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RegisterHVDs/HVDPs: global harmonization?! [Power / Sample Size]
posted by Helmut 
– Vienna, Austria, 2010-12-22 17:59 (5295 d 18:46 ago) – Posting: # 6330
Views: 13,600
Dear Boonchai!
Convention (aka old hat).
Was first stated at the Bio-International ’89 in Toronto, Canada as 25% CV being “problematic” and 30% considered highly variable. ≥30% Was agreed upon at the Bio-International ’92 in Bad Homburg, Germany.1,2
Nitpicking terminology: We distinguish between HVDs (Highly Variable Drugs: CV of a solution ≥30%) and HVDPs (Highly Variable Drug Products: CV of a formulation ≥30%). EMA adopted this wording in the current guideline.
No and no.
In some countries widening of the BE-limits is acceptable:
![[image]](img/uploaded/image66.png)
Note that the bioequivalence limits are displayed in ln-scale in order to show the symmetry around 1:
ln(1) = 0 and ln(0.80, 1.25) = ∓0.2231.
❝ Who define HVD?
Convention (aka old hat).
Was first stated at the Bio-International ’89 in Toronto, Canada as 25% CV being “problematic” and 30% considered highly variable. ≥30% Was agreed upon at the Bio-International ’92 in Bad Homburg, Germany.1,2
Nitpicking terminology: We distinguish between HVDs (Highly Variable Drugs: CV of a solution ≥30%) and HVDPs (Highly Variable Drug Products: CV of a formulation ≥30%). EMA adopted this wording in the current guideline.
❝ Does it subject to the regulator in each country? Is it useless?
No and no.
In some countries widening of the BE-limits is acceptable:
- Arbitrary to 75–133% for Cmax if based on clinical grounds: old EMEA guideline, Australia, ASEAN states,…
- For Cmax and AUC in product-specific GLs of the FDA (no clinical justification); RSABE-scaling, GMR restriction 80–125%.
- For Cmax according to current EMA-GL: ABEL limited with CV≤50%, clinical justification, GMR restriction 80–125%. Note that generally HVDs/HVDPs are defined with CV at least 30%; EMA states CV greater than 30%.
- For AUC according to Canada’s TPD drafted-GL: unlimited ABEL, no GMR restriction.
Note that the bioequivalence limits are displayed in ln-scale in order to show the symmetry around 1:
ln(1) = 0 and ln(0.80, 1.25) = ∓0.2231.
- Blume HH, Midha KK. Bio-International ’92, Conference on Bioavailability, Bioequivalence and Pharmacokinetic Studies. Int Pharm J. 1993;7(5):201–5. doi:10.1002/jps.2600821125.
- Blume HH, Midha KK, editors. Bio-International. Bioavailability, Bioequivalence and Pharmacokinetics. Stuttgart: medpharm Scientific Publishers; 1993.
—
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Helmut Schütz
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The quality of responses received is directly proportional to the quality of the question asked. 🚮
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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
Complete thread:
- How is the calculated Sample Size? bjkim97 2010-12-22 02:42 [Power / Sample Size]
![[Mix]](https://static.bebac.at/img/mix.png "open in Mix view")
- How is the calculated Sample Size? boonchai_l 2010-12-22 05:55
- How is the calculated Sample Size? VRP 2010-12-22 06:54
- How is the calculated Sample Size? bjkim97 2010-12-22 07:40
- How is the calculated Sample Size? boonchai_l 2010-12-22 09:06
- How is the calculated Sample Size? Dr_Dan 2010-12-22 11:06
- HVDs/HVDPs: global harmonization?!Helmut 2010-12-22 16:59
- How is the calculated Sample Size? boonchai_l 2010-12-22 09:06
- Pantoprazole CVs d_labes 2010-12-22 12:05
- Pantoprazole CVs boonchai_l 2010-12-22 21:26
- Expectation ElMaestro 2010-12-22 22:22
- Opinions Ohlbe 2010-12-23 01:23
- Pooling... Helmut 2010-12-23 15:29
- Choosing CVs d_labes 2011-01-03 08:43
- Pantoprazole CVs bjkim97 2010-12-23 14:43
- Pooling: example Helmut 2010-12-23 16:11
- Pantoprazole CVs boonchai_l 2010-12-22 21:26
- How is the calculated Sample Size? boonchai_l 2010-12-22 05:55
Ing. Helmut Schütz