Examples of drugs with such variability include those with:
Therapeutic drug monitoring (TDM) has become an essential aspect of clinical management. The process is based on the assumption there is a relationship between plasma drug concentration/dosage and between the blood drug concentration/pharmacodynamic effects. Clinicians identify the effects of pharmacokinetic and immunosuppressive drugs variability to differences in dosage requirements by measuring drug concentration at a steady state.
The drug concentration is also modified to attain the desired concentration associated with efficacy, not toxicity. For this reason, toxicology studies are sometimes tied to therapeutic drug monitoring programs. However, the significant interindividual pharmacodynamic variability at any given plasma concentration requires the use of a range of concentrations.
That’s why sampling techniques like remote patient monitoring and microsampling have become widely accepted. Microsampling enables researchers to collect smaller blood samples for quantitative analysis of drug concentrations, biomarkers, and metabolites.
It has particularly become an essential part of off-site pharmacokinetic studies in early drug development as it facilitates:
Microsampling devices like the Mitra have been developed as a result. Mitra is a volumetric absorptive microsampling equipment designed for nonclinical plasma and blood collection. It is mainly instrumental in plasma collection, which is often preferred to blood matrices.
Liquid matrices are easy to use in existing analytical workflows, and the remaining samples applied for other purposes; e.g., in the study of biomarkers, reassay, and the identification of metabolites.
Additionally, dried sampling techniques need more method development and often have non-standard bio-analytical workflows in comparison with liquid matrices.
Most studies support the application of microsampling in early discovery projects of drugs. Some reasons for fewer later-phase studies using this technique include high attrition rates, slow drug progression in candidates, and reluctance by organizations to change from traditional blood sampling approaches.
More information about remote microsampling for TDM can be found via our Microsampling for Drug Monitoring page.