Principles of antimicrobial use

Question 1

What is the systematic approach to antimicrobial use?

Answer 1

1. Confirm presence of infection
2. Identification of pathogens
3. Selection of antimicrobial and regimen
4. Monitor response

Question 2

What are data used in confirming presence of infection?

Answer 2

Risk factors for infections
Subjective evidence
Objective evidence
Site of infection (Possible source)

Question 3

What are data used in identifying pathogens?

Answer 3

Likely pathogens

Microbiological tests

Question 4

What do we consider when selecting antimicrobial and the regimen?

Answer 4

Emipiric, definitive or prophylaxis
Consider organism, host and drug factors
Decide Agent, ROA, regimen

Question 5

What are key things in monitoring response?

Answer 5

Efficacy (therapeutic response)

Safety (ADRs)

Question 6

What are some localized symptoms of infection? (subjective)

Answer 6

D/V/N/abdominal distention
Cough/purulent sputum
Dysuria/frequency/Urgency
Pain and inflammation at site of infection
Purulent discharge

Question 7

What are data used in confirming presence of infection?

Answer 7

Risk factors for infections
Subjective evidence
Objective evidence
Site of infection (Possible source)

Question 8

What is the normal range of CRP and the factors that affect it?

Answer 8

Normal: <10mg/L
Mild inflammation/viral infection: 10-40mg/L
Active inflammation/bacterial infection: 40-200mg/L
Severe bacterial infection/burns: >200mg/L

Question 9

What are key things in monitoring response?

Answer 9

Efficacy (therapeutic response)

Safety (ADRs)

Question 10

What are some risk factors for infections?

Answer 10

Disruption of natural protective barriers
Age (very young/old)
Immunosuppression
Alteration in normal flora (i.e. hospital/use of abx)

Question 11

What are some systemic symptoms of infection? (subjective)

Answer 11

Feeling Feverish, chills, rigors
Malaise
Fast HR
SOB
Mental status changes
Weakness

Question 12

What are things to note in identifying pathogens?

Answer 12

Take cultures before starting antibiotics
consider contaminant/colonizer/pathogen
consider Starting or Streamlining definitive therapy using susceptibility test results

Question 13

What are the objective evidence of infection (labs)?

Answer 13

Elevated WBCs (>10 x 10^9) or depressed WBCs (<4 x 10^9)
Increased neutrophils (note baseline)
Increased procalcitonin/CRP/erythrocyte sedimentation rate ESR (acute phase reactants)
Radiology
- X-ray (chest,bone)
- Ultrasound
- CT scan
- MRI

Question 14

What are the key thresholds when using procalcitonin to STARTING antibiotics?

Answer 14

1. <0.25ug/L: abx strongly DIScouraged
2. Between 0.25ug/L (inclusive) to less than 0.5ug/L: abx DIScouraged (grey)
3. Between 0.5ug/L (inclusive) to less than 1ug/L: abx encouraged
4. 1ug/L or higher: abx strongly encouraged

Question 15

What are the benefits of combination therapy?

Answer 15

Extended spectrum of activity (for polymicrobials or resistant strains)
Synergistic killing
Prevent development of resistance

• i.e. pip-tazo (pseudomonas) + IV vancomycin (MRSA) for HAP
• i.e. pip-tazo + cipro for pseudomonas
• i.e. gentamicin + ampicillin for enterococcus endocarditis (synergism)
• i.e. trimethoprim + sulfamethoxazole (synergism)

Question 16

What are the key thresholds when using procalcitonin to STOPPING antibiotics?

Answer 16

1. <0.25ug/L: STOPPING abx strongly encouraged
2. Between 0.25ug/L (inclusive) to less than 0.5ug/L: STOPPING abx encouraged (grey)
3. Between 0.5ug/L (inclusive) to less than 1ug/L: CONTINUING abx encouraged
4. 1ug/L or higher: CONTINUING abx strongly encouraged

Question 17

How can we determine the site of infection?

Answer 17

Clinical presentation
Risk factors
O/S evidences
Common sites: urinary tract, skin and soft tissues

Question 18

Which kind of infections are likely to be anaerobic infections?

Answer 18

Intra-abdominal infections from perforated viscus (Bacteriodes, Clostridium)
Diabetic foot infections (polymicrobial process)

Question 19

What should we note regarding wound swabs?

Answer 19

Usually superficial and carry alot of commensals

- But if there are no other results, we can cover all organisms and streamline therapy when pt is better

Question 20

What does empiric therapy mean?

Answer 20

Microbiological results unavailable
Agent use based on clinical presentation, likely site of infection, likely organism and likely resistant pattern (antibiogram)

Question 21

What are the disadvantages of combination therapy?

Answer 21

Increased toxicity and allergic reactions
Increased risk for DDI
Increased Cost
Selection for Multi-drug-resistant (MDR) bacteria
Increased risk of superinfections (fungal, CDAD)

Question 22

What are some key host factors to note?

Answer 22

Age
Allergies and ADR hx
G6PD deficiency
Pregnancy/Lactation
Renal/Hepatic impairment 
Immune status
Severity of infection
Recent antimicrobial use
Healthcare associated factors

Question 23

Abx to avoid when pt has G6PD deficiency?

Answer 23

Sulfonamides and nitrofurantoin

Question 24

Abx to avoid when pt is pregnant/lactating?

Answer 24

Fluroquinolones
Co-trimoxazole
Tetracyclines

Question 25

Abx to avoid in children?

Answer 25

Fluoroquinolones

Tetracyclines

Question 26

Abx to avoid in hepatic impairment?

Answer 26

Pyrazinamide

Augmentin

Question 27

Abx to avoid in renal impairment?

Answer 27

High dose vancomycin

Aminoglycosides

Question 28

Why are combination therapy and bactericidal abx recommended for immunocompromised patients?

Answer 28

More vulnerable to polymicrobial infections (combination therapy better covers these)
Bactericidal abx better help lower cell count (vs bacteriostatic)

Question 29

What are the abx consideration in severely ill pts?

Answer 29

Start active abx asap

Broader spectrum cover needed

Question 30

What are things to think about when pt has recent anti-microbial use?

Answer 30

Risk factor for drug resistant organism

If there was tx failure, avoid the same abx

Question 31

What are we referring to when discussing MDR organisms?

Answer 31

ESBLs producing gram negative organisms and MRSA

Question 32

What are healthcare associated risk factors?

Answer 32

Hospitalization in the last 90 days
Current hospitalization (2 or more days)
Residence in nursing home
Antimicrobial use in last 90 days
Home infusion therapy (catheter risk factor for MRSA)
Chronic dialysis

Question 33

What are Drug Associated factors?

Answer 33

Activity against suspected organism
Ability to reach site of infection
PK-PD characteristics
ROA
Side effect profile
Drug interactions
Cost

Question 34

Can ertapenem (carbapenem class) be used for pseudomonas?

Answer 34

No

Question 35

MRSA abx options?

Answer 35

Vancomycin, linezolid, daptomycin, ceftaroline

Question 36

Pseudomonas aeruginosa abx options?

Answer 36

3rd and 4th gen cephalosporins, pip-tazo, ciprofloxacin, AGs (gentamicin and amikacin), aztreonam, meropenem and imipenem

Question 37

ESBLs abx options?

Answer 37

Carbapenems (1st line), AGs

- FQs, Bactrim (co-trimoxazole) have increasing resistance rates, only for culture directed tx

Question 38

Anaerobe Cover?

Answer 38

Clindamycin, Metronidazole, Augmentin, Pip-tazo, carbapenems

Question 39

Can daptomycin be used for pneumonia?

Answer 39

No. It is inactivated by lung surfactant

Question 40

Should we use Aminoglycosides (AGs) for abscesses?

Answer 40

No. AGs are less effective in the low oxygen/pH, high protein environment. Prefer beta lactams

Question 41

Drug of choice for prostatitis?

Answer 41

Ciprofloxacin and Bactrim

Question 42

Drug of choice for CNS infections?

Answer 42

Penicillins (G and ampicillin), 3rd and 4th gen cephalosporins, meropenem and vancomycin

Question 43

Which abx cannot be used for CNS infections?

Answer 43

1st and 2nd gen cephalosporins, AGs, Clindamycin, macrolides

Question 44

Which abx feature concentration dependent killing?

Answer 44

Aminoglycosides, Fluroquinolones

Question 45

Which abx feature time dependent killing?

Answer 45

Beta lactams

Question 46

What is the Optimum Cmax/MIC or AUC/MIC ratio for concentration dependent kill?

Answer 46

8-10x above MIC

Question 47

Advantages of OD AG dosing?

Answer 47

Concentration dependent kill
Post abx effect
Prevents adaptive resistance
Less nephrotoxicity
Lower labour/equipment cost

Question 48

What is the dose adjustment of AGs for renally impaired pts?

Answer 48

Increase the dosing interval without reducing dose

Question 49

What is the optimum Time above MIC for abx exhibiting time dependent kill?

Answer 49

40-70% of dosing interval above MIC

Question 50

What are some strategies for improve time above MIC?

Answer 50

More frequent dosing 
Continuous IV infusion
Block excretion (i.e. probenecid)

Question 51

Which abx exhibits time-dependent bacterial kill with persistent effect?

Answer 51

Vancomycin

- Rate and extent of kill related to overall drug exposure (AUC) vs MIC

Question 52

What is the target AUC:MIC ratio for vancomycin treating MRSA?

Answer 52

400-600

Question 53

Why is the PO route favored over other ROA?

Answer 53

Less need for line/injections and lowers blood infection risk
Avoids thrombophlebitis (iv needles can cause vein irritation)

Question 54

What are some situations where PO is not preferred?

Answer 54

Absorption problem (GI issue)
No suitable PO abx
High tissue conc needed (i.e. meningitis, endocarditis, bone/joint infection)
Urgent tx needed
Non-compliance

Question 55

Examples of abx with good oral bioavailability?

Answer 55

Co-trimoxazole, fluoroquinolones, metronidazole, linezolid

Question 56

Can carbapenems be used together with valporate?

Answer 56

No. Carbapenems reduce the conc of valporate, potentially leading to pt seizures

Question 57

What are some CYP450 inhibitors?

Answer 57

Azoles and macrolides

Question 58

What are is an example of an CYP450 inducer?

Answer 58

Rifampicin

Question 59

Expected abx duration for surgical prophylaxis (Chlamydia cervicititis)?

Answer 59

24h or single dose

Question 60

Expected abx duration for UTI/Respiratory/Skin tx?

Answer 60

5-14 days

Question 61

Expected abx duration for endocarditis/osteomyelitis?

Answer 61

4-6weeks

Question 62

Expected abx duration for tuberculosis (chronic suppression)

Answer 62

6 Months

Question 63

Expected abx duration for HIV?

Answer 63

life long

Question 64

What is monitored under therapeutic response?

Answer 64

Resolution of s/sx
Microbiological eradication
Absence of complications/progression of infection

Question 65

Common ADRs for abx to monitor for?

Answer 65

Allergies (rash, itch, angioedema)

Question 66

When should we think of modifying/streamlining therapy?

Answer 66

When test results are available

When pt shows good clinical response

Question 67

Some reasons for poor clinical response?

Answer 67

Wrong drug
Wrong dose/conc
Wrong organism
Wrong treatment (i.e. should have I&D for abscesses)
Wrong diagnosis
Impaired host defense 
Toxicity of drug
Non-compliance
Improving renal function and clearance
Resistance

Question 68

When do we evaluate initial abx response?

Answer 68

48-72h later