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Cmax ☆ India, 2010-08-27 22:10 (5357 d 23:47 ago) Posting: # 5862 Views: 7,756 |
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Dear anyone, Can any one suggest how we can calculate sample size for a partial replicate study with scaled approach... for example considering CV 45%  in normal cross over we may have to do with 100+ subjects... what would be the sample size if we propose a partial replicate...thanks in advance |
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Helmut ★★★   Vienna, Austria, 2010-08-30 18:02 (5355 d 03:56 ago) @ Cmax Posting: # 5868 Views: 7,187 |
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Dear Cmax! ❝ Can any one suggest how we can calculate sample size for a partial replicate study with scaled approach... considering CV 45% in normal cross over we may have to do with 100+ subjects... Sounds like you are aiming at T/R 0.95 with 90% power? Would need 110 subjects (and 82 for unscaled partial replicate). ❝ what would be the sample size if we propose a partial replicate... In theory RSABE should adjust the acceptance range according to the intra-subject variability of the reference. In other words, power (and therefore the sample size) is independent from CV. For details see: Tóthfalusi L, Endrényi L and A García-Arieta ![[image]](img/uploaded/image54.png) Fig. 3. Power curves of simulated three-period crossover studies evaluated by average bioequivalence (ABE) and by scaled ABE (SABE) with two different regulatory constants. Three-period test-reference-test/reference-test-reference bioequivalence trials were simulated with 36 subjects and different within-subject variabilities. (a) Coefficient of variation (CV) = 35%. (b) CV= 45%. (c) CV= 55%. The simulated bioequivalence studies were evaluated using ABE with the conventional criterion and by SABE with two regulatory cutoff values. The regulatory cutoff sigmaS = 0.760 was proposed by Tothfalusi and Endrenyi, whereas the US FDA suggestion is 0.893. In both cases, an additional criterion was applied, which constrained the point estimate of the geometric mean ratio to values between 0.80 and 1.25. These figures show the percentage of crossover studies that successfully declare bioequivalence as the true geometric mean ratio gradually increases. Notice that for the same sample size power drops in the conventional (unscaled 2×2 cross-over) ABE design, but is only fairly affected in the scaled methods. The sample size for a unscaled partial replicate is 75 % of a 2×2 Xover. Now for the pitfalls:
— Dif-tor heh smusma 🖖🏼 Довге життя Україна! ![[image]](https://static.bebac.at/pics/Blue_and_yellow_ribbon_UA.png) Helmut Schütz ![[image]](https://static.bebac.at/img/CC by.png) The quality of responses received is directly proportional to the quality of the question asked. 🚮 Science Quotes |
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Cmax ☆ India, 2010-09-04 10:51 (5350 d 11:06 ago) @ Helmut Posting: # 5885 Views: 6,660 |
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Dera Helmut, Thanks and if we are not in our desired power then. regards cmax |
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Helmut ★★★ Vienna, Austria, 2010-09-04 15:42 (5350 d 06:15 ago) @ Cmax Posting: # 5887 Views: 6,685 |
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Dear Cmax! ❝ Thanks and if we are not in our desired power then. First see this post. Please try to formulate your questions in an unambigious way. If you are within the CV-range where scaling is allowed (FDA >30%, EMA >30%-50%) there is no 'desired power then'. Either the study demonstrated bioequivalence - or not. — Dif-tor heh smusma 🖖🏼 Довге життя Україна! Helmut Schütz The quality of responses received is directly proportional to the quality of the question asked. 🚮 Science Quotes |
Ing. Helmut Schütz