The invention relates to the use of a plasma treated silicone oil layer as a coating for a medical injection device comprising a barrel and a stopper in a gliding engagement within the barrel, for limiting the number of particles released in a pharmaceutical composition contained in the injection device.
Medical injection devices that comprise a sealing stopper in a gliding engagement within a container are widely used to deliver drug by injection to a patient.
Such injection devices include syringes, cartridges but also auto-injectors.
Many different types of injection devices have been designed for administering medicines. Injection devices usually comprise a container intended to receive the product to be injected and a plunger rod intended to move a stopper within the container so as to expel the product therefrom at the time of injection. Empty and pre-filled disposable injection devices exist but prefilled devices are now preferred because they are more convenient, safe and efficient and may be used directly in emergency cases.
Such injection devices would be appropriate for containing the new high-value drugs that are commonly named “biotech” drugs, and that are currently developed and launched on the pharmaceutical market.
These biotech drugs are made out of living cell cultures, instead of the simple molecules used to create traditional pharmaceuticals, and can comprise for example biological elements such as proteins, peptides, DNA, RNA and the like, as well as sensitive drugs.
A major constraint with such drugs is their sensitivity towards their environment and therefore there is a need to find an appropriate container able to maintain the integrity of the drugs when they are stored for a long time in injections devices.
Traditional injections devices comprise a container made of glass or plastic and a stopper made of rubber.
Optionally, coatings can be applied on the surface of the container and/or on the surface of the stopper in order to improve the lubrication of the injection device.
But in some cases, it has been shown that such injections devices are not appropriate for long storage of high-value drugs due to the high and long interaction with their containers.
Indeed, it has been shown that some degradations of the drug (aggregation, denaturing, etc. . . . ) occur with time, leading to the rejection of the prefilled device and therefore leading to a high loss for pharmaceutical companies.
Therefore there is a need to have a prefilled injection device having a medical container compatible with biotech drugs, meaning a container that avoids any denaturing and/or aggregation of the drug.
Besides, such prefilled injection devices should also have good gliding properties i.e. a low gliding force to move the stopper within the container.
Moreover, if a coating is applied on the surface of the prefilled injection device, the integrity of the coating layer has to be maintained from the deposition of the layer on the surface(s) of the medical device until the injection of the drug to the patient.
It means that any delaminating or breaking phenomena of the layer are to be avoided.
This is particularly the case for lubrication layers that should be required to enhance the gliding properties of the injection devices.
Finally, the integrity of the drug, the integrity of the coating and the gliding properties of the prefilled device need to be maintained over time i.e. to be stable for at least the shelf life of the prefilled injection device.
Some documents such as U.S. Pat. No. 5,338,312 and EP 0 201 915 describe an injection device having enhanced gliding properties by using a lubricant layer that is crosslinked in order to immobilize the layer on the surface of the container of the injection device.
However, said former injection devices were not necessarily compatible with sensitive drugs such as biotech drugs and/or vaccines.
Besides, these documents do not address the issue of providing a coating that would keep its integrity within time and that would not have any, or at least any significant or adverse, interaction with the drug contained inside the injection device.
The document EP 1 060 031 describes a lubricated medical container that exhibits good gliding properties as well as low protein adsorption on the inner surface of the container.
Nevertheless, this document does not disclose any coating compatible with sensitive drugs such as vaccines and/or biotech drugs.
Indeed, as the coating described is not directed to be used with high-value drugs, even if the adsorption may be avoided, some denaturing of the drugs could occur.
This would be the case for example, with some polymers described in this document such as phosphorylcholine, 2-hydroxymethacrylate.
Additionally, this document is not directed to the integrity of the coating over time, after a long storage period.
However, the issue of storage is essential for prefilled syringes, as the coating needs to be stable over time not only before the filling of the drug in the injection device but also after the drug has been placed in the injection device.
Document U.S. Pat. No. 6,461,334 also addresses the problem of drug adsorption on the coating and provides either a silicone coating crosslinked by irradiation or a silicone copolymer coating rendered hydrophilic by a plasma treatment.
Alternatively, document JP 2005-160888 provides a polyparaxylylene coating on the stopper to avoid drug adsorption on the stopper.
Document WO 2011/092536 discloses a medical injection device comprising a barrel and a stopper in gliding engagement within the barrel, wherein the inner volume of the barrel is composed of a distal portion containing a drug and a proximal portion containing a propelling fluid, said distal and proximal portions having different surface conditions and the drug being isolated from the piston and the proximal region where it slides.
The surface conditions of said distal and proximal portions are thus able to address different objectives, which may be incompatible.
On the one hand, the distal portion may be coated with a coating suited for drug stability.
In particular, said coating may be a hydrophilic coating, e.g. a hydrophilic polymer, possibly covering a hydrophobic pre-coating, e.g. PDMS, so as to obtain a barrier effect.
On the other hand, the proximal portion may be coated with a coating suited for a smooth gliding of the stopper.
In particular, said coating may be made of plasma-treated silicone.
Due to the isolation between the distal and proximal portions of the barrel, the coating of the proximal portion cannot be in contact with the drug contained in the distal portion; said coating can thus be chosen among coatings that would be likely to interact with the drug.
Recently, a new problem was raised by specialists of biotech drugs, which is the presence of particles in the pharmaceutical composition that could appear after the filling of the container, due to interaction of the drug with the coating present on the inner walls.
Indeed, these specialists have observed that significant amounts of subvisible particles (i.e. particles having a size comprised between 0.1 μm and 100 μm), in particular protein aggregates, in the pharmaceutical solution may be hazardous for the patients and they thus recommend that the level of particles in this size range be carefully controlled.
One can refer in this respect to “Overlooking Subvisible Particles in Therapeutic Protein Products: Gaps That May Compromise Product Quality”, by John F. Carpenter et al., Journal of Pharmaceutical Sciences, Vol. 98, No 4, April 2009.
These recommendations result in more severe norms with regard to the maximum authorized particle level defined by the United States Pharmacopeia (USP 31 <788>) and the European Pharmacopeia (EP 6 <2.9.19>).
These norms not only place a heavy burden onto the pharmaceutical companies themselves but also onto the manufacturers of injection devices, since the release of particles from the containers into the pharmaceutical composition has to be avoided.
Document WO 2010/092536 discloses a pyrolyzing technique for forming a coating in a medical injection device in order to improve the gliding of the stopper.
However, this document does not address the above-mentioned problem of particles.
It is thus necessary to provide a medical injection device that exhibits a good compatibility with sensitive drugs stored inside for long time period in order to meet the pharmacopeia norms with regard to the level of particles in the drug, while still providing good performance with regard to the gliding of the stopper within the barrel, and where the lubrication layer keeps its integrity over time.
A goal of the invention is to provide such injection devices.
An object of the invention is the use of plasma treated silicone oil as a coating in a medical injection device comprising a barrel and a stopper in gliding engagement within the barrel, for limiting the number of particles present on the surface of the coating and for limiting the number of particles released in a pharmaceutical composition contained in the injection device.
At least part of the pharmaceutical composition contained in said medical injection device is in contact with said coating.
According to an advantageous embodiment of the invention, the coating consists of crosslinked silicone.
According to an advantageous embodiment of the invention, said use is for increasing the gliding force of the stopper within the barrel as compared to a medical injection device having a not plasma-treated silicone coating.
The thickness of the coating is advantageously comprised between 90 and 400 nm.
The gliding force of the stopper is comprised between 1 and 8 N, preferably between 1.5 and 6 N.
According to an embodiment of the invention, the barrel is made of glass.
According to an embodiment of the invention, the silicone oil consists of 900 to 1200-centistoke polydimethylsiloxane (PDMS), preferably 1000-centistoke polydimethylsiloxane.
According to an embodiment of the invention, the injection device is a syringe having an internal volume of 1 ml and a diameter of 6.35 mm.
According to an embodiment of the invention, the weight of the coating is of between 0.1 and 0.4 mg.
According to an embodiment of the invention, the injection device is a prefilled syringe.
According to an embodiment of the invention, the pharmaceutical composition contained in the injection device is a biotech drug.
A further object of the invention is a medical injection device having:
a barrel having an inner surface;
a stopper in gliding engagement with the barrel; and
a pharmaceutical composition within the medical injection device and in contact with the inner surface of the barrel, the inner surface of the barrel comprising a coating of plasma treated silicone oil in contact with the composition,
wherein the plasma treatment of silicone oil reduces the number of particles present on the surface of the coating and the number of particles released into the pharmaceutical composition contained in the medical injection device as compared to silicone oil that is not plasma treated.
According to advantageous embodiments of said device, that may be considered independently or in combination:
the particle level released in a solution contained within the medical injection device is less than 2.11 particles per mm2 of the barrel surface in contact with the solution when measured by light obscuration method;
the particle level released in a solution contained within the medical injection device is less than 10.56 particles per mm2 of the barrel surface in contact with the solution when measured by microflow imaging method;
said solution contained within the medical injection device is a mixture of Phosphate Buffered Saline and filtered Tween 80;
the stopper is coated with silicone oil;
the plasma treated silicone oil coating comprises a thickness between 90 and 400 nm;
the plasma treated silicone oil coating increases a gliding force for moving the stopper within the barrel;
a gliding force for moving the stopper within the barrel is between 1 and 8 N, more preferably said gliding force is between 1.5 and 6 N;
the barrel is made of glass;
the silicone oil comprises polydimethylsiloxane (PDMS);
the silicone oil comprises a viscosity between 900 and 1200 centistoke;
the medical injection device is a syringe having an internal volume of 1 mL and a diameter of 6.35 mm;
the plasma treated silicone oil coating comprises a weight between 0.1 and 0.4 mg;
the device is filled with said pharmaceutical composition to allow long term storage of the pharmaceutical composition meeting pharmacopeia norms with regard to the level of particles in the pharmaceutical composition;
the device comprises a biotech drug within the barrel;
the device comprises one or more of a protein, a peptide, a vaccine, DNA, or RNA within the barrel;
the particles present on the surface of the coating and/or the particles released into the pharmaceutical composition contained in the medical injection device have a size ranging between approximately 0.1 μm and 100 μm.
A further object of the invention is a method of treating a medical injection device, the device comprising a barrel having a coated inner surface, a stopper in gliding engagement with the barrel, and, comprising:
(1) coating the inner surface of the barrel with a layer of a silicone oil; and
(2) exposing the silicone oil layer to a plasma treatment, thereby reducing the number of particles present on a surface of the coating or the number of particles released into a pharmaceutical composition contained in the medical injection device when the pharmaceutical composition is in contact with the inner surface of the barrel, as compared to a device having a barrel coated with silicone oil that is not plasma treated.
A further object of the invention is a method of reducing a number of particles present on a surface of a coating or a number of particles released into a pharmaceutical composition contained in a medical injection device, the device comprising a barrel having a coated inner surface, a stopper in gliding engagement with the barrel, the pharmaceutical composition being in contact with the inner surface of the barrel, said method comprising, prior to disposing the pharmaceutical composition within the device, preparing the coating by:
(1) coating the inner surface of the barrel with a layer of a silicone oil; and
(2) exposing the silicone oil layer to a plasma treatment, thereby reducing the number of particles present on the inner surface of the coating or reducing the number of particles released into the pharmaceutical composition contained in the medical injection device as compared to a device comprising a barrel coated with silicone oil that is not plasma treated.
According to embodiments of either of those methods, that may be considered alone or in combination:
the stopper is coated with silicone oil and the silicone oil coated stopper is exposed to a plasma treatment;
the plasma treated silicone oil coating comprises a thickness between 90 and 400 nm;
the plasma treated silicone oil coating increases a gliding force for moving the stopper within the barrel;
the gliding force for moving the stopper within the barrel is between 1 and 8 N, preferably, said gliding force is between 1.5 and 6 N;
the barrel is made of glass;
the silicone oil comprises polydimethylsiloxane (PDMS);
the silicone oil comprises a viscosity between 900 and 1200 centistoke;
the pre-filled medical injection device is a syringe having an internal volume of 1 mL and a diameter of 6.35 mm;
the plasma treated silicone oil coating comprises a weight between 0.1 and 0.4 mg;
the device is filled with said pharmaceutical composition to allow long term storage of the pharmaceutical composition meeting pharmacopeia norms with regard to the level of particles in the pharmaceutical composition;
the composition within the device is a biotech drug;
the composition within the device is one or more of a protein, a peptide, a vaccine, DNA, or RNA;
the plasma treated silicone oil coating comprises a cross-linked silicone;
at least 90% of a surface of the inner surface of the barrel is coated with silicone oil;
the plasma is produced by radio-frequencies;
the plasma treatment comprises an oxidative plasma treatment performed under a mixture of oxygen and argon;
the particle level released in a solution contained within the medical injection device is less than 2.11 particles per mm2 of the barrel surface in contact with the solution when measured by light obscuration method;
the particle level released in a solution contained within the medical injection device is less than 10.56 particles per mm2 of the barrel surface in contact with the solution when measured by microflow imaging method;
preferably, said solution contained within the medical injection device is a mixture of Phosphate Buffered Saline and filtered Tween 80;
the particles present on the surface of the coating and/or the particles released into the pharmaceutical composition contained in the medical injection device have a size ranging between approximately 0.1 μm and 100 μm.
Other features and advantages of the invention will become apparent from the detailed description to follow, with reference to the appended drawings, in which:
Referring to
The container 2 of the injection device may be made of any kind of glass or plastics suitable for medical applications.
The stopper 3 may be made of any elastomeric material, e.g. rubber, butyl rubber, silicone rubber.
The container 2 and /or the stopper 3 may be laminated with any suitable coating e.g. hydrophilic, hydrophobic coating as well as fluorinated coating.
The stopper 3 may be adapted to be connected to a plunger rod of a syringe or of an injection pump, for example.
To that end, it includes any suitable connecting means, e.g. a threaded portion 31, etc.
The end 20 of the barrel 2 opposed to the stopper 3 may be adapted to be connected to a needle 4, a cap or a catheter, or may comprise a staked needle.
The inner wall 21 of the barrel 2 is coated with a lubricant layer 5, which is a plasma-treated silicone layer.
The formation of the coating 5 according to an embodiment of the invention preferably comprises, in a first step, coating the inner walls of the barrel with silicone oil.
According to a preferred embodiment of the invention, the lubricant layer is sprayed onto the interior wall of the barrel 2.
To that end, a device comprising one or several nozzles may be introduced in the barrel 2 and moved along the barrel so as to uniformly deposit a silicone layer onto the inner wall of the barrel.
In a second step, the method comprises the exposure of the silicone oil layer to a plasma treatment.
To that end, the lubricated container is placed in a plasma reactor and plasma is generated in the reactor.
Numerous plasma processes are possible to achieve the plasma treatment.
However, in a preferred embodiment, the plasma treatment would be an oxidative plasma realized for example, under a mixture of oxygen and argon, such as 15% to 30% of oxygen and 30% to 70% of argon, preferably 25% of oxygen and 75% of argon.
The plasma may be produced by radio-frequency (i.e. with a frequency from 10 to 20 MHz, preferably from 11 to 14 MHz), with a power ranging from 50 W to 300 W, preferably from 150 to 220 W and under a vacuum of 10-100 mTorr in absolute value.
The exposure time of the coating is typically chosen to be between 1 second and 60 seconds, preferably from 10 to 40 seconds.
It should be clear to the skilled person that such parameters would be selected depending on the plasma reactor geometry, the volume of the injection device the arrangement of the injection devices inside the plasma reactor, the lubricant layer thickness, etc. in order to have the appropriate treatment according to the equipment used but also to the objects to be treated.
As a result of the plasma treatment, the silicone of the coating is crosslinked.
According to a preferred embodiment, the lubricant layer 5 is a silicone layer such as a polydimethylsiloxane (PDMS).
The viscosity of the silicone layer can be preferably comprised between 900 and 1200 centistoke.
More preferably, the lubricant layer is a 1000-centistoke PDMS.
The lubricant layer is applied so as to coat the major part of the interior wall 21 of the barrel.
Preferably, the lubricant coating 5 covers at least 90% of the interior surface of the barrel 2.
Preferably, the lubricant coating 5 has a thickness comprised between 90 nm and 400 nm, preferably about 150 nm.
According to an advantageous embodiment of the invention, the stopper is also lubricated in order to further reduce the gliding force.
In a preferred example, the stopper is a rubber stopper covered by a Flurotec® barrier sold by West Pharmaceutical Services and further siliconized by PDMS DC-360.
Since the particles are induced by the interaction of the pharmaceutical composition 6 and the lubricant coating 5, there is a direct link between the number of particles and the surface area of the coating: the larger the surface of the coating is, the higher the amount of particles is.
It has been shown that with the coating according to an embodiment of the invention, the level of particles present in the solution 6 is below 2.11 particles by mm2 of lubricant coating surface when measured by HIAC and below 10.56 particles by mm2 of lubricant coating area when measured by MFI.
As shown on the enlarged view of
The first issue consists of silicone particles A (e.g. droplets) released into the pharmaceutical composition 6 and are thus present in the solution.
A second issue consists of aggregates or denatured drugs (referred to as B) that are present in the pharmaceutical solution 6 and that have been formed by the interaction of the pharmaceutical composition 6 and the silicone particles A.
A third issue consists of silicone particles (referred to as C) from the coating 5 that are released in the pharmaceutical solution 6 due to the mechanical friction of the stopper along the walls of the barrel.
With the plasma treated silicone layer according to an embodiment of the invention, the level of particles present on the surface of the coating is significantly reduced, which implies that the level of subvisible particles that may be released into the pharmaceutical composition or be in contact with the pharmaceutical composition during the life of the injection device is reduced.
As a consequence, the risk of aggregation of proteins in the solution itself, due to the adsorption generated at the silicone droplets, as well as the risk of adsorption of proteins at the surface of the barrel, are significantly reduced.
Therefore, the coating of the prefilled injection device remains stable over time meaning that no or no more aggregation neither denaturing of the drugs occur due to potential interaction with the coating present on the surface of the container.
Besides, since silicone particles are likely to be released in a very small amount into the pharmaceutical composition, they do not generate any background noise that would be detrimental to the monitoring of protein aggregation.
The coating in the medical container in accordance with an embodiment of the present invention also shows favorable mechanical properties. For example, no delaminating or break-up of the coating occurs under strong movement (from for example, transportation), as well as under dramatic changes in temperature. The coating remains attached to the barrel and no element is removed from it.
A further effect in accordance with an embodiment of the present invention is that the above-mentioned technical effects i.e. good gliding properties and favorable mechanical properties, remains stable during a long period of time, for example from 12 to 24 months.
This is particularly important when the prefilled medical container is stored in different conditions and positions, transport over long distances and then finally used to inject a pharmaceutical composition into a patient after a long period of storage after being filled.
Another advantage of an embodiment of the invention is that no further chemical species is introduced in the medical container, since the only chemical consists in a classic silicone oil, already used and authorized for such use.
This diminishes the risk of unpredictable side effects.
With a particle level below 2.11 particles/mm2 of surface of the barrel in contact with the drug if measured by HIAC and below 10.56 particles/mm2 of surface of the barrel in contact with the drug if measured by MFI, the obtained medical injection device fulfills the above-mentioned requirements, i.e. a high compatibility with vaccines and biotech drugs, good gliding performance, favorable mechanical properties and maintaining these properties over a long period of time (e.g. 12 to 24 months).
When comparing the amount of particles present in a container having plasma-treated silicone versus a similar container comprising a silicone oil coating that is not plasma-treated, the above values correspond respectively to a reduction of particles of at least 70% (when measured by HIAC) and of at least 90% (when measured by MFI).
The experimental protocols for these measurements are described in detail below.
In a preferred embodiment, the gliding force, i.e. the force required to move the stopper 3 in the barrel 2 is increased of 0.75 to 1.0 N as compared to a similar container comprising a not plasma-treated silicone oil lubricant.
Even if increasing the gliding force is usually strongly avoided by the skilled person, the applicant was able to correlate this increase, together with the dramatic decrease in term of particle level, with the expected properties of the medical injection device.
As a consequence, the medical injection device in accordance with an embodiment of the invention may advantageously be used as a prefilled injection device, i.e. an injection device that is filled with a pharmaceutical composition before being sold or delivered to end-users.
By pharmaceutical composition is meant any fluid manufactured in the pharmaceutical industry and delivered to patients in a therapeutic or diagnostic purpose.
In particular, the pharmaceutical composition that fills the medical injection device according to the invention may be a drug containing proteins, e.g. a vaccine, immunoglobulin or any other biotech drug.
For example, the medical injection device is a prefilled syringe.
Particle Level Measurement Methods
To measure the level of particles present on the surface of the barrel, the injection device is filled with a solution and the level of particles released in said solution is measured.
The solution that is used is a mixture of 10 g/L of Phosphate Buffered Saline and 2.13 mg/L of Tween 80 filtered with a 0.22 microns Stericup™ filter.
Then, the solution is stored for 2 hours before being introduced in a syringe. Once the syringes are filled, they are stirring during 48 h and the measurement of the particles is realized.
Depending on the size of the particles to be detected and quantified, different methods and equipments may be used.
In accordance with an embodiment of the present invention, the particles that are quantified in the lubricated medical injection device have a size of between 1 μm and 100 μm, preferably between 1 μm and 10 μm.
With a size ranging from 1 to 100 μm, the particles are called “subvisible particles”, whereas above 100 μm, the particles are called “visible particles”.
For such particle sizes, the most suitable counting methods are based on optical technologies: a first method is Light Obscuration (LO), a second method is Micro Flow Imaging (MFI), both of which being described in detail below.
Light Obscuration
Light obscuration is routinely used to detect and measure subvisible particles present in parenteral solutions.
As illustrated on
This signal change is then equated to a particle's equivalent spherical diameter based on a calibration curve created using polystyrene spheres of a known size.
Devices based on this technique are sold under the brand HIAC by Hach Lange, for example.
Advantages of such light obscuration device are that it is easy to used, automated and fast.
The measured particles size range with such a device is typically comprised between 2 and 400 μm.
To provide good accuracy, the device has to be used with a large volume of solution (more than 3 ml, which is greater than the volume of a single 1 ml syringe), which implies that it does not allow analyzing containers one by one.
Therefore, as illustrated on
The fluid used to carry out the particles level measurement is WFI (water for injection).
The protocol is the following.
The HIAC equipment is first cleaned with a mixture of WFI and isopropanol alcohol (50/50 proportion), then with WFI only.
All the glassware (intermediate containers for flushing the content of the containers that have to be tested) is also cleaned with WFI, so that the number of particles having a size of 10 μm is of less than 1 particle/ml.
Between each run, a blank with WFI is launched so as to check cell probe and glassware cleanliness.
Then the pharmacopeia norms are conducted on the WFI flushed from the containers. This means that the stopper is moved towards the distal direction in order to eject the WFI through the nozzle of the container into the intermediate container 10.
Usually, the program consists of four runs of 3 ml with the first run discarded, with 3 more ml in order to avoid air bubbles.
In the case of 1 ml injection device, 15 devices are flushed to a common recipient 10 in order to obtain the required analysis volume.
Micro Flow Imaging
MFI is a flow microscopic technology which operates by capturing images of suspended particles in a flowing stream.
Different magnification set-points are available to suit the desired size range and image quality.
The images are used to build a particle database including count, size, transparency and shape parameters.
Said database can be interrogated to produce particle size distributions and isolate sub-populations using any measured parameter.
Suitable equipments are for example sold by Brightwell Technologies (e.g. MFI DPA4200).
The solution is pumped from the injection tip of the container and goes through a flow cell.
As illustrated on
On each picture, pixel contrast differences with calibrated background mean that there is a particle P.
The particle is then digitally imaged.
Supplementary characteristics are thus given (size, shape, etc.).
Due to the particles imaging, the advantage of this device is that it allows making the difference between an air bubble and a silicone oil droplet.
The measured particles size range is typically of between 1 and 100 μm.
The protocol is the following.
First, flow cell integrity is checked to ensure that the measures will be precise.
Then the cleanliness of the flow cell and the tubing is controlled by a blank with WFI (the particle number has to be below 100 particles/mL).
A run with certified beads (e.g. with a size of 5 or 10 μm and with a concentration of 3000 particles/ml) may be carried out.
The measurement program usually consists of 0.5 ml runs separated by 0.2 ml purge.
In this case, and unlike the analysis protocol used for Light Obscuration, several syringes are not flushed to a common recipient.
Instead, as shown on
A rinsing step is performed between the analyses of each syringe.
Depending on the selected method for counting the particles, the measured particle level may vary significantly.
According an embodiment of the present invention, the particle level when measured by HIAC as described above is of less than 2.11 particle/mm2 of surface of contact between the barrel and the solution, whereas a measurement by MFI as described above indicates a particle level of less than 10.56 particle/mm2 of surface of contact between the barrel and the solution.
Gliding Properties Measurement
In order to evaluate the gliding forces, a 1 ml long glass syringe closed by a Daikyo Flurotec® stopper is filled with WFI before being connected to a traction-compression bench (Lloyd LRX Plus) to induce gliding of the stopper within the container.
Then, in order to estimate the comportment of the coating during time, measurement of the gliding forces is performed on syringes coated with 0.25 mg of silicone submitted to plasma treatment at “T0” meaning immediately after the formation of the coating on the syringe surface, and at “T1” meaning after 1 month under 40° C. and 75% of relative humidity.
In parallel, a visual check is performed to ensure that no delaminating or break-up occurred during the one month period.
The results of such experiments can be seen on
Therefore, it can be concluded that the plasma treated coating is not deteriorated with time as the gliding measurements remain in acceptable ranges, meaning between 1 N and 8 N.
Experimental Data
The following illustrates experimental data obtained on a medical container consisting of a 1 ml Long glass syringe.
For such a syringe, the barrel has an inner diameter of 6.35 mm.
The stopper was a rubber stopper with a Flurotec® barrier and further siliconized with PDMS DC-360.
To obtain a silicone layer having a thickness of between 90 and 400 nm, with an average thickness of 150 nm, between 0.1 and 0.4 mg of silicone oil have been sprayed within the barrel with a spraying device.
The silicone oil used was 1000-ctsk DC-360 PDMS.
Then, a plasma treatment with a mixture of oxygen and argon was produced by radio-frequency, with a power ranging from 50 to 300 W and under a vacuum of 10-100 mTorr in absolute value.
The particles level has been measured both by HIAC light obscuration and by MFI method according to the experimental protocols described above.
With the first method, the particle level was of below 1500 particles/mL.
Curve (a) corresponds to a weight of silicone of 0.25 mg, wherein curve (b) corresponds to a weight of silicone of 0.40 mg.
The greater the weight of silicone, the longer the plasma treatment has to be applied to reach the same particle level.
With the second method, the particle level was of below 7500 particles/ml and even below 4800 particles/mL.
Boxplots (a) corresponds to an injection device with a silicone coating of 0.15 mg, whereas boxplots (b) correspond to an injection device with a silicone coating of 0.40 mg.
Since the surface of the barrel in contact with the pharmaceutical composition is of about 710 mm2, the particle levels correspond to less than 2.11 particles by mm2 of coating and less than 10.56 particles by mm2 of coating, respectively.
While specific embodiments of the invention are described with reference to the figures, those skilled in the art may make modifications and alterations to such embodiments without departing from the scope and spirit of the invention. Accordingly, the above detailed description is intended to be illustrative rather than restrictive. The invention is defined by the appended claims, and all changes to the invention that fall within the meaning and range of equivalency of the claims are to be embraced within their scope.
Number | Date | Country | Kind |
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11306236.8 | Sep 2011 | EP | regional |
Filing Document | Filing Date | Country | Kind | 371c Date |
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PCT/EP2012/069119 | 9/27/2012 | WO | 00 | 3/27/2014 |