S34.
52
Glycopeptide-resistant Enterococci
VanS Membrane-associated sensor kinase VanR
Cytoplasmic response regulator
53
Glycopeptides Spectrum of Activity

Gram-positive bacteria
MSSA, MRSA, MSSE, MRSE
S. pneumoniae (including PRSP)
Streptococcus sp.
Enterococcus sp.
Corynebacterium, Bacillus, Listeria, Actinomyces
Rhodococcus equi
Clostridium sp. (including C. difficile),
Peptococcus, Peptostreptococcus
No activity against gram-negative aerobes or
anaerobes

54
Vancomycin Pharmacology

Bactericidal effect except for Enterococcus spp.
Time-dependent bactericidal action
Short PAE effect
Administration IV, oral (poor oral absorption),
intraperitoneum, intrathecal, intraventricular,
intraocular
Protein binding 30-55
Poor CSF/aqueous humor penetration
Primarily excrete unchanged by glomerular
filtration, higher clearance in burn patients

55
Vancomycin Pharmacology

IV administration
Concentration lt 5 mg/ml
Rate lt 15 mg/min
Dosage in normal renal function
30 mg/kg/day divided into 2-4
dosages
Intraperitoneal administration
In CAPD patient, therapeutic serum level can be
obtained.
Intrathecal or intraventricular administration
Recommend for treatment of shunt
infection/ventriculitis
Dosage 10-20 mg/day (diluted up to 2 ml in 0.9
NSS conc. 2.5-25 mg/ml)
Monitor CSF trough level 10-20 ?g/ml

56
Vancomycin Dosage in Renal Insufficiency

Hemodialysis 15 mg/kg q 7-10 days
If high-flux membrane is used, 20 mg/kg loading
dose with 500 mg after each dialysis
CVVH 0.5-1.5 g q 24 hours
CVVHD 0.8-1.75 g q 24 hours
Renal impairment
Loading dose 15 mg/kg, followed by
Dose (mg/day) 15.4 x CCr (mL/min)
Loading dose 25 mg/kg, followed by 19 mg/kg at
calculated interval
Interval normal interval (86 0.689 x CCr
3.66)

57
Indications for Vancomycin Dosage Monitoring

Concomitantly received another nephrotoxic agents
Receiving high-dose vancomycin
Rapidly changing renal function
Undergoing hemodialysis
Receiving vancomycin for treatment CNS infection
Neonate
Extremely ill patients
Suspected therapeutic failure
Morbid obesity
Burn patient

Optimal Targets Peak serum concentration 30-40
?g/ml Trough level 10-15 ?g/ml Average steady
state 15 ?g/ml
58
Teicoplanin Pharmacology

Administration IV, IM, oral (poor absorption),
intraperitoneum, intrathecal
90 protein binding, highly bound in tissue
Better bone concentration compared to vancomycin
More active against Streptococci, including
Enterococci than vancomycin
Eliminated by kidney

59
Teicoplanin Pharmacology

IV/IM administration
Loading 6 mg/kg q 12 hours x 3 doses then q 24
hours
In S. aureus endocarditis or septic arthritis,
and in burn pt.
12 mg/kg q 12 hours x 3 doses then q 24 hours
Intraperitoneal administration
In CAPD patient, therapeutic serum level can be
obtained.
20 mg/L in each exchange (4 times daily) x 10
days or for 5 days after bacterial clearance
Intrathecal or intraventricular administration
Dosage 10-20 mg/day q 24-48 hours

60
Teicoplanin Dosage in Renal Insufficiency

Hemodialysis 6-12 mg/kg q 72 hours
CVVHD 800 mg D1, 400 mg D2 3 then 400 mg q
48-72 hours
Renal impairment
CCr 40-60 mL/min 6-12 mg/kg q 48 hours
Maintenance daily dose normal dose x pts
CCr/normal CCr
Extended Interval normal CCr/pts CCr

61
Indications for Teicoplanin Dosage Monitoring

Receiving high-dose teicoplanin
Rapidly changing renal function
Undergoing CVVHD
Suspected therapeutic failure
Trough level lt 20 ?g/ml is correlated with
treatment failure.
IVDU with endocarditis
Burn patient

62
Glycopeptides Adverse Reaction

Ototoxicity
Rare, Reversible
Co-administer with AG augment this event
Vertigo and tinnitus may precede hearing loss
Nephrotoxicity Vancomycin gt Teicoplanin
Rate increase when co-administer with AG
Acute interstitial nephritis has been reported.
Neutropenia, Thrombocytopenia
Thrombophrebitis

63
Glycopeptides Adverse Reaction

Red neck or Red man syndrome
Infusion-related reaction from vancomycin, rarely
from teicoplanin
Anaphylactoid reaction
Rapid onset of erythematous rash and/or pruritus
affecting head, face, neck, and upper trunk with
or without angioedema and hypotension
Probably related to histamine release
Prevention by
Decreasing infusion rate or concentration
Using antihistamine (H1 receptor antagonist)
Drug rash, Drug-related fever

64
Glycopeptides Drug Interaction

Drug precipitation when mixed with
ceftazidime, heparin, chloramphenicol,
corticosteroid, aminophylline, barbiturate,
diphenylhydantoin, sodium bicarbonate
Anion-exchange resins can bind vancomycin and
decrease activity of vancomycin in the gut lumen.

65
PART II
...... to be continue

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