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KR ★ India, 2009-04-17 08:34 (6269 d 19:20 ago) Posting: # 3550 Views: 5,134 |
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Dear all, Can anyone throw some focus on dose normalization for two way crossover study? i.e if reference product is of 30 mg given once daily and test product is of 10 mg given thrice daily then how to do pharmacokinetic and statistical analysis? What is the effect of this dose on concentration values? Thanks and regards, KR |
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Helmut ★★★   Vienna, Austria, 2009-04-21 15:44 (6265 d 12:10 ago) @ KR Posting: # 3574 Views: 4,154 |
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Dear KR! ❝ Can anyone throw some focus on dose normalization for two way crossover ❝ study? i.e if reference product is of 30 mg given once daily and test ❝ product is of 10 mg given thrice daily then how to do pharmacokinetic and ❝ statistical analysis? Your design sounds a little bit strange. The reference obviously is an MR formulation and you want to develop an IR? Is there no IR reference available? What's the rationale to come up with an IR formulation (compliance issues)? But if you want to do that:
❝ What is the effect of this dose on concentration values? OK, you will have three Cmax values for the IR formulation. Whether they will be different or not depends on the dosage interval (thrice daily for some antibiotics means strictly 8/8/8 hours; for many drugs morning/after lunch/after dinner would mean 6/6/12 hours) and the half life of the drug (accumulation?). With some knowledge of the PK it is possible to get an idea about the expected levels for test/reference. This is useful in designing the sampling scheme. But again: it does not make sense to compare the rate of BA. — 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 |
Ing. Helmut Schütz