Bioequivalence and Bioavailability Forum • Mesalazine tablets for Europe Market

balakotu
★

India,
2015-10-19 11:47
(3103 d 22:16 ago)

Posting: # 15570
Views: 8,777

Mesalazine tablets for Europe Market [RSABE / ABEL]

Dear All,

Please provide the valuable suggestion for below mentioned product for Europe submission,

1) We would like to know what kind of studies required for Mesalazine Gastro-resistant MR tablets for Europe Market.

2) Do we need to conduct the studies on 400 mg & 800 mg or any one of the strengths? At what dose the study should be conducted.

3) Please also propose the approx. number of subjects required for your proposed studies.

Regards
Kotu.

Edit: Category changed. [Helmut]

komodo
☆

Turkey,
2015-10-23 10:52
(3099 d 23:11 ago)

@ balakotu
Posting: # 15576
Views: 7,266

Mesalazine tablets for Europe Market

Post reply

❝ We would like to know what kind of studies required for Mesalazine Gastro-resistant MR tablets for Europe Market.

Dear Kotu,

Since it has enteric coated form most probably it will require semi or fully replicate design but to decide it better to perform a pilot study with 18 sub at least to have a meaningful results. as per literature sources ISCV >30% :confused:

Edit: Full quote removed. Please delete everything from the text of the original poster which is not necessary in understanding your answer; see also this post! [Helmut]

Helmut
★★★

Vienna, Austria,
2015-10-23 15:09
(3099 d 18:54 ago)

@ komodo
Posting: # 15579
Views: 7,285

Generic of an extremely HVDP possible?

Post reply

Hi komodo & balakotu,

❝ […] it will require semi or fully replicate design but to decide it better to perform a pilot study with 18 sub at least to have a meaningful results. as per literature sources ISCV >30% :confused:

>30% is correct; see this post: C_max ~200%, AUC ~300%!
Applying the EMA’s ABEL-method for C_max, CV 200%, GMR 0.90, power 80%, 4-period full replicate:

library(PowerTOST) sampleN.scABEL(CV=2, theta0=0.9, targetpower=0.8, design="2x2x4", details=FALSE) +++++++++++ scaled (widened) ABEL +++++++++++ Sample size estimation --------------------------------------------- Study design: 2x2x4 (full replicate) log-transformed data (multiplicative model) 1e+05 studies for each step simulated. alpha = 0.05, target power = 0.8 CVw(T) = 2; CVw(R) = 2 Null (true) ratio = 0.9 ABE limits / PE constraints = 0.8 ... 1.25 Regulatory settings: EMA Sample size n power 156 0.8001

In Europe generally it is not acceptable to scale AUC. That would mean for a CV of 300%:

sampleN.TOST(CV=3, theta0=0.9, targetpower=0.8, design="2x2x4", details=FALSE) +++++++++++ Equivalence test - TOST +++++++++++ Sample size estimation ----------------------------------------------- Study design: 2x2x4 replicate crossover log-transformed data (multiplicative model) alpha = 0.05, target power = 0.8 BE margins = 0.8 ... 1.25 Null (true) ratio = 0.9, CV = 3 Sample size (total) n power 1028 0.800468

However, the MR-GL does allow reference-scaling for partial AUCs. I would not dare to walk that road without a scientific advice. Yet:

sampleN.scABEL(CV=3, theta0=0.9, targetpower=0.8, design="2x2x4", details=FALSE) +++++++++++ scaled (widened) ABEL +++++++++++ Sample size estimation --------------------------------------------- Study design: 2x2x4 (full replicate) log-transformed data (multiplicative model) 1e+05 studies for each step simulated. alpha = 0.05, target power = 0.8 CVw(T) = 3; CVw(R) = 3 Null (true) ratio = 0.9 ABE limits / PE constraints = 0.8 ... 1.25 Regulatory settings: EMA Sample size n power 224 0.8016

IMHO, a pilot study in 18 subjects is just a waste of time & money. For a product with such a high variability you don’t get any meaningful information out of a small study. Let’s assume that the true CV is 300% and you run a 4-period full replicate in 18 subjects. The 95% CI of the CV is:

round(100*CVCL(CV=3, df=3*18-4, side="2-sided", alpha=0.05), 0) lower CL upper CL 203 565

Another issue is that the point estimate of HVDPs “jumps around” between studies. Let’s assume that you were extremely lucky and found a GMR of 1 in the pilot. You could calculate a 80% CI (i.e., accepting a 20% risk that the true value lies outside):

round(CI.BE(alpha=0.2, pe=1, CV=3, n=18, design="2x2x4"), 4) lower upper 0.7382 1.3547

I’m asking myself whether it is possible to show BE for such a HVDP at all. Maybe therapeutic equivalence is a better option?

—
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

nobody nothing 2015-10-23 16:46 (3099 d 17:17 ago) @ Helmut Posting: # 15580 Views: 7,186	Generic of an extremely HVDP possible? Post reply
	Hi! http://onlinelibrary.wiley.com/doi/10.1111/j.1365-2036.2005.02442.x/full http://www.surreyandsussex.nhs.uk/wp-content/uploads/2013/04/UKMi-Oral-Mesalazine-Bioequivalence.doc Have fun! — Kindest regards, nobody