Antibiograms and Antimicrobial Susceptibility Testing Information

• Interpretive Guidelines
• Definitions and Abbreviations
• Gram-Positive Bacteria
• Enterococci – non-urine isolates
• Staphylococci
• Viridans group Streptococci
• Beta-hemolytic Streptococci
• Gram-Negative Bacteria
• Enteric Gram Negative Rods (Enterobacteriacae)
• Yeast

Interpretive Guidelines

Definitions and Abbreviations

• CLSI: Clinical Laboratory Standards Institute
• EUCAST: European Committee on Antimicrobial Susceptibility Testing

Gram-Positive Bacteria

Enterococci – non-urine isolates

Gentamicin (500 mcg/mL)

• A result of "Synergy likely" indicates that an isolate does not have high level resistance to gentamicin. This drug is therefore likely to be synergistic with a cell wall-active agent (e.g., ampicillin, penicillin, and vancomycin) provided the organism is susceptible to that agent.
• A result of "Synergy unlikely" indicates high-level resistance to gentamicin, meaning it is not synergistic with cell wall-active agents.

Streptomycin (1000 mcg/mL)

• A result of "Synergy likely" indicates that an isolate does not have high level resistance to streptomycin. This drug is therefore likely to be synergistic with a cell wall-active agent (e.g., ampicillin, penicillin, and vancomycin) provided the organism is susceptible to that agent.
• A result of "Synergy unlikely" indicates high-level resistance to streptomycin, meaning it is not synergistic with cell wall-active agents.

Imipenem

EUCAST breakpoints; susceptible ≤4, resistant ≥16

Moxifloxacin

Currently there are no breakpoints for this antibiotic. However, moxifloxacin demonstrates in vitro activity against some Enterococcus species and a provisional breakpoint of susceptible ≤1 has been suggested (Andrews, et al. 1999). An infectious disease consult may be useful if you are considering using moxifloxacin for the treatment of Enterococcal infections.

Staphylococci

Clindamycin

A result of "R(comment)" or "Resistant (with comment)" indicates that an isolate has inducible clindamycin resistance. Clindamycin may still be used in combination regimes but should not be used alone to treat infections caused by bacteria with inducible resistance.

Viridans group Streptococci

Clindamycin

A result of "R(comment)" or "Resistant (with comment)" indicates that an isolate has inducible clindamycin resistance. Clindamycin may still be used in combination regimes but should not be used alone to treat infections caused by bacteria with inducible resistance.

Penicillin

In patients with streptococcal endocarditis, use American Heart Association (AHA) breakpoints for penicillin:

• Susceptible ≤0.12µg/ml

• Intermediate >0.12 to ≤0.5µg/ml

• Resistant >0.5µg/ml

For further information, please see: Baddour, et al. 2015.

Imipenem

EUCAST breakpoint; susceptible ≤2, resistant ≥4

Moxifloxacin

Currently there are no existing breakpoints for this antibiotic. However, a provisional susceptible breakpoint of ≤1 has been suggested for S. pneumoniae and could be considered applicable to viridans group streptococci (Andrews, et al. 1999).

S. pneumoniae

Clindamycin

A result of "R(comment)" or "Resistant (with comment)" indicates that an isolate has inducible clindamycin resistance. Clindamycin may still be used in combination regimes but should not be used alone to treat infections caused by bacteria with inducible resistance.

Penicillin and Ceftriaxone

In the event that a patient is thought to have meningitis, but a CSF specimen has not been obtained, the “meningitis” interpretation should be used to guide therapeutic decisions.

Beta-hemolytic Streptococci

Clindamycin

A result of "R(comment)" or "Resistant (with comment)" indicates that an isolate has inducible clindamycin resistance. Clindamycin may still be used in combination regimes but should not be used alone to treat infections caused by bacteria with inducible resistance.

Imipenem

Per EUCAST: susceptibility can be inferred from the penicillin susceptibility result.

Moxifloxacin

EUCAST breakpoints; susceptible ≤0.5, resistant ≥2

Gram-Negative Bacteria

Enteric Gram Negative Rods (Enterobacteriacae)

Cefepime

Current CLSI interpretive breakpoints may not predict clinical efficacy. Only strains with MIC ≤1.0 may be regarded as fully susceptible. Strains with MICs 2.0-4.0 should be considered to have dose-dependent susceptibility. A cefepime MIC = 8 has been associated with clinical failure. (Bhat, et al. 2007; Crandon, et al. 2010; Lee, et al. 2007; Paterson, et al. 2001).

Piperacillin-Tazobactam

CLSI interpretive breakpoints may not predict clinical efficacy. PK/PD analyses support the EUCAST recommendation that only strains with piperacillin-tazobactam MICs ≤ 8 be considered susceptible (DeRyke, et al. 2007).

Fluoroquinolones – non-urine isolates

For serious infections, CLSI interpretive breakpoints may not predict clinical efficacy. PK/PD analyses suggest that ciprofloxacin and levofloxacin MICs should be ≤0.125-0.25 and ≤0.25-0.5, respectively, for isolates to be considered susceptible (DeRyke, et al. 2007; Frei, et al. 2008).

Moxifloxacin – urine isolates only

No CLSI interpretive breakpoints are available. EUCAST interpretive breakpoints: susceptible ≤0.5, resistant ≥2

Pseudomonas aeruginosa

Cefepime

Current CLSI interpretive breakpoints may not predict clinical efficacy.Only strains with MIC ≤1.0 may be regarded as fully susceptible. Strains with MICs 2.0-4.0 should be considered to have dose-dependent susceptibility. A cefepime MIC = 8 has been associated with clinical failure. (Bhat, et al. 2007; Crandon, et al. 2010; Lee, et al. 2007; Paterson, et al. 2001).

Fluoroquinolones – non-urine isolates

For serious infections, CLSI interpretive breakpoints may not predict clinical efficacy. PK/PD analyses suggest that ciprofloxacin and levofloxacin MICs should be ≤0.125-0.25 and ≤0.25-0.5, respectively, for isolates to be considered susceptible (DeRyke, et al. 2007; Frei, et al. 2008). Many authorities recommend combination therapy for serious P. aeruginosa infections.

Acinetobacter

Tigecycline

No CLSI interpretive breakpoints are available. The FDA interpretive breakpoint for Enterobacteriacae (susceptible ≤2) is unlikely to predict clinical efficacy. Tigecycline only achieves steady-state serum concentrations of 0.4-0.6, and PK/PD analyses suggest that MICs should be ≤0.25 to be considered susceptible. Treatment failures have been reported with tigecycline monotherapy for serious Acinetobacter infections (Pankey, et al. 2005; Ambrose, et al. 2009; Anthony, et al. 2008).

Cefepime

Current CLSI interpretive breakpoints may not predict clinical efficacy.Only strains with MIC ≤1.0 may be regarded as fully susceptible. Strains with MICs 2.0-4.0 should be considered to have dose-dependent susceptibility. A cefepime MIC = 8 has been associated with clinical failure. (Bhat, et al. 2007; Crandon, et al. 2010; Lee, et al. 2007; Paterson, et al. 2001).

Fluoroquinolones – non-urine isolates

For serious infections, CLSI interpretive breakpoints may not predict clinical efficacy. PK/PD analyses suggest that ciprofloxacin and levofloxacin MICs should be ≤0.125-0.25 and ≤0.25-0.5, respectively, for isolates to be considered susceptible (DeRyke, et al. 2007; Frei, et al. 2008).

Piperacillin-Tazobactam

PK/PD analyses suggest that only strains with piperacillin-tazobactam MICs ≤8 should be considered susceptible (DeRyke, et al. 2007).

Stenotrophomonas maltophilia

Moxifloxacin

No CLSI or EUCAST breakpoints are available. However, EUCAST breakpoints for Enterobacteriacae may be tentatively used for guidance: susceptible ≤0.5, resistant ≥2

Yeast

Candida species

Susceptible Dose Dependent (SDD)

Susceptibility is dependent on achieving the maximal possible blood level. ID consult recommended.

Flucytosine

Flucytosine should be used in combination with another antifungal agent to prevent emergence of resistance (Drew, et al. 2013).

Candida glabrata

Voriconazole

Current data are insufficient to demonstrate a correlation between in vitro susceptibility testing and clinical outcome for Candida glabrata (CLSI 2012)

Candida parapsilosis

Micafungin

EUCAST interpretive criteria for C. parapsiolosis and micafungin: susceptible ≤2, resistant >2. C. parapsilosis harbors an alteration in the echinocandin target gene and the MIC's of the echinocandins are higher than for other Candida species (EUCAST 2013). Multiple studies have shown C. parapsilosis to be intrinsically less susceptible to micafungin and breakthrough cases of C. parapsilosis invasive infection have been reported (Pfeiffer, et al. 2010).

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