CVintra ≠ CVtotal [Power / Sample Size]

posted by Helmut Homepage – Vienna, Austria, 2017-06-01 17:47 (3306 d 16:56 ago) – Posting: # 17440
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Hi Laura,

❝ We are planning a XO BE study to support a manufacturing change, and have only data from a single administration (from which we extracted %CV).


That’s the total CV. It is pooled from the between- and within-subject variability. The fact that you administered the product only once, does not mean that the within-subject variability (or inter-occasion variability) does not exist.
Only from a Xover you could estimate (besides CVtotal) both CVintra and CVinter (see this presentation, slides 12–13).

❝ In order to calculate sample size, do I need information regarding expected correlation between PK parameters in period 1 (test) vs period 2 (ref)?


In a Xover you have two sequences (RT|TR). Hence, T in ½N in period 1 and ½N in period 2. Same for R: ½N in period 1 and ½N in period 2. Administering T and R without randomization (T in period 1 and R in period 2) would be a paired design which is not acceptable in BE (requires lacking period effects).

❝ What would be a reasonable assumption when there is no prior data?


None. You need the within-subject CV which you cannot obtain from the data you have. In most (!) cases CVintra < CVinter but the actual relationship is unknown till you have data from a Xover. I know, that’s a vicious circle.
Don’t be tempted to design the Xover based on your CVtotal (e.g., your company is “wealthy” enough and the guy in the Armani-suit tells you “We have the budget. Go ahead!”).Sorry, there are no shortcuts. Either perform a pilot study or – if you don’t have to deal with a HVD(P) – a two-stage design.

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