Table II.
Tool, information | Outcome |
---|---|
Dose | Defined normal (most common) dose and maximum dose for which the breakpoints are valid. |
Clinical indication(s) | Clinical indications for which there was reasonable clinical evidence and for which breakpoints are valid. |
Target species | Species for which there was reasonable clinical evidence and for which breakpoints are valid. |
MIC distributions for target species to define the epidemiological cut-off values (ECOFF). | Epidemiological cut-off value (ECOFF). Defined MIC distributions made available on the EUCAST website and the determination of the ECOFF for species where enough MIC values were obtained. The importance of this is that the final clinical breakpoint should not divide wild-type MIC distributions of important target organisms. This would obviate reproducible susceptibility testing. |
Resistance mechanisms in target organisms | When there is obvious correlation between the presence of a defined resistance mechanism (or gene), the breakpoint should separate organisms without and with the resistance mechanism (gene). When the correlation is stronger with the MIC of the organism than with the presence or absence of a resistance mechanism, the breakpoint should be allowed to divide organisms without and with the mechanism (gene). |
Pharmacokinetics of the agent; Pharmacodynamics of the agent; Mathematical simulations | PK/PD cut-off value. |
Clinical outcome data (when related to MIC)—to determine if the clinical success rates are related to MICs or specific resistance mechanisms | Clinical cut-off value. |