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Antibiotics

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Title: Antibiotics

1
Antibiotics

MR. H GEE MD, FRCOG
Hon. Assoc. Clinical Professor
University of Warwick

2
Objectives

By the end of this lecture you should be able to
Classify commonly used antibiotics into six major
antibiotic classes of
Beta lactams
Aminoglycosides
Fluoroquinolones
Macrolides
Tetracyclines
Glycopeptides
Metronidazole
Understand the mechanism of action of each
antibiotic class.
Understand clinical use of each class of
antibiotic
Possible major side effects.

3
There are Three in this Relationship
Drug
Toxicity
Resistance
Pharmacokinetics (PK)
Pharmacodynamics(PD)
Infection
Bacteria
Host
Host defence
4
Improving the probability of positive outcomes

Window of opportunity
Early recognition and treatment of infection
Selection of appropriate antibiotic(e.g. through
in vitro susceptibility determination)
Optimization of DOSE using Pharmacodynamic
principles
Use optimized dosing that would allow for the
minimization of selecting further resistance

5
Early recognition of infection (Sepsis)

Systemic inflammatory response syndrome (SIRS)
(Bone et al Crit Care med 1989.17 389)
Systemic activation of the immune response
? 2 of the following in response to an insult
T gt 38 .C or lt 36.C
HR gt 90 bpm
RR gt 20 bpm
WBC gt 12 000 cells/mm3
Sepsis
SIRS suspected or confirmed infection

6
Key Message 1

Diagnose sepsis early and give antibiotics
promptly to reduce mortality from sepsis

7
Antibiotics

Actions
Bactericidal
Kills bacteria, reduces bacterial load
Bacteriostatic
Inhibit growth and reproduction of bacteria
All antibiotics require the immune system to work
properly
Bactericidal appropriate in poor immunity
Bacteriostatic require intact immune system

8
ß-Lactams
?-Lactam Ring
Thiazolidine Ring
9
ß-Lactams
ß-Lactams

Penicillin
Narrow Spectrum
Benzylpenicillin (Penicillin G)
Phenoxymethylpenicillin (Pen V)
Flucloxacillin
Broad Spectrum
Amoxicillin/Co-amoxiclav
Ampicillin
Piperacillin with Tazobactam (Tazocin)

Cephalosporin
Cefalexin
Cefuroxime
Cefotaxime
Ceftriaxone

Carbapenem
Meropenem
Imipenem
Doripenem
Ertapenem

10
Mechanisms of Action

Anti Cell Wall Activity
Bactericidal

11
Beta Lactams Against Bacterial Cell Wall
Cell wall
Osmotic Pressure
Cell Membrane
Antibiotic against cell wall
Osmotic Pressure
Cell membrane Rupture
12
Spectrum of Activity

Very wide
Gram positive and negative bacteria
Anaerobes
Spectrum of activity depends on the agent and/or
its group

13
Adverse Effects

Penicillin hypersensitivity 0.4 to 10
Mild rash
Severe anaphylaxis death
There is cross-reactivity among all Penicillins
Penicillins and cephalosporins 5-15

14
Resistance to ß-Lactams

ß-Lactamase
Other mechanisms are of less importance
Augmentin

15
Important Points

Beta lactams need frequent dosing for successful
therapeutic outcome
Missing doses will lead to treatment failure
Beta lactams are the safest antibiotics in renal
and hepatic failure
Adjustments to dose may still be required in
severe failure

16
Summary

Cell wall antibiotics
Bactericidal
Wide spectrum of use
Antibiotics of choice in many infections
Limitations
Allergy
Resistance due to betalactamase
Very safe in most cases
No monitoring required

17
Aminoglycosides

Inhibit bacterial protein synthesis by
irreversibly binding to 30S ribosomal unit
Naturally occurring
Streptomycin
Neomycin
Kanamycin
Tobramycin
Gentamicin
Semisynthetic derivatives
Amikacin (from Kanamycin)
Netilmicin (from Sisomicin)

18
30S Ribosomal Unit Blockage by Aminoglycosides

Causes mRNA decoding errors

19
Spectrum of Activity

Gram-Negative Aerobes
Enterobacteriaceae
E. coli, Proteus sp., Enterobacter sp.
Pseudomonas aeruginosa
Gram-Positive Aerobes (Usually in combination
with ß-lactams)
S. aureus and coagulase-negative staphylococci
Viridans streptococci
Enterococcus sp. (gentamicin)

20
Adverse Effects

Nephrotoxicity
Direct proximal tubular damage - reversible if
caught early
Risk factors High troughs, prolonged duration of
therapy, underlying renal dysfunction,
concomitant nephrotoxins
Ototoxicity
8th cranial nerve damage irreversible
vestibular and auditory toxicity
Vestibular dizziness, vertigo, ataxia
Auditory tinnitus, decreased hearing
Risk factors as for nephrotoxicity
Neuromuscular paralysis
Can occur after rapid IV infusion especially
with
Myasthenia gravis
Concurrent use of succinylcholine during
anaesthesia

21
Prevention of Toxicity

Levels need to be monitored to prevent toxicity
due to high serum levels
To be avoided where risk factors for renal damage
exist
Dehydration
Renal toxic drugs

22
Mechanisms of Resistance

Inactivation by Aminoglycoside modifying enzymes
This is the most important mechanism

23
Important Points

Aminoglycosides should be given as a large single
dose for a successful therapeutic outcome
Multiple small doses will lead to treatment
failure and likely to lead to renal toxicity
Aminoglycosides are toxic drugs and require
monitoring
Avoid use in renal failure but safe in liver
failure
Avoid concomitant use with other renal toxic
drugs
Check renal clearance, frequency according to
renal function

24
Summary

Restricted to aerobes
Toxic, needs level monitoring
Best used in Gram negative bloodstream infections
Good for UTIs
Limited or no penetration
Lungs
Joints and bone
CSF
Abscesses

25
Macrolides
26
Macrolides

Lactone Ring
14
14

Erythromycin
Telithromycin
14
15

Clarithromycin
Azithromycin

27
Mechanism of Action

Bacteriostatic- usually
Inhibit bacterial RNA-dependent protein synthesis
Bind reversibly to the 23S ribosomal RNA of the
50S ribosomal subunits
Block translocation reaction of the polypeptide
chain elongation

28
Spectrum of Activity

Gram-Positive Aerobes
Activity ClarithromycingtErythromycingtAzithromycin
MSSA
S. pneumoniae
Beta haemolytic streptococci and viridans
streptococci
Gram-Negative Aerobes
Activity AzithromycingtClarithromycingtErythromycin
H. influenzae, M. catarrhalis, Neisseria sp.
NO activity against Enterobacteriaceae
Anaerobes upper airway anaerobes
Atypical Bacteria

29
Mechanisms of Resistance - Microlides

Altered target sites
Methylation of ribosomes preventing antibiotic
binding
Cross-resistance occurs between all macrolides

30
Clinical Use

Cellulitis/Skin and soft tissue
Beta haemolytic streptococci
Staphylococcus aureus
Intra-cellular organisms
Chlamydia
Gonococcus

31
Summary

Bacteriostatic
ALL hepatic elimination
Gastrointestinal Sideeffects (up to 33 )
(especially Erythromycin)
Nausea
Vomiting
Diarrhoea
Dyspepsia
Best used in atypical pneumonia
Excellent tissue and cellular penetration
Very useful in susceptible intracellular
infections

32
Fluoroquinolones
33
Fluoroquinolones
Quinolone pharmacore
34
Mechanism of Action

Prevent
Relaxation of supercoiled DNA before replication
DNA recombination
DNA repair

35
Spectrum of Activity

Gram-positive
Gram-Negative (Enterobacteriaceae H. influenzae,
Neisseria sp. Pseudomonas aeruginosa)
Ciprofloxacin is most active
Atypical bacteria all have excellent activity

36
Summary

Wide range of activity against Gram positive and
negative bacteria.
Sepsis from Intra-abdominal and Renal Sources
Coliforms (Gram negative bacilli)
UTI
E. coli
Very good tissue penetration
Excellent oral bioavailability
High risk for C.difficile

37
Tetracyclines

Hydronaphthacene nucleus containing four fused
rings
Tetracycline
Short acting
Doxycycline
Long acting

38
Mechanism of Action

Inhibit protein synthesis
Bind reversibly to bacterial 30S ribosomal
subunits
Prevents polypeptide synthesis
Bacteriostatic

39
Spectrum of Activity

All have similar activities
Gram positives aerobic cocci and rods
Staphylococci
Streptococci
Gram negative aerobic bacteria
Atypical organisms
Mycoplasmas
Chlamydiae
Rickettsiae
Protozoa

40
Adverse Effects

Oesophageal ulceration
Photosensitivity reaction
Incorporate into foetal and children bone and
teeth

Avoid in pregnancy and children
41
Summary

Very good tissue penetration
Use usually limited to
Skin and soft tissue infections
Chlamydia

42
Glycopeptides

Vancomycin
Teicoplanin

Vancomycin
43
Mechanism of Action

Inhibit peptidoglycan synthesis in the bacterial
cell wall
Prevents cross linkage of peptidoglycan chains

44
Summary

Large molecule
Only active against Gram positive bacteria
Second choice in all its uses except
MRSA
C.difficile

45
Metronidazole

Antibiotic
Amoebicide
Anti-protozoal
Trichomonas Vaginalis

46
Mechanisms of Action

Molecular reduction
Nitroso intermediates
Sulfamides
Melatbolised
Bacterial DNA de-stabilised

47
Spectrum of Activity Uses

Anaerobes
Bacterial Vaginosis
Pelvic Inflammatory Disease
C. Diff

48
Bio-Availability

Oral
Intra-venous
Expensive
Rectal
Cheap

49
Summary

Wide spectrum of activity
Anaerobes
In combination

50
Use of Pharmacokinetics in Treatment

Beta lactams
Good/variable (Dependant on individual
antibiotic)
Soft tissue
Bone and joints
Lungs
CSF
Poor
Abscesses

Aminoglycosides
Good
Circulating organisms
Poor
Soft tissue
Bone and joints
Abscesses
Lungs
CSF

Examples of good Tissue Penetrators Tetracyclines
Macrolides Quinolones Clindamycin
51
Key Message 2

When selecting an antibiotic consider the
following
Where is the infection?
Which antibiotics will reach the site of
infection
Match the two and select your antibiotic

52
Key Message 3

Always check the impact of an antibiotic on other
drugs that a patient is on
Consult BNF or equivalent

53
PHEW!!!

Any Questions?

54
Chlamydia Trachomatis

Obligate, intracellular bacterium
Rigid cell wall but NO peptidoglycan layer
Cervicitis
Slapingitis
Pelvic Inflammatory Disease
Neonate - mucopurulent conjunctivitis
Reiter's syndrome(urethritis, uveitis, arthritis)
Lymphogranuloma Venereum

55
Chlamydia Trachomatis

Diagnosis
Giemsa stain
Inclusion bodies in epithelial cells
Gram stain of no value
ELISA - antigens in exudates or urine
Immunofouresence
PCR
Culture

56
Chlamydia Trachomatis

Life Cycle

Elementary Body
Cell
Reticulate Body
Release from Cell
Binary Fission
Daughter Elementary Bodies
57
Chlamydia Trachomatis

Treatment
Tetracyclines (Doxicycline)
Erythromycin
Azythromycin

58
PK/PD Principles in Antibiotic Prescribing And
Prescribing in Organ FailureSAHD May 17, 2013

Peter Gayo Munthali
Consultant Microbiologist
UHCW
Honorary Associate Clinical Professor
University of Warwick

59
Pharmacokinetics - Beta-Lactams

Absorption
PO forms have variable absorption
Food can delay rate and extent of absorption
Distribution
Widely to tissues fluids
CSF penetration
IV limited unless inflamed meninges
Metabolism Excretion
Primarily renal elimination
Some have a proportion of drug eliminated via the
liver
ALL ?-lactams have short elimination half-lives

60
Clinical Use - Beta- Lactams

Cellulitis/Skin and soft tissues
Commonest causes
Beta haemolytic streptococci
Staphylococcus aureus
Which Antibiotics?
Benzylpenicillin (Streptococci only)
Flucloxacillin (Staphylococcus aureus and
streptococci)
Other beta lactams can be used but spectrum too
wide

61
Clinical Use - Beta- Lactams

UTI
Commonest cause
E. coli
Which antibiotics
Cephalexin
Co-Amoxiclav
Secondary choice, better non beta lactam
alternatives exist
Nitrofurantoin
Trimethoprim

62
Clinical Use - Beta- Lactams

Sepsis from Intra-abdominal and Renal Sources
Commonest causes
Coliforms (Gram negative bacilli)
Which antibiotics?
Co-Amoxiclav
Tazocin
Meropenem/imipenem/ertapenem (ESBL suspected)

63
Pharmacokinetics - Aminoglycosides

All have similar pharmacologic properties
Gastrointestinal absorption unpredictable but
always negligible
Distribution
Hydrophilic widely distributes into body fluids
but very poorly into
CSF
Vitreous fluid of the eye
Biliary tract
Prostate
Tracheobronchial secretions
Adipose tissue
Elimination
85-95 eliminated unchanged via kidney
t1/2 dependent on renal function
In normal renal function t1/2 is 2-3 hours

64
Clinical Use 1 - Aminoglycosides

Sepsis from Intra-abdominal and Renal Sources
Commonest causes
Coliforms (Gram negative bacilli)
Which antibiotics?
Gentamicin/Amikacin (with beta lactam and or
metronidazole)

65
Clinical Use 2 - Aminoglycosides

UTI
Very effective in UTI as 85-95 of the drug is
eliminated unchanged via kidney
Commonest cause
E. coli
Which antibiotics
Gentamicin
Secondary choice, better alternatives exist
Nitrofurantoin
Trimethoprim
Beta lactams

66
Pharmacokinetics 1- Microlides

Erythromycin ( Oral absorption 15 - 45)
Short t1/2 (1.4 hr)
Acid labile
Absorption (Oral)
Erythromycin variable absorption of 15 - 45
Clarithromycin 55
Azithromycin 38
Half Life (T1/2)
Erythromycin 1.4 Hours
Clarithromycin (250mg and 500mg 12hrly) 3-4 5-7
hours respectively
Azithromycin 68hours
Improved tolerability
Excellent tissue and intracellular concentrations
Tissue levels can be 10-100 times higher than
those in serum
Poor penetration into brain and CSF
Cross the placenta and excreted in breast milk

67
Pharmacokinetics 2 - Microlides

Metabolism Elimination
ALL hepatic elimination

68
Adverse Effects - Microlides

Gastrointestinal (up to 33 ) (especially
Erythromycin)
Nausea
Vomiting
Diarrhoea
Dyspepsia
Thrombophlebitis IV Erythromycin Azithromycin
QTc prolongation, ventricular arrhythmias
Other ototoxicity with high dose erythromycin in
renal impairment

69
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70
Pharmacokinetics - Fuoroquinolones

Absorption
Good bioavailability
Oral bioavailability 60-95
Divalent and trivalent cations (Zinc, Iron,
Calcium, Aluminum, Magnesium) and antacids reduce
GI absorption
Distribution
Extensive tissue distribution but poor CSF
penetration
Metabolism and Elimination
Combination of renal and hepatic routes

71
Adverse Effects - Fluoroquinolones

Cardiac
Prolongation QTc interval
Assumed to be class effect
Articular Damage
Cartilage damage
Induced in animals with large doses

72
Resistance - Fluoroquinolones

Altered target sites due to point mutations.
The more mutations, the higher the resistance to
Fluoroquinolones
Most important and most common
Altered cell wall permeability
Efflux pumps
Cross-resistance occurs between fluoroquinolones

73
Clinical Use 1- Fluoroquinolones

Sepsis from Intra-abdominal and Renal Sources
Commonest causes
Coliforms (Gram negative bacilli)
Which antibiotics?
Ciprofloxacin
High risk for C.difficile, safer alternatives
should be used

74
Clinical Use 2 - Fluoroquinolones

UTI
Commonest cause
E. coli
Which antibiotics
Ciprofloxacin
High risk for C.difficile, safer alternatives
should be used

75
Pharmacokinetics - Tetracyclines

Incompletely absorbed from GI, improved by
fasting
Metabolised by the liver and concentrated in bile
(3-5X higher than serum levels)
Excretion primarily in the urine except
doxycycline ( 60 biliary tract into faeces,40
in urine)
Tissue penetration is excellent but poor CSF
penetration
Incorporate into foetal and children bone and
teeth

76
Resistance - Tetracyclines