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Antimicrobial Fundamental Concepts(抗菌基本概念)
Antimicrobial Fundamental Concepts
Pharmacodynamics and Therapeutic Drug Monitoring
Pharmacokinetics versus pharmacodynamics
Pharmacokinetics mathematically describe the relationship of antibiotic concentration to time.
Terminology that is typically associated with pharmacokinetics includes: absorption, distribution,
metabolism, elimination, half-life, volume of distribution, and area under the concentration-time
curve (AUC).
Pharmacodynamics describe the relationship of antibiotic concentration to pharmacologic effect
or microorganism death. The three main pharmacodynamic parameters that are used are the
peak to minimal inhibitory concentration ratio (peak/MIC), the AUC to MIC ratio (AUC/MIC), and
the time the drug concentration remains above the MIC (TMIC).
Concentration independent versus concentration dependent
Concentration independent (time dependent) means that the rate and extent of microorganism
killing remain unchanged regardless of antimicrobial concentration. The pharmacodynamic
parameter that is most often predictive of outcome for concentration independent drugs is
TMIC, although the AUC/MIC can be used because the AUC takes both the antimicrobial
concentration and time into account. Examples of concentration independent antimicrobials
include: beta-lactams, vancomycin, macrolides, aztreonam, carbapenems, clindamycin,
tetracyclines, quinupristin/dalfopristin, flucytosine, and azole antifungals.
Concentration dependent (time independent) means that the rate and extent of microorganism
killing are a function of the antimicrobial concentration (increase as the concentration
increases). The pharmacodynamic parameter that is most often predictive of outcome for
concentration dependent drugs is peak/MIC, although the AUC/MIC can be used because the
AUC takes both the antimicrobial concentration and time into account. Examples of
concentration dependent antimicrobials include: fluoroquinolones, aminoglycosides, and
amphotericin B.
B
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