Clinical Pharmacokinetics and Pharmacodynamics
Summary
Antimicrobial agents work by killing or preventing the growth of a microorganism whilst having little or no impact on the host. Antimicrobials include agents that act against all types of microorganisms: bacteria (anti-bacterial), viruses (anti-viral), fungi (anti-fungal) and protozoa (antiprotozoal). Dosing regimens of antimicrobials should be optimised to prevent or minimise resistance. Suboptimal dosing has been attributed to poorer clinical outcomes and cure rates, as well as increasing the risk of morbidity and mortality.
Pharmacokinetics (PK) is the study of the time course of drug absorption, distribution, metabolism and elimination i.e. what the body does to a drug. Pharmacodynamics (PD) is the study of the relationship between drug concentration at the site of action and the resulting effect i.e. what the drug does to the body.
Target PK* and PD* indices are crucial to achieving maximal antibiotic activity and effective treatment of infection. However, adequate antimicrobial dosing to achieve PK/PD targets remains a challenge. The administered drug doses are frequently obtained from data from healthy individuals and often do not account for PK/PD differences in different patient populations, such as septic patients. Thus, optimising antimicrobial dosing regimens requires robust knowledge of the pharmacokinetics and pharmacodynamics of the antimicrobial agent.
It should be noted that PK/PD principles relate to all drugs but for the purpose of this eModule the focus being on antimicrobial agents.
General Information
Enrolled trainees 1986
Open 11.09.2018
Available for ESICM members
Student effort 2
Last Updated September 11, 2018
Intended Learning Outcomes
After studying this module on Clinical Pharmacokinetics and Pharmacodynamics, you should be able to:
- Describe the main aspects of PK and PD and explain how these two concepts connect regarding the use of antimicrobial agents.
- Define MIC and breakpoint and explain how these concepts affect antimicrobial resistance.
- Describe the main pharmacokinetic changes that occur in septic patients.
Relevant competencies in CoBaTrICE
- 4.2 Manages antimicrobial drug therapy
Enrollment Options
You are currently NOT enrolled in this course.
This course is available only for registered ESICM members.
If you are an ESICM member you can enrol yourself by clicking the Enrol Me button.
If there is no Enrol button on the top left of this card please check that you have login and that you are an ESICM Member.
Verify that you are logged in the Academy using your valid ESICM account to enrol yourself in the course.
Disclaimer
All authors of ACE courses sign a document declaring absence or any actual or potential conflicts of interest. In addition, they sign a copyright document confirming the work is their own and that they have obtained the necessary permission for any copyrighted material. The latter document also transfers the intellectual copyright to the ESICM. Both the conflict of interest and copyright forms are filed and stored in compliance with GDPR and are available for inspection upon request.