Table 1.
Comparisons of the performance of selective reaction monitoring (SRM), parallel reaction monitoring (PRM), data-dependent acquisition (DDA), and data-independent acquisition (DIA)a.
| Techniques | Performance | |||||
|---|---|---|---|---|---|---|
| Sensitivity | Specificity | Reproducibility | Multiplexing | Assay development | Prevalence in DMET studyb | |
| SRM | + + + | + + + | + + + + | + | + | + + + + |
| PRM | + + + + | + + + + | + + + + | + | + + | + + |
| DDA | + | + | + | + + + + | + + + + | + |
| DIA | + + | + + | + + | + + + + | + + + | + |
aThe number of “+” indicates the performance of a specific technique with “+ + + +” denoted to the best performance and “+” for the lowest performance. b The prevalence of each technique used in drug-metabolizing enzymes and transporters (DMET) proteomics research was estimated from the literature collected by the writing of this paper (May, 2020).