AU2002230589A1

AU2002230589A1 - Fast dissolving tablet

Info

Publication number: AU2002230589A1
Application number: AU2002230589A
Authority: AU
Inventors: Khawla A. Abu-Izza; Vincent H. Li; Jee L. Look; Graham D. Parr; Matthew K. Schineller
Original assignee: PF Consumer Healthcare 1 LLC
Current assignee: PF Consumer Healthcare 1 LLC
Priority date: 2000-12-06
Filing date: 2001-12-04
Publication date: 2002-08-22
Anticipated expiration: 2021-12-04

Description

FAST DISSOLVING TABLET

This application claims priority under 35 U.S.C. § 119 rom U.S. Nonprovisional Application No. 09/731,479, filed on December 6, 2000 and is incorporated herein by reference in its entirety.

FIELD OF THE INVENTION

The current invention relates to tablets of low hardness but good physical stability, in particular fast dissolving tablets that can be made at very low compression force, yet have acceptable stability, and methods for preparing such tablets.

BACKGROUND OF THE INVENTION Several processes are presently available by which a tablet, which dissolves quickly in the mouth, may be formulated. However, various disadvantages are associated with these currently available methods for producing fast dissolving tablets. For example the addition of high levels of disintegrants is disclosed by Cousin et al (U.S. Patent 5,464,632). Cousin et al. add two disintegrants to the disclosed tablet formulations, for example 16% starch 1500 and 13.3 % crosspovidone. The oral-disintegration time of these tablets is 35 seconds to 45 seconds. However, tablets including high levels of disintegrants have a chalky or dry feel when placed in the mouth.

Another process for producing fast dissolving tablets involves freeze drying or lyophilizing solutions or suspensions of an active ingredient and matrix forming excipients. Pebley et al. (U.S. Patent 5,298,261) disclose freeze-drying a slurry or paste comprising an active ingredient and excipients placed in blister packets. Humbert-Droz et

al. (WO 97/36879) disclose vacuum drying, at room temperature or a slightly elevated temperature, a suspension including the active drug, a sugar alcohol, PEG 6000, talc, sweeteners and flavors in preformed blisters. The disadvantages of the freeze drying or vacuum drying methods are time (very slow process), cost of the equipment (not done on conventional tablet manufacturing equipment), and that it is limited to low dose actives.

Fast-dissolving tablets may also be formulated by the inclusion of effervescent coupled compounds. Wehling et al. (US Patent 5,178,878 and WO 91/04757) disclose the addition of an effervescent couple (such as sodium bicarbonate and citric acid) to a tablet. Exposure of the tablet to moisture results in contact and chemical reaction between the effervescent couple which leads to gas production and tablet disintegration. For this reason, tablets which include effervescent pairs are highly sensitive to moisture and have an unpleasant mouth feel. Tablets formed by compression under low compression force also dissolve more rapidly than tablets formed by high compression force. However, tablets produced by these processes have a high degree of friability. Crumbling and breakage of tablets prior to ingestion may lead to uncertainty as to the dosage of active ingredient per tablet. Furthermore, high friability also causes tablet breakage leading to waste during factory handling.

The present invention addresses these and other problems associated with the prior art. The invention provides fast-dissolving tablets of low hardness, low friability and high stability which have the added advantage of cost-effective methods of manufacture. In particular, the fast-dissolving tablets of the invention melt rapidly in the mouth and provide an excellent mouth feel.

SUMMARY OF THE INVENTION

The present invention advantageously provides compositions and methods for preparing a fast dissolving tablet of low hardness but good physical stability that can be made at very low compression force.

Thus, the invention provides a tablet comprising a low melting point compound that melts or softens at or below 37 °C, a water soluble excipient, and an active ingredient. Preferably, the low melting point compound comprises from about 2.5% to about 20% (wt/wt) of the composition (e.g., 2.5, 5, 7.5, 10, 12, 14, 16, 18, or 20%

(wt/wt)). Preferably the tablet has a hardness of about 3 kP or less, more preferably about 2kP or less, and still more preferably about IkP or less. Preferably, the minimum hardness of the tablet is about 0.1 kP, although lower values, including 0.05 kP, are possible.

The invention further provides a method of producing a tablet composition.

The method comprises combining an active agent (also termed "active ingredient" or

"active") with a fast dissolving granulation. The fast dissolving granulation comprises a low melting point compound and a water soluble excipient. Preferably, the low melting compound is present in an amount that will yield values of about 2.5% to about 20% (wt/wt) in a final tablet composition (e.g., 2.5, 5, 7.5, 10, 12, 14, 16, 18, or 20% (wt/wt)). The accompanying Detailed Description, Examples and Drawings further elaborate the invention and its advantages. DESCRIPTION OF THE DRAWINGS

Figure 1 shows a graph of tablet hardness as a function of compression

force for tablets of the invention prepared by a melt granulation process (diamonds), and tablets prepared by direct compression (squares).

Figure 2 shows a graph of friability as a function of tablet hardness;

"Number of Rotations" indicates a number of rotations in a Friabilator which occur before

a tablet breaks. Tablets prepared by melt granulation (diamonds) or by direct compression (squares) were evaluated.

Figure 3 shows a graph of time of onset of disintegration (Tl) as a function

of compression force for tablets of the invention (diamonds) and for tablets formed by

direct compression (squares).

Figure 4 shows a graph of disintegration time (T2) as a function of

compression force for tablets of the invention (diamonds) and for tablets formed by direct

compression (squares).

Figure 5 shows a graph of disintegration time as a function of the friability

(as measured by the number of rotations in a Friabilator before a first tablet breaks) for

tablets of the invention (diamonds) and for tablets formed by direct compression (squares).

Figure 6 shows a graph of time to dissolve (mean of disintegration time in

seconds for 34 samples of a tablet of the invention (MG), two types of tablets formed by

direct compression (DC1 and DC2), and a commercial fast dissolving tablet (KIDTAB^®).

Figure 7 shows a graph of grittiness score (adjusted mean determined by

least squares from ANON A). Subjects scored this sensory attribute on a scale of 1 (low grittiness) to a 9 (high grittiness). Tablets were as described for Figure 6. Figure 8 shows a graph of chalkiness score (adjusted mean determined by

least squares from ANON A). Subjects scored this sensory attribute on a scale of 1 (low

chalkiness) to a 9 (high chalkiness). Tablets were described for Figure 6.

Figure 9 shows a graph of overall preference ranking for each product (as

described in Figure 6), represented by the percentage of subjects ranking each product 1 ^st,

2^nd, 3^rd, or 4^th.

DETAILED DESCRIPTION

The current invention provides fast dissolving tablet formulations that can

be formed by compression into a conventional tablet. Tablet friability is lower than

conventional fast dissolving tablets prepared by low compression. The fast dissolving

tablet has at least one compound which partially or fully melts or softens at or below body

temperature and a water soluble excipient. The low melting point excipient may be

hydrophilic or hydrophobic. The tablets of the invention may also include an active

ingredient and may also include one or more disintegrants, flavors, colorants, sweeteners,

souring agents, glidants or lubricants.

The hardness of the tablets is low (less than or equal to about 3 kP),

preferably less than or equal to about 2 kP, and more preferably less than or equal to about

1 kP, with a minimum hardness of greater than or equal to about 0.1 kP (e.g., 0.05, 0.07,

0.1, 0.2, 0.3, 0.4, 0.5, 0.6, 0.7, 0.8, 0.9, 1.0, 1.3, 1.6, 1.9, 2.0, 2.1, 2.3, 2.5, 2.7, 2.8 or 3.0

kP). In a specific embodiment, hardness ranges from about 0.2 to about 1 kP. Attributes such as (1) fast tablet dissolution; (2) good tablet mouth feel; and (3) good tablet physical

stability are of greater importance than minimum and maximum values of tablet hardness.

Nevertheless, the tablets are somewhat pliable, and are less f agile than conventional tablets that have the same crushing strength. The tablets have an excellent mouth feel resulting from the low melting point component which melts or softens in the mouth to

produce a smooth feel and masks the grittiness of insoluble ingredients. Unlike other fast

dissolving tablets, the disintegration of this fast dissolving tablet occurs by a combination

of melting, disintegration of the tablet matrix, and dissolution of the water soluble

excipient. Therefore, a dry feel does not occur. Disintegration time is 10 to 30 seconds

(e.g., 10, 12, 14, 16, 18, 20, 22, 24, 26, 28 or 30 seconds), depending on the tablet size and

amount of insoluble ingredients, e.g., coated active. Even though the tablet contains a low

melting point ingredient, it is relatively stable to high temperatures. Heating the tablet

above the melting point of its low melting point component will not significantly reduce

its physical stability.

The friability of conventional tablets is measured by the percentage weight

loss after a typical friability test (rotating 10 tablets in a friability apparatus for 100

rotations). This test is very harsh for conventional fast dissolving tablets and so cannot be used to measure their friability. Fast dissolving tablets made by direct compression at low

force crumble after a few rotations in the -friability apparatus. Fast dissolving tablets

manufactured by the method in the current invention can withstand 20-50 rotations in the

friability apparatus before any tablet breaks. After 20 rotations, the friability (% weight

lost) is typically less than 1%. The term "low melting point compound" may include any edible

compound which melts or softens at or below 37°C which is suitable for inclusion in the

tablets of the invention. Materials commonly used for manufacturing suppositories usually

have a melting point at or just below body temperature and can be used in the invention. The low melting point compound can be hydrophilic or hydrophobic. Examples of hydrophilic low-melting point compounds include, but are not limited to, polyethylene glycol; the preferred mean molecular weight range of polyethylene glycol for use in the tablets of the invention is from about 900 to about 1000. Mixtures of polyethylene glycol with different molecular weights (200, 300, 400, 550, 600, 1450, 3350, 8000 or 10,000) are within the scope of the invention if the mixture melts or softens at or below 37 degrees celcius.

Examples of hydrophobic low-melting point compounds include, but are not limited to, low melting point triglycerides, monoglycerides and diglycerides, semisynthetic glyceride (e.g., EUTECOL^®, GELUCIRE^®(available from Gatteffosse SA of France), hydrogenated oils , hydrogenated oil derivatives or partially hydrogenated oils

(e.g., partially hydrogenated palm kernel oil and partially hydrogenated cottonseed oil), fatty acid esters such as myristyl lactate, stearic acid and palmitic acid esters, cocoa butter

or its artificial substitutes, palm oil/palm oil butter, and waxes or mixtures of waxes, which melt at 37° C or below. In preferred embodiments, the hydrogenated oil is WECOBEE^® M (available of Stepan Co. of Northfield, Illinois). To be effective in the tablet compositions, the low melting point compound must be edible.

Mono- di- and triglycerides are rarely used as pure components. Hydrogenated vegetable oils, and solid or semisolid fats are usually mixtures of mono- di- and triglycerides. The melting point of the fat or hydrogenated vegetable oil is characteristic of the mixture and not due to a single component. Examples include, but are not limited to WITESPOL^® (available from Condea of Germany), SUPPOCIRE^® (available from Gattefosse SA of France), and NON AT A^® (available from Henkel of Austria), commonly used in manufacturing suppositories because they melt at body temperature. All are mixtures of triglycerides, monoglycerides and diglycerides. In preferred embodiments, the low melting point compound comprises from about 2.5% to about 20%, by weight, of a tablet composition (e.g., about 2.5, 5, 7.5, 10, 12, 14, 15, 16, 18, or 20% (wt/wt)).

The tablets of the present invention also include a water soluble excipient. As used herein, the term "water soluble excipient" refers to a solid material or mixture of materials that is orally ingestible and readily dissolves in water. Examples of water soluble excipients include but are not limited to saccharides, amino acids, and the like. Saccharides are preferred water soluble excipients. Preferably, the saccharide is a mono-, di- or oligosaccharide. Examples of saccharides which may be added to the tablets of the invention may include sorbitol, glucose, dextrose, fructose, maltose and xylitol (all monosaccharides); sucrose, lactose, glucose, galactose and mannitol (all disaccharides). In a specific embodiment, exemplified below, the saccharide is lactose. Preferably, the saccharide is mannitol. Other suitable saccharides are oligosaccharides. Examples of oligosaccharides are dextrates and maltodextrins. Other water soluble excipients may include amino acids such as alanine, arginine, aspartic acid, asparagine, cysteine, glutamic acid, glutamine, glycine, histidine, isoleucine, leucine, lysine, methionine, phenylalanine, proline, serine, threonine, tryptophan, tyrosine and valine; glycine and lysine are preferred

amino acids.

In preferred embodiments, the water soluble excipient comprises from about 25% to about 97.5%, by weight, of a tablet composition. The preferred range is about 40% to about 80%. For example, tablet compositions comprising about 25, 30, 35, 40, 45, 50, 55, 60, 65, 70, 75, 80, 85, 90, 95 or 97.5%, by weight, saccharide are within the scope of the invention. As used herein, the term "about" (or "approximately") means a particular value can have a range acceptable to those of skill in the art given the nature of the value and method by which it is determined. In a specific embodiment, the term means within 50% of a given value, preferably with 20%, more preferably within 10%, and more preferably still within 5%.

Active Ingredients

As used herein, the term "active ingredient" or "active agent" refers to one or more compounds that have some pharmacological property. Accordingly, more than one type of active ingredient compound may be added to the tablets of the invention. The

tablets of the invention may comprise any active ingredient which may be orally administered to a subject. Tablets including active ingredients in amounts appropriate for the desired pharmacological properties at the dosage administration can be formulated. Any amount of active ingredient that does not significantly affect beneficial tablet features, such as hardness, friability and mouth feel are within the scope of the invention. Placebo tablets, which lack an "active ingredient" having a known pharmacologic activity, are also within the scope of the invention. An "active ingredient" of a placebo can be the water soluble excipient (i.e., lacking any identifiable "active"), a different water soluble compound, or any non-active compound.

A non-limiting list of acceptable active ingredients may include but is by no means limited to:l) antipyretic analgesic anti-inflammatory agents such as indomethacin, aspirin, diclofenac sodium, ketoprofen, ibuprofen, mefenamic acid, dexamethasone, dexamethasone sodium sulfate, hydrocortisone, prednisolone, azulene, phenacetin, isopropylantipyrin, acetaminophen, benzydamine hydrochloride, phenylbutazone, flufenamic acid, mefenamic acid, sodium salicylate, choline salicylate, sasapyrine,

clofezone or etodolac; 2) antiulcer agents such as ranitidine, sulpiride, cetraxate

hydrochloride, gefarnate, irsogladine maleate, cimetidine, lanitidine hydrochloride, famotidine, nizatidine or roxatidine acetate hydrochloride; 3) coronary vasodilators such as

nifedipine, isosorbide dinitrate, diltiazem hydrochloride, trapidil, dipyridamole, dilazep

dihydrochloride, methyl

2,6-dimethyl-4-(2-nitrophenyl)-5-(2-oxo- 1 ,3 ,2-dioxaphosphorinan-2-yl)- 1 ,4- dihydropyridine-3-carboxylate, verapamil, nicardipine, nicardipine hydrochloride or

verapamil hydrochloride; 4) peripheral vasodialtors such as ifenprodil tartrate, cinepazide

maleate, cyclandelate, cinnarizine or pentoxyfyline; 5) oral antibacterial and antifungal

agents such as penicillin, ampicillin, amoxicillin, cephalexin, erythromycin ethylsuccinate, bacampicillin hydrochloride, minocycline hydrochloride, chloramphenicol, tetracycline,

erythromycin, fluconazole, itraconazole, ketoconazole, miconazole or terbinafine; 6)

synthetic antibacterial agents such as nalidixic acid, piromidic acid, pipemidic acid

trihydrate, enoxacin, cinoxacin, ofloxacin, norfloxacin, ciprofloxacin hydrochloride, or

sulfamethoxazole trimethoprim; 7) antipasmodics such as propantheline bromide, atropine

sulfate, oxapium bromide, timepidium bromide, butylscopolamine bromide, rospium chloride, butropium bromide, N-methylscopolamine methylsulfate, or methyloctatropine

bromidebutropium bromide; 8) antitussive, anti-asthmatic agents such as theophylline,

aminophylline, methylephedrine hydrochloride, procaterol hydrochloride, trimetoquinol

hydrochloride, codeine phosphate, sodium cromoglicate, tranilast, dextromethorphan

hydrobromide, dimemorfan phosphate, clobutinol hydrochloride, fominoben hydrochloride, benproperine phosphate, tipepidine hibenzate, eprazinone hydrochloride,

clofedanol hydrochloride, ephedrine hydrochloride, noscapine, calbetapentane citrate, oxeladin tannate, or isoaminile citrate; 9) broncyodilators such as diprophylline, salbutamol sulfate, clorprenaline hydrochloride, formoterol fumarate, orciprenalin sulfate, pirbuterol hydrochloride, hexoprenaline sulfate, bitolterol mesylate, clenbuterol hydrochloride, terbutaline sulfate, mabuterol hydrochloride, fenoterol hydrobromide, or methoxyphenamine hydrochloride; 10) diuretics such as -turosemide, acetazolarmide, trichlormethiazide, methyclothiazide, hydrochlorothiazide, hydroflumetliiazide, ethiazide, cyclopenthiazide, spironolactone, triamterene, fluorothiazide, piretanide, metruside, ethacrynic acid, azosemide, or clofenamide; 11) muscle relaxants such as chlorphenesin carbamate, tolperisone hydrochloride, eperisone hydrochloride, tizanidine hydrochloride,

mephenesin, chlorozoxazone, phenprobamate, methocarbamol, chlormezanone, pridinol mesylate, afloqualone, baclofen, or dantrolene sodium; 12) brain metabolism altering drugs such as meclofenoxate hydrochloride; 13)minor tranquilizers such as oxazolam, diazepam, clotiazepam, medazepam, temazepam, fludiazepam, meprobamate, nitrazepam, or chlordiazepoxide; 14) major tranquilizers such as sulpirid, clocapramine hydrochloride,

zotepine, chlorpromazine, or haloperidol; 15) β-blockers such as pindolol, propranolol

hydrochloride, carteolol hydrochloride, metoprolol tartrate, labetalol hydrochloride, acebutolol hydrochloride, butetolol hydrochloride, alprenolol hydrocl loride, arotinolol hydrochloride, oxprenolol hydrochloride, nadolol, bucumolol hydrochloride, indenolol hydrochloride, timolol maleate, befunolol hydrochloride, or bupranolol hydrocliloride; 16) antiarrhythmic agents such as procainamide hydrochloride, disopyramide, ajimaline, quinidine sulfate, aprindine hydrocliloride, propafenone hydrochloride, or mexiletine hydrochloride; 17) gout suppressants allopurinol, probenecid, colchicine, sulfinpyrazone, benzbromarone, or bucolome; 18) anticoagulants such as ticlopidine hydrochloride, dicumarol, or warfarin potassium; 19) antiepileptic agents such as phenytoin, sodium valproate, metharbital, or carbamazepine; 20) antihistaminics such as chlorpheniramine

maleate, cremastin fumarate, mequitazine, alimemazine tartrate, or cycloheptazine

hydrochloride; 21) antiemetics such as difenidol hydrochloride, metoclopramide,

domperidone, betahistine mesylate, or trimebutine maleate; 22) hypotensives such as

5 dimethylaminoethyl reserpilinate dihydrochloride, rescinnamine, methyldopa, prazosin

hydrochloride, bunazosin hydrochloride, clonidine hydrochloride, budralazine, or urapidin;

23) sympathomimetic agents such as dihydroergotamine mesylate, isoproterenol

hydrochloride, or etilefrine hydrochloride; 24) expectorants such as bromhexine

hydrochloride, carbocysteine, ethyl cysteine hydrochloride, or methyl cysteine

0 hydrochloride; 25) oral antidiabetic agents such as glibenclamide, tolbutamide, or

glymidine sodium; 26) circulatory agents such as ubidecarenone or ATP-2Na; 27) iron

preparations such as ferrous sulfate or dried ferrous sulfate; 28) vitamins such as vitamin

Bl, vitamin B2, vitamin B6, vitamin B12, vitamin C, vitamin A, vitamin D, vitamin E,

vitamin K or folic acid; 29) pollakiuria remedies such as flavoxate hydrocliloride,

5 oxybutynin hydrochloride, terodiline hydrochloride, or

4-diethylamino-l,l-dimethyl-2-butynyl (I)- α-cyclohexyl-α-phenylglycolate hydrochloride

monohydrate; 30) angiotensin-converting enzyme inhibitors such as enalapril maleate,

alacepril, or delapril hydrochloride; 31) anti- viral agents such as trisodium

phosphonoformate, didanosine, dideoxycytidine, azido-deoxythymidine,

-0 didehydro-deoxythymidine, adefovir dipivoxil, abacavir, amprenavir, delavirdine,

efavirenz, indinavir, lamivudine, nelfinavir, nevirapine, ritonavir, saquinavir or stavudine;

32) high potency analgesics such as codeine, dihydrocodeine, hydrocodone, morphine,

dilandid, demoral, fentanyl, pentazocine, oxycodone, pentazocine or propoxyphene; 33) antihistamines such as brompheniramine maleate and 34) nasal decongestants such as phenylpropanolamine HCl. Active ingredients in the foregoing list may also have

beneficial pharmaceutical effects in addition to the one mentioned.

Other Tablet Ingredients

The term "tablet" refers to a pharmacological composition in the form of a small, essentially solid pellet of any shape. Tablet shapes may be cylindrical, spherical,

rectangular, capsular or irregular. The term "tablet composition" refers to the substances

included in a tablet. A "tablet composition constituent" or "tablet constituent" refers to a

compound or substance which is included in a tablet composition. These can include, but

are not limited to, the active agent and any excipients in addition to the low melting

compound and the water soluble excipient. An excipient is any ingredient in the tablet

except the active agent, and includes binders, disintegrants, flavorants, colorants, glidants,

souring agents and sweeteners.

For the purposes of the present application, "binder" refers to one or more

ingredients added before or during granulation to form granules and/or promote cohesive

compacts during compression. A "binder compound" or "binder constituent" is a

compound or substance which is included in the binder. Binders of the present invention

include, at least, the low melting compound.

Additionally, and optionally, other substances commonly used in

pharmaceutical formulations can be included such as flavors (e.g., strawberry aroma,

raspberry aroma, cherry flavor, magnasweet 135, key lime flavor, grape flavor trusil art 5-

11815, fruit extracts and PROSWEET™), flavor enhancers and sweeteners (e.g.,

aspartame, sodium saccharine, sorbitol, glucose, sucrose), souring agents (e.g. citric acid),

dyes or colorants. The tablet may also contain one or more glidant materials which improve

the flow of the powder blend and minimize tablet weight variation. Glidants such as

silicone dioxide may be used in the present invention.

Additionally, the tablets of the invention may include lubricants (e.g.

magnesium stearate) to facilitate ejection of the finished tablet from dies after compression

and to prevent tablets from sticking to punch faces and each other.

Any method of forming a tablet of the invention into a desired shape which

preserves the essential features thereof are within the scope of the invention.

Tablet Formation

A preferred method of forming the tablet compositions of the invention

includes mixing a fast dissolving granulation, which includes a low-melting point

compound and a water soluble excipient, preferably a saccharide. The term "fast dissolving granulation" refers to a composition of the low melting point compound and the

water soluble excipient prepared for use in manufacture of tablets of the invention. A

portion of the fast dissolving granulation may then be added to the remaining ingredients.

However, methods of forming the tablets of the invention wherein all tablet constituents

are combined simultaneously or wherein any combination of tablet constituents are combined separate from the other constituents are within the scope of the invention.

Granulation end point can be determined visually (visual inspection). It can

also be determined using a load cell that measures power consumption. Tablet

manufacturing and granulation routinely employ both techniques.

The tablet compositions of the invention can be formed by melt granulation

which is a preferred method. In particular, the melt granulation can be performed in a high shear mixer, low shear mixer or fluid bed granulator. An example of high shear mixer is

DIOSNA^® (available Diosna Dierks & Sδhne GmbH). Examples of low shear mixers are

various tumbling mixers (e.g., twin shell blenders or N-blender). Examples of fluid bed

granulators are Glatt and Aeromatic fluid bed granulators.

There are three ways of manufacturing the granulation:

- Melting the low melting point ingredient, then combining it with the

water soluble ingredient(s) in the granulator and mixing until granules

form.

- Loading the water soluble excipient in the granulator and spraying

the molten low melting point compound on it while mixing.

- Combining the two (water soluble component and low melting point

component) and possibly other ingredients and mixing while heating to a temperature around or higher than the melting point of the low melting point component until the

granules form.

After the granulation congeals, it may be milled and/or screened. Examples

of mills that can be used are COMILL^® and STOKES OSCILLATOR^®. Any mills that are

commonly used for milling tablet granulations may be used.

Melt extrusion can be used to form the fast dissolving granulation. An

example of an extruder that can be used is the ΝICA SYSTEM™ (available from

Νiro- Aeromatic of Columbia, Maryland). The low melting point compound and the water

soluble saccharide are mixed and heated in a planetary mixer bowl (low shear mixer) that is usually part of the extruder. The soft mass is then fed to the extrusion chamber and

forced through small holes or orifices to shape it into thin rods or cylinders. After the

extruded material congeals it can be milled or spheronized using standard equipment. In the spheronization step, the extrudate is dumped onto the spinning plate of the spheronizer and broken up into small cylinders with a length equal to their diameter, then rounded by frictional forces (See, International Journal of Pharmaceutics 1995, 116:131-146, especially p. 136.).

Spray congealing or prilling can also be used to form the tablet compositions of the invention. Spray congealing includes atomizing molten droplets of compositions which include a low melting point compound onto a surface or, preferably, other tablet constituents. Equipment that can be used for spray congealing includes spray driers (e.g., Nero Spray Drier) and a fluid bed coater/granulation with top spray (e.g., Glatt Fluid Bed Coater/Granulator). In preferred embodiments, a fast-dissolve granulation is formed wherein, preferably a water soluble excipient, more preferably a saccharide, is suspended in a molten low melting point ingredient and spray congealed. After spray congealing, the resulting composition is allowed to cool and congeal. Following congealing of the mixture, it is screened or sieved and mixed with the remaining tablet constituents. Spray congealing processes wherein fast-dissolve granulations comprising any combination of low melting point compound and other tablet constituents are melted and spray congealed onto other tablet constituents are within the scope of the present invention. Spray congealing processes wherein all tablet constituents, including the low- melting point compound, are mixed, the low melting point compound is melted and the mixture is spray congealed onto a surface are also within the scope of the invention.

After spray congealing, the mixture may be milled and then combined with other tablet constituents. Following formation of the final tablet composition, the composition may be further processed to form a tablet shape. Mixing and milling of tablet constituents during the preparation of a tablet

composition may be accomplished by any method which causes the composition to

become mixed to be essentially homogeneous. In preferred embodiments the mixers are

high-shear mixers such as the DIOSNA^®, COMILL^® or N-BLENDER^®.

Once tablet compositions are prepared, they may be formed into various

shapes. In preferred embodiments, the tablet compositions are pressed into a shape. This

process may comprise placing the tablet composition into a form and applying pressure to

the composition so as to cause the composition to assume the shape of the surface of the

form with which the composition is in contact. In preferred embodiments, the tablet is

compressed into the form at a pressure which will not exceed about 10 kN, preferably less

than 5 kN. For example, pressing the tablets at less than 1, 1, 1.5, 2, 2.5, 3, 3.5, 4, 4.5, 5,

6, 7, 8, 9, or 10 kN is within the scope of the invention. The tablets of the invention

generally have a hardness of about 3kP or less; preferably the tablets have a hardness of about 2 kP or less and more preferably about IkP or less. For example, tablets of about

0.05, 0.07, 0.1, 0.2, 0.3, 0.4, 0.5, 0.6, 0.7, 0.8, 0.9, 1.0, 1.3, 1.6, 1.9, 2.0, 2.1, 2.3, 2.5, 2.7,

2.8 or 3.0 or less than 0.1 kP are within the scope of the invention. Hydraulic presses such

as a CARVER PRESS^® or rotary tablet presses such as the STOKES VERSA PRESS^® are

suitable means by which to compress the tablet compositions of the invention.

Tablets may also be formed by tumbling melt granulation (TMG)

essentially as described in Maejima et al, Chemical Pharmacology Bulletin. (1997) 45(3):

518-524; which is incorporated herein by reference. Tumbling melt granulation can be

used for preparing the melt granulation and can be done in a tumbling mixer. The molten

low melting point compound is sprayed on the crystalline saccharide and powdered saccharide in the blender and are mixed until granules form. In this case, the low melting ingredient is the binder and the crystalline saccharide is the seed. An alternative method is to combine the unmelted low melting point ingredient, crystalline sugar (e.g. sucrose or maltose), and water-soluble ingredient in the powder form (e.g., mannitol or lactose) in the tumbling mixer and mix while heating to the melting point of the low melting point binder or higher. The seed should be a crystalline or granular water soluble ingredient

(saccharide), e.g., granular mannitol, crystalline maltose, crystalline sucrose, or any other sugar. An example of tumbling mixers is the twin-shell blender (V-BLENDER^®), or any other shape of tumbling mixers. Heating can be achieved by circulating heated air through the chamber of the granulator and by heating the bottom surface of the chamber. As the seed material and the powdered tablet constituents circulate in the heated chamber, the low-melting point compound melts and adheres to the seeds. The unmelted, powdered material adheres to the seed-bound, molten low-melting point material. The spherical beads which are formed by this process are then cooled and screen sifted to remove nonadhered powder.

EXAMPLES

EXAMPLE 1: Fast Dissolving Granulations

Compositions of Fast Dissolving Granulations. In these compositions, the

water soluble excipient is a saccharide. As described above, the tablets of the invention may be formulated by a method wherein a fast dissolving granulation, comprising a low melting point compound and a water soluble excipient, is mixed separately from other tablet constituents. A portion of the fast dissolving granulation may then be combined with the other tablet constituents. In this example, several specific examples of fast dissolving granulations are set forth. Table 1. Fast dissolving granulation formulations.

Fast dissolving granulations 1 and 2 were prepared by heating the low melting compound to 50°C. At 50°C, WECOBEE^® M and GELUCIRE^® 33/01 become molten. The molten material was gradually added to the mannitol powder in a high shear granulator (DIOSNA^®). The granulation was mixed at high speed. When the granulation end point was reached as determined by visual inspection, the granulation was allowed to congeal. The congealed granulation was then milled using a COMILL^®.

Granulation 3 was granulated by combining melted WECOBEE^® M with the mannitol in a high shear mixer (Robot Coupe) and blending until the granules formed. Granulation 4 was made by combining the melted PEG with fructose powder in a planetary mixer (low shear mixer) and mixing until the granules formed. The granulations were allowed to cool, then were screened.

EXAMPLE 2: Fast dissolving ibuprofen tablets

The following is an example of a fast dissolving tablet wherein the active ingredient is ibuprofen. Ingredient Amount (mg tablet) -

Coated ibuprofen (active ingredient 121.9 (equivalent to 100 mg

ibuprofen)

Citric acid (souring agent) 11.0

Magnasweet 135 (sweetening agent) 3.9

Aspartame (sweetening agent) 6.5

Cherry flavor (flavoring agent) 7.8

Crosscarmellose sodium (disintegrant) 39.0

Silicone dioxide (glidant flow aid) 1.95

Magnesium stearate (lubricant) 3.25

Fast dissolving granulation 4 457.9

Total 653.2

Ingredients were screened, then mixed in a V-BLENDER^®. Tablets were

compressed using a hydraulic press (CARVER PRESS^®) at 600 lb (about 2.7 kN). The

tablets had a hardness of 0.2-0.5 kP and disintegrated in less than 15 seconds.

EXAMPLE 3: Fast dissolving antihistamine/decongestant tablets

The following is an example of a fast dissolving tablet comprising the

active ingredients of many common allergy medications, Phenylpropanolamine HCl and

Brompheniramine Maleate.

Ingredient Amount (mg/tablef.

Phenylpropanolamine HCl (active ingredient) 6.25

Bromphemramine Maleate (active ingredient) 1.0

Citric acid (souring agent) 6.0 Magnasweet 135 (sweetening agent) 1.80

Aspartame (sweetening agent) 4.5

Cherry flavor (flavoring agent) 3.60

Crosscarmellose sodium (disintegrant) 21.0

Lecithin (creamy mouthf eel) 3.0

Corn Starch (anti-adherent) 30.0

Silicone dioxide (glidant flow aid) 3.0

Fast dissolving granulation 4 219.25

Magnesium stearate (lubricant) 2.1

Total 301.5

Tablets were compressed on a hydraulic press (CARVER PRESS^®) at

approximately 3 kN. Tablet hardness was 0.2-0.5 kP and disintegration time 10 seconds.

EXAMPLE 4: Fast dissolving ibuprofen tablets

The following is an example of a fast dissolving tablet wherein the active

ingredient is ibuprofen.

Ingredient Amount (mg/tablet)

Coated ibuprofen (active agent) 119.0

Citric Acid (souring agent) 20.0

Magnasweet 135 (sweetening agent) 7.5

Aspartame (sweetening agent) 7.5

Grape flavor Trusil Art 5-11815 (flavoring agent) 5.00

Prosweet™ (flavor and sweetness enhancer) 5.00

Crosscarmellose sodium (enhancer) 20.0 Corn Starch, NF (anti-adherent) 40.0

Silicone dioxide (Syloid^® 244) (glidant flow aid) 5.00

Fast dissolving granulation 1 271

Total 500

Tablets were compressed using a rotary tablet press (STOKES VERSA PRESS^®) at 3.3.-3.5 kN, resulting in a hardness of 0.2-0.9 kP. In vivo disintegration time was 19 seconds (average of 34 subjects).

Sensory study: The melt granulation tablets of Example 4 were evaluated for in vivo disintegration time and mouthfeel in an in-house sensory study. The comparator was Kidtab^®, an 80 mg acetaminophen fast dissolving tablet prepared by direct compression. Two other ibuprofen fast dissolving tablets prepared by direct compression were also included in the study. The study included 34 subjects. The subjects were asked to record the time for the tablet to completely dissolve in the mouth and give scores for mouthfeel attributes and overall liking of the product. The melt granulation prototype (based on this invention) performed best on disintegration time (Figure 6) and mouthfeel attributes (least grittiness (Figure 7) and least chalkiness (Figure 8)) and were ranked best on the overall performance by the panelists.

Table 2 shows the ranking results of the sensory study on disintegration time and mouthfeel attributes: MG is the melt granulation tablet of the invention. DC1 and DC2 are the two direct compression prototypes. Table 2

The tablets of the invention were ranked the highest (1, best) in all four

categories tested (dissolution time, grittiness, chalkiness and overall performance) against DCl, DC2 and KIDTAB^®.

As illustrated in Figure 6, the tablets of the invention exhibited superior

fast dissolving characteristics as compared to the direct compression tablets which were

also evaluated (DCl, DC2 and KIDTAB^®); the average time for the tablet of the invention (MG) to dissolve was 19 seconds wherein the time for DCl, DC2 and KIDTAB^® to

dissolve were about 20, 22 and 25 seconds, respectively. The tablets of the invention also

exhibited a mouth feel which was superior to the DCl, DC2 and KIDTAB^® tablets.

Figures 7 and 8 indicate the 34 individuals who participated in the study perceived a lower

level of grittiness and chalkiness associated with the tablets of the invention as compared

to the direct compression tablets (DCl, DC2 and KIDTAB^®).

Overall preference was also scored (least squares mean from ANOVA) on a

scale from 1 (most preferred) to 9 (least preferred). As indicated in Figure 9, the tablet of

the invention scored highest (2.11), followed by the KIDTAB^® (2.29), and the two direct compression tablets (DC2-2.52, DC 1-3.05)

banking (1 = best, 4 = worst) EXAMPLE 5: Fast dissolving ibuprofen tablets

The following is an example of a fast dissolving tablet wherein the active

ingredient is ibuprofen

Ingredient mg/tablet

Coated ibuprofen (active agent) 238.0

Citric Acid (souring agent) 17.5

Magnasweet 135 (sweetening agent) 9.75

Aspartame (sweetening agent) 9.75

Key Lime flavor (flavoring agent) 6.50 Vanilla powder (flavoring agent) 0.650

Corn Starch, NF (anti-adherent) 52.0

Silicone dioxide (Syloid^® 244) (glidant/flow aid) 6.50

Sodium stearyl fumarate (Pruv) (lubricant) 4.88

Fast dissolving granulation 1 304 Total 650

Tablets were compressed using a rotary tablet press (STOKES VERSA

PRESS^®) at 3 kN, resulting in a hardness of 0.35-0.60 kP. In vivo disintegration time was

16 seconds.

EXAMPLE 6: Compressibility and in vitro evaluation of tablets

To compare fast dissolving tablets of the invention with fast dissolving tablets prepared by direct compression, the following two examples were prepared. Melt granulation fast dissolving tablet:

Ingredient mg/tablet

Ibuprofen microcaps 119.0

Citric Acid, anhydrous, fine granular 20.0

Magnasweet 135 7.5

Aspartame (Nutrasweet) 7.5

Cherry Berry flavor 4.25

Sweet AM 2.50

Crosscarmellose sodium 20.0

Corn Starch, NF 40.0

Silicone dioxide (Syloid^® 244) 5.00

Fast dissolve granulation 274.25

TOTAL 500

* The granulation is 85.0% Mannitol powder, USP and 15.0% WECOBEE^® M

(hydrogenated vegetable oil). The granulation was prepared similar to granulation 1 in

Table 1.

Direct compression fast dissolving tablet:

Ingredient mg/tablet

Ibuprofen microcaps 119.0

Citric Acid, anhydrous, fine granular 20.0

Magnasweet 135 7.5

Aspartame (Nutrasweet) 7.5

Sweet AM 2.50

Fruit Punch flavor 3.50 Crosscarmellose sodium 20.0

Corn Starch, NF 40.0

Silicone dioxide (Syloid^® 244) 5.00

Mg Stearate 3.50 Granular mannitol 271.5

TOTAL 500

Melt granulation tablets and direct compression tablets were prepared based on the same formula, except that granular mannitol was used instead of the fast dissolve melt granulation. The compressibility of the two tablet formulations (melt granulation and direct compression) were compared. The two blends were compressed at different compression forces and the resulting tablets were evaluated for hardness and in vitro disintegration time. Tablet hardness (crushing strength) was measured using a high resolution texture analyzer (Stable Microsystems) with an acrylic cylindrical probe.

In vitro disintegration was performed in a texture analyzer. A tablet was held on a net that was then attached to a 1/4" stainless steal ball probe. The disintegration medium was 5 ml of water in a 50 ml beaker. The height of water was barely enough to submerge the tablet, and the water temperature was kept at 37 ± 1°C. The texture analyzer was instructed to apply a small force (20 g) when the tablet hit the bottom of the beaker. The time for disintegration onset and total disintegration time were recorded. Compressibility: Fast dissolving tablets in general are soft and need to be blister-packaged directly off the tablet press. The tablets manufactured according to the invention can be compressed at very low compression forces, which cannot be used with tablets prepared by direct compression or wet granulation. For fast dissolving tablets containing a coated active, it is important to compress at the lowest force possible so that the coating will not be ruptured under compression. With the melt granulation approach,

tablets that are robust enough to withstand packaging right off the tablet press were obtained using a compression force as low as 2 kN, whereas for a similar direct

compression formulation, acceptable tablets could not be obtained at compression forces

below 5 kN (Figure 1).

Hardness and Friability: Although the melt granulation tablets had a lower

hardness compared to direct compression tablets that are compressed at the same force (Figure 1), the melt granulation tablets were somewhat pliable and less fragile. As

illustrated in Figure 2, the softest melt granulation prototype, with a hardness of about 0.2

kP, was able to withstand at least 9 rotations in the friabilator (friability apparatus) before

any tablet breaks. At 0.5 kP, these tablets survived 20-30 rotations. Direct compression

tablets at about 0.45 kP started breaking after 4 rotations, while the hardest direct

compression prototype with about 0.9 kP hardness only survived 12 rotations. In the same

friability test, Kidtab^® tablets (marketed fast dissolving tablets prepared by direct

compression) started breaking after 5-10 rotations. The average hardness of Kidtab^®

tablets was 1.8 kP. Moreover, at the end of the test, the direct compression tablets showed

more chipping around the edges than melt granulation prototypes. Direct compression tablets with hardness greater than 1 kP were not fast dissolving (took 1 minute or more to

dissolve in the mouth of a subject).

In vitro Disintegration: The onset of disintegration was faster for the melt

granulation prototypes compared to direct compression prototypes prepared at the same

compression force (Figure 3). Furthermore, the total time for in vitro disintegration was

dependent on compression force regardless of the formulation (Figure 4). Acceptable

tablets were obtained from the melt granulation processing low compression force. Direct

compression tablets could not be obtained at the same compression force. Therefore, for tablets with similar friability, the melt granulation approach produced faster disintegration

time (Figure 5).

The melt granulation formulation was less sensitive to small changes in

compression force, whereas for the direct compression formulation, both hardness and

onset of disintegration increased sharply with increasing the compression force (Figures 1

and 3).

EXAMPLE 7: Example of melt granulation tablets with higher hardness:

Ingredient mg/tablet

Ibuprofen microcaps (encapsulated ibuprofen) 121.9

Citric Acid, anhydrous, fine granular 11.0

Magnasweet 135 4.0

Aspartame (Nutrasweet) 6.0

Cherry flavor 6.0

Sweet AM 0.5

Crosscarmellose sodium 45.0

Corn Starch, NF 40.0

Silicone dioxide (Syloid^® 244) 2.50

Fast dissolve granulation 263.1

TOTAL 500

* The granulation is 85.0% Mannitol powder, USP and 15.0% WECOBEE^® M

(hydrogenated vegetable oil).

Tablets were compressed on STOKES VERSA PRESS^®. Compression force was not recorded. Tablet hardness was 1.5 kP. The tablets had a friability of less

than 1.0% after 50 rotations in the friabilator, i.e, lost less than 1% of their initial weight and no tablet broke. Mean in vivo disintegration time was 25.8 seconds (12 subjects were asked to take the tablets and record the time it takes for the tablet to completely dissolve without chewing).

The present invention is not to be limited in scope by the specific embodiments described herein. Indeed, various modifications of the invention in addition to those described herein will become apparent to those skilled in the art from the foregoing description and the accompanying figures. Such modifications are intended to fall within the scope of the appended claims.

It is further to be understood that all values are approximate, and are provided for description.

Patents, patent applications, publications, product descriptions, and protocols are cited throughout this application, the disclosures of which are incorporated herein by reference in their entireties for all purposes.

Claims

WHAT IS CLAIMED

1. A tablet comprising a low melting point compound that melts or softens at or below 37°C, a water soluble excipient and an active ingredient, wherein the low melting point compound comprises from about 2.5% to about 20% (wt/wt) of the composition, and wherein the tablet has a hardness of about IkP or lower.

2. The tablet of claim 1 , wherein the water soluble excipient comprises about 25% to about 97.5% (wt/wt) of the tablet.

3. The tablet of claim 1 wherein the water soluble excipient comprises about 40% to about 85% (wt/wt) of the tablet.

4. The tablet of claim 1 wherein the water soluble excipient is a saccharide.

5. The tablet of claim 4 wherein the water soluble excipient is a saccharide and the saccharide is one or more substances selected from the group consisting of maltose, fructose, sucrose, lactose, glucose, galactose, xylitol, sorbitol, dextrates, maltodextrins and mannitol.

6. The tablet of claim 1 wherein the water soluble excipient is an amino acid.

7. The tablet of claim 6 wherein the water soluble excipient is an amino acid and the amino acid is one or more compounds selected from the group consisting of glycine and lysine.

8. The tablet of claim 1 further comprising one or more components selected from the group consisting of a disintegrant, a colorant, a sweetener, a souring agent, a glidant, a binder, a lubricant and a flavorant.

9. The tablet of claim 1 wherein the low melting point compound is one or more compounds selected from the group consisting of hydrogenated oil, polyethylene glycol, low melting point triglycerides, low melting point diglycerides, low melting point monoglycerides, synthetic glycerides, fatty acid esters, semisynthetic glycerides, partially hydrogenated oil, palm oil, palm butter, wax and cocoa butter.

10. The tablet of claim 9 wherein the low melting point compound comprises a mixture of a monoglyceride, a diglyceride and a triglyceride and wherein the mixture is one or more substances selected from the group consisting of WITEPSOL^®, SUPPOCIRE^® and NOVATA^®.

11. The tablet of claim 9 wherein the low melting point compound is a partially hydrogenated oil and wherein the partially hydrogenated oil is one or more substances selected from the group consisting of partially hydrogenated palm kern oil and partially hydrogenated cotton seed oil.

12. The tablet of claim 9 wherein the low melting point compound is a hydrogenated oil and the hydrogenated oil is WECOBEE^® M.

13. The tablet of claim 9 wherein the low melting point compound is a fatty acid ester and the fatty acid ester is one or more compounds selected from the group consisting of stearic acid ester, palmitic acid ester and myristyl lactate ester.

14. A method of producing a tablet composition, which method comprises combining an active agent with a fast dissolving granulation, wherein the fast dissolving granulation comprises a low melting point compound and a water soluble excipient.

15. The method of claim 14, which further comprises adding one or more components selected from the group consisting of a disintegrant, a colorant, a sweetener, a lubricant, a souring agent, a glidant, a binder and a flavorant.

16. The method of claim 14, which further comprises molding the tablet composition into a tablet form.

17. The method of 14, wherein the fast dissolving granulation is prepared by high sheer granulation.

18. The method of claim 17 wherein the low melting point compound is molten.

19. The method of claim 18 wherein the fast dissolving granulation is prepared by spraying the molten low melting point compound onto the water soluble excipient and allowing the resulting composition to congeal.

20. The method of claim 18 wherein the fast dissolving granulation is prepared by suspending the water soluble excipient in molten low melting point compound and spray congealing the resulting composition.

21. The method of claim 18 wherein the fast dissolving granulation is made by a method comprising extruding the composition comprising the active agent and the fast dissolving granulation through a nozzle and allowing the resulting composition to congeal.

22. The method of claim 18 wherein the water soluble excipient is one or more saccharides selected from the group consisting of maltose, fructose, sucrose, lactose, glucose, galactose, xylitol, sorbitol, and mannitol.

23. The method of claim 18 wherein the low melting point compound is one or more compounds selected from the group consisting of hydrogenated oil, polyethylene glycol, low melting point triglycerides, low melting point diglycerides, low melting point monoglycerides, synthetic glycerides, fatty acid esters, semisynthetic glycerides, partially hydrogenated oil, palm oil, palm butter, wax and cocoa butter.

24. The method of claim 18 which comprises congealing a mixture comprising molten low melting point compound and the water soluble excipient.

25. The method of claim 24, which further comprises granulating the congealed mixture by a method selected from the group consisting of sifting the congealed mixture through a screen and milling the congealed mixture.

26. The method of claim 25 which further comprises molding the granulated mixture into a tablet shape.

27. A placebo tablet comprising a low melting point compound that melts or softens at or below 37°C and a water-soluble excipient. The low melting point compound comprises from about 2.5% to about 20% (wt/wt) of the composition wherein the tablet has a hardness of about IkP or lower.

28. A tablet comprising a low melting point compound that melts or softens at or below 37°C, a water soluble excipient and an active ingredient, wherein the low melting point compound comprises from about 2.5% to about 20% (wt/wt) of the composition, and wherein the tablet disintegrates in an oral cavity in 10 to 30 seconds.

29. The tablet of claim 28 comprising a hardness of about 3 kP or less.

30. The tablet of claim 29 comprising a hardness of about 2 kP or less.

31. The tablet of claim 30 comprising a hardness of about 1 kP or less.

32. The tablet of claim 28, wherein the water soluble excipient comprises about 25% to about 97.5% (wt/wt) of the tablet.

33. The tablet of claim 28 wherein the water soluble excipient comprises about 40% to about 85% (wt/wt) of the tablet.

34. The tablet of claim 28 wherein the water soluble excipient is a saccharide.

35. The tablet of claim 34 wherein the saccharide is one or more ^' substances selected from the group consisting of maltose, fructose, sucrose, lactose, glucose, galactose, xylitol, sorbitol, dextrates, maltodextrins and mannitol.

36. The tablet of claim 28 wherein the water soluble excipient is an amino acid.

37. The tablet of claim 36 wherein the water soluble excipient is an amino acid and the amino acid is one or more compounds selected from the group consisting of glycine and lysine.

38. The tablet of claim 28 further comprising one or more components selected from the group consisting of a disintegrant, a colorant, a sweetener, a souring agent, a glidant, a binder, a lubricant and a flavorant.

39. The tablet of claim 28 wherein the low melting point compound is one or more compounds selected from the group consisting of hydrogenated oil, polyethylene glycol, low melting point triglycerides, low melting point diglycerides, low melting point monoglycerides, synthetic glycerides, fatty acid esters, semisynthetic glycerides, partially hydrogenated oil, palm oil, palm butter, wax and cocoa butter.

40. The tablet of claim 39 wherein the low melting point compound comprises a mixture of a monoglyceride, a diglyceride and a triglyceride and wherein the mixture is one or more substances selected from the group consisting of WITEPSOL^®, SUPPOCIRE^® and NOVATA^®.

41. The tablet of claim 39 wherein the low melting point compound is a partially hydrogenated oil and wherein the partially hydrogenated oil is one or more substances selected from the group consisting of partially hydrogenated palm kern oil and partially hydrogenated cotton seed oil.

42. The tablet of claim 39 wherein the low melting point compound is a hydrogenated oil and the hydrogenated oil is WECOBEE^® M.

43. The tablet of claim 39 wherein the low melting point compound is a fatty acid ester and the fatty acid ester is one or more compounds selected from the group consisting of stearic acid ester, palmitic acid ester and myristyl lactate ester.

44. A placebo tablet comprising a low melting point compound that melts or softens at or below 37°C and a water-soluble excipient, wherein the low melting point compound comprises from about 2.5% to about 20% (wt/wt) of the composition and the tablet disintegrates in an oral cavity in 10 to 30 seconds.