Aeri Park: Hello. My name is Aeri Park. I am a Director of US Operations in Almac Group in the US, providing all the services for your blinded material, which is over-encapsulated products, how to perform the analytical testing, why we have to perform the analytical testing and what type of testing that's required
So, I will talk about all of this today. But, first, when you talk about blinded material, obviously, that's over-encapsulated material, the key considerations we have to consider are, first of all, the true product because there are more than one types of manufacturers for the same drug products and different sizes and shapes
Because they have to go into another capsule shell, size and shape can be important, impacting the size of the final capsule shell you have to put in, and also amount of excipients you have to fill in as a backfill. And also, you have to consider the type of excipient because that may impact performance of your blinded products
The capsule shell is obviously also very important, and we will talk about a little more of this later
Now, analytical data is very important because your study results have to have the right test to make sure you have the right placebo that's labeled as placebo and the active is right active and the right amount of active if you're using multiple potencies
Now, today, we'll mostly talk about oral dosage forms. But, you know, same principle can be applied to many different variety of products, which I'll have some examples of that later during the presentation
So, there are just two pictures here. If you look at the top picture, it shows some tablets and some of the over-encapsulated products and some capsules
So, when you first blind your product, either it's tablet or capsule, putting into another big capsule and fill it with the backfill, the most important testing to be performed are listed here. It's identity, because you have to make sure the placebo is indeed just a placebo, active contains your product, potency because if you have a multiple strength of the product you are blinding, you have to make sure the potencies are correctly prepared
Now, the most important test for all blinded products is performance. Because you have--even though you have taken commercial product, the commercial product are now inside another capsule with another backfill. So, you don't know if this tablet or capsule will now perform exactly same way as intended as the original commercial product
That's why performance is important, and that is tested by something called dissolution testing. And we'll talk about that in detail later
Now, if you look at the bottom picture - so, all these over-encapsulated blinded products are put into a packaging. The picture shows example of a blister packaging. That's put into another box
So, once it's packaged, either blisters or bottles--again, identity has to be checked, make sure the right placebos and right potencies and right products is in the product, in the blister package or bottles
Now, now it comes shelf life--the original commercial product we purchased to blind may have its own shelf life. But, now we have taken it, put it into another capsule, filled it with a backfill, and then packaged it again differently. So, new shelf life has to be determined, and this is determined by something we call stability testing
And so, during the duration of clinical trials, stability testing needs to be performed to ensure these products, these blinded products are still safe and okay to use
Here, it's a very simple scheme showing how these products are tested at different time points. So, if you think about the very simplistic view, initial--very initial point, the original commercial products--let's say it's tablet, it's over-encapsulated, that’s the first blinding step
Once it's over-encapsulated, you have these bulk products of capsules. Now, this is a good point to do the testing, and I'll explain to that in a few minutes
So, these bulk products can be tested for ID. That's identification, make sure there's a right product in it, placebo's a placebo, there's only backfill in it obviously for placebos, assay and impurity--assay is for testing for potency, impurity obviously important for later. I will talk about why impurity is important
Dissolution--I talked about the performance, make sure that blinding did not alter any of the performance of the original product. And microbiology - this is to ensure that there's no microbial problems with over-encapsulated products
So, once all the testing is performed, certificate of analysis will be issued--that's a C of A in the slides--so that the product can be now released for the next step. Either it can go directly to the clinic if it's a bulk product that's released or prescribed to the patients, or it can be packaged into various configurations
So, for example, as the slide shows, if it's packaged into blisters or bottles--the reason it's good to have all the bulk products tested before it's blistered or bottled is because, most of the time in the clinical trials, blistering and bottling is done many different configurations. So, you will have blisters with one or two products in it, maybe seven or eight depending on one week supply, one month supply, it may be a one day supply. Same thing with the bottles - many different variety of counts are placed into the bottles
So, if you bottle it blister first and then try to do complete release testing, we might have to test same product ten times. So, it's better to test in bulk. And then, once it's blistered or bottled, just to do the stability testing and the identification testing
Obviously, stability is important for the shelf life determination, but simple identification testing will tell us, yes, we have the right product into the right blisters or right columns of the blisters
And then, individual blisters and bottles can go to the next step. That's the final part of this slide. Blisters can put it into columns or rows in a kit, in a wallet, or different bottles can go into another bigger box to make it a one week supply or a one month supply
Again, identification testing can be performed to ensure the right products are placed into the right location as is intentional--originally intended
As shown here, the stability testing is normally performed on the initial blisters and bottles because that is the point you want to ensure that products are stable. Once it's done into secondary [unintelligible] kits, you don't have to have a stability testing because product's not impacted in any other way
So, as you can imagine, you can have as many as three different types of certificate of analysis, depending on how your products are designed and how your products are packaged. Obviously, if you have only one blister packaging type, we can do all of the release testing such as ID, assay dissolution, microbiology, all on the single blister package
So, I talked about different analytical testing. So, there are basically three big steps that we have to think about. The first is obviously method
Each [unintelligible] products, commercial products have a unique component, unique drugs inside, active components. And therefore, they have to have a unique analytical method that's designed for their specific product. So, we need to have a method
Second one is reference standards. Without the reference standards, we will not know, we will not have anything to compare against. And then, finally, stability studies are required for determining shelf life
So, first, let's talk about the analytical methods. There are many variety of sources that we can find analytical methods for the commercial products. The most common is pharmacopeia. Most commonly--this slides shows US pharmacopeia, normally called USP, or British pharmacopeia has a lot of commercial products that compendium methods already listed there
Oftentimes, though, many of the commercial products that customer wishes to use it as a competitor testing, the products do not have any compendium method because it's so new and there are no genetic products available, so obviously, no compendium methods available. Often, we can find published articles that describes how those products are tested
In addition, every commercial product in the United States already have dissolution methods available in the FDA dissolution database. It describes the medium dissolution method, the time points and when to test it. So, all these are listed in detail
If none of the methods are available, it is possible to develop the methods from scratch to a full method development. So, all of these choices are available
Now, where do you find your reference standard? Again, pharmacopeia, so this USP is the biggest source of reference standard samples. If USP does not have it available, there are many commercial sources available. You can purchase them
Many API suppliers will--happy to sell you five or ten grams of reference standards, or Sigma Aldrich will supply them, as well
In rare cases, we may not be able to find reference standards from any sources because the product is so new to the market. In that case, it is possible to use the commercial product as a reference product and then use that to test all of the blinded product
Obviously, it's a lot more difficult to do so, but it is possible to perform that way
Now, this slide shows a very simple pictorial showing the flow of how analytical test is done such as assays or impurities for those of you who may not be familiar with analytical testing. So, we start with packaged product, remove the products from the packaging, and they are ground with normal [unintelligible]
Once they are completely pulverized [sp] into a white powder, we dissolve it completely and then analyze it, normally instrument called HPLC, and that stands for High Performance Liquid Chromatography. So, this instrument will tell us identity of the drug, how much of drug is in it--so, in other words, potency--as well as all of the impurities that might be present in the product
Now, analytical methods--let's say we have taken the methods from a compendium method such as USP. The compendium method's already validated. However, we still have to do some additional validation
The reason is we are not dealing with original commercial products. We are dealing with blinded product, which is over-encapsulated with a capsule present and with additional backfill in it. So, that might interfere with the analysis itself. So, we have to do some specificity validation
And sometimes, the color of the shell can impact the analytical method, so that has to be also taken into consideration. So, minimum specificity has to be tested and validated for individual existing methods
Now, let me talk about the dissolution testing. I talked about performance of the blinded products, the over-encapsulated products. So, this is how we do the dissolution testing
So, the over-encapsulated products are removed from the packaging, and that's placed into an equipment called dissolution bath. And that's shown on the slide on the right
And normally, we put it into six different identical vessels. It's filled with about a liter of a medium. Normally, it's water or acidic media, depending on how the drug is developed, dissolved in the body
And then, when we stir them or whatever method that's required or specified in the compendium method, the samples are pulled at specific time points - say 15 minutes, 30 minutes, 45 minutes or two hours, depending on the product, and that those pulled samples are again analyzed by HPLC to determine how much is drug is dissolved in the dissolution media within a specified time
There are two normal dissolution apparatus [sp] used for blinded product testing. The one on the left is apparatus one. The one on the right is apparatus two
So, if you look at apparatus two, that's just showing a paddle in the middle. That's the metal piece. And then, it's just sitting inside a round dissolution bath
The dissolution bath is filled with up to the rim almost a liter of the liquid, normally water. And then, as you can see, there's a pink tablet on the bottom, and as the paddle stirs, the tablet dissolves into the dissolution media, and then it releases the drug. And that's how we test, make sure the tablet is dissolving properly, depending on the different product, obviously, different speed and different media is determined
The one on the left is normally used for capsules because tablet, when you put it into the liquid, it sinks to the bottom. Capsules will float
So, if something has to hold a capsule--so, instead of using the paddles, we'll put it into a basket. So, the picture, if you can imagine, this basket is on the place of the paddle on the right inside dissolution bath. So, the capsule is kept inside a basket, and the basket itself is rotating to help to dissolve the drug product inside
Now, if you imagine your blinded product, most of the blinded products start with a tablet. So, the USP method, compendium method will be apparatus two, which requires the paddle
But, because it is a capsule now, you put it into another capsule with a backfill, it will float to the top. So, to be able to use the same apparatus that's in the compendium method, we will use something called sinkers [sp]
So, this slide shows on the bottom right hand slide various types of spiral sinkers and thongs [sp] that holds down the tablet or the capsules to the bottom of the vessel, so when the paddle's spinning, you have your product on the bottom. So, eventually, the capsule will disintegrate and the backfill will dissipate, and then your tablet will be exposed to dissolve inside the vessel
Now, if you already have capsules starting as a commercial product, then you make a blinded product, obviously, you'll be using the same basket. So, in the picture in the slide, there are various types of baskets. They can be used for different various products
So, to continue this talk about the dissolution techniques, the reason dissolution is such an important technique for determining the performance of your blinded product is shown on this slide. Because you have taken the commercial product and put it inside another capsule shell with a backfill, that oftentimes delay the dissolution
So, if your over-encapsulated product dissolves slower than the original commercial product, you may have a failure and you may have questions with the bio equivalence. So, because of that, oftentimes, we will do comparative dissolution, which I'll talk about in the next slides
So, in this slide, there is a very nice diagram of dissolution profile. So, if you look at the X axis, that's the time points. The Y axis shows percent dissolved. So, the dissolution results are shown from zero all the way to the 100 percent
And the dark blue line on the top, that profile is the original commercial tablet. So, it's dissolving, as you can see, about 60 minutes, about 70 percent dissolved, at 120 minutes, it's over 80 percent dissolved
The pink line on the bottom is over-encapsulated tablets. So, that's your blinded material. As you can see already immediately, the pink line is much lower in terms of dissolution than the commercial product so that you already have delayed dissolution
So, the question is, is this a bioequivalent. And when we test that, we answer that question is this a bioequivalent by calculating something called similarity factor. That's shown on this slide
So, in order to calculate similarity factor, we perform the dissolution with [unintelligible] 12. That means you perform the dissolution of 12 original tablets, original product, and 12 of the blinded over-encapsulated product
And after the dissolution testing is completed, something called similarity factor is calculated, the equations are shown here. And if the answer is between 50 to 100, that indicates two products are similar, and that passes the similarity factor, that means the over-encapsulated products are performing similarly to the commercial products. So, it can be released to the clinic
Now, here is an example, again showing two dissolution profiles with original tablet, and then the pink line on the bottom is the over-encapsulated blinded product
As we can see, the pink line is not dissolving very well at all. So, if you look at time points such as 40, 40 minutes, about 40 and 50 minutes, the original product dissolves almost 100 percent whereas the over-encapsulated product, the pink line is dissolved only about 60 percent
The reason is obvious. If you look at the picture on the right shows bottom of dissolution vessel
So, what this is shown is that the capsule that's outside has already disintegrated. But, inside the capsule, you have a backfill, which is normally excipient
Now, most excipient used for backfill are polymers. So, they're not water soluble
So, if you have very small tablet and use large quantities of backfill, the backfill will sit right on top of your tablet, and that's what we call coning [sp]. When it's coning, no matter how much the paddle is spinning above it, the excipient might be just happily sit there on top of your tablet. And when that happens, the drug is not released because it's covered inside a mound of your backfill, which is the polymer excipient
So, as you can see from the graph from the dissolution profiles that the over-encapsulated product is very slowly dissolving. Even after almost between 40 and 50 minutes, it's really released about 60 percent. And only after 60 minutes, it's released more than 80 percent
So, let's assume if this product specification was 80 percent dissolved after 60 minutes, this product will pass. The over-encapsulated product will also pass the specification. But, this will fail the similarity factor
That's why it's important to know, not only meeting the specification of dissolution percent dissolved, but the two different profiles of the unmodified product and the blinded product has to have a similar dissolution profile to pass it. That's why similarity factor, which is done by comparative dissolution, and normal specification of how much to dissolve have to both pass
Now--so, what do you do if this happens to your own product? Well, there are two ways to solve this problem. Obviously, the easiest way is change your backfill
If you change to different excipient, oftentimes, finer smaller particles will dissipate far easier, and that will solve the problem. However, oftentimes, it might be too late to change excipient because the product may have been already manufactured. In that case, we'll have to modify the dissolution method
So, once the dissolution method is modified, it has to be validated. And then, comparative dissolution has to be repeated against a modified, the commercial product, and the blinded material using the identical modified method to show that the similarity factor is passing and everything is dissolving in a similar way
The next slide shows a different kind of problem. It's something called cross-linking
Because over-encapsulation is normally happening with a hard gelatin capsule, the gelatin material can, over time, cross link and becomes very hard to disintegrate. Normal gelatin capsule will disintegrate in water in about five minutes
When they cross-link, they may not want to disintegrate at all and might hold onto it for a very long time, which will cause failure on the dissolution testing
The reason it's happening is because, sometimes, your product, your product, commercial product itself, or the backfill might react with gelatin capsule because they are not compatible, and that might cause cross-linking. Oftentimes, the true product tablets that are coated with the various materials, the coating can cause cross-linking of the gelatin capsules. And sometimes, the solubility is decreased because of the storage at high temperature and high humidity
So, if you look at the right hand side picture, again, this is showing a bottom of the dissolution vessel, and you can see there's a pink capsule--no, it's blue capsules inside, not pink, blue capsules inside. And as you can see, the capsule is held up by a spiral stainless steel sinker. So, you can see the sinker on the picture
Now, normally, when you put the capsules in the media, within five minutes, capsules will disintegrate, and then the--you will immediately see the backfill and the tablets inside
In this case, even after long time of storing, instead of capsules disintegrating, it absorbs media and becomes bigger and bigger and turns into a big sponge. And then, it doesn't release the product
Now, that's evident from the left hand side where the dissolution profile is shown. Again, X axis is tie [sp], Y axis is percent dissolved. The dark blue line on the top is a tablet. And it's dissolved about, after 30 minutes, almost 100 percent dissolved
And then, the red line under it is the blinded material, which is over-encapsulated tablet. And that gives a very good profile, as well - at 30 minutes, close to 100 percent is dissolved, about 90 percent dissolved. So, it looks really good
But, if you look at the bottom graph, which is green, that's your blinded product, over-encapsulated product. After one month, that's one--M stands as one month--40/75--we'll talk about the stability study later, but 40/75 indicates it was stored for one month at 40 degrees C, 75 percent humidity
So, after one month, as you can see the dissolution profile, for 30, first 30 minutes, no drugs dissolved. Obviously, the capsule shell is expanding, expanding. It's not releasing any of the drug
And then, about 45 minutes, you see a little bit of drug is dissolved, about 30 percent dissolved. And 60 minutes, another 40 percent is dissolved
Obviously, if this happens, this product will fail after one month on stability
So, when this happens, there are other ways to overcome it. USP allows two different types of enzymes to be used to basically digest the capsule shells when it's cross-linked and not dissolving, and those are pepsin and pancreatic
So, depending on the PH of the dissolution media, you can choose one of the enzymes to help digest the capsule shells because those enzymes are obviously present in our body. And so, you can successfully complete the dissolution testing during stability studies
So, we've been talking about the stability and some additional things that we have to think about, because every over-encapsulated blinded product has to be placed on the stability study to determine the new shelf life. Again, we have to think about excipient interactions and the capsule shell itself because these two can have a big impact on the stability of a blinded material
Excipients are normally selected by what's already in the tablet. So, if the tablet contains specific excipient, normally, that same excipient is selected for over-encapsulation. However, that doesn't always guarantee the stability. Sometimes, additional excipient can impact the stability of the product
Now, capsule shells - the biggest drawback of capsule shells is that it has 11 percent moisture. So, if the true product is very moisture sensitive, they can interact with the capsule shell and interfere with the stability and even increase the degradation rate. And sometimes, capsule shell itself, the material itself may not be comparable with the API itself
So, there are different types of capsule shells. Instead of gelatin capsule shells, there are vegetable capsule shells with a different moisture content
Or sometimes, a customer will overcome the moisture problems by adding additional drying cylinders inside containers such as [unintelligible] into the bottles to avoid having API degradation
So, to perform the stability study, we normally advise to place not only your modified, the over-encapsulated blinded products into the stability, but also put the original commercial product in its original packaging in the same condition and the placebo products. The reason you want to do that is, sometimes, your blinded product may fail stability studies, but it may not be because of blinding itself. It might be because the original product is unstable
So, you want to always eliminate the question why it's failing. Maybe it's original question. So, that has to be always done concurrently
You don't have to test both products at every time point, but have it available so that if your blinded material fails the stability study, then you can go back to the original commercial product that's placed in the same condition and analyze that to see where the failure came from
Obviously, you want to test placebo even though we are only doing visual testing for placebo because you don't want to have placebo inactive [sp] changing to different colors for any blinded studies
Now, if you have a multiple strength, because a lot of clinical trials will have more than three to five strengths tested for blinding test, then bracketing can be used as long as the formulation is consistent between the low strengths to high strength
Some of the delayed release or the extended release tablets, we may not be able to do bracketing studies because of different strength may have a quite different formulations. So, all of them may have to be tested for stability
And I've listed four different conditions, and these are very common conditions for stability studies. So, for example, for North America and most of Europe, the normal storage conditions are climactic zone two, that's 25 degrees C, 60 percent RH
So, the product will be placed in that stability condition to monitor during the duration of our clinical trials. At the same time, products are placed in something called accelerated conditions. That’s on the bottom list. That's 40 degrees C, 75 percent RH
So, depending on your climactic zone, you have your zone temperature and then the accelerated conditions
So, there is more details of how the stability study is done on this current slide, and it shows all the different time points. So, this is example of North America and most of Europe where the climactic zone is two. So, our standard condition is 25 degrees C, 60 percent RH
The testing frequency is--required is every three months up to one year--so, it's three, six, nine, 12 months--and then every six months after two years--so, 12, 18, 24. And after that, it's annual testing if it's required to be stored longer
And then, on the bottom, there's accelerated condition. That's 40 degrees C, 75 percent humidity. And that's tested only up to six months
Now, normally, it's three months and six months testing, but most customers prefer testing at one month because one month data gives you a lot of information how stable this product would be
We also recommend putting samples in 30 degrees C, 65 percent RH. The reason is because some products might be unstable at 40 but might be stable at 30. So, if it fails at 40 degrees C, accelerated conditions, we test up to one year at 30 degrees C, 65 percent humidity to confirm--to have that as accelerated conditions
Obviously, if the commercial product is stored at refrigerated conditions, then refrigerated condition would be the long term and 25 degrees C, 60 percent will be the accelerated. So, as you can see, depending on where the current drug storage condition is, we have to determine what the accelerated condition is
So, we talked about the stability study. So, what do we do at each time point? The stability testing time point, the very important first thing, visual inspection. We make sure the capsules didn't change in color, shape, the backfill didn't discolor it and the tablets inside didn't change visually
And then, what's the point of doing stability testing? It's because you want to make sure the product is stable over the period of time
Therefore, we always do assay. That's to determine the potency, so the drug's not decreasing in potency, and the related substances. That's to determine that impurity's not increasing
If the impurity's increasing above and beyond over what's specified for the product to be acceptable, if there is increase, that means the stability study's over. You can no longer use that sample. And that will determine the shelf life of that sample as up to that point
Obviously, dissolution testing has to be always included because dissolution testing determines--ensures that the blinded over-encapsulated products are not changing in terms of performance during the storage, during the duration of your shelf life and the clinical trials
Now, moisture is tested on some of the products, especially if you know this commercial product is moisture sensitive. Then, moisture may be tested at each time point, make sure that there is no change of the true product and no moisture is taken in from the environment
So, if I summarize all the process that we discussed today, the very first step for performing all of the analytical testing for the blinded products is analytical methods, either from literature, compendium method, whichever source have to have analytical method. And then, secondly, we need to have a reference standard material. So, I talked about where to get those reference standard materials
And also, there is some developing analytical methods, some validation is always involved because it's over-encapsulated product. Therefore, it's not the same as a commercial product, so compendium method cannot be used verbatim. It has to be always validated, make sure it works for these modified blinded product, as well
Now, comparative dissolution - I talked about how important it is to determine the performance did not change and to confirm the blinded products, the over-encapsulated products are bio equivalent to the commercial product, we have to perform the comparative dissolution
Finally, stability study we discussed because during the duration of your clinical trials, you want to make sure that you have sufficient shelf life to use the same lot, same lot of product continuously
Now, I will talk about, something about the timelines. As you can imagine, all these analytical methods, validations, some upfront work, we like to have at least three months of stability data before starting the clinical trials because you don't want to have any surprises on your huge clinical batch and have an unexpected failure
So, it is a very common practice to make a very small batch of stability batch just to solely purpose of testing for stability data only. So, it's a fairly small batch, even though it's manufactured identical way as a clinical batch would. So, you do that ahead of time and obtain three month stability data, and then that gives the confidence that the clinical batch would go fairly well and you'll have no surprises or problems during the clinical trials
So, to discuss clinical trial materials, this means you have to start the discussion at least six months before that because you want to have at least three months stability data
Now, I will briefly talk about different types of testing required at each different time point. So, first, let's talk about release testing, what type of testing do we have to do
For over-encapsulated material, obviously, you need to have a specification indicating what is a pass fail limit. Comparative dissolution data is important for the release testing. That's most important. That's the minimum important you need to have, absolute minimum
In addition to that, oftentimes, assay and related substance are included into the release testing. The reason is because you want to compare the data to the stability data later
Appearance, obviously, is always included, and at the end, a certificate of analysis released to release a product into the clinic
I have an example of a placebo inhaler devices because, you know, inhaler devices are often tested, but placebo is not often tested. So, I'd like to talk about it a little bit because it is important to test placebos
Obviously, same story - you need to have analytical method. And specification has to be set
Now, the placebo devices can be tested in two different ways. We can test disassembled device, or we can actually test the immediate dose. The reason is we want to make sure there is no active present in the placebo device, and the certificate of analysis is issued
Now, wallets [sp] will have been already tested before it's put into wallets, either it's in a blister stage or bulk stage. But, once put it into wallets, it's oftentimes very important to do additional ID testing, that's identification testing. The reason is wallet designs are very oftentimes complex, and you want to make sure the right dose and right product is in the right column or right row, because sometimes, you'll have different strength or active and placebo mixed in the same wallet cards
So, obviously, method, specification has to be all present before that
Assay method - that's to determine strength if you have different doses inside same wallet cards. And certificate of analysis will be issued
So, I have next slide an example of a wallet. This is a fairly extreme case that we have. But, as you can see, there is a morning column and the evening column. And there are various different strength put into the wallet cards
So, if you have different strength, unless individual capsules can be opened and we can identify it by looking at visually what strength of tablets they're in--sometimes, we can focal measure products--we have to do actual assay testing to determine the right product is in the right location of the wallet card
I have two case studies, just to give you a little bit of flavor for how this clinical trial product manufacturing goes from the beginning to the point of clinical batch production begins
So, in this first case study one, we studied discussion and planning--obviously, month one from the beginning. And then, month two, we did a feasibility study. What does a feasibility study mean? We don't know if this commercial product can be put into certain capsules, and then what type of excipients do you use, and will it meet the dissolution parameters, will it pass the performance testing
So, to do all of that, we did initial feasibility study. To do that, it's very simple. You make man encapsulations in the lab. You can make 50 to 100 blinded products by hand. And then, we will test them to make sure performance is not impacted. You can even test various different excipients, make sure you can select the right excipient. You can use the same capsules for validation studies
Once that study's done, obviously, we already know what capsules to use, what excipient to use. So, month three, stability batch can be produced. That stability batch is that the over-capsulated product that's put into either bottles or some type of blister packages
While the stability batch is under production, then analytical lab will perform validation studies to make sure this over-encapsulated--over-encapsulation process is not impacting actual analytical test, and then the methods are also specific for the product
Month four, the stability batch production was completed. So, we were able to put all of the products into the stability conditions on the various conditions
Now, in this case, we only did up to six months stability studies. It's depending on the customer. Some customers wish to do full 24 month stability study, even on the stability batch, not on the clinical batch, but the stability batch, because it always gives them three months data before they get the data for the clinical batch. So, it gives a nice advanced notice if something might go wrong
However, some customers have to do a short term stability study on stability batch, and in this case, we did actually three months stability studies with a six months as optional. If we see something funny or something concerned at three months, we might do another six months poll
The next follow month, month five, we did a one month stability testing. Everything looked okay. And then, so since everything looked good, clinical batch production was scheduled
And then, month seven, we were able to do three months stability testing. Now, remember this is both conditions, 25 degrees C, 60 percent RH, which is normal conditions, and the accelerated conditions, that's 40 degrees C, 75 percent RH
So, at both conditions, we test at three months, and that gave confidence to the customer to give a green light to start the clinical batch production
So, the whole process took about seven months to begin the production
Now, next, this is the final slide for case study, second case study. This one was a little bit shorter because we took a little bit of risk
So, you can see from these timelines that it is possible to even make the timeline even shorter, depending on how much risk you want to--you're willing to take
So, at first month, we started discussion and the planning of the analytical testing. At month two, we studied dissolution testing and then start validating all the methods
But, at the same time, stability batch production began. So, stability batch production started before we confirmed that this product will have possible or acceptable performance once we blinded, because that was assumed that it'll work
And so, month three, as soon as stability batch was produced, we started stability studies. Now, this case, we had 24 month stability study
Month four--so, by that time, month four arrived, we had all of the methods validated. So, we did T Zero [sp] testing, which is initial testing, and one month testing all together at month four using the stability batch
So, obviously, one month testing is from the samples that already in stability condition, the accelerated condition. T Zero testing is the samples, the original samples that we have not put it into the stability conditions yet
Obviously, we can do this for various reasons. First of all, we knew that the customer's taking the risk because the timeline was shorter. And secondly, this is a stability batch, not the clinical batch. Therefore, we can test times zero point and one month point at the same time
Now, one month data was good. There was nothing concerning. And then, six months time point, we were able to perform three month stability testing so that clinical batch production was able to start at the end of six months
Now, it is possible for some customers to skip stability batch production entirely. There are multiple ways--multiple reasons why you can do that
Obviously, one, sometimes, the timeline is so tight, because you only have two months to discuss and you don't have time to make stability batches and clinical trial batches. However, because companies like us, if you come to service companies like us, because we have performed hundreds of stability studies in the past, we might have already performed stability study on the same commercial product that you are wishing to test
It may not be the same manufacturers, but it might be the same product. And therefore, we might have already advanced knowledge or information to tell you that, yes, we have test this product with this configuration and it was stable up to two years. And that might give you confidence, even though you have very little time, to start immediately, to start clinical batch production without going through all the stability batch production
In some cases, some products are known to be very, very stable. And those cases, oftentimes, customers will skip stability batch production and go straight to the clinical batch production
So, today, I talked about all the important points of testing, blinded, over-encapsulated clinical products. So, those testing requirements, you have to have a method. And I talked about how to get those method
And I also talked about what type of parameters have to be validated at minimum. And I talked about how to get the reference standard materials and talked about importance of performance testing using dissolution and comparative dissolutions and also talked about some of the issues that we have encountered during the dissolution and how you can overcome that and make improvements
And finally, I talked about the stability testing, the importance of it and what type of things that has to be tested for stability studies
And thank you for your time, and if you have any questions, please feel free to contact any of us Almac. Thank you. Have a good day.