33/34 - Antimicrobial Resistance Flashcards

1
Q

Antimicrobial Stewardship

PRIMARY GOAL

A

IMPROVE PATIENT OUTCOMES

Systematic process to optimize ABx use to improve patient outcomes
while:
Minimizing unintended consequences

Optimizing:
Utilized only when indicated
Ideal Agent
Dose/ Route/Duration

SAFETY

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2
Q

ABx Stewardship
CORE STRATEGIES

A
  • *Formulary Management**
  • *Restrictions + Preauthorization**

Prospective AUDIT
with intervention + feedback

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3
Q

ABx Stewardship

Supplemental Strategies

A

IV to PO Switch
for HIGHLY BIOAVAILABLE AGENTS - Fluoroquinolones
Indications and durations
Education
Dosing protocols
Including optimization of PK/PD through alternative dosing schemes
Guideline development
Use of CPOE/CDS

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4
Q

Formulary Management
Abx Stewardship

A

RESTRICTIONS

  • *Pre-Authorization Chalenges:**
  • *Staff/coverage**
  • *Documentation / Challenging Physicians autonomy**
  • *DELAYS IN THERAPY**
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5
Q

Antimicrobial TIME-OUT

A

@48-96 hours to RE-ASSESS NEED for continued therapy

Transition from:
Empiric –> DEFINITIVE THERAPY

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6
Q
  • *NNIS report from 2004**
  • *showed notable increases in resistance:**
A

Kleb. Pneumonia
resistance to 3rd Gen Cephs
Ceftazadime / Ceftriaxone / Cefotaxime

MRSA

Pseudomonas AUREGINOSA
increase in quinolone + 3rd gen cephs

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7
Q
  • *Bad Bugs, No Drugs**
  • *Campaign**
A

Developed by IDSA in 2004
to increase awareness of RESISTANCE RATES

INCENTIVES FOR R&D
within pharmaceutical industry for ABx development

Followed up by:
2011 ESKAPE PATHOGENS

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8
Q

2011 ESKAPE PATHOGENS
Cause significant # of Healthcare infxns:
HAP/VAP - IntraAbdominal - UTI - CRSBI

Update to IDSA’s “Bad bugs, No Drugs” campaign

A

Considered to cause significant burden of healthcare infections which can “escape” effects of current abx agents.

+ Enterococus faceum +
+ S. aureus
+

Below are gram NEGATIVE:

  • K*lebsiella pneumonia
  • *Acinetobacter** species
  • *P.** aeruginosa
  • *Enterobacteriacea** (gut ones)
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9
Q

3 Mecanisms of Gram NEGATIVE Resistance

INTRINSIC

A

INTRINSIC

Characteristic of the organism

EFFLUX pumps

Enzymes = AmpC

Low permeability membrane

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10
Q

3 Mecanisms of Gram NEGATIVE Resistance

ACQUIRED

A

ACQUIRED

Incorporation of “extra” genetic material

Plasmids** / **Transposons** / **Integrons

  • *BETA-LACTAMASES**
  • *Enzymes**
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11
Q

3 Mecanisms of Gram NEGATIVE Resistance

ADAPTIVE

A

ADAPTIVE

Baceria develops ability to RESIST by:
modifying DNA/genetic material

Typically due to:
REPEAT ABx exposure

Subtherapeutic Conc.** + **OVERUSE

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12
Q

Beta-Lactamase Mutations

Arose from mutations from WHAT?

A

TEM

+

SHV

B-lactamases

had activity against:
ampicillin / cephalothin / 3rd gen Cephs.
CeftriaXone - CeftaZadime - CefotaXime

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13
Q
  • *ESBLs**
  • *Extended Spectrum B-Lactamases**

Resistant to WHAT + What ORGANISMS?

A

Resistance is:
ACQUIRED - Plasmid Mediated

CEPHalosporims 1st-3rd gen + Penicillins
also typically resistant to:
Quinolones

Typically seen in:
Enterobecteriacea
esp Kleb + E. Coli

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14
Q
  • *ESBLs**
  • *Extended Spectrum B-Lactamases**

TREATMENT OF CHOICE

CEPHalosporims 1st-3rd gen + Penicillins
also typically resistant to:
Quinolones

Typically seen in:
Enterobecteriacea
esp Kleb + E. Coli

A
  • *CARBAPENEM**
  • *Mero**penem / Imipenem / Ertapenem

Cefepime
4th gen ceph - may have some activity

Fofsomycin / Tigecycline

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15
Q

AmpC - B-Lactamases
Aka - cephalosporinases

Resistant to WHAT + What ORGANISMS?

A

Resistance is: INDUCED
might NOT show resistance NOW –> will be INDUCED after ABX given

  • *CEPHalosporims** 1st-3rd gen + Penicillins
  • similar to ESBLs*

Seen in:
SPACE organisms

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16
Q

SPACE BUGS

What are they?

KNOW THIS

A

AmpC - B-lactamase producers
INDUCIBLE, will see suceptibility first –> INDUCED RESISTANCE

Serratia marcescens

Pseudomonasaureginosa

Acinetobacter baumannii

Citrobacter feundii

Enterobacter cloacae

17
Q

AmpC TREATMENT
INDUCIBLE, need to closely monitor those with:

Serratia marcescens

Pseudomonas aureginosa

Acinetobacter baumannii

Citrobacter feundii

Enterobacter cloacae

A

AmpC Treatment

CARBAPENEMS
Meropenem / Imipenem / Ertapenem

  • *Cefipime**
  • above same as ESBL treatment*

Quinolones** + **Bactrim

18
Q

Carbapenamase Producers

Resistant to WHAT + What ORGANISMS?

A

Similar to ESBL+ AmpC but now resistant to:
CARBAPENEMS
Typically also show resistance to:
Quinolones** + **AminoGlycosides

Typically Seen in:
CRE = Carbapenamase Resistant Enterobacter
Klebsiella**+**E.Coli**+**Enterobacter

Also:
P. Aeurginosa + A. Baumanni
can pick up MANY resistant genes

19
Q

Carbapenamase Producers

TREATMENT OPTIONS?

CRE = Carbapenamase Resistant Enterobacter
Klebsiella**+**E.Coli**+**Enterobacter

Also:
P. Aeurginosa + A. Baumanni

A

B-Lactam + Inhibitor Combos

CEFTAZIDIME** + **AVIBACTAM
Avycaz

MEROPENEM** + **VABORBACTAM
Vabomere

Tigecycline ?

20
Q

Multidrug-Resitant Isolates

Which ORGANISMS often PICK UP many INDUCIBLE RESITANT GENES?

A

Pseudomonas. Aeruginosa + Acinetobacter. Baumanni
both are SPACE bugs - AmpC B-lacamase producers

Typically only
Susceptible < 2 classes of ABx

Have Numerous mechanisms for drug resistance:
Inducible ceph / B-lactamase / enzymes
Porins
Efflux Pumps

21
Q

Colistin** / **Polymyxin B

Option for Resistant Gram-Pathogens?

A
  • *Old drug**
  • no GRAM POS activity*

issue is:
NEPHROTOXICITY

can use inhalation

22
Q

TIGECYCLINE

Drug Option / Issues?

KNOW THIS

A

does NOT cover
_PSEUDOMONAS
_
meaning that you can NOT use it for:
HAP

“Minocycline on Steroids

Covers:
MRSA / MDR Acinetobacter / ESBLs
good for POLYMICROBIAL infxns

Barf-a-cycline

23
Q

Drug of Choice for Resistant Phenotype?

AmpC B-Lactamase
SPACE ORGAMISMS
Enterobacter / Citrobacter Freundii / Serratia

Resistant to:
ALL B-Lactamases except cefepime + carbapenems

A

CEFEPIME
preferred

CARBAPENEMS

FQ** + **SMX/TMP

24
Q

Drug of Choice for Resistant Phenotype?

ESBL
Extended spectrum B-lactamase
CTX-M / SHV/TEM

Enterobacteriacae = E. Coli + Kleb

A

CARBAPENEMS

pip/tazo too but not used

25
Q

Drug of Choice for Resistant Phenotype?

CARBAPENAMASES
KPC / NDM / OXA

enterobactericiae

A

CEFTAZ** + **AVI

MERO** + **VABO

Polymixins / Aminoglycosides