AI Article Synopsis
- Microdosing is a method in early drug development that uses very low doses of drugs to gather data on how the body processes them, known as pharmacokinetics (PK).
- It combines these low doses with advanced testing techniques to predict how higher, clinically relevant doses will behave in the body, assuming a linear relationship.
- While it simplifies some regulatory requirements and reduces costs, it requires the creation of labeled compounds and complex testing methods to be effective.
Article Abstract
Microdosing offers a faster and potentially less expensive approach to obtaining human in vivo PK data in early clinical drug development. It encompasses the use of pharmacologically inactive doses of test drug in the low microgram range along with ultrasensitive assay methods (PET, AMS) to assess human exposure in order to extrapolate the PK of higher, clinically more relevant doses, assuming linear PK. This strategy allows early evaluation of systemic clearance, oral bioavailability as well as sources of intersubject variability and questions of specific metabolite formation. It does take advantage of reduced regulatory requirements of preclinical safety studies, bulk drug synthesis (CMC requirements) and easier formulation options, e.g., as part of an exploratory IND; however, this is counterbalanced by a need to synthesize radiolabeled test compound and the development of a sophisticated analytical method. Ongoing studies will determine the predictability of human PK using Microdosing methods.
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| http://dx.doi.org/10.1007/978-3-540-49529-1_2 | DOI Listing |
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