Linganisha mbinu
Pitia mbinu ulizochagua bega kwa bega; safu zinazotofautiana zinaangaziwa.
| Jaribio la Msalaba la Mikono Mingi× | Crossover Randomized Controlled Trial× | |
|---|---|---|
| Nyanja | Muundo wa Majaribio | Muundo wa Majaribio |
| Familia | Process / pipeline | Process / pipeline |
| Mwaka wa asili≠ | Mid-20th century; multi-arm extensions formalized by 1970s–1980s | 1960s (Grizzle 1965 for statistical foundations); widely used in clinical research since the 1970s |
| Mwanzilishi≠ | Developed from early crossover trial methodology (Williams 1949; Cochran & Cox 1957) | Early formalized by statisticians including Bradford Hill and colleagues in clinical trials; theoretical framework developed by Grizzle (1965) and later Senn (2002) |
| Aina≠ | Within-subject experimental design with multiple treatment arms | Experimental within-subject design |
| Chanzo asilia≠ | Jones, B., & Kenward, M. G. (2003). Design and Analysis of Cross-Over Trials (2nd ed.). Chapman and Hall/CRC. ISBN: 978-1584883869 | Senn, S. (2002). Cross-over Trials in Clinical Research (2nd ed.). Wiley. ISBN: 978-0471496533 |
| Majina mbadala | multi-arm crossover trial, multi-period multi-treatment crossover, CMAT, multi-treatment crossover experiment | crossover RCT, crossover trial, within-subject RCT, AB/BA crossover design |
| Zinazohusiana | 5 | 5 |
| Muhtasari≠ | A crossover multi-arm experiment is a within-subject experimental design in which each participant receives three or more treatments (arms) across successive periods, with random assignment to sequence. Because every participant experiences all arms, the design eliminates between-subject variability from treatment comparisons, dramatically increasing statistical power for a given sample size. It is widely used in clinical pharmacology, psychology, agriculture, and behavioral research. | A crossover randomized controlled trial (crossover RCT) is an experimental design in which each participant receives all study interventions in a randomized sequence, separated by a washout period. Because every participant serves as their own control, within-subject variability is eliminated from the treatment comparison, yielding greater statistical power per participant than a parallel-group RCT of equal size. |
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