TREA

A NOVEL PHARMACEUTICAL COMPOSITION OF A LIPID LOWERING COMPOUND

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Information

  • Patent Application
  • 20190142741
  • Publication Number
    20190142741
  • Date Filed
    June 07, 2017
    7 years ago
  • Date Published
    May 16, 2019
    5 years ago
Information
Abstract
The present invention provides liquid oral dosage form of lipid lowering agent suitable for oral administration to human or animals.
Description
FIELD OF THE INVENTION

The present invention is related to liquid oral dosage form of lipid lowering compound preferably statin products suitable for oral administration.


BACKGROUND OF THE INVENTION

Statins are HMG-CoA reductase inhibitors, a class of drug used to lower the cholesterol level by inhibiting HMG-CoA reductase. Currently available in the market either as tablets, capsules, or solutions for injection. An individual may have difficulty swallowing the usual solid dosage form, and daily injections are difficult to administer. For children, dose management is difficult if tablet to cut or crush because of no accuracy of dose. Based on that a patent application US20120270933 claims liquid solution comprising statin and at least one solubilizer with statement that liquid statin formulation are not available due to poor solubility or insolubility


Still using solubilizer there is an increase in the unknown impurity. So to avoid this in the present invention solubilizer is avoided.


OBJECT OF INVENTION

The primary objective of present invention is to provide liquid oral dosage form of lipid lowering compound.


Another objective of present invention is to provide oral suspension/solution having dose flexibility for patients who need special doses of the drug and have difficulties in swallowing oral dosage forms.


Still another objective of present invention is to provide oral suspension/solution with improved taste having high patient compliance.


It is yet another objective of present invention to provide process of preparation of oral suspension/solution of statin products suitable for oral administration.


It is yet another objective of present invention to provide oral suspension/solution of atorvastatin products suitable for oral administration and process for preparation thereof without use of stabilizer and buffering agent.


SUMMARY OF THE INVENTION

The present invention provides liquid oral dosage form of lipid lowering agent, statin suitable for oral administration to human or animals. These formulations are useful for administration of the lowest dose of statin for treatment of high cholesterol level and any diseases due to high cholesterol. This liquid oral dosage form formulation statins include atorvastatin, simvastatin, rosuvastatin etc. a preferred is atorvastatin.







DETAIL DESCRIPTION OF THE INVENTION

The present invention relates to suspension of statin products suitable for oral administration to humans or animals.


Statins are HMG-CoA reductase inhibitors, used for the treatment of high cholesterol level or any disease due to high cholesterol level in human and animals. Currently available doses of statins are either as tablets, capsules, or solutions for injection. Present invention is liquid oral dosage form of statin for oral administration without use of solubilizerand/or a stabiliser such as an antioxidant. Formulation of present invention is useful even to administer the lowest dose of the composition.


This liquid oral dosage form formulation statins include atorvastatin, simvastatin, rosuvastatin etc. wherein preferred is atorvastatin.


Statins are known for poor aqueous solubility and stability but present invention provides dosage form without use of stabilizer, buffering agent and optionally solubilizer.


Common formula of present invention comprises statin between of 0.1 and 5% and at least one suspending agent between 0.2 and 6%. In addition the composition comprises viscosity modifier, sweetener, flavors, colors, preservatives and water.


In a preferred form of present invention excipients used can be selected from vehicle, co-solvent, preservative, sweetener, chelating agent, buffer, flavoring agent and sweetness/flavor enhancing agent.


Vehicles used in pharmaceutical formulations are mainly liquid bases which carries drugs and other excipients in dissolved or dispersed state. Pharmaceutical vehicles are of two types:

    • 1) Aqueous vehicles
    • 2) Oily vehicles


Aqueous vehicles can be selected from but not limited to purified water, hydro-alcoholic, polyhydric alcohols and buffers, while oily vehicles can be selected from vegetable oils, oils, organic oily bases or emulsified bases.


Co-solvents are used to increase solubility of drugs that show low solubility in water. It is also used to improve viscosity, taste and flavor. Co-solvent system comprises of solvents selected from but not limited to propylene glycol, glycerin, alcohol, polyhydric alcohol and water for injection which is used alone or in combination.


Preservatives are included in pharmaceutical solutions to control the microbial bioburden of the formulation having broad spectrum of antimicrobial activity, must be chemically and physically stable over the shelf-life of the product and have low toxicity. Preservative can be selected from group but not limited to alcohol, benzyl alcohol, chlorobutol, chlorocresol, alkyl esters of paraben, phenol, phenyl ethanol, sodium benzoate, antimicrobial solvents like propylene glycol, chloroform.


Sweetener can be selected from but not limited to sucrose, liquid glucose, glycerol, sorbitol, saccharin sodium, sucrose and aspartame to impart sweetness to the formulation.


Chelating agent is used for drug stabilization, to maintain potency of active ingredients and to stabilize colors and flavors. Chelating agent can be selected from but not limited to citric acid monohydrate, disodium edetate, dipotassium edetate, edetic acid, fumaric acid, malic acid, phosphoric acid, sodium edetate, tartaric acid and trisodium edetate.


pH of the formulation is between 5 and 10 can be controlled and optimize the physicochemical performance of the formulation by using base or buffer can be selected from but not limited to sodium acetate, sodium hydroxide, sodium citrate, sodium phosphate and disodium phosphate.


Flavouring agents are mainly use to increase the palatability and enhance the aesthetic qualities of the formulation. Flavouring agent can be selected but not limited to oil based flavouring agent such as essential oils including peppermint oil, orange oil, lemon oil etc.


In aspect of present invention, oral pharmaceutical solution of atorvastatin is formulated which comprises of an active ingredient, atorvastatin and other excipients selected from vehicle, co-solvent, preservative, sweetener, chelating agent, buffer, flavouring agent and sweetness/flavour enhancing agent, wherein pH of formulation is maintained between 5 and 10, more particularly between 6 and 9.


Oral liquid composition without use of stabilizer, buffering agent and optionally solubilizer can be oral suspension or oral solution.


Examples

The present invention can be described by way of example or strategy only. It is to be recognized that modifications falling within the scope and spirit of the description or claims, which would be obvious to a person skilled in the art based upon the disclosure herein, are also considered to be included within the scope of this disclosure.


Composition is general for oral liquid dosage form of statin is as under:














Sr.
Ingredients for Statin Oral



No.
Solution
Range (% w/w)







1.
Active Ingredient
  2-10%


2.
Solubilizer
0.0-15%


3.
Co-solvent
0.0-15%


4.
Suspending agent
0.0-10%


5.
Complexing agent
 0-5%


6.
Sweetner
  0-50%


7.
Flavor
0.0-2% 


8.
Surfactant
 0.0-0.2%


9.
Vehicle
0.0-95%









For the composition of atorvastatin 1 mg/ml, drug and excipients with its range are shown below in table:












Strategy I & II


With antioxidant and without antioxidant










Sr.

STRATEGY I
STRATEGY II


No.
Ingredients
20 mg/5 ml
20 mg/5 ml













1
Atorvastatin
20.00
20.00


2
Propylene Glycol
250.00
250.00


3
Carboxymethyl cellulose
33.33
33.33



sodium


4
Magnesium Aluminium silicate
66.67
66.67


5
Butylatedhydroxyanisole
0.00
2.00


6
Purified water
qs 5 ml
qs 5 ml









Manufacturing Process for (Strategy I)





    • 1. Sodium Carboxymethyl Cellulose were slowly added in 30% W/W purified water and stir well till clear solution was obtained.

    • 2. Dispensed quantity of Magnesium Aluminium silicate was added in step 1, additional 20% w/w a purified water add in Step 1 and stir well till all solid mass was get mixed properly i.e. homogeneously dispersed.

    • 3. API was added into propylene glycol and mixed properly where solubilizer was used. This mixture was added in to step 2 and stirred through simple stirrer properly to get homogenized suspension.

    • 4. Add 50% w/w of remaining purified water for makeup the suspension.





Manufacturing Process for (Strategy II)





    • 1 Sodium Carboxymethyl Cellulose were slowly added in 30% W/W purified water and stir well till clear solution was obtained.

    • 2 Dispensed quantity Magnesium Aluminium silicate was added in STEP 1, additional 20% w/w a purified water add in Step 1 and stir well till all solid mass was get mixed properly at i.e. homogeneously dispersed RPM (600-800).

    • 3 BHA and API was added into propylene glycol and mixed properly where solubilizer was used. This mixture was added in to step 2 and stirred through simple stirrer properly to get homogenized suspension.

    • 4 Add remaining purified water for makeup the suspension





Result achieved for strategy I and II based on stability are as under:















Trial









Stability
Strategy I
Strategy II













condition
Initial
25° C./60% RH
40 C./75% RH
Initial
25° C./60% RH
40° C./75% RH





Impurity A
0.05%
0.02%
0.02%
0.05%
0.02%
0.05%


Impurity C
0.01%
ND
ND
ND
ND
ND


Impurity D
0.02%
0.01%
0.01%
0.03%
0.01%
0.01%


Lactone
0.03%
 0.1%
0.06%
0.04%
0.05%
0.05%


Ester
ND
ND
ND
ND
ND
ND


Unknown
0.08%
0.15%
1.40%
0.12%
0.63%
1.10%


Impurities
(RRT0.74)
(RRT0.80)
(RRT0.80)
(RRT0.74)
(RRT0.80)
(RRT0.80)


Total
0.53%
0.42%
 2.1%
0.42%
1.00%
 1.7%


Impurities









Conclusion:

On based of 3M 25° C./60% RH, impurity profile of Strategy I & Strategy II, antioxidant having no effective role.


Based on the results achieved with or without use of stabilizer, we have also tried for avoiding buffering agent as described in strategy III and IV along with avoiding stabilizing agent.












Strategy III & IV


With buffering agent without buffering agent












STRATEGY
STRATEGY


Sr.
Ingredients for Atorvastatin Oral
III
IV


No.
Suspension
20 mg/5 ml
20 mg/5 ml













1.
Atorvastatin
20.00
20.00


2.
Carboxymethyl cellulose sodium
33.33
33.33


3.
Magnesium Aluminium silicate
66.66
66.66


4.
Sucralose
50.00
50.0


5.
Acesulfame K
5.00
5.0


6.
Methyl parahydroxybenzoate
5
5


7.
Ethyl parahydroxybenzoate
1
1


8.
Potassium Di-Hydrogen Phosphate
0.959



9.
Di-potassium Hydrogen Phosphate
0.078



10.
Orange flavour
15.0
15.0



Purified water
Up to 5 ml
Up to 5 ml









Manufacturing Process for Strategy III





    • 1. 50% w/w Purified water was heated till the temperature reached to 80-90° C.





Dispensed quantity of Methyl parahydroxybenzoate and Ethyl parahydroxybenzoate was added in to this and stirred to get clear solution. Cool down solution at room temperature.

    • 2. Add sucralose, Acesulfame K in step 1, stir well till clear solution.
    • 3. Sodium Carboxymethyl Cellulose were slowly added in step 1, stir well till clear viscous solution.
    • 3 Magnesium Aluminium silicate were add in step 2 stir well till all solid mass was get mixed properly i.e. homogeneously dispersed.
    • 4 Add and disperse Atorvastatin in 10% w/w purified water in separate vessel mix properly for 30 min, with high speed homogenization.
    • 5 Step 4 is add in step 3, mix well through simple stirrer till get homogenized suspension.
    • 6 Add Potassium Di-Hydrogen Phosphate, Di-potassium Hydrogen Phosphate in 20% w/w purified water, add slowly in step 5 to achieve pH 6.0-9.0
    • 7 Add flavour in step 6.
    • 8 Add purified water and makeup the volume.


Manufacturing Process for Strategy IV





    • 1 50% w/w Purified water was heated till the temperature reached to 80-90° C. Dispensed quantity of Methyl parahydroxybenzoate (E218) and Ethyl parahydroxybenzoate (E214) was added in to this and stirred to get clear solution. Cool down solution at room temperature.

    • 2 Add sucralose, Acesulfame K in step 1, stir well till clear solution.

    • 3 Sodium Carboxymethyl Cellulose were slowly add in step 1, stir well till clear viscous solution.

    • 4 Magnesium Aluminium silicate were add in step 2 stir well till all solid mass was get mixed properly i.e. homogeneously dispersed.

    • 5 Add and disperse Atorvastatin in 10% w/w purified water in separate vessel mix properly for 30 min i.e. homogeneously dispersed.

    • 6 Step 4 is add in step 3, mix well through simple stirrer and get homogenize medium i.e. homogeneously suspension.

    • 7 Add flavour in step 6.

    • 8 Add purified water and makeup the volume.





The results we achieved for strategy III and IV are as under:















Trial










Strategy III
Strategy IV











3 M

3 M













Stability condition
Initial
25° C./40% RH
40 C./25% RH
Initial
25° C./40% RH
40 C./25% RH












%













Impurity A
ND
0.07
0.07
0.04
0.06
0.06


Impurity C
ND
ND
ND
ND
ND
ND


Impurity D
0.03
0.04
0.05
0.06
0.02
0.02


Lactone
0.05
0.08
0.11
0.18
0.1 
0.08


Ester
ND
ND
ND
ND
ND
ND


Unknown Impurities
0.05
0.25
0.76
0.07
0.09
0.12



(0.81RRT)
(0.78RRT)
(0.78 RRT)
(0.80 RRT)
(0.79 RRT)
(0.79 RRT)


Total Impurities
0.1 
0.62
1.4 
0.57
0.44
0.44









Conclusion:

Based on 3M 25° C./40% RH & 3M 40° C./25% RH impurity profile of Strategy III & Strategy IV, stabilizer buffering agent is having partial or no effective role.


Strategy V












For effective homogenization.











STRATEGY V


Sr. No.
Ingredients for Atorvastatin Oral Suspension
20 mg/5 ml












1.
Atorvastatin
20.00


2.
Carboxymethyl cellulose sodium
33.33


3.
Magnesium Aluminium silicate
66.66


4.
Sucralose
50.00


5.
Acesulfame K
5.00


6.
Methyl parahydroxybenzoate
5


7.
Ethyl parahydroxybenzoate
1


8.
Orange flavour
15.0


9.
Purified water
Up to 5 ml









Manufacturing Process for Strategy V





    • 1 50% w/w Purified water was heated till the temperature reached to 80-90° C. Dispensed quantity of Methyl parahydroxybenzoate (E218) and Ethyl parahydroxybenzoate (E214) was added in to this and stirred to get clear solution. Cool down solution at room temperature.

    • 2 Add sucralose, Acesulfame K in step 1, stir well till clear solution.

    • 3 90% quantity of Sodium Carboxymethyl Cellulose were slowly add in step 1, stir well till clear viscous solution.

    • 4 Magnesium Aluminium silicate were add in step 2 stir well till all solid mass was get mixed properly i.e. homogeneously dispersed.

    • 5 In a separate vessel take 10% v/v of purified water and remaining qty of sodium carboxymethyl cellulose and disperse Atorvastatin. Homogenize through high speed for 30 min, achieve particle size d90 1 micron-15 micron.

    • 6 Step 5 is add in step 4, mix well through simple stirrer and get homogenize medium i.e. homogeneously suspension.

    • 7 Add flavour in step 6.

    • 8 Add purified water to make up and homogenize through high speed for 45 min.





Trial Results:

Based on the homogenization trials, final formulation with different particle size distribution was evaluated with Reference marketed product (Lipitor 40 mg Film coated tablet) at a dose of 40 mg per volunteer. And the results of the bio equivalence (BE) study is as mentioned below:












BE STUDY I: Formulation particle size (D90-22.39 μm)









Pharma-




cokinetic
Ln-transformed
90%


Pa-
Geometric Least Squares Mean
ConfidenceInterval











rameters
TestProduct
ReferenceProduct
T/R
(Parametric)












(Units)
(T)
(R)
(%)
Lower
Upper















Cmax
36.1290
53.2937
67.79
52.49
87.56


(ng/mL)


AUC0-t
164.7519
176.0092
93.60
86.32
101.50


(ng · hr/


mL)



















BE STUDY II: Formulation particle size (D90-6.02 μm)









Pharma-




cokinetic
Ln-transformed
90%


Pa-
Geometric Least Squares Mean
ConfidenceInterval











rameters
TestProduct
ReferenceProduct
T/R
(Parametric)












(Units)
(T)
(R)
(%)
Lower
Upper















Cmax
55.6268
61.7538
90.08
63.43
127.92


(ng/mL)


AUC0-t
212.8483
215.5457
98.75
82.91
117.61


(ng · hr/


mL)









Conclusion:

Based on above data, (a) stabilizer and buffering agent have partial or no effective role and (b) suitable particle size of API in finished product to get bioequivalent product, can be achieved from effective homogenization


Observation from Study 2:


The ratios of geometric least squares means of test product (T) and reference product (R) for Ln-transformed pharmacokinetic parameters (Cmax and AUC0-t) of atorvastatin were found to be 67.79 and 93.60%, respectively for formulation strategy IV (homogenized product with API particle size D90=22.39 μm), which is not within acceptable range of 90.00-110.00%.


The ratios of geometric least squares means of test product (T) and reference product (R) for Ln-transformed pharmacokinetic parameters (Cmax and AUC0-t) of atorvastatin were found to be 90.08% and 98.75% respectively, which is in between range of 90.00-110.00% for formulation strategy V (homogenized product with API particle size D90=6.02 μm). Furthermore, the 90% confidence intervals for the ratio of geometric least squares means for Ln-transformed pharmacokinetic parameter AUC0-t is within the acceptable bioequivalence interval of 80.00-125.00%, while that of Cmax is not within the acceptable bioequivalence interval of 80.00-125.00% due to limited number of subjects and lower power of the study. By adding more number of subjects and higher power in the study, the 90% confidence intervals for the ratio of geometric least squares means for Ln-transformed pharmacokinetic parameter Cmax may be within the acceptable bioequivalence interval of 80.00-125.00%.


From the study it was concluded that effective homogenization-particle size reduction method is required to produce the product having comparative pharmacokinetic profile to Innovator product (Lipitor).


The same strategy and manufacturing process can be applicable to all HMG-CoA reductase inhibitors like simvastatin, rosuvastatin.


Further, formulation trials were also tried for atorvastatin oral solution without using stabilising and buffering agent. Few strategies are mentioned below:












Atorvastatin oral solution









STRATEGY













Ingredients for
I
II
III
IV


Sr.
Atorvastatin Oral
20 mg/
20 mg/
20 mg/
20 mg/


No.
Solution
5 ml
5 ml
5 ml
5 ml















1.
Atorvastatin
20.00
20.0
20.0
20.00


2.
Propylene glycol
250

150



3.
Ethanol


5% v/v
20% v/v


4.
HPBCD



400


5.
Sorbitol solution
300
300
300
300


6.
Peppermint flavor
0.5
0.5

0.5


7.
Orange flavor

0.5
0.5



8.
Polysorbat 80
1
3




9.
Glycerine
Up to 5 ml


Up to 5 ml


10
Purified water

Up to 5 ml
Up to 5 ml










Manufacturing Process Strategy I





    • 1. Add atorvastatin in Propylene glycol mix well till clear solution obtained.

    • 2. Add sorbitol solution in 50% v/v of total quantity of glycerine mix well to obtain homogeneous mixture.

    • 3. Add step 2 in to step 1 mix well.

    • 4. Add polysorbate 80 in step 3 to obtain clear viscous solution.

    • 5. Add peppermint in step 4 and mix well till homogeneous solution obtained.

    • 6. Make up the volume with glycerine pH of solution (4.0-7.0)





Manufacturing Process Strategy II





    • 1 Add atorvastatin in purified water mix well than add polysorbate 80 and mix well till clear solution obtain.

    • 2 Add sorbitol solution in Step 1 stir well till clear solution.

    • 3 Add Orange flavor in step 2 stir well till clear solution.

    • 4 Make up the volume with purified water pH of solution (5.0-9.0)





Manufacturing Process Strategy III





    • 1 Add atorvastatin in ethanol mix well in separate vessel.

    • 2 Add propylene glycol in step 1 till clear solution obtain.

    • 3 Add sorbitol solution in 50% purified water in separate vessel mix well to obtain homogeneous mixture

    • 4 Add Orange flavor in step 3 stir well till clear solution.

    • 5 Step 1 add in step 4 stir well till clear solution obtain.

    • 6 Make up the volume with purified water. Ph of solution (5.0-8.0)





Manufacturing Process Strategy IV





    • 1 Add atorvastatin in ethanol mix well in separate vessel.

    • 2 Add HPBCD in step 1 stir well till complete complex is formed.

    • 3 Add sorbitol solution in 50% purified water in separate vessel mix well to obtain homogeneous mixture.

    • 4 Add peppermint flavor in step 3 stir well till clear solution.

    • 5 Step 1 add in step 4 stir well till clear solution obtain.

    • 7 Make up the volume with glycerine. pH of solution (4.0-7.0)





The same strategy can be applicable to all other HMG-CoA reductase inhibitors like simvastatin, rosuvastatin, etc.

Claims
  • 1-10. (canceled)
  • 11. A suspension suitable for oral administration comprising a statin, at least one suspending agent, at least one preservative and water, wherein the suspension does not include a solubilizer, an antioxidant, or a buffering agent.
  • 12. The suspension of claim 11, wherein the statin is selected from the group consisting of atorvastatin, rosuvastatin, simvastatin, or a combination thereof.
  • 13. The suspension of claim 11, wherein the at least one suspending agent is selected from the group consisting of sodium carboxymethyl cellulose, magnesium aluminum silicate, or a combination thereof.
  • 14. The suspension of claim 11, wherein the at least one preservative is selected from the group consisting of alcohol, benzyl alcohol, chlorobutol, chlorocresol, alkyl esters of paraben, phenol, phenyl ethanol, sodium benzoate, propylene glycol, chloroform, methyl parahydroxybenzoate, ethyl parahydroxybenzoate, or a combination thereof.
  • 15. The suspension of claim 11, further comprising at least one of the following: a sweetener, flavoring, or a combination thereof.
  • 16. The suspension of claim 15, wherein the sweetener is selected from the group consisting of glycerol, sucrose, liquid glucose, sorbitol, saccharin sodium, aspartame, sucralose, acesulfame K, or a combination thereof.
  • 17. The suspension of claim 15, wherein the sweetener is in an amount of 0.1% w/w to 2% w/w.
  • 18. The suspension of claim 15, wherein the flavoring is in an amount of 0.01% w/w to 2% w/w.
  • 19. The suspension of claim 11, wherein the suspending agent is in an amount of 0.2% w/w to 6% w/w.
  • 20. The suspension of claim 11, wherein the preservative is in an amount of 0.01% w/w to 0.5% w/w.
  • 21. The suspension of claim 11, wherein the statin is in an amount of 0.1% w/w to 2% w/w.
  • 22. The suspension of claim 11, wherein the D90 of the statin particles are less than 50 microns.
  • 23. The suspension of claim 11, wherein the D90 of the statin particles are less than 10 microns.
  • 24. The suspension of claim 11, wherein the pH of the suspension is 6.0 to 9.0.
  • 25. A method of lowering high cholesterol levels in a human or animal, comprising administering the suspension of claim 11.
  • 26. A suspension for oral administration comprising 0.1%-2% w/w of atorvastatin, 0.2%-6% w/w of a suspending agent, 0.01%-0.5% of a preservative, and water; wherein the suspension does not include a solubilizer, an antioxidant, or a buffering agent.
  • 27. The suspension of claim 26, wherein the pH of the suspension is 6.0 to 9.0.
  • 28. A method of lowering high cholesterol levels in a human or animal, comprising administering the suspension of claim 26.
Priority Claims (1)
Number Date Country Kind
201621019719 Jun 2016 IN national
PCT Information
Filing Document Filing Date Country Kind
PCT/IB2017/053348 6/7/2017 WO 00