Brainscape's Knowledge GenomeTM

Browse over 1 million classes created by top students, professors, publishers, and experts.


See full index

3151 Therapeutics > LRTI (Nosocomial Pneumonia - HAP/VAP) > Flashcards

LRTI (Nosocomial Pneumonia - HAP/VAP) Flashcards

1
Q

What are the risk factors for HAP/VAP?

A

Patient-related factors

  • Elderly
  • Smoking
  • COPD, cancer, immunosuppression
  • Prolonged hospitalization
  • Coma, impaired consciousness (affect pt breathing and swallowing)
  • Malnutrition (immunosuppression)

Infection control-related factors

  • Lack of hand hygiene compliance
  • Contaminated respiratory care devices (e.g., ventilator, intubation)

Healthcare-related factors

  • Prior antibiotic use
  • Sedatives (when pt are sedated, don’t breathe well, require supplemental O2, innate immunity down)
  • Opioid analgesics
  • Mechanical ventilation
  • Supine position
How well did you know this?
1
Not at all
2
3
4
5
Perfectly
2
Q

How to prevent HAP/VAP?

A
  • Practice hand hygiene
  • Judicious use of antibiotics and medications with sedative effect

VAP specific:

  • Limit duration of mechanical ventilation
  • Minimize duration and deep levels of sedation
  • Elevate head of bed by 30 degrees
How well did you know this?
1
Not at all
2
3
4
5
Perfectly
3
Q
  1. Identification of pathogens [HAP/VAP]

List the common causative pathogens

A

Pseudomonas Aeruginosa
Staphylococcus Aureus
Enteric gram-negative (Enterobacter, Klebsiella, E. Coli)
Acinetobacter spp.
Strenotrophomonas maltophilia

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
4
Q
  1. Identification of pathogens [HAP/VAP]

Unlike CAP, HAP/VAP is not likely caused by ________

A

HAP/VAP not likely caused by:
- Streptococcus pneumoniae
- Haemophilus influenzae
- Atypicals
- Burkholderia pseudomallei

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
5
Q
  1. Selection of antimicrobial and regimen [HAP/VAP]

At the minimum, empiric cover for HAP/VAP should cover?

A
  1. Pseudomonas Aeruginosa
  2. Staphylococcus Aureus
How well did you know this?
1
Not at all
2
3
4
5
Perfectly
6
Q
  1. Selection of antimicrobial and regimen [HAP/VAP]

HAP/VAP choice of antibiotics should be selected based on…?

A
  1. Local distribution of pathogens associated with HAP/VAP and their antimicrobial suscpetibilities
  2. ICU-specific antibiogram for VAP
  3. Empirically be able to cover Pseudomonas Aeruginosa and Staphylococcus Aureus
How well did you know this?
1
Not at all
2
3
4
5
Perfectly
7
Q
  1. Selection of antimicrobial and regimen [HAP/VAP]

In what situations would additional cover be needed (e.g., MRSA, ESBL producing gram-negative)

A
  • MDRO risk factors
  • Mortality risk factors (severely ill patients)
  • Hospital or unit’s distribution of pathogen associated with HAP/VAP and their susceptibilities (antibiogram)
How well did you know this?
1
Not at all
2
3
4
5
Perfectly
8
Q
  1. Selection of antimicrobial and regimen [HAP/VAP]

Should empirically cover for MRSA if?

*MRSA risk factors

A

MRSA risk factors:

  • Prior intravenous antibiotic use within 90 days
  • Isolation of MRSA in last 1 year
  • Hospitalization in a unit where >20% of S. aureus are MRSA
  • Prevalence of MRSA in the hospital is unknown, but pt is at high risk for mortality (i.e. need ventilatory support due to HAP and septic shock)
How well did you know this?
1
Not at all
2
3
4
5
Perfectly
9
Q
  1. Selection of antimicrobial and regimen [HAP/VAP]

When is empiric double antipseudomonal antibiotic cover required?

*Pseudomonas aeruginosa risk factors (that require double cover)

A

Pseudomonas aeruginosa risk factors (that require double cover):

  • Risk factor for antimicrobial resistance (e.g., prior intravenous antibiotic use within 90 days, isolation of P. aeruginosa in last 1 year, acute renal replacement therapy prior to VAP onset)
  • Hospitalization in a unit where >10% of P. aeruginosa isolates are resistant to an agent being considered for monotherapy
  • Prevalence of P. aeruginosa in the hospital is unknown, but pt is at high risk for mortality (i.e. need ventilatory support due to HAP and septic shock)

*The two agents should be from different class to ensure at least one is active against the bug

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
10
Q
  1. Selection of antimicrobial and regimen [HAP/VAP]

In what situation can a single antipseudomonal agent be used for empiric cover?

Which agent must be AVOIDED as the sole antipseudomonal agent?

A

When the monotherapy considered has >=90% susceptibility

*Aminoglycoside CANNOT be used as monotherapy due to:

  • Nephrotoxicity (many HAP/VAP patients in ICU are hemodynamically unstable, low BP can lead to reduced perfusion of the kidney and AKI)
  • Low perfusion/distribution into lungs especially with abscess

(If used, at most 1 week)

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
10
Q
  1. Selection of antimicrobial and regimen [HAP/VAP]

What is the general double antipseudomonal agent combination?

A

Beta-lactam + Fluroquinolone
OR
Beta-lactam + Aminoglycoside

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
11
Q
  1. Selection of antimicrobial and regimen [HAP/VAP]

Name the antibiotic selection and their doses

Cover for:
Pseudomonas Aeruginosa
Staphylococcus Aureus
Enteric gram-negative (Enterobacter, Klebsiella, E. Coli)

A

Beta lactam

  • IV Piperacillin/Tazobactam 4.5g q6-8h
  • IV Cefepime 2g q8h
  • IV Ceftazidime 2g q8h
  • IV Meropenem 1g q8h
  • IV Imipenem/Cilastatin 500mg q6h

AND/OR

  • IV Levofloxacin 750mg q24h
  • IV Ciprofloxacin 400mg q8-12h / PO 500mg q12h
  • IV Amikacin 15-20mg/kg q24h
  • IV Gentamicin 5-7mg/kg q24h

If MRSA risk factors, ADDITIONAL:

  • IV Vancomycin 25-30mg/kg LD, 15mg/kg q8-12h, to achieve AUC/MIC 400-600
  • IV/PO Linezolid 600mg q12h

*Avoid use of Ceftazidime or Ciprofloxacin, if theres no MRSA cover with Vanco/Linezolid (bc these two agents need Vanco/Linezolid to help cover MSSA)

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
12
Q
  1. Selection of antimicrobial and regimen [HAP/VAP]

Why is Meropenem the last line Beta-lactam?

A

No need broad spectrum Carbapenem to cover ESBL-producing enteric GNR (unless there is MDRO risk, that require double cover)

Hence, okay to use Pip-Tazo/Cefepime/Ceftazidime first as single agents

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
13
Q
  1. Selection of antimicrobial and regimen [HAP/VAP]

Discuss when and how deescalation / IV to oral conversion of CAP antibiotic regimen can be done

A

When to de-escalate?

  • Pt is hemodynamically stable
  • Pt has improved clinically
  • Pt able to ingest oral medication

How to de-escalate?

=>Postive culture

  • Use AST to guide selection of narrower spectrum and/or PO antibiotics
  • For P. aeruginosa, SWITCH to SINGLE antipseudomonal agent based on AST

=> If no positive culture

  • De-escalate but maintain cover according to local HAP/VAP antibiogram
  • If antibiogram not available, then minimally cover for P. aeruginosa, enteric GNR, MSSA (can remove MRSA cover - may do MRSA screening)
  • De-escalation is NOT possible for pt with significant risk for MDRO (still need MRSA, keep empiric for 7 days)
  • IV to oral (either Cipro + Augmentin or Levo) (*Augmentin to cover MSSA)
How well did you know this?
1
Not at all
2
3
4
5
Perfectly
14
Q
  1. Selection of antimicrobial and regimen [HAP/VAP]

What is the treatment duration for HAP/VAP?

A

7 days recommended regardless of pathogen (*no diff in recurrence and mortality b/w short 7d and long course 8-14d)

*Provided pt achieved clinical stability:

  • Resolution of vital signs abnormalities
  • Baseline mental status for HAP (*VAP sedated, unable to assess)

*Most patient should achieve clinical stability within first 48-72h

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
15
Q
  1. Selection of antimicrobial and regimen [HAP/VAP]

When might longer treatment duration be required for HAP/VAP?

A

Longer courses of therapy for:

  • HAP/VAP complicated with other deep-seated infections (e.g., meningitis, lung abscess) ~2-3 weeks
16
Q
  1. Monitor response [HAP/VAP]
    - Involves therapeutic response + ADRs

How is therapeutic response monitored?

A
  • Most patients achieve clinical stability within 48-72h
  • Elderly pt and those with multiple comorbidities may take longer (4-5 days)
  • Do not escalate Abx in the first 72h (unless 1. Culture-directed, or 2. Significant clinical deterioration) *send another culture e.g., BAL if culture comes back negative
  • Radiographic improvement lags behind clinical improvement for resolution (takes 6weeks to a few months, hence only repeat if clinical deterioration and suspect new pneumonia/spread)
  • No need to repeat microbiological test (clinical improvement is sufficient)
17
Q
  1. Monitor response [HAP/VAP]

What might clinical deterioration after having started empiric antibiotics suggest?
*think other bugs not yet covered

A

May be Acinetobacter or Strenotrophomonas maltophilia
=> Need to add cover for these if pt gets worse with normal empiric regimen

  • Acinetobacter and Strenotrophomonas have high resistance against Meropenem (which is the last line anti-pseudomonal and ESBL cover)
  • May treat with Levofloxacin or Polymyxin

3151 Therapeutics (12 decks)

Brainscape helps you reach your goals faster, through stronger study habits.
© 2025 Bold Learning Solutions. Terms and Conditions