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Orodispersible tablets

a technology of oral administration and tablets, applied in the direction of tablets, digestive system, metabolism disorders, etc., can solve the problems of reducing economic and energetic manufacturing costs, unpleasant taste, and reducing patient compliance, and achieves low friability, high mechanical resistance, and low resistance

Inactive Publication Date: 2016-10-27
LAB LESVI SL
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Benefits of technology

[0021]The authors of the present invention have surprisingly found that a formulation based on a dry powdered mixture comprising up to 15% by weight, at least 50% by weight of a diluent and a disintegrant, allows preparing orodispersible tablets by direct compression, with disintegration times very similar to those obtained using more complex techniques. In fact, the orodispersible tablets can be disintegrated in the mouth cavity in less than 15 seconds, having also a high mechanical resistance, a low friability and higroscopicity, which involve important advantages with respect to other technologies which require preparing tablets with low resistance and high porosity in order to get short disintegration times.
[0022]Direct compression provides important advantages over other complex techniques since the active ingredient is not subjected to humidity conditions (water or other solvents) or to high temperatures, conditions which are known to diminish the stability of the oral formulation. In addition, due to its simplicity, it only requires simple machinery leading to a reduction in economic and energetic manufacturing costs.
[0023]Unlike other typical formulations used in direct compression, which are not only rather expensive but also very coarse and granular in nature resulting in a coarse dispersion in the mouth, the formulation used in the invention to prepare the orodispersable tablets provides an improved palatability. This technical feature is mainly derived from the incorporation of calcium silicate as excipient which avoids the remaining excipients to agglutinate forming agglomerates which render difficult the dispersion of the tablet in the mouth leading to an unpleasant taste and therefore to a diminished patient compliance.
[0024]Furthermore, one of the main advantages conferred by this formulation is the possibility of providing tablets with a thickness less than 30% of its major diameter, thus favouring the disintegration in the mouth and also improving the palatability. These features make even easier the administration of active ingredients to patients who have difficulty in swallowing. In addition, since the amount of calcium silicate is very low, it is also possible to elaborate tablets with a high content of active ingredient, without affecting the final size of the tablet.
[0030]Moreover, the inventors have found that by incorporating an effervescent component in the formulation, an even higher improvement in the palatability of the tablets is achieved. Consequently, the formulation of the invention can further comprise an effervescent component.

Problems solved by technology

In addition, due to its simplicity, it only requires simple machinery leading to a reduction in economic and energetic manufacturing costs.
This technical feature is mainly derived from the incorporation of calcium silicate as excipient which avoids the remaining excipients to agglutinate forming agglomerates which render difficult the dispersion of the tablet in the mouth leading to an unpleasant taste and therefore to a diminished patient compliance.

Method used

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Examples

Experimental program
Comparison scheme
Effect test

example 1

[0064]Orodispersible tablets were made according to the method defined below using the formulation having the ingredients shown in table I:

TABLE Img% (w / w) 1. Olanzapine10.00 mg 12.50%  2. Lactose monohydrate54.61 mg 68.26%  3. Hydroxypropylcellulose3.20 mg4.00%low-substituted 4. Crospovidone2.40 mg3.00% 5. Calcium silicate7.20 mg9.00% 6. Aspartame1.07 mg1.33% 7. Banana Flavor0.16 mg0.20% 8. Orange Flavor0.16 mg0.20% 9. Colloidal anhydrous silica0.40 mg0.50%10. Magnesium stearate0.80 mg1.00%Total  80 mg 100%

Manufacturing Method

[0065]The orodispersible tablet was obtained according to the following procedure:[0066]a) the components of the formulation were weighted;[0067]b) components 4 and 5 were sieved through a screen with a mesh size of 0.5-0.6 mm;[0068]c) the materials of stage “b” were mixed in a suitable container until a homogeneous mixture was obtained;[0069]d) components 1, 2, 3, 6, 7, 8 and 9 were sieved through a screen with a mesh size of 0.5-0.6 mm;[0070]e) the materials...

example 2

[0078]The tablet was prepared according to the procedure described below using the formulation having the ingredients shown in table II:

TABLE IImg% (w / w) 1. Olanzapine10.00 mg 13.33%  2. Lactose monohydrate40.98 mg 54.63%  3. Hydroxypropylcellulose3.00 mg4.00%low-substituted 4. Crospovidone3.00 mg4.00% 5. Calcium silicate9.00 mg12.00%  6. Aspartame1.00 mg1.33% 7. Calcium carbonate3.00 mg4.00% 8. Tartaric acid3.75 mg5.00% 9. Banana Flavor0.15 mg0.20%10. Colloidal anhydrous silica0.38 mg0.50%11. Magnesium stearate0.75 mg1.00%Total  75 mg 100%

Manufacturing Method

[0079]The orodispersible table was obtained according to the following procedure:[0080]a) components of the formulation were weighted;[0081]b) components 4 and 5 were sieved through a screen with a mesh size of 0.5-0.6 mm;[0082]c) the materials of stage “b” were mixed in a suitable container until a homogeneous mixture has been obtained;[0083]d) components 1, 2, 3, 6, 7, 8, 9 and 10 were sieved through a screen with a mesh size...

example 3

[0087]The tablet was prepared according to the procedure described below using the formulation having the ingredients shown in table III:

TABLE IIIPR-42mg% (w / w)1. Zolmitriptan2.52.772. Mannitol granular73.4581.613. Crospovidone4.554. Calcium silicate6.375. Aspartame0.916. Orange Flavour0.917. Strawberry Flavour0.10.118. Magnesium Stearate1.351.5Total90100

Manufacturing Method

[0088]The orodispersible table was obtained according to the following procedure:[0089]a) the components of the formulation were weighted;[0090]b) component 1, enough amount of 2 to achieve a homogeneous mixture, 3 and 4 were sieved through a screen with a mesh size of 0.5-0.6 mm;[0091]c) the materials of stage “b” were then mixed together in a suitable container until a homogeneous mixture was obtained;[0092]d) the rest of component 2, and components 5, 6, and 7 were sieved through a screen with a mesh size of 0.5-0.6 mm;[0093]e) the materials of stage “d” were mixed together in a suitable container until a homo...

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Abstract

This invention relates to a an orally disintegrating tablet obtainable by direct compression of a dry powdered mixture, said mixture comprising up to 15% by weight of calcium silicate, at least 50% of a diluent, a disintegrant agent and an active ingredient. It also relates to a process for preparing the tablets by homogeneous blending the specific excipients in powder form and subsequent direct compression of the mixture. Said tablets disintegrate quickly in the cavity of the mouth, in particular in less than 15 seconds.

Description

FIELD OF THE INVENTION[0001]The present invention relates to solid pharmaceutical formulations, in particular it relates to a tablet for oral administration which disintegrates rapidly by the action of saliva in the oral cavity, having also good palatability, friability, mechanical strength properties and employing a conventional manufacturing method to obtain them.BACKGROUND OF THE INVENTION[0002]The development of solid formulations that disintegrate quickly in the mouth without requiring water are very interesting due to the advantages that these pharmaceutical formulations provide for patients who have difficulty in swallowing, such as old people, infants, patients with mental problems and non-cooperative patients, as well as the population in general; since it makes it possible for the drug to be administered without the need for water. Moreover, since the formulation disintegrates inside the mouth, the drug may be absorbed in the oral, pharyngeal and gastrointestinal regions. ...

Claims

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Application Information

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Patent Type & Authority Applications(United States)
IPC IPC(8): A61K31/4196A61K9/20A61K31/519A61K31/4178A61K31/422A61K31/5513A61K9/00A61K9/46
CPCA61K31/4196A61K9/0056A61K9/2095A61K9/2009A61K9/0007A61K31/519A61K9/2027A61K9/2054A61K31/4178A61K31/422A61K31/5513A61K9/2018A61K31/551A61P1/00A61P3/06A61P3/10A61P7/02A61P9/00A61P9/12A61P11/06A61P15/00A61P15/10A61P25/00A61P25/06A61P25/18A61P25/20A61P25/22A61P25/24A61P29/00A61P31/12A61K9/2013A61K9/2072
Inventor BEDA PEREZ, CARMEND EZ MART N, IGNACIOPABLO ALBA, PABLO
Owner LAB LESVI SL
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