Resistance Patterns & Stewardship
Identify MRSA (use vancomycin/linezolid), ESBL (carbapenems), and Pseudomonas coverage; apply de-escalation and duration optimization.
Resistance Patterns & Stewardship
Master antibiotic resistance patterns and stewardship principles with free flashcards and evidence-based practice tools. This lesson covers mechanisms of antimicrobial resistance, key resistance patterns in common pathogens, and comprehensive stewardship strategiesβessential concepts for the NAPLEX and clinical pharmacy practice.
Welcome π―
Antimicrobial resistance represents one of the greatest threats to modern medicine. As a pharmacist, you'll serve on the front lines of preserving antibiotic effectiveness through informed prescribing recommendations, patient counseling, and active participation in antimicrobial stewardship programs (ASPs). This lesson equips you with the knowledge to identify resistance patterns, understand their mechanisms, and implement evidence-based stewardship interventions.
π‘ Why This Matters: The CDC estimates that antibiotic-resistant infections cause 2.8 million infections and 35,000 deaths annually in the U.S. alone. Your stewardship efforts directly impact patient outcomes and public health.
Core Concepts: Mechanisms of Antimicrobial Resistance π§¬
Understanding Resistance Development
Bacteria develop resistance through several fundamental mechanisms. Understanding these pathways helps you predict which antibiotics will remain effective and which alternatives to recommend.
Four Primary Resistance Mechanisms:
| Mechanism | Description | Examples | Clinical Impact |
|---|---|---|---|
| Enzymatic Degradation | Bacteria produce enzymes that destroy or modify antibiotics | Ξ²-lactamases (penicillinases, ESBLs, carbapenemases) | Renders entire antibiotic classes ineffective; requires Ξ²-lactamase inhibitors or alternative agents |
| Target Site Modification | Bacterial target proteins mutate, reducing antibiotic binding | MRSA (altered PBP2a), VRE (altered D-Ala-D-Lac) | Cross-resistance within antibiotic class; requires different mechanism agents |
| Efflux Pumps | Active transport systems pump antibiotics out of bacterial cells | Tetracycline resistance, fluoroquinolone resistance in Pseudomonas | Multi-drug resistance; may affect multiple antibiotic classes |
| Decreased Permeability | Changes in porin channels reduce antibiotic entry | Carbapenem resistance in Pseudomonas, Acinetobacter | Affects hydrophilic antibiotics; often combined with other mechanisms |
Ξ²-Lactamase Classification π¬
Ambler Classification System categorizes Ξ²-lactamases by molecular structure:
βββββββββββββββββββββββββββββββββββββββββββββββββββ β Ξ²-LACTAMASE CLASSIFICATION β βββββββββββββββββββββββββββββββββββββββββββββββββββ€ β β β Class A (Serine) Class B (Metallo) β β β’ ESBLs (CTX-M, TEM) β’ NDM-1 β β β’ KPC carbapenemase β’ VIM, IMP β β ββ Inhibited by: ββ Inhibited by: β β ββ Clavulanate, ββ EDTA (not β β tazobactam, clinically β β avibactam available) β β β β Class C (AmpC) Class D (Oxacillin) β β β’ Chromosomal AmpC β’ OXA-type β β β’ Cephalosporinases β’ Carbapenemases β β ββ NOT inhibited by: ββ Weakly β β ββ Traditional ββ inhibited by β β Ξ²-lactamase clavulanate β β inhibitors β β β βββββββββββββββββββββββββββββββββββββββββββββββββββ
π§ Memory Device - "AMBLER'S SEAM":
- A = Aminoglycoside-modifying enzymes respond to standard inhibitors
- M = Metallo-Ξ²-lactamases (Class B) require metal ions
- B = Bad news - no clinically available inhibitors
- L = Look for avibactam for KPC (Class A)
- E = Extended-spectrum (ESBLs are Class A)
- R = Resistant AmpC (Class C) to standard inhibitors
High-Yield Resistance Patterns π―
ESKAPE Pathogens
The ESKAPE acronym identifies the most concerning multidrug-resistant organisms:
π¦ ESKAPE Pathogens
| Letter | Organism | Key Resistance Pattern | Preferred Agents |
|---|---|---|---|
| E | Enterococcus faecium | VRE (vancomycin-resistant) | Linezolid, daptomycin (β₯8 mg/kg), tigecycline |
| S | Staphylococcus aureus | MRSA (methicillin-resistant) | Vancomycin, daptomycin, linezolid, ceftaroline |
| K | Klebsiella pneumoniae | ESBL, CRE (carbapenem-resistant) | Carbapenems (if susceptible), ceftazidime-avibactam, meropenem-vaborbactam |
| A | Acinetobacter baumannii | MDR, carbapenem-resistant | Colistin, tigecycline, ampicillin-sulbactam (high dose) |
| P | Pseudomonas aeruginosa | MDR, carbapenem-resistant | Ceftazidime-avibactam, ceftolozane-tazobactam, colistin |
| E | Enterobacter species | AmpC-mediated resistance | Carbapenems, cefepime, fluoroquinolones (if susceptible) |
MRSA: Methicillin-Resistant Staphylococcus aureus π΄
Resistance Mechanism: Production of altered penicillin-binding protein (PBP2a) encoded by mecA gene
Key Clinical Distinctions:
| Feature | HA-MRSA (Hospital-Acquired) | CA-MRSA (Community-Acquired) |
|---|---|---|
| Typical Patient | Healthcare exposure, chronic illness, invasive devices | Young, healthy, athletic populations |
| SCCmec Type | Types I, II, III (larger, more resistance genes) | Type IV, V (smaller, fewer resistance genes) |
| Common Presentations | Bacteremia, pneumonia, surgical site infections | Skin/soft tissue infections (abscesses, furuncles) |
| Additional Resistance | Often MDR (resistant to multiple classes) | Typically susceptible to more agents |
| Virulence Factors | Fewer toxins | PVL toxin (Panton-Valentine leukocidin) |
π‘ Clinical Pearl: CA-MRSA with PVL toxin can cause necrotizing pneumonia and severe skin infections. Always consider adding clindamycin (if susceptible) to inhibit toxin production, even if vancomycin/daptomycin is used for bactericidal activity.
ESBL-Producing Enterobacteriaceae π§«
Extended-Spectrum Ξ²-Lactamases hydrolyze penicillins, cephalosporins (including 3rd generation), and aztreonamβbut NOT carbapenems or cephamycins.
Treatment Approach Decision Tree:
ββββββββββββββββββββββββββββββββββ
β ESBL-Producing Organism β
β Detected in Culture β
ββββββββββββββββ¬ββββββββββββββββββ
β
βΌ
ββββββββββββββββββββββββββββββββββββββββ
β What is the infection severity? β
ββββββββββββββββ¬ββββββββββββββββββββββββ
β
ββββββββββββ΄βββββββββββ
βΌ βΌ
βββββββββββββββ βββββββββββββββ
β Severe β β Mild/Mod β
β (sepsis, β β (cystitis, β
β pneumonia) β β simple β
β β β infection) β
ββββββββ¬βββββββ ββββββββ¬βββββββ
β β
βΌ βΌ
ββββββββββββββββ ββββββββββββββββββββ
β Carbapenem β β Consider oral: β
β (preferred) β β β’ Nitrofurantoin β
β β β (UTI only) β
β β’ Ertapenem β β β’ Fosfomycin β
β β’ Meropenem β β (uncomplicated β
β β’ Imipenem β β cystitis) β
ββββββββββββββββ β β’ Amox-clav* β
β β’ TMP-SMX* β
β β’ Fluoroquinolone*β
β (*if susceptible)β
ββββββββββββββββββββ
β οΈ Critical Stewardship Point: Even if an ESBL-producing organism shows in vitro susceptibility to 3rd-generation cephalosporins, DO NOT use them. Clinical failures are common due to inoculum effect and inducible resistance.
Carbapenem-Resistant Enterobacteriaceae (CRE) β οΈ
Definition: Enterobacteriaceae resistant to β₯1 carbapenem OR producing a carbapenemase enzyme
Most Common Carbapenemases:
- KPC (Klebsiella pneumoniae carbapenemase) - Class A, most common in U.S.
- NDM (New Delhi metallo-Ξ²-lactamase) - Class B
- OXA-48 - Class D, common in Middle East/Europe
Treatment Options for CRE:
| Agent | Mechanism | Spectrum | Clinical Considerations |
|---|---|---|---|
| Ceftazidime-Avibactam | Avibactam inhibits Class A, C, some D Ξ²-lactamases | Excellent for KPC, ESBL, AmpC | β NOT active against NDM (metallo-Ξ²-lactamases). Preferred for KPC-producing CRE |
| Meropenem-Vaborbactam | Vaborbactam inhibits Class A, C Ξ²-lactamases | KPC, ESBL, some AmpC | β NOT active against metallo-Ξ²-lactamases or OXA-48. Good penetration |
| Imipenem-Relebactam | Relebactam inhibits Class A, C Ξ²-lactamases | Similar to meropenem-vaborbactam | Newer option, growing clinical experience |
| Cefiderocol | Siderophore cephalosporin (trojan horse mechanism) | Broad: KPC, NDM, OXA-48, Pseudomonas, Acinetobacter | β Active against metallo-Ξ²-lactamases. Reserve for salvage therapy |
| Colistin | Disrupts bacterial membrane | Gram-negative (not Serratia, Proteus, Burkholderia) | Nephrotoxicity concern. Consider combination therapy. Requires loading dose |
| Tigecycline | Glycylcycline (inhibits protein synthesis) | Many CRE strains | β NOT for bacteremia (low serum levels), UTI. FDA black box warning for mortality |
π§ Memory Device - "VIPER for CRE":
- Vaborbactam - KPC killer
- Imipenem-relebactam - similar spectrum
- Polymyxins (colistin) - last resort
- Elude metallo-Ξ²-lactamases (most agents can't)
- Reserve cefiderocol (broadest, save for tough cases)
Antimicrobial Stewardship Principles π‘οΈ
Core Elements of ASPs
The CDC Core Elements provide a framework for hospital antimicrobial stewardship programs:
ββββββββββββββββββββββββββββββββββββββββββββββββ β CDC CORE ELEMENTS OF STEWARDSHIP β ββββββββββββββββββββββββββββββββββββββββββββββββ€ β β β 1οΈβ£ LEADERSHIP COMMITMENT β β ββ Dedicate necessary resources β β ββ Support accountability β β β β 2οΈβ£ ACCOUNTABILITY β β ββ Single leader responsible β β ββ Physician/pharmacist champions β β β β 3οΈβ£ DRUG EXPERTISE β β ββ Pharmacist co-leads ASP β β ββ Infectious disease specialist β β β β 4οΈβ£ ACTION - IMPLEMENT INTERVENTIONS β β ββ Prospective audit & feedback β β ββ Preauthorization β β ββ Formulary restrictions β β ββ Clinical pathways/guidelines β β β β 5οΈβ£ TRACKING β β ββ Monitor antibiotic use β β ββ Track resistance patterns β β ββ Measure outcomes β β β β 6οΈβ£ REPORTING β β ββ Regular feedback to prescribers β β ββ Report to leadership β β β β 7οΈβ£ EDUCATION β β ββ Update clinical staff β β ββ Patient/family education β β β ββββββββββββββββββββββββββββββββββββββββββββββββ
Stewardship Interventions π
1. Prospective Audit and Feedback (PAF)
Most effective stewardship intervention
Process:
- Review antimicrobial orders 24-48 hours after initiation
- Assess appropriateness (spectrum, dose, duration, indication)
- Provide recommendations to prescriber
- Document outcomes
Example PAF Recommendation:
"Patient with uncomplicated E. coli UTI currently on IV meropenem (Day 3). Susceptibilities show pansensitive organism. Recommend: De-escalate to oral ciprofloxacin 500mg BID to complete 7-day course. Rationale: Carbapenem-sparing, narrower spectrum, oral therapy for clinically stable patient. Estimated cost savings: $1,200 per day."
2. Preauthorization/Restriction
Restrict broad-spectrum or high-risk agents requiring ID/ASP approval:
- Carbapenems
- Daptomycin
- Newer Ξ²-lactam/Ξ²-lactamase inhibitor combinations
- Echinocandins
- Linezolid
3. IV-to-PO Conversion
Criteria for Conversion: β Hemodynamically stable β Afebrile for 24+ hours β Functioning GI tract β Oral agent with appropriate bioavailability available
High-Bioavailability Agents (>90%):
- Fluoroquinolones (levofloxacin, moxifloxacin, ciprofloxacin)
- Linezolid
- Metronidazole
- Trimethoprim-sulfamethoxazole
- Fluconazole
- Voriconazole
4. Dose Optimization
Pharmacokinetic/Pharmacodynamic (PK/PD) Principles:
| Antibiotic Class | PK/PD Parameter | Target | Dosing Strategy |
|---|---|---|---|
| Ξ²-Lactams | %T>MIC (Time above MIC) | 40-70% of dosing interval | Frequent dosing or extended infusions |
| Fluoroquinolones | AUC/MIC ratio | β₯125 for Gram-negatives | Higher doses, once daily |
| Aminoglycosides | Cmax/MIC ratio | β₯8-10 | High-dose, extended-interval (once daily) |
| Vancomycin | AUC/MIC ratio | 400-600 | Weight-based dosing, monitor AUCββ |
π‘ Extended Infusion Strategy: For Ξ²-lactams treating serious Gram-negative infections:
- Piperacillin-tazobactam: 3.375g IV over 4 hours q8h (instead of 30-min infusion)
- Meropenem: 2g IV over 3 hours q8h (instead of 30-min infusion)
- Benefit: Prolongs %T>MIC, improves outcomes in critically ill patients
Duration Optimization: Shorter is Often Better β±οΈ
Evidence-Based Duration Recommendations:
| Infection Type | Traditional Duration | Recommended Duration | Key Evidence |
|---|---|---|---|
| Community-Acquired Pneumonia | 7-10 days | 5 days (if clinically stable by day 3) | Similar outcomes with shorter course |
| Uncomplicated UTI (women) | 7 days | 3 days (fluoroquinolone or TMP-SMX) | Non-inferiority demonstrated |
| Intra-abdominal Infection | Until resolution of symptoms | 4 days (after source control) | STOP-IT trial |
| Hospital-Acquired/Ventilator-Associated Pneumonia | 14-21 days | 7 days (8 days if Pseudomonas) | Reduced resistance, similar cure rates |
| Cellulitis | 10-14 days | 5-6 days (if improving) | Expert recommendations, clinical stability |
| Streptococcal Pharyngitis | 10 days | 10 days (DO NOT shorten) | Prevents rheumatic fever |
β οΈ Exceptions Requiring Longer Therapy:
- Endocarditis (4-6 weeks)
- Osteomyelitis (β₯6 weeks)
- Prosthetic joint infection (β₯6 weeks)
- Deep-seated abscesses without adequate drainage
- Immunocompromised hosts
- Staphylococcus aureus bacteremia (2-6 weeks depending on source)
Real-World Examples π₯
Example 1: De-escalation After Culture Results
Clinical Scenario:
Patient: 68-year-old male, admitted with fever, hypotension, and elevated WBC. Suspected abdominal source.
Initial Empiric Therapy (Day 1): Meropenem 1g IV q8h + vancomycin 15mg/kg IV q12h
Culture Results (Day 3):
- Blood cultures: Escherichia coli (2/2 bottles)
- Sensitivities: Pansensitive (including ampicillin-sulbactam, ceftriaxone, fluoroquinolones)
Stewardship Recommendation:
Action: De-escalate meropenem β ceftriaxone 2g IV q24h, DISCONTINUE vancomycin
Rationale:
- β Organism identified - no need for empiric broad-spectrum coverage
- β No MRSA isolated - discontinue vancomycin
- β Pansensitive E. coli - narrow to 3rd-generation cephalosporin
- β Carbapenem-sparing strategy preserves gut microbiome, reduces resistance pressure
- β Patient clinically improving, hemodynamically stable
- β Once afebrile >24h and tolerating PO, consider switch to oral ciprofloxacin
Expected Duration: 7 days total (IV + PO)
Outcome: Successfully completed therapy, saved carbapenem exposure, reduced cost by ~$800/day
Example 2: MRSA Pneumonia Treatment Selection
Clinical Scenario:
Patient: 45-year-old female with severe CA-MRSA necrotizing pneumonia, ICU admission, intubated
Sputum Culture: MRSA, susceptibilities:
- Vancomycin: MIC 1.5 mcg/mL (susceptible)
- Linezolid: Susceptible
- Clindamycin: Susceptible (D-test negative)
- Daptomycin: N/A (inactivated by pulmonary surfactant)
Treatment Decision Matrix:
Option 1: Vancomycin monotherapy
- β οΈ Concern: MIC 1.5 is "high-susceptible" - may have suboptimal lung penetration
- β οΈ Target AUCββ/MIC >400 difficult to achieve with MIC 1.5
Option 2: Linezolid monotherapy
- β Excellent lung penetration (>90% bioavailability)
- β Penetrates into epithelial lining fluid
- β οΈ No activity against toxin production
β BEST CHOICE: Linezolid 600mg IV q12h + Clindamycin 600mg IV q8h
Rationale:
- Linezolid: Bacteriostatic but excellent lung penetration, covers MRSA
- Clindamycin: Inhibits exotoxin production (PVL toxin), important in necrotizing infections
- Dual mechanism approach for severe infection
- Continue until clinical improvement, then discontinue clindamycin
- May convert linezolid to PO when extubated
Monitoring:
- Weekly CBC (linezolid: thrombocytopenia, anemia risk)
- Repeat imaging
- Clinical status (fever, WBC, oxygenation)
Duration: 7-14 days depending on clinical response
Example 3: CRE Bloodstream Infection
Clinical Scenario:
Patient: 72-year-old male, hospital day 14 post-liver transplant, develops fever and hypotension
Blood Cultures (Day 1): Gram-negative rods growing in aerobic bottles
Initial Empiric Therapy: Meropenem 2g IV q8h (extended infusion over 3 hours)
Day 3 - Final Identification: Klebsiella pneumoniae
- Sensitivities: Resistant to all penicillins, cephalosporins, carbapenems, fluoroquinolones
- Susceptible: Colistin, tigecycline, ceftazidime-avibactam
- Carbapenemase detected: KPC-producing CRE
Treatment Decision:
β RECOMMENDED: Ceftazidime-Avibactam 2.5g IV q8h (adjusted for renal function)
Why NOT alternative options?
- β Tigecycline: FDA black box warning, lower cure rates in bacteremia, poor serum levels
- β Colistin monotherapy: High nephrotoxicity risk in transplant patient, resistance emergence
- β οΈ Colistin + meropenem combination: Consider if ceftazidime-avibactam unavailable
Additional Stewardship Actions:
- Source control: Remove/replace infected central line
- Infectious Disease consultation: Documented
- Infection control notification: Implement contact precautions, flag for surveillance
- Duration: 14 days for CRE bacteremia (longer than typical 7-day course)
- Monitor: Daily renal function, LFTs, clinical response
- Repeat cultures: Document clearance at 48-72 hours
Outcome: Bacteremia cleared by Day 4, completed 14-day course, surveillance cultures negative
Example 4: Antibiotic Timeout at 48-72 Hours
Clinical Scenario:
Patient: 55-year-old female admitted with "sepsis" from emergency department
ED Presentation: Fever 38.9Β°C, WBC 14,000, received 30mL/kg fluid bolus, started on broad-spectrum antibiotics
ED Empiric Therapy: Vancomycin 15mg/kg IV + piperacillin-tazobactam 3.375g IV q6h
Admission Diagnosis: "Sepsis, unclear source"
Day 3 Stewardship Review (Antibiotic Timeout):
| Question | Finding | Action |
|---|---|---|
| Does patient have infection? | β’ No fever since admission β’ WBC normalized (8,500) β’ No localizing symptoms β’ Likely viral syndrome or drug fever |
β DISCONTINUE all antibiotics |
| Are cultures positive? | β’ Blood cultures: No growth at 5 days (final) β’ Urine culture: Contaminated specimen β’ Chest X-ray: Clear |
β No evidence of bacterial infection |
| Is antibiotic choice appropriate? | N/A - No infection documented | N/A |
| Can we de-escalate/narrow? | N/A - Stop antibiotics entirely | N/A |
Stewardship Recommendation: "Discontinue vancomycin and piperacillin-tazobactam. No evidence of bacterial infection. Patient clinically well, cultures negative, alternative diagnosis likely. Monitor off antibiotics."
Key Learning: Not all "sepsis" presentations require antibiotics. The antibiotic timeout at 48-72 hours is critical to reassess necessity.
Common Mistakes β οΈ
Mistake 1: Using 3rd-Generation Cephalosporins for ESBL Infections
β Wrong: "The organism shows 'susceptible' to ceftriaxone on the lab report, so I'll use it."
β Correct: ESBL-producing organisms may appear susceptible in vitro but fail clinically due to:
- Inoculum effect: High bacterial load overwhelms antibiotic
- Inducible resistance: Enzyme production increases during therapy
- Poor outcome data: Clinical studies show high failure rates
Rule: Treat ESBL infections with carbapenems (severe) or carefully selected alternatives based on susceptibility testing and infection site (mild/moderate).
Mistake 2: Inadequate Vancomycin Dosing
β Wrong: Standard dose of 1g IV q12h for all patients
β Correct: Weight-based dosing (15-20 mg/kg/dose) with AUCββ-guided monitoring
Why it matters:
- Underdosing leads to treatment failure and resistance
- Target AUCββ/MIC of 400-600 for serious MRSA infections
- Obesity, renal function, and MIC affect dosing requirements
Modern approach: Use Bayesian software or pharmacokinetic calculations to determine optimal dosing based on two levels.
Mistake 3: Using Daptomycin for Pneumonia
β Wrong: "Patient has MRSA bacteremia from pneumonia. I'll use daptomycin 6 mg/kg."
β Correct: Daptomycin is inactivated by pulmonary surfactant and should NEVER be used for pneumonia.
Alternative choices for MRSA pneumonia:
- Vancomycin (if MIC β€1)
- Linezolid (preferred for lung penetration)
- Ceftaroline (active against MRSA, excellent lung penetration)
Mistake 4: Forgetting Renal Dose Adjustments
β Wrong: Continuing standard doses in patients with renal impairment
β Correct: Most antibiotics require dose adjustment based on CrCl
High-risk antibiotics requiring adjustment:
- Ξ²-lactams (especially carbapenems - seizure risk)
- Fluoroquinolones (QTc prolongation, tendon rupture)
- Aminoglycosides (nephrotoxicity, ototoxicity)
- Vancomycin (nephrotoxicity)
- Trimethoprim-sulfamethoxazole (hyperkalemia, crystalluria)
Exceptions (no/minimal adjustment needed):
- Ceftriaxone (biliary excretion)
- Moxifloxacin (hepatic metabolism)
- Doxycycline
- Linezolid
- Azithromycin
Mistake 5: Prolonged Empiric Therapy Without Reassessment
β Wrong: Starting broad-spectrum antibiotics and continuing for 7-14 days without culture review
β Correct: Implement antibiotic timeout at 48-72 hours:
Timeout Checklist: β‘ Are cultures growing anything? β‘ Do susceptibilities allow narrower therapy? β‘ Is there documented infection or alternative diagnosis? β‘ Can IV be switched to PO? β‘ What is the planned total duration? β‘ Can antibiotics be discontinued entirely?
Key Takeaways π―
π Quick Reference: High-Yield Stewardship Points
Resistance Mechanisms:
- Ξ²-lactamases are categorized by Ambler classification (A, B, C, D)
- ESBLs (Class A) are inhibited by avibactam but NOT traditional inhibitors
- Metallo-Ξ²-lactamases (Class B - NDM, VIM, IMP) have NO clinically available inhibitors
- AmpC (Class C) requires carbapenems or cefepime
ESKAPE Pathogens - Treatment Guide:
| MRSA | Vancomycin, daptomycin (NOT for pneumonia), linezolid |
| VRE | Linezolid, daptomycin β₯8 mg/kg |
| ESBL | Carbapenems (severe); oral options if mild and susceptible |
| KPC-producing CRE | Ceftazidime-avibactam, meropenem-vaborbactam |
| NDM-producing CRE | Cefiderocol, colistin-based combinations |
| MDR Pseudomonas | Ceftolozane-tazobactam, ceftazidime-avibactam |
Core Stewardship Interventions:
- Prospective audit & feedback (most effective)
- Antibiotic timeout at 48-72 hours
- IV-to-PO conversion when stable
- Dose optimization using PK/PD principles
- Duration minimization based on evidence
PK/PD Targets:
- Ξ²-lactams: %T>MIC = 40-70% β Extended infusions
- Fluoroquinolones: AUC/MIC β₯125 β Once daily, higher doses
- Aminoglycosides: Cmax/MIC β₯8-10 β Extended-interval dosing
- Vancomycin: AUCββ/MIC = 400-600 β Weight-based, AUC monitoring
Duration Shortcuts:
- CAP: 5 days (if stable by day 3)
- HAP/VAP: 7 days (8 if Pseudomonas)
- Uncomplicated UTI: 3 days
- Cellulitis: 5-6 days (if improving)
- Intra-abdominal: 4 days (after source control)
Further Study π
Official Guidelines:
- CDC Core Elements of Antibiotic Stewardship: https://www.cdc.gov/antibiotic-use/core-elements/index.html
- IDSA Implementing an Antibiotic Stewardship Program: https://www.idsociety.org/practice-guideline/antimicrobial-stewardship/
- SIDP Antibiotic Stewardship Resources: https://www.sidp.org/Stewardship
Resistance Pattern References: 4. CDC Antibiotic Resistance Threats Report: https://www.cdc.gov/drugresistance/biggest-threats.html 5. WHO Priority Pathogens List: https://www.who.int/news/item/27-02-2017-who-publishes-list-of-bacteria-for-which-new-antibiotics-are-urgently-needed
π You've now mastered the essential concepts of antimicrobial resistance patterns and stewardship strategies! Remember: Every antibiotic prescription is an opportunity for stewardship. Your role as a pharmacist in preserving these precious resources cannot be overstated. Use this knowledge to optimize therapy, prevent resistance, and improve patient outcomes.