GB2630304A

GB2630304A - Pharmaceutical formulations

Info

Publication number: GB2630304A
Application number: GB2307626.8A
Authority: GB
Inventors: Jacob Givoni Nathan; Huynh Julie; Michael Wynne Paul; Tolotchkov Kristina
Original assignee: Gelteq Ltd
Current assignee: Gelteq Ltd
Priority date: 2023-05-22
Filing date: 2023-05-22
Publication date: 2024-11-27
Also published as: WO2024241210A1; GB202307626D0

Abstract

A formulation comprising a Biopharmaceutics Classification System (BCS) class II active pharmaceutical ingredient, a combination of gelling agents comprising agar, carrageenan and alginate, at least one cation donor, a pH modifier, a preservative and water. The formulation may further comprise a flavouring. The BCS class 2 API may be ibuprofen, naproxen, diclofenac or hydrochlorothiazide, preferably a sodium salt of ibuprofen, naproxen or diclofenac, the agar may be agar-agar, the carrageenan may be kappa-carrageenan, the alginate may be sodium alginate, the cation donor may be a calcium, magnesium or sodium salt, preferably magnesium or potassium chloride, the pH modifier may be citric acid, and the preservative may be potassium sorbate. The composition may comprise 0.47-0.948% agar, preferably 0.47-0.71% or 0.632-0.948% agar, 0.312-0.47% carrageenan and 0.16-0.24% alginate.

Description

PHARMACEUTICAL FORMULATIONS

[0001] This invention relates to pharmaceutical formulations and more particularly to one for an Active Pharmaceutical Ingredient (API) which is recognised under the Biopharmaceutics Classification System (BCS) as a Class II drug.

BACKGROUND

[0002] API's can be difficult to formulate as their properties differ from API to API. Two of the parameters that challenge a formulation chemist are an API's solubility and its permeability. Accordingly, API's are broadly defined as those falling into one of four classification types based on these two parameters. These four types are illustrated in Fig 1.

[0003] Class I API's have high permeability and high solubility a. An Examples is Metoprolol.

b. Class I compounds are well absorbed, and their absorption rate is usually higher than excretion.

[0004] Class II API's have high permeability and low solubility.

a. Examples include Ibuprofen and Naproxen.

b. The bioavailability of those products is limited by their solvation rate. A correlation between the in vivo bioavailability and the in vitro solvation can be found.

[0005] Class III API's have low permeability and high solubility.

a. An example is Cimetidine b. The absorption is limited by the permeation rate, but the drug is solvated very fast. If the formulation does not change the permeability or gastro-intestinal duration time, then class I criteria can be applied. [0006] Class IV API's have low permeability and low solubility.

a. An example is Bifonazole b. These compounds have a poor bioavailability. Usually, they are not well absorbed over the intestinal mucosa and a high variability is expected.

[0007] The API's are classified in BCS on the basis of solubility, permeability, and also dissolution.

[0008] Solubility class boundaries are based on the highest dose strength of an immediate release product. A drug is considered highly soluble when the highest dose strength is soluble in 250 ml or less of aqueous media over the pH range of 1 to 7.5. The volume estimate of 250 ml is derived from typical bioequivalence study protocols that prescribe administration of a drug product to fasting human volunteers with a glass of water.

[0009] Permeability class boundaries are based indirectly on the extent of absorption of a drug substance in humans and directly on the measurement of rates of mass transfer across human intestinal membrane. Alternatively non-human systems capable of predicting drug absorption in humans can be used (such as in-vitro culture methods). A drug substance is considered highly permeable when the extent of absorption in humans is determined to be 90% or more of the administered dose based on a mass-balance determination or in comparison to an intravenous dose.

[0010] Dissolution class boundaries include an immediate release product, namely one which is rapidly dissolving, i.e. when no less than 85% of the labelled amount of the drug substance dissolves within 15 minutes using USP Dissolution Apparatus 1 at 100 RPM or Apparatus 2 at 50 RPM in a volume of 900 ml or less in the following media: 0.1 M HCI or simulated gastric fluid or pH 4.5 buffer and pH 6.8 buffer or simulated intestinal fluid.

[0011] Most oral formulations take the form of filled capsules or tablets.

[0012] Other formulation types are known, and Applicant has developed a number of drinkable gel-based formulations in areas such as glucose tolerance testing and for delivering nutraceuticals -see respectively: W02017/075672 and W02019215641.

[0013] It is an object of the present invention to provide alternative pharmaceutical formulations for BCS Class II drugs as exemplified by, for example, Ibuprofen and Naproxen.

[0014] Ibuprofen belongs to the drug class called nonsteroidal anti-inflammatory drugs (NSAIDs).

[0015] It comes in various oral dosage forms including oral tablets, oral capsules, oral suspension and chewable tablets.

[0016] Branded Ibuprofens include: US: Equate, Advil, and Motrin I B; AU: Nurofen, Wagner Health, and Rafen; and UK: Boots, Nurofen, Calprofen, Ibuleve, Cuprofen, and Flarin [0017] Naproxen is also a NSAID.

[0018] It comes in various oral dosage forms including tablets, enteric coated tablets, suspensions and liquid filled capsules.

[0019] Branded Naproxens include: Aflaxen, Aleve, Aleve Arthritis, Anaprox, Anaprox DS, EC Naprosyn, Naprelan, Naprelan 500, Naprelan Dose Card and Naprosyn.

[0020] From a regulatory perspective it is possible to obtain registration for a new dosage form using an abridged process such as that provided by the FDA using 505(B)(2) regulatory pathways. See for example: hito!livyyvvv.fdactoviniedall56350/downloac incorporated by reference.

[0021] It is an object of the present invention to develop alternative dosage forms for BSC class II drugs as exemplified with reference to Ibuprofen and Naproxen, and in particular "drinkable" gel-based formulations which can be targeted at patient groups that find swallowing tablets difficult, such as the elderly and children.

BRIEF SUMMARY OF THE DISCLOSURE

[0022] In accordance with the present inventions there is provided a BCS class II formulation comprising: i) a Biopharmaceutics Classification System (BCS) class II Active Pharmaceutical Ingredient (API), or a salt or solution thereof; ii) a combination of gelling agents comprising or consisting of: a. agar, b. carrageenan, and c. an alginate; iii) at least one cation donator; iv) a pH modifier; v) a preservative; and vi) water.

[0023] Preferably, the BCS class II formulation further comprises: vii) a flavouring.

[0024] Non-limiting examples of BCS class II formulations include formulations in which the API is ibuprofen or naproxen, or a salt or solution thereof [0025] Preferred ibuprofen or naproxen formulations are sodium salts or solutions thereof.

[0026] Other exemplary BCS class II API's include: [0027] Hydrochlorothiazide and Diclofenac.

[0028] Hydrochlorothiazide is a diuretic medication often used to treat high blood pressure.

[0029] Diclofenac is another non-steroidal anti-inflammatory.

[0030] The alternative gel formulations of the invention comprise agar as a primary gelling agent, as on sucking it shears to release water making the delivery system particularly attractive as a delivery means for children and the elderly who find swallowing tablets difficult. However, in order to accommodate different class II API's, provide dissolution, stability and texture Applicant determined that both specific secondary and tertiary gelling agents were required.

[0031] The terms primary, secondary and tertiary are used to reflect the relative amounts of each gelling agent, with the primary gelling agent being present in the greatest amount by weight and the tertiary the least amount by weight.

[0032] As noted above the primary gelling agent is Agar.

[0033] Agar is outstanding among hydrocolloids. Agar-agar gels can be formed in very dilute solutions, containing as little as 0.5% to 1.0% of agar-agar. These gels are rigid, brittle, have well defined shapes, as well as sharp melting and gelling points. Moreover, they clearly demonstrate the interesting phenomenon of syneresis (spontaneous extrusion of water through the surface of the gel), and hysteresis (temperature interval between melting and gelling temperatures). Gelling occurs at temperatures far below the gel melting temperature. A 1.5% solution of agar-agar forms a gel on cooling to about 32° to 45° C that does not melt below 85° C. This hysteresis interval is a novel property of agar-agar that finds many uses in food applications. The gel strength of the agar-agar is influenced by concentration, time, pH, and sugar content. The pH noticeably affects the strength of the agar gel; as the pH decreases, the gel strength weakens. Sugar content also has a considerable effect over agar gel. Increasing levels of sugar make gels with harder but a less cohesive texture.

[0034] The secondary agent is a carrageenan, more particularly kappa carrageenan.

[0035] Carrageenan's are large, highly flexible molecules that form curling helical structures. This gives them the ability to Form a variety of different gels at room temperature. They are widely used in the food and other industries as thickening and stabilizing agents.

[0036] Ail carrageenan's are high-molecular-weight polysaccharides and are mainly made up of alternating 3-linked 13-0-galac-topyranose (G-units) and 4-linked o-Dgalactopyranose (0-units) or 4-linked 3,6-anhydro-cr-D-galactopyranose (DA-uni forming the disaccharide repeating unit of carrageenan's.

[0037] There are three main commercial classes of carrageenan: * Kappa which forms strong, rigid gels in the presence of sodium and potassium ions.

* Iota which forms soft gels in the presence of calcium ions, and * Lambda which does not gel.

[0038] The tertiary gelling agent is an alginate. The alginates include: * Sodium alginate (NaC51-1706), * Potassium alginate (KC6H706), and * Calcium alginate (CaC,2H,4©:2).

[0039] The three gelling agents are optimally used in the relative proportions of about: Agar: Carrageenan: Alginate of 4-3: 2.5-1.5: 1.

[0040] The preferred gelling agents are: a. agar-agar, b. kappa carrageenan, and c. sodium alginate.

[0041] To facilitate gelling one or more cation donators are judicially selected.

[0042] Preferably the iii) at least one cation donator is one of a divalent or monovalent cation, more preferably a calcium, magnesium, or potassium salt. Preferred salts include magnesium and potassium chloride.

[0043] In a preferred embodiment the iii) cation donator consists or comprises potassium chloride. [0044] Preferably the iv) the at least one pH modifier is an acidifying agent, alkalizing agent or buffering agent. Exemplary modifiers include: acetic acid, citric acid, hydrochloric acid, phosphoric acid and sodium hydroxide.

[0045] In a preferred embodiment the BCS class II formulation has as the acidifying agent citric acid.

[0046] The citric acid may be used in an amount of up to 2.88% (by weight). [0047] Preferably the v) at least one preservative is selected from lactic acid, potassium sorbate and sodium benzoate.

[0048] In a preferred embodiment the BCS class II formulation has as v) the at least one preservative, potassium sorbate.

[0049] The potassium sorbate may be used in an amount of from 0.07 to 0.12% [0050] Generally, for a BCS class II formulation the gelling agents comprise a primary, secondary, and tertiary gelling agent comprising respectively, by weight percent of the total formulation as claimed: a. agar -0.47% -0.95%, b. carrageenan -0.31% -0.47%, and c. an alginate -0.16% -0.24%.

[0051] With respect to the weight percent figures, these are based on the essential components specified in the claims and exclude optional excipients such as a favouring which may, for example, be added in amounts of up to 2% by weight.

[0052] The actual amounts vary with the API selected.

[0053] In a first embodiment, where the API is Ibuprofen, the gelling agents are present in an amount by weight of: a. agar -0.47% -0.71%, b. carrageenan -0.31% -0.47%, and c. an alginate -0.16% -0.24%.

[0054] More particularly the formulation is as illustrated in Table 1 below:

Table 1

Excipient Weight percent (Range) Mean Ibuprofen (sodium salt) 0.69 -1.03% 0.86% Water L78.18% 97.7% Potassium sorbate 0.078% -0.117% 0.1% Magnesium chloride 0.034% -0.052% 0.04% Potassium chloride 0.016% -0.024% 0.02% Agar 0.469% -0.704% 0.59% Ka rapageenan Capr 0.313% -0.469% 0.39% Sodium alginate 0.157% -0.235% 0.20% Citric acid 0.066% -0.099% 0.08% TOTAL 100% [0055] Actual excipient amounts are illustrated in Table 2a and 2b below: Table 2a Ibuprofen gel (200 mg/25 ml) -pH 6.8 INGREDIENT MASS UNIT % Ibuprofen 0.200 g 0.78% Water 25 g 97.80% Potassium sorbate 0.025 g 0.10% Magnesium chloride 0.011 g 0.04% Potassium chloride 0.005 g 0.02% Agar 0.150 g 0.59% Karapageenan Capr 0.100 g 0.39% Sodium alginate 0.050 g 0.20% Citric acid 0.021 g 0.08% TOTAL 25.562 g 100.00%

Table 2b

Ibuprofen gel (220 mg/25 ml) -pH 6.8 INGREDIENT MASS UNIT % Ibuprofen 0.220 g 0.86% Water 25 g 97.72% Potassium sorbate 0.025 g 0.10% Magnesium chloride 0.011 g 0.04% Potassium chloride 0.005 g 0.02% Agar 0.150 g 0.59% Kappa Carrageenan 0.100 g 0.39% Sodium alginate 0.050 g 0.20% Citric acid 0.021 g 0.08% TOTAL 25.582 g 100.00% [0056] In a second embodiment, where the API is Naproxen, the gelling agents are present in an amount by weight of: a. agar -0.63% -0.95%, b. carrageenan -0.31% -0.47%, and c. an alginate -0.16% -0.24%.

[0057] More particularly the formulation is as illustrated in Table 3 below: Table 3 Excipient Weight percent (Range) Mean Naproxen 0.69% -1.03% 0.86% Water 78.12% 97.7% Potassium sorbate 0.08% -0.12% 0.10% Potassium chloride 0.16% -0.23% 0.20% Agar 0.63% -0.94% 0.78% Kappaa 0.31% -0.47% 0.39%

C

Sodium alginate 0.16% -0.23% 0.20% Citric acid 0.0009% -0.0014% 0.0012% TOTAL 100% [0058] Actual excipient amounts are illustrated in Table 4 below: Table 4 Naproxen gel (220 mg/25 ml) -pH 7.5 INGREDIENT MASS UNIT ok Naproxen 0.22 g 0.86% Water 25.00 g 97.66% Potassium sorbate 0.025 g 0.10% Potassium chloride 0.005 g 0.02% Agar 0.200 g 0.78% Karapageenan Capr 0.100 g 0.39% Sodium alginate 0.050 g 0.20% Citric acid 0.0003 g 0.0012% TOTAL 25.60 g 100.00% [0059] In a third embodiment, where the API is Diclofenac, the gelling agents are present in an amount by weight of: a. agar -0.47% -0.71%, b. carrageenan -0.32% -0.47%, and c. an alginate -0.16% -0.24%.

[0060] More particularly the formulation is as illustrated in Table 5 below: Table 5 Excipient Weight percent (Range) Mean Diclofenac 0.038% -0.057% 0.05% Water a.78.88% 98.6% Potassium sorbate 0.076 -0.114 % 0.09% Potassium chloride 0.015 -0.023 % 0.02% Agar 0.53 -0.79 % 0.66% Kappaageenan C 0.30 -0.46 % 0.38% Sodium alginate 0.15 -0.23 % 0.19% Citric acid 0.0012 -0.0018 % 0.0015% TOTAL 100% [0061] Actual excipient amounts are illustrated in Table 6 below: Table 6 Diclofenac gel (12.5 mq/25 ml) -pH 7.5

INGREDIENT MASS UNIT

Diclofenac 0.0125 g 0.05% Water 26.00 g 98.60% Potassium sorbate 0.025 g 0.09% Potassium chloride 0.005 g 0.02% Agar 0.175 g 0.66% Kappa 0.100 g 0.38% Carrageenan Sodium alginate 0.050 g 0.19% Citric acid 0.0004 g 0.0015% TOTAL 26.3679 g 100.00% [0062] In a fourth embodiment, where the API is Hydrochlorothiazide, the gelling agents are present in an amount by weight of: a. agar -0.47% -0.71%, b. carrageenan -0.32% -0.47%, and c. an alginate -0.16% -0.24%.

[0063] More particularly the formulation is as illustrated in Table 7 below:

Table 7

Excipient Weight percent (Range) Mean Hydrochlorothiazide 0.038 -0.057 % 0.05 % Water 78.9 % 98.65 % Potassium sorbate 0.076 -0.11 % 0.10 % Potassium chloride 0.015-0.023 % 0.02 % Magnesium chloride 0.034 -0.050 % 0.04 % Agar 0.46 -0.069 % 0.57 % Kappa 0.31 -0.46 % 0.38 % Carrageenan Sodium alginate 0.15-0.23 % 0.19 % Citric acid 0.0012 -0.0018% 0.0015 % TOTAL 100 % [0064] Actual excipient amounts are illustrated in Table 8 below:

Table 8

Hydrochlorothiazide (12.5 mg/25 ml) -pH 7.5 INGREDIENT MASS UNIT ok Hydrochlorothiazide 0.0125 g 0.05% Water 25.87 g 98.65% Potassium sorbate 0.025 g 0.10% Potassium chloride 0.005 g 0.02% Magnesium chloride 0.011 g 0.04% Agar 0.150 g 0.57% Kappa Carrageenan 0.100 g 0.38% Sodium alginate 0.050 g 0.19% Citric acid 0.0004 g 0.0015% TOTAL 26.2239 g 100.00% [0065] The invention is further described, by way of example only, with reference to the drawings, Examples and detailed description given below.

BRIEF DESCRIPTION OF THE DRAWINGS

[0066] Embodiments of the invention are further described hereinafter with reference to the accompanying drawings, in which: Fig 1 is a diagram illustrating the Biopharmaceutics Classification System (BCS); Fig 2 is a graph illustrating the dissolution of five individual gels; and Figs 3a and 3b are graphs illustrating the dissolution of the preferred triple combination with ibuprofen at 200mg and 220mg respectively vs Advil and Motrin (alternative dosage forms).

DETAILED DESCRIPTION

[0067] In developing alternative formulations for BCS class II formulations Applicant looked at a variety of standard gelling agents with a first Exemplary API (Ibuprofen).

Experimental series 1 [0068] From a stock solution of ibuprofen (Table 9 below), a number of mono-gel formulations were produced, and dissolution was tested.

[0069] Table 9

(1) Ibuprofen sodium stock solution (Ibu-Na solution) Ingredient Mass Unit % Ibuprofen 1.20 g 0.79 Sodium hydroxide 0.23 g 0.15 Water 150.00 g 99.06 [0070] Using this stock solution gels the following mono gels were produced and the formulations are provided in Tables 10 to 14:

1) Agar Table 10

Excipients Agar only Unit g % Ibu-Na soln 25 99.16 Magnesium chloride 0.011 0.04 Potassium sorbate 0.01 0.04 Agar 0.19 0.75 2) Kappa carrageenan,

Table 11

Excipients Kappa Carrageenan only Unit g Ibu-Na soln 25 99.1 Magnesium chloride 0.011 0.04 Potassium sorbate 0.01 0.04 Potassium chloride 0.005 0.02 Kappa carrageenan 0.2 0.79 3) Low acyl gellan gum Table 12 Excipients Low acyl gellan gum only Unit g Ibu-Na soln 25 99.12 Magnesium chloride 0.011 0.04 Potassium sorbate 0.01 0.04 Low acyl gellan gum 0.2 0.79 4) Sodium alginate Table 13 Excipients Sodium alginate only Unit g Ibu-Na soln 25 99.52 Magnesium chloride 0.011 0.04 Potassium sorbate 0.01 0.04 Sodium alginate 0.1 0.40 Notes Formulation remained as a liquid 5) Pectin

Table 14

Excipients Pectin only Unit g Ibu-Na soln 25 99.52 Magnesium chloride 0.011 0.04 Potassium sorbate 0.01 0.04 Pectin 0.1 0.40 Formulation Notes remained as a liquid Results [0071] The dissolution data for these formulations are provided in Fig 2.

[0072] As can be seen from Fig 2, the results showed the "gels" to perform differently.

[0073] The two "gels", which did not actually gel in the given formulations, namely -sodium alginate (red circle) and pectin (blue diamond), perhaps unsurprisingly given their state, showed the most rapid dissolution, releasing their full dose inside of 5 minutes.

[0074] On the other hand, Agar (yellow diamond) and Gellan gum (pink triangle) took about 60 minutes to fully release the Ibuprofen.

[0075] Surprisingly, the Kappa carrageenan, which forms gels via ionic association with potassium ions, produced the fastest dissolution profile with 0.02% potassium chloride, releasing the full dose of ibuprofen within 5 minutes. The gel had a soft and bouncy texture and therefore fully disintegrated. Although this is great for a therapeutic it proved not to be temperature stable, and therefore a second series of experiments (Experimental series 2) looked at utilising the kappa carrageenan and modifying it with other gelling agent(s) to improve its stability (and texture) was undertaken.

Experimental series 2 [0076] To strengthen the kappa carrageenan gel base, agar was introduced. In contrast to kappa carrageenan, agar forms gels via cold-set gelation. Agar was dissolved and dispersed in boiling water. Upon cooling, inter-chain helices form between the polymers, leading to a three-dimensional network. The introduction of agar with kappa carrageenan produced semi-solid gels compared to kappa carrageenan alone. However, the gels remained soft and bouncy, rather than rigid and firm.

[0077] Concentrations of agar from 0.20-0.32% resulted in a soft gel which crumbled when crushed. Agar concentrations of 0.44-0.55% resulted in a firmer gel that broke apart when squished. When the kappa carrageenan concentration changed from 0.28-0.75%, the gel texture was soft but there was no noticeable difference. Therefore, contrary to the indications from Experimental series 1, agar became the primary gelling agent and kappa the secondary gelling agent.

[0078] An exemplary, two gel combination is provided in Table 15 below:

Table 15

Kappa & Agar Ingredient Mass % Unit Ibu-Na soln 25 99.10% g Magnesium chloride 0.011 0.04% g Potassium sorbate 0.01 0.04% g Potassium chloride 0.005 0.02% g Kappa 0.09 0.36% g Agar agar 0.11 0.44% g TOTAL 25.226 100.00% g Observations Semi-clear gel, firm, holds shape. clean interior cut. good texture gel when squished, collapses under the spatula but not too soft [0079] However, the two gelling agent composition, whilst having suitable dissolution and stability characteristics, had a texture which was unsatisfactory. Therefore, a third gelling agent was introduced -Series 3.

Experimental series 3 [0080] Following extensive experimentation Applicant determined that sodium alginate should be added, and a desirable formulation was obtained that was temperature stable.

[0081] An exemplary formulation is illustrated in Table 16 below:

Table 16.

Kappa Agar & Alginate Ingredient Mass % Unit Ibu-Na soln 25 98.71 g Magnesium chloride 0.011 0.04 g Potassium sorbate 0.01 0.04 g Potassium chloride 0.005 0.02 g Kappa 0.1 0.39 g carrageenan Agar agar 0.15 0.59 g Sodium 0.05 0.20 g alginate TOTAL 25.326 100.00 Observations Firm gel, homogenous, cloudy appearance due to gelling agents. Clean cut. Collapses when squished (not pasty) [0082] However, the ibuprofen sodium solution had a pH of 9.90. Therefore, a series of experiments were undertaken to modify the pH.

[0083] Hydrochloric acid and citric acid were tested as pH adjustors. Hydrochloric acid precipitated and was not compatible with the formulation. Citric acid changed the pH significantly. As a consequence, it was selected as the preferred pH adjusting agent.

[0084] Further details of the ibuprofen gels of the invention are set out in Example 1.

EXAMPLE 1 (Ibuprofen) [0085] The preferred Ibuprofen formulations are set out in Tables 2a and 2b reproduced below:

Table 2a

Ibuprofen gel (200 mg/25 ml) -pH 6.8 INGREDIENT MASS UNIT % Ibuprofen 0.200 g 0.78% Water 25 g 97.80% Potassium sorbate 0.025 g 0.10% Magnesium chloride 0.011 g 0.04% Potassium chloride 0.005 g 0.02% Agar 0.150 g 0.59% Karapageenan Capr 0.100 g 0.39% Sodium alginate 0.050 g 0.20% Citric acid 0.021 g 0.08% TOTAL 25.562 g 100.00%

Table 2b

Ibuprofen gel (220 mg/25 ml) -pH 6.8 INGREDIENT MASS UNIT % Ibuprofen 0.220 g 0.86% Water 25 g 97.72% Potassium sorbate 0.025 g 0.10% Magnesium chloride 0.011 g 0.04% Potassium chloride 0.005 g 0.02% Agar 0.150 g 0.59% Kappa Carrageenan 0.100 g 0.39% Sodium alginate 0.050 g 0.20% Citric acid 0.021 g 0.08% TOTAL 25.582 g 100.00% [0086] The selected ibuprofen gel formulation was modified to produce a product with "bio equivalence" to an approved ibuprofen formulation so that the FDA 505 pathway could be used to expedite approval.

Formulating the gel [0087] To prepare the ibuprofen solution, dissolve sodium hydroxide pellets in water. Add ibuprofen powder slowly until completely dissolved. Add citric acid to obtain a pH -7. Using a stirring hot plate, heat the ibuprofen solution to 95°C. Add agar and mix until completely dissolved and clear. Add potassium sorbate, magnesium chloride, potassium chloride and mix until dissolved. Add citric acid and mix. Slowly add the remaining gelling agents, kappa carrageenan and sodium alginate and mix until completely dissolved. Hot fill the gel into the pouch and cap immediately. Let it cool to room temperature. Pouches may require air to inflate the pouch prior to filling.

Preparing the gel for dissolution testing [0088] Once cool and set, squeeze the pouch 5 times prior to opening.

Dissolution test [0089] Fill dissolution vessel with 900 mL medium (phosphate-buffered saline, PBS pH 7.2). Using the paddle attachment, set rotating speed at 50 rpm and temperature of the water bath at 37.5°C. Dispense squished gel from the pouch into the dissolution vessel and start experiment. Sample buffer medium at the following time points: 5, 10, 15, 20, 30, 45, 60, 120 minutes and filter immediately after sampling. Replace removed buffer after sampling.

High performance liquid chromatography [0090] The HPLC was performed as set out in Table 17 below:

Table 17

Parameter Value Instrument Shimadzu Nexera X2 UHPLC system attached to Shimadzu SPD-M30A Diode array detector and Shimadzu CTO-20AC column oven Column Phenomenex Kinetex® 2.6pm C18 100,E (100 x 2.1mm) LC Column UV Wavelength 220 nm Mobile Phase 0.1% formic acid in H2O

A

Mobile Phase 0.1% formic acid in ACN

B

Flow rate 0.5 mlimin Gradient Time (min) % Mobile phase B 0 20 20 90 90 20 20 0.05 Temperature 40°C Injection volume 1 pL Peak retention time 4.28 min Concentration range 50-300 pg/mL Validation [0091] The assay was validated based on replicates at three concentrations and were considered valid when precision and accuracy were within ±10%.

Results [0092] Figs 3a and 3b show the dissolution profile of a 200mg and 220mg formulation of ibuprofen respectively against formulations of Advil and Motrin respectively.

EXAMPLE 2 (Naproxen) Table 4 Naproxen gel (220 mg/25 ml) -pH 7.5 INGREDIENT MASS UNIT 0/0 Naproxen 0.22 g 0.86% Water 25.00 g 97.66% Potassium sorbate 0.025 g 0.10% Potassium chloride 0.005 g 0.02% Agar 0.200 g 0.78% Kappa 0.100 g 0.39% Carrageenan Sodium alginate 0.050 g 0.20% Citric acid 0.0003 g 0.0012% TOTAL 25.60 g 100.00% EXAMPLE 3 (Diclofenac) Table 6 Diclofenac gel (12.5 mq/25 ml) -pH 7.5 INGREDIENT MASS UNIT % Diclofenac 0.0125 g 0.05% Water 26.00 g 98.60% Potassium sorbate 0.025 g 0.09% Potassium chloride 0.005 g 0.02% Agar 0.175 g 0.66% Kappa 0.100 g 0.38% Carrageenan Sodium alginate 0.050 g 0.19% Citric acid 0.0004 g 0.0015% TOTAL 26.3679 g 100.00% EXAMPLE 4 (Hydrochlorothiazide)

Table 8

Hvdrochlorothiazide (12.5 ma/25 ml) -pH 7.5 INGREDIENT MASS UNIT % Hydrochlorothiazide 0.0125 g 0.05% Water 25.87 g 98.65% Potassium sorbate 0.025 g 0.10% Potassium chloride 0.005 g 0.02% Magnesium chloride 0.011 g 0.04% Agar 0.150 g 0.57% Kappa Carrageenan 0.100 g 0.38% Sodium alginate 0.050 g 0.19% Citric acid 0.0004 g 0.0015% TOTAL 26.2239 g 100.00%

Claims

CLAIMS 1. 2. 3. 4. 6. 7.A Biopharmaceutics Classification System (BCS) class II formulation comprising: i) a Biopharmaceutics Classification System (BCS) class II Active Pharmaceutical Ingredient (API), or a salt or solution thereof, a combination of gelling agents comprising or consisting of: a. agar, b. carrageenan, and c. alginate, iii) at least one cation donator, iv) a pH modifier, v) a preservative, and vi) water.
A BCS class II formulation as claimed in claim 1 which further comprises: vii) a flavouring.
A BCS class II formulation as claimed in any of the preceding claims wherein i) the API is ibuprofen, naproxen, diclofenac or hydrochlorothiazide, or a salt or solution thereof.
A BCS class II formulation as claimed in claim 3 wherein i) the ibuprofen, naproxen or diclofenac is a sodium salt or solution.
A BCS class II formulation as claimed in any of the preceding claims wherein ii) a. the agar is agar-agar, b. the carrageenan is kappa carrageenan, and c. the alginate is sodium alginate.
A BCS class II formulation as claimed in any of the preceding claims wherein iii) the at least one cation donator is one of a calcium, magnesium, or potassium salt.
A BCS class II formulation as claimed in claim 6 wherein iii) the at least one cation donator comprises magnesium and potassium chloride.
8. A BCS class II formulation as claimed in claim 6 wherein iii) the at least one cation donator consists of potassium chloride.
9. A BCS class II formulation as claimed in any of the preceding claims wherein iv) the at least one pH modifier is citric acid.
10. A BCS class II formulation as claimed in any of the preceding claims wherein v) the at least one preservative is potassium sorbate.
11. A BCS class II formulation as claimed in any of the preceding claims wherein ii) the gelling agents are present in an amount percent by weight of: a. agar -0.47% -0.948% b. carrageenan -0.312% -0.47%, and c. an alginate -0.16% -0.24%. 15
12. A BCS class II formulation as claimed in claim 11 wherein ii) the gelling agents are present in an amount percent by weight of: a. agar -0.47% -0.71% b. carrageenan -0.32% -0.47%, and c. an alginate -0.16% -0.24%.
13. A BCS class II formulation as claimed in claim 11 wherein ii) the gelling agents are present in an amount percent by weight of: a. agar -0.632% -0.948% b. carrageenan -0.312% -0.468%, and c. an alginate -0.16% -0.24%.
14. A BCS class II formulation as claimed in claim 12 comprising the excipients of Table 1 in the range as set out below: Excipient Weight percent (Range) Ibuprofen (sodium salt) 0.69 -1.03% Water 78.18% Potassium sorbate 0.078% -0.117% Magnesium chloride 0.034% -0.052% Potassium de chlori 0.016% -0.024% Agar 0.469% -0.704% Kappa 0.313% -0.469%, C geenan Sodium alginate 0.157% -0.235%.Citric acid 0.066% -0.099%
15. A BCS class II formulation as claimed in claim 14 comprising by mean weight:INGREDIENT MASS UNITIbuprofen 0.200 g Water 25 g Potassium sorbate 0.025 g Magnesium chloride 0.011 g Potassium chloride 0.005 g Agar 0.150 g Kappa 0.100 g Carrageenan Sodium alginate 0.050 g Citric acid 0.021 g TOTAL 25.562 g orINGREDIENT MASS UNITIbuprofen 0.220 g Water 25 g Potassium sorbate 0.025 g Magnesium chloride 0.011 g Potassium chloride 0.005 g Agar 0.150 g Kappa Carrageenan 0.100 g Sodium alginate 0.050 g Citric acid 0.021 g TOTAL 25.582 g
16. A BCS class II formulation as claimed in claim 13 comprising the excipients of Table 3 in the range as set out below: Excipient Weight percent (Range) Naproxen 0.69% -1.03% Water a.78.12% Potassium sorbate 0.08% -0.12% Potassium chloride 0.16% -0.23% Agar 0.63% -0.94% Kappa 0.31% -0.47% Car rageenan Sodium alginate 0.16% -0.23%.Citric acid 0.0009% -0.0014%
17. A BCS class II formulation as claimed in claim 16 comprising by mean weight the excipients of Table 4 as set out below:INGREDIENT MASS UNITNaproxen 0.22 g Water 25.00 g Potassium sorbate 0.025 g Potassium chloride 0.005 g Agar 0.200 g Kappa 0.100 g Carrageenan Sodium alginate 0.050 g Citric acid 0.0003 g TOTAL 25.60 g
18. A BCS class II formulation as claimed in claim 11 comprising the excipients of Table 5 in the range as set out below: Excipient Weight percent (Range) Diclofenac 0.038% -0.057% Water 78.88% Potassium sorbate 0.076 -0.114 % Potassium chloride 0.015 -0.023 % Agar 0.53 -0.79 % Kappa 0 % Carrageenan.30 -0.46 Sodium alginate 0.15 -0.23 % Citric acid 0.0012 -0.0018 %
19. A BCS class II formulation as claimed in claim 18 comprising by mean weight the excipients of Table 6 as set out below:INGREDIENT MASS UNITDiclofenac 0.0125 g Water 26.00 g Potassium sorbate 0.025 g Potassium chloride 0.005 g Agar 0.175 g Kappa 0.100 g Carrageenan Sodium alginate 0.050 g Citric acid 0.0004 g TOTAL 26.3679 g
20. A BCS class II formulation as claimed in claim 11 comprising the excipients of Table 7 in the range as set out below: Excipient Weight percent (Range) Hydrochlorothiazide 0.038 -0.057 cro Water 78.9 % Potassium sorbate 0.076 -0.11 % Potassium chloride 0.015-0.023 % Magnesium chloride 0.034 -0.050 Agar 0.46 -0.069 % Kappa 0 % Carrageenan.31 -0.46 Citric acid 0.0012 -0.0018%
21. A BCS class II formulation as claimed in claim 20 comprising by mean weight the excipients of Table 8 as set out below:INGREDIENT MASS UNITHydrochlorothiazide 0.0125 g Water 25.87 g Potassium sorbate 0.025 g Potassium chloride 0.005 g Magnesium chloride 0.011 g Agar 0.150 g Kappa 0.100 g Carrageenan Sodium alginate 0.050 g Citric acid 0.0004 g TOTAL 26.2239 g