TREA

SPRAYABLE ANALGESIC COMPOSITIONS

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Information

  • Patent Application
  • 20180271813
  • Publication Number
    20180271813
  • Date Filed
    November 04, 2015
    8 years ago
  • Date Published
    September 27, 2018
    5 years ago
Information
Abstract
A sprayable analgesic composition is an aqueous ethanolic solution which contains a nonsteroidal anti-inflammatory drug (NSAID), lauryl lactate, lactic acid, glyceryl monolaurate, propylene glycol and optionally an alkoxylated alcohol.
Description
FIELD OF INVENTION

This invention relates to analgesic compositions. More particularly, this invention relates to sprayable compositions containing nonsteroidal anti-inflammatory drugs.


BACKGROUND OF THE INVENTION

Nonsteroidal anti-inflammatory drugs (NSAIDs) are known medications with analgesic and antipyretic effects. NSAIDs are used to treat pain and discomfort such as muscle strain/sprain, fever, inflammation such as rheumatoid arthritis, joint pain, and the like.


The present invention provides topical dosage forms of NSAIDs that can be applied as a spray or as an aerosol.


SUMMARY OF INVENTION

A sprayable analgesic preparation contains a nonsteroidal anti-inflammatory drug (NSAID) together with lauryl lactate, lactic acid, and glyceryl monolaurate dissolved in a mixture of water and ethanol. The obtained aqueous ethanolic solution is useful for extended pain relief.


Optionally, the aqueous ethanolic solution can contain propylene glycol, a non-ionic surfactant having a HLB value of at least 12, and a thickener such as cellulose ethers, cross-linked alkyl acrylates, and the like.


Preferred NSAID's are the propionic acid derivatives ketoprofen, ibuprofen and naproxen, as well as the acetic acid derivatives diclofenac, indomethacin and etodolac.





BRIEF DESCRIPTION OF DRAWINGS

In the drawings,



FIG. 1 is a bar graph showing skin permeation by ketoprofen, applied as spray compositions, at selected time intervals after application, and comparison with a commercially available, ketoprofen-containing topical gel (Profenid® Sanofi-Aventis; 2.5% ketoprofen);



FIG. 2 is a bar graph showing skin permeation by naproxen, applied as spray compositions, at selected time intervals after application, and comparison with a commercially available naproxen-containing topical gel (Naprosyn®, Syntex, 10% naproxen free acid);



FIG. 3 is a bar graph showing skin permeation by ibuprofen, applied as a spray composition, at selected time intervals after application, and comparison with a commercially available ibuprofen-containing topical gel (Ibuleve®, DDD ltd., 5% ibuprofen);



FIG. 4 is a bar graph showing skin permeation by diclofenac, and pharmaceutically acceptable salts thereof, applied as spray compositions, and comparison with a commercially available diclofenac sodium gel (Swiss Relief™, Mika Pharma GmbH, Fug, Switzerland, 4% diclofenac sodium);



FIG. 5 is a bar graph showing the effect of propylene glycol on skin permeation in ibuprofen-containing spray compositions, and comparison with a commercially available ibuprofen-containing topical gel (Ibuleve®, DDD ltd., 5% ibuprofen);



FIG. 6 is a bar graph showing skin permeation by ketoprofen with Brij 58 as a permeation enhancer, applied as spray compositions, at selected time intervals after application, and comparison with a commercially available, ketoprofen-containing topical gel (Profenid®, Sanofi-Aventis; 2.5% ketoprofen);



FIG. 7 is a bar graph showing skin permeation by ketoprofen with propylene glycol laurate as a permeation enhancer, applied as spray compositions, at selected time intervals after application, and comparison with a commercially available, ketoprofen-containing topical gel (Profenid®, Sanofi-Aventis; 2.5% ketoprofen);



FIG. 8 is a bar graph showing skin permeation by ketoprofen with propylene glycol caprylate as a permeation enhancer, applied as spray compositions, at selected time intervals after application, and comparison with a commercially available, ketoprofen-containing topical gel (Profenid®, Sanofi-Aventis; 2.5% ketoprofen);



FIG. 9 is a bar graph showing skin permeation by ketoprofen with Sorbitan monolaurate as a permeation enhancer, applied as spray compositions, at selected time intervals after application, and comparison with a commercially available, ketoprofen-containing topical gel (Profenid®, Sanofi-Aventis; 2.5% ketoprofen);



FIG. 10 is a bar graph showing skin permeation by ketoprofen with various Brij derivatives as a permeation enhancer, applied as spray compositions, at selected time intervals after application, and comparison with a commercially available, ketoprofen-containing topical gel (Profenid®, Sanofi-Aventis; 2.5% ketoprofen);



FIG. 11 is a bar graph showing skin permeation by ketoprofen, applied as a spray composition after 3 months stored at 25° C. and 40° C., at selected time intervals after application, and comparison with a commercially available, ketoprofen-containing topical gel (Profenid®, Sanofi-Aventis; 2.5% ketoprofen);



FIG. 12 is a bar graph showing skin permeation by naproxen using 5% Naproxen sodium salt and Brij 58, applied as spray compositions, at selected time intervals after application, and comparison with a commercially available naproxen-containing topical gel (Naprosyn®, Syntex, 10% naproxen free acid);



FIG. 13 is a bar graph showing skin permeation by naproxen using 2.5% Naproxen sodium salt and Brij 58, applied as spray compositions, at selected time intervals after application, and comparison with a commercially available naproxen-containing topical gel (Naprosyn®, Syntex, 10% naproxen free acid);



FIG. 14 is a bar graph showing skin permeation by ibuprofen with and without isopropyl myristate (IPM), applied as spray compositions, at selected time intervals after application, and comparison with a commercially available ibuprofen-containing topical gel (Ibuleve®, DDD ltd., 5% ibuprofen);



FIG. 15 is a bar graph showing skin permeation by ibuprofen with isopropyl myristate (IPM) and Brij 58, applied as spray compositions, at selected time intervals after application, and comparison with a commercially available ibuprofen-containing topical gel (Ibuleve®, DDD ltd., 5% ibuprofen);



FIG. 16 is a bar graph showing skin permeation by diclofenac, and pharmaceutically acceptable salts thereof, applied as cream compositions, and comparison with a commercially available diclofenac sodium gel (Voltaren®, Novartis Pharma Productions GmbH, Wehr, Germany, 1% diclofenac sodium);



FIG. 17 is a bar graph showing skin permeation by diclofenac, and pharmaceutically acceptable salts thereof, applied as spray compositions, and comparison with a commercially available diclofenac sodium gel (Swiss Relief™, Mika Pharma GmbH, Fug, Switzerland, 4% diclofenac sodium);



FIG. 18 is a bar graph showing skin permeation by diclofenac sodium with Brij 58, and different levels of propylene glycol and lactic acid, applied as spray compositions, and comparison with a commercially available diclofenac sodium gel (Voltaren®, Novartis Pharma Productions GmbH, Wehr, Germany, 1% diclofenac sodium);



FIG. 19 is a bar graph showing skin permeation by diclofenac diethylamine with Brij 58, and different levels of propylene glycol and lactic acid, applied as spray compositions, and comparison with a commercially available diclofenac sodium gel (Voltaren®, Novartis Pharma Productions GmbH, Wehr, Germany, 1% diclofenac sodium); and



FIG. 20 is a bar graph showing skin permeation by ketoprofen compositions containing different levels of propylene glycol and hydroxypropyl cellulose thickeners.





DESCRIPTION OF PREFERRED EMBODIMENTS

The present topical compositions are clear, sprayable, aqueous ethanolic solutions that contain dissolved therein a nonsteroidal anti-inflammatory drug (NSAID). Preferred NSAIDs are the acetic acid derivatives such as indomethacin, sulindac, etodolac, tolmetin, ketorolac, nabumetone, diclofenac, and the like, including the pharmaceutically acceptable salts thereof, as well as the propionic acid derivatives such as ibuprofen, naproxen, fenoprofen, ketoprofen, flurbiprofen, oxaprozin, and the like, including the pharmaceutically acceptable salts thereof.


Illustrative NSAID salts suitable for use as active ingredients in the spray compositions are pharmaceutically acceptable salts of the aforementioned acetic acid derivatives, e.g., indomethacin salts such as indomethacin sodium, indomethacin meglumine, and the like, tolmetin salts such as tolmetin sodium, and the like, ketorolac salts such as ketorolac tromethamine, and the like, diclofenac salts such as diclofenac sodium, diclofenac diethylamine, diclofenac epolamine, and the like, as well as pharmaceutically acceptable salts of the aforementioned propionic acid derivatives, e.g., ibuprofen salts such as ibuprofen lysine, ibuprofen methylglucamine, and the like, naproxen salts such as naproxen piperazine, naproxen sodium, and the like, fenoprofen salts such as fenoprofen calcium, and the like.


Also suitable are NSAIDs such as aspirin, the enolic acid derivatives such as pizoxicam, meloxicam, tenoxicam, and the like, the fenamic acid derivatives such as mefenamic acid, meclofenamic acid, flufenamic acid, and the like, and selective COX-2 inhibitors such as celecoxib and the like, including the pharmaceutically acceptable salts thereof.


The aqueous ethanolic solutions preferably contain the NSAID in an amount in the range of about 1 to about 10 percent by weight preferably about 5 percent by weight, based on the total weight of the solution.


Also present in the solutions is lauryl lactate (C15H30O3), the ester of lauryl alcohol and lactic acid having the formula




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Preferably, lauryl lactate is present in the solution in an amount in the range of about 1 to about 5 weight percent, more preferably about 3 weight percent, based on the total weight of the solution.


The aqueous ethanolic solution also contains lactic acid (C3H6O3; 2-hydroxypropanoic acid), preferably in an amount in the range of about 0.5 to about 5 weight percent, more preferably about 1.5 weight percent, based on the total weight of the solution; glyceryl monolaurate (C15H30O4; dodecanoic acid 2,3-dihydroxypropyl ester), preferably in an amount in the range of about 2 to about 5 weight percent, more preferably about 3 weight percent, based on the total weight of the solution. Optionally, propylene glycol (C3H8O2; propane-1,2-diol) can be present, preferably in an amount in the range of about 5 to about 30 weight percent, more preferably about 10 weight percent, based on the total weight of the solution.


The remainder of the solution is constituted by water and ethanol, preferably present in a respective weight ratio of about 0.3:1 to about 2.6:1, more preferably in a respective weight ratio of about 1:1.


The aqueous ethanolic solution can also contain, as an optional ingredient, a non-ionic surfactant having a Hydrophile-Lipophile balance (HLB) value of at least 12. Preferred non-ionic surfactants are the alkoxylated alcohols. Particularly preferred is polyethylene glycol ether of cetyl alcohol represented by the formula CH3(CH2)14CH2(OCH2CH2)nOH, where n has an average of 10, and having a HLB value of about 15.7.


The foregoing clear aqueous ethanolic solutions are prepared by first combining the NSAID with lauryl lactate, lactic acid, and glyceryl monolaurate and thereafter dissolving the obtained admixture by gradual addition, at ambient temperature, of propylene glycol followed by the addition of alternating aliquots of water and ethanol. The non-ionic surfactant, if desired, is added to the admixture prior to the addition of water and ethanol.


Skin permeation studies of illustrative compositions embodying the invention were performed using dermatoned human female (46 years old) cadaver skin pieces from the back (Science Care, Aurora, Colo.; 250 Micrometers thick) Franz cells (3.65 ml volume, 0.55 cm2 surface area) at 35° C. using heating/stirring blocks. Receptor compartment contained saline with sodium azide (pH 7.4). Two or three replicates (25 μl and control 25 mg) were made for each solution. Sampling volume was 300 μl. Fresh buffer was replaced after each sample removal. Sampling was carried out at 2, 4, 6 and 24 hours. The samples were assayed using high performance liquid chromatography (HPLC).


Respective controls were NSAID containing gels: Profenid® gel (2.5% ketoprofen; Sanofi Aventis, France), Ibuleve® gel (5% ibuprofen; DDD Ltd., UK), Naprosyn® gel (10% naproxen free acid; Syntex, Turkey), Swiss Relief™ Spray Gel (4% diclofenac sodium) Mika Pharma GmbH, Switzerland), and Voltaren® gel (1% diclofenac sodium) Novartis Pharma Productions GmbH, Wehr, Germany.


The experimental results obtained with a ketoprofen spray composition are presented in Tables 1 and 2 below, and in FIG. 1.









TABLE 1







Ketoprofen Spray Composition









Composition, wt. %











Ingredients
KeS47
KeS73
KeS74
KeS75














Ketoprofen
5
5
5
5


Propylene glycol
10
10
10
10


Lauryl lactate
3
3
3
3


Lactic acid
1.5
1.5
1.5
1.5


Ceteth-201

3


Imwitor 4122


3


Capmul PG-83



3


Glyceryl monolaurate
3
3
3
3


Ethanol
37.5
27.25
39.5
34.5


Water
40
47.25
35
40


TOTAL
100
100
100
100






1CH3(CH2)14CH2(OCH2CH2)nOH, n average value 20; HLB 15.7; also Brij 58



2Propylene glycol laurate, HLB 4-5



3Propylene glycol monocaprylate, HLB 5-6













TABLE 2







Permeation Data









Cumulative Amount in Receptor, μg/cm2

















Time,








Profenid



hours
KeS47
±SD
KeS73
±SD
KeS74
±SD
KeS75
±SD
2.5%
±SD




















2
92.35
14.49
112.54
49.36
88.47
16.40
88.95
49.36
2.93
5.93


4
189.43
40.72
252.20
54.87
166.05
52.11
188.46
65.71
15.74
21.11


6
253.32
53.34
363.38
54.64
222.65
77.00
267.87
66.92
32.57
33.53









The above data show that spray compositions provided better skin permeation for ketoprofen than a ketoprofen containing gel composition, and that skin permeation could be further enhanced by an alkoxylated alcohol having an HLB value of 15.7.


The experimental results obtained with a naproxen spray composition are presented in Table 3 and 4 below, and in FIGS. 2.









TABLE 3







Naproxen Spray Composition









Composition, wt. %











Ingredients
NapS05
NapS05a
NapS20
Naprosyn ®














Naproxen



10


Naproxen Na
5
4.7
5


Propylene glycol
10
9.5
10


Lauryl lactate
3
2.8
3


Isopropyl myristate


3


Lactic acid
1.5
1.4
1.5


Ceteth-201

2.8
3


Glyceryl monolaurate
3
2.8
3


Ethanol
55.5
42.7
41.5


Water
22
33.2
30


TOTAL
100
100
100
















TABLE 4







Naproxen Permeation Data








Time,
Cumulative Amount in Receptor, μg/cm2















hours
NapS05
±SD
NapS05a
±SD
NapS20
±SD
Naprosyn ®
±SD


















2
78.92
37.94
68.91
0.54
64.42
11.20
1.65
0.28


4
206.15
65.01
187.63
11.82
187.47
15.16
9.67
1.17


6
293.37
81.72
277.23
23.83
292.88
38.90
20.38
2.42









The above data show that naproxen containing spray compositions provided better skin permeation for naproxen than the Naprosyn® 10% naproxen gel. The incorporation of higher levels of water did not reduce the permeation of naproxen.


The experimental results obtained with an ibuprofen spray composition are presented in Tables 5 and 6 below, and in FIG. 3. The experimental procedure was the same as that for the ketoprofen and naproxen spray compositions, except that the dermatomed cadaver skin was that of a human male, 72 years old.









TABLE 5







Ibuprofen Spray Composition










Composition, wt. %












Ingredients
Ibu17
Ibuleve ®















Ibuprofen
5
5



Lauryl lactate
3



Lactic acid
1.5



Glyceryl monolaurate
3



Ethanol
47.5



Water
40



TOTAL
100

















TABLE 6







Ibuprofen Permeation Data









Time,
Cumulative Amount in Receptor, μg/cm2












hours
Ibu17
±SD
Ibuleve ®
±SD














2
17.59
0.96
4.12
1.22


4
45.81
0.75
16.31
0.45


6
68.39
0.16
31.47
0.32









The above data show that an ibuprofen containing spray composition provided better skin permeation for ibuprofen than the Ibuleve® ibuprofen gel.


The experimental results obtained with a diclofenac spray composition are presented in Tables 7 and 8 below, and in FIG. 4. The experimental procedure was the same as that for the ketoprofen and naproxen spray compositions except that the dermatomed cadaver skin was that of a 79-year old human male.









TABLE 7







Diclofenac Spray Composition










Composition, wt. %











Ingredients
DcS02
DcS03
Swiss Relief ™













Diclofenac Na
1

44


Diclofenac diethylamine

1


Propylene glycol
10
10


Lauryl lactate
3
3


Lactic acid
1.5
1.5


Glyceryl monolaurate
3
3


Ethanol
48.5
48.5


Water
33
33


TOTAL
100
100






4Swiss Relief ™ spray gel contains 4 wt. % diclofenac sodium together with inactive ingredients isopropyl alcohol, soy bean lecithin, ethanol, disodium phosphate dodecahydrate, sodium dihodrogen phosphate dehydrate, sodium edetate, propylene glycol, peppermint oil, ascorbyl palmitate, hydrochloric acid (10% w/w), sodium hydroxide (10% w/w), purified water.













TABLE 8







Diclofenac Permeation Data









Cumulative Amount in Receptor, μg/cm2













Time,




Swiss Relief ™



hours
DcS-02
±SD
DcS-03
±SD
spray gel
±SD
















2
14.16
3.67
9.71
1.25
4.64
3.11


4
21.51
6.42
17.30
0.93
11.08
1.33


6
27.31
8.43
23.39
1.76
16.62
1.70









The above data show that a diclofenac containing spray composition provided better skin permeation for diclofenac than a spray gel composition that has a relatively larger concentration of diclofenac.


The effect of propylene glycol in an ibuprofen spray composition was investigated using cadaver skin from a 72 year-old human male. The experimental results are presented in Tables 9 and 10 below, and in FIG. 5.









TABLE 9







Ibuprofen Spray Compositions









Composition, wt. %












Ingredients
Ibu17
Ibu24
Ibuleve ®
















Ibuprofen
5
5
5



Propylene glycol

10



Lauryl lactate
3
3



Lactic acid
1.5
1.5



Glyceryl monolaurate
3
3



Ethanol
47.5
37.5



Water
40
40



TOTAL
100
100

















TABLE 10







Ibuprofen Permeation Data








Time,
Cumulative Amount in Receptor, μg/cm2













hours
Ibu17
±SD
Ibu24
±SD
Ibuleve ®
±SD
















2
20.22
5.59
19.36
12.52
7.17
12.42


4
69.45
5.95
71.08
27.82
8.65
1.80


6
127.06
2.01
138.70
35.68
20.97
8.20









The above data show that propylene glycol in the spray composition enhanced the skin penetration of ibuprofen.


The experimental results obtained with a ketoprofen spray composition and a nonionic surfactant, polyoxyethylene (20) cetyl ether (Brij 58), as a permeation enhancer are presented in Tables 11 and 12 below, and in FIG. 6.









TABLE 11







Ketoprofen and a Nonionic Surfactant Spray Composition









Composition, wt. %












Ingredients
KeS47
KeS61
KeS67
KeS73
KeS73a















Ketoprofen
5
5
5
5
5


Propylene glycol
10
10
10
10
10


Lauryl lactate
3
3
0
3
3


Lactic acid
1.5
1.5
1.5
1.5
1.5


Brij 581

3
3
3
3


Glyceryl monolaurate
3
0
3
3
3


Ethanol
37.5
37.5
37.5
27.25
25.25


Water
40
40
40
47.25
49.25


TOTAL
100
100
100
100
100
















TABLE 12







Permeation Data









Cumulative Amount in Receptor, μg/cm2

















Time,








Profenid



hours
KeS47
±SD
KeS61
±SD
KeS67
±SD
KeS73
±SD
2.5%
±SD




















2
92.35
14.49
84.55
25.06
71.71
49.49
112.54
49.36
15.60
5.93


4
189.43
40.72
186.97
15.02
182.54
64.55
252.20
54.87
70.75
21.11


6
253.32
53.34
267.88
3.95
275.99
47.09
363.38
54.64
134.62
33.53









The above data show that the addition of Brij 58 helped to increase water levels. All formulations exhibited similar permeation behavior; however, KeS73 showed slightly higher permeation. KeS73a was slightly cloudy.


The experimental results obtained with a ketoprofen spray composition and propylene glycol laurate as a permeation enhancer are presented in Tables 13 and 14 below, and in FIG. 7.









TABLE 13







Ketoprofen and Propylene Glycol Laurate Spray Composition









Composition, wt. %











Ingredients
KeS47
KeS62
KeS68
KeS74














Ketoprofen
5
5
5
5


Propylene glycol
10
10
10
10


Lauryl lactate
3
3
0
3


Lactic acid
1.5
1.5
1.5
1.5


Propylene glycol laurate

3
3
3


Glyceryl monolaurate
3
0
3
3


Ethanol
37.5
42.5
42.5
39.5


Water
40
35
35
35


TOTAL
100
100
100
100
















TABLE 14







Permeation Data









Cumulative Amount in Receptor, μg/cm2













Time,




Profenid



hours
KeS47
±SD
KeS74
±SD
2.5%
±SD
















2
92.35
14.49
88.47
16.40
15.60
5.93


4
189.43
40.72
166.05
52.11
70.75
21.11


6
253.32
53.34
222.65
77.00
134.62
33.53









Only formulations KeS47 and KeS74 gave clear solutions. The above data show that the KeS47 and KeS74 formulations exhibited nearly the same permeation behavior.


The experimental results obtained with a ketoprofen spray composition and propylene glycol caprylate as a permeation enhancer are presented in Tables 15 and 16 below, and in FIG. 8. The experimental procedure was the same as that for the previous ketoprofen spray compositions, except that the dermatomed cadaver skin was that of a human male, 79 years old.









TABLE 15







Ketoprofen and Propylene Glycol Caprylate Spray Composition









Composition, wt. %











Ingredients
KeS47
KeS63
KeS69
KeS75














Ketoprofen
5
5
5
5


Propylene glycol
10
10
10
10


Lauryl lactate
3
3
0
3


Lactic acid
1.5
1.5
1.5
1.5


Propylene glycol caprylate

3
3
3


Glyceryl monolaurate
3
0
3
3


Ethanol
37.5
37.5
37.5
34.5


Water
40
40
40
40


TOTAL
100
100
100
100
















TABLE 16







Permeation Data









Cumulative Amount in Receptor, μg/cm2

















Time,








Profenid



hours
KeS47
±SD
KeS63
±SD
KeS69
±SD
KeS75
±SD
2.5%
±SD




















2
77.12
12.81
64.90
9.02
57.22
10.33
58.98
10.81
2.27
0.44


4
140.68
16.03
144.77
13.15
131.23
21.40
128.25
34.31
13.60
2.05


6
183.17
22.46
198.59
10.20
184.99
21.11
172.43
52.30
21.69
4.50









The above data show that all of the formulations exhibited comparable permeation behavior.


The experimental results obtained with a ketoprofen spray composition and Sorbitan monolaurate as a permeation enhancer are presented in Tables 17 and 18 below, and in FIG. 9. The experimental procedure was the same as that for the previous ketoprofen spray compositions, except that the dermatomed cadaver skin was that of a human male, 79 years old.









TABLE 17







Ketoprofen and Sorbitan Monolaurate Spray Composition









Composition, wt. %











Ingredients
KeS47
KeS66
KeS72
KeS78














Ketoprofen
5
5
5
5


Propylene glycol
10
10
10
10


Lauryl lactate
3
3
0
3


Lactic acid
1.5
1.5
1.5
1.5


Sorbitan monolaurate

3
3
3


Glyceryl monolaurate
3
0
3
3


Ethanol
37.5
57.5
57.5
34.5


Water
40
20
20
40


TOTAL
100
100
100
100
















TABLE 18







Permeation Data









Cumulative Amount in Receptor, μg/cm2













Time,




Profenid



hours
KeS47
±SD
KeS78
±SD
2.5%
±SD
















2
77.12
12.81
45.37
4.10
2.27
0.44


4
140.68
16.03
101.16
16.60
13.60
2.05


6
183.17
22.46
137.44
27.22
21.69
4.50









Only formulations KeS47 and KeS78 gave clear solutions. The above data show that permeation from KeS78 was slightly lower than KeS47.


The experimental results obtained with a ketoprofen spray composition and various Brij derivatives as a permeation enhancer are presented in Tables 19 and 20 below, and in FIG. 10. The experimental procedure was the same as that for the previous ketoprofen spray compositions, except that the dermatomed cadaver skin was that of a human male, 79 years old.









TABLE 19







Ketoprofen and Non-ionic Surfactant Spray Composition









Composition, wt. %













Ingredients
KeS73
KeS79
KeS80
KeS81
KeS82
KeS83
















Ketoprofen
5
5
5
5
5
5


Propylene
10
10
10
10
10
10


glycol


Lauryl lactate
3
3
3
3
3
3


Lactic acid
1.5
1.5
1.5
1.5
1.5
1.5


Brij 581
3


Brij 305

3


Brij 356


3


Brij 727



3


Brij 988




3


Brij 7219





3


Glyceryl
3
3
3
3
3
3


monolaurate


Ethanol
27.25
27.25
27.25
27.25
27.25
27.25


Water
47.25
47.25
47.25
47.25
47.25
47.25


TOTAL
100
100
100
100
100
100






5poly(oxyethylene)(4) lauryl ether



6poly(oxyethylene)(23) lauryl ether



7poly(oxyethylene)(2) stearyl ether



8poly(oxyethylene)(20) oleyl ether



9poly(oxyethylene)(21) stearyl ether













TABLE 20







Permeation Data









Cumulative Amount in Receptor, μg/cm2





















Time,












Profenid



hours
KeS73
±SD
KeS79
±SD
KeS80
±SD
KeS81
±SD
KeS82
±SD
KeS83
±SD
2.5%
±SD
























2
58.92
11.11
53.39
10.39
54.79
13.75
61.91
16.23
67.06
20.54
59.12
6.21
7.15
0.42


4
138.70
11.05
125.49
22.77
125.93
21.40
141.07
30.91
139.71
32.62
134.15
17.36
21.66
1.94


6
185.84
18.67
176.90
31.52
171.52
24.45
191.21
38.25
189.49
39.15
178.84
23.19
37.41
3.53









The above data show that all formulations containing the non-ionic surfactants permitted higher water content while showing similar behavior with respect to permeation.


The experimental results showing permeation of a ketoprofen spray composition after storage for three (3) months at 25° C. and 40° C. is presented in Tables 21 and 22 below, and in FIG. 11. The experimental procedure was the same as that for the previous ketoprofen spray compositions, except that the dermatomed cadaver skin was from the thigh of a human male, 79 years old.









TABLE 21







Ketoprofen Spray Composition










Composition, wt. %












Ingredients
KeS38/25° C.
KeS38/40° C.















Ketoprofen
5
5



Lauryl lactate
3
3



Lactic acid
1.5
1.5



Glyceryl monolaurate
3
3



Ethanol
47.5
47.25



Water
40
40



TOTAL
100
100

















TABLE 22







Permeation Data









Cumulative Amount in Receptor, μg/cm2













Time,




Profenid



hours
KeS38/25° C.
±SD
KeS38/40° C.
±SD
2.5%
±SD
















2
85.61
35.14
72.35
7.44
6.97
1.23


4
178.97
66.42
154.72
19.61
25.34
3.96


6
251.24
89.44
220.46
29.64
45.35
6.86









The above data show that both formulations exhibited similar permeation behavior after three months of storage.


The experimental results obtained with a naproxen spray composition using 5% Naproxen sodium and Brij 58 are presented in Table 23 and 24 below, and in FIG. 12. The experimental procedure was the same as that for the previous spray compositions, except that the dermatomed cadaver skin was from the thigh of a human male, 79 years old.









TABLE 23







Naproxen Spray Composition Using 5%


Naproxen Sodium and a Non-ionic Surfactant









Composition, wt. %












Ingredients
NapS05
NapS21a
NapS22a
NapS23a
NapS24















Naproxen
0
0
0
0
0


Naproxen Na
5
5
5
5
5


Propylene glycol
10
10
10
10
10


Lauryl lactate
3
3
3
3
3


Lactic acid
1.5
0.5
3
0.5
3


Brij 581

0
0
3
3


Glyceryl
3
3
3
3
3


monolaurate







Ethanol
55.5
34.5
46
30
47


Water
22
44
30
45.5
26


TOTAL
100
100
100
100
100
















TABLE 24







Naproxen Permeation Data








Time,
Cumulative Amount in Receptor, μg/cm2















hours
NapS05
±SD
NapS21a
±SD
NapS23a
±SD
Naprosyn ®
±SD


















2
60.77
16.57
44.92
14.84
22.70
18.23
1.67
2.90


4
139.90
28.22
101.66
22.94
52.91
36.06
2.37
4.10


6
186.06
27.93
147.81
27.39
77.01
48.09
3.61
6.25









The above data show that by decreasing the level of water and lactic acid, formulations with higher levels of ethanol were prepared. Reduction in lactic acid and addition of Brij 58 resulted in lower skin permeation. A precipitate was noted in NapS22a and NapS24.


The experimental results obtained with a naproxen spray composition using 2.5% Naproxen sodium and Brij 58 are presented in Table 25 and 26 below, and in FIG. 13. The experimental procedure was the same as that for the previous spray compositions, except that the dermatomed cadaver skin was from the thigh of a human male, 79 years old.









TABLE 25







Naproxen Spray Composition Using 2.5% Naproxen Sodium and a Non-ionic Surfactant









Composition, wt. %














Ingredients
NapS05
NapS25
NapS25a
NapS26
NapS26a
NapS27
NapS28

















Naproxen
0
0
0
0
0
0
0


Naproxen Na
5
2.5
2.5
2.5
2.5
2.5
2.5


Propylene glycol
10
10
10
10
10
10
10


Lauryl lactate
3
3
3
3
3
3
3


Lactic acid
1.5
0.5
0.5
1.5
1.5
0.5
1.5


Brij 581

3
3
3
3
0
0


Glyceryl monolaurate
3
3
3
3
3
3
3


Ethanol
55.5
22
32
37
40
36
45


Water
22
56
46
40
37
45
35


TOTAL
100
100
100
100
100
100
100









A precipitate was noted in NapS05, NapS25, NapS26 and NapS28.









TABLE 26







Naproxen Permeation Data








Time,
Cumulative Amount in Receptor, μg/cm2

















hours
NapS05
±SD
NapS25a
±SD
NapS26a
±SD
NapS27
±SD
Naprosyn ®
±SD




















2
60.77
16.57
26.05
7.07
43.55
1.01
34.57
11.52
1.67
2.90


4
139.90
28.22
57.48
16.40
79.99
7.85
83.28
17.65
2.37
4.10


6
186.06
27.93
82.19
21.96
104.69
8.99
119.11
23.73
3.61
6.25









The above data show that reduction of Naproxen levels to 2.5% caused a significant reduction in skin permeation.


The effect of isopropyl myristate in an ibuprofen spray composition was investigated. The experimental results are presented in Tables 27 and 28 below, and in FIG. 14. The experimental procedure was the same as that for the previous spray compositions, except that the dermatomed cadaver skin was from the thigh of a human male, 79 years old.









TABLE 27







Ibuprofen with and without Isopropyl Myristate Spray Compositions










Composition,




wt. %












Ingredients
Ibu24
Ibu30














Ibuprofen
5
5



Propylene glycol
10
10



Isopropyl myristate
0
3



Lauryl lactate
3
3



Lactic acid
1.5
1.5



Glyceryl monolaurate
3
3



Ethanol
37.5
39.5



Water
40
35



TOTAL
100
100
















TABLE 28







Ibuprofen with and without Isopropyl Myristate Permeation Data








Time,
Cumulative Amount in Receptor, μg/cm2













hours
Ibu24
±SD
Ibu30
±SD
Ibuleve ®
±SD
















2
177.88
34.92
149.67
43.10
53.86
36.32


4
324.99
58.07
271.38
62.99
129.82
74.30


6
415.42
62.34
344.02
61.75
177.62
89.78









The above data show that addition of isopropyl myristate in the spray composition did not further enhance the skin permeation of ibuprofen.


The effect of isopropyl myristate and Brij 58 in an ibuprofen spray composition was investigated. The experimental results are presented in Tables 29 and 30 below, and in FIG. 15. The experimental procedure was the same as that for the previous spray compositions, except that the dermatomed cadaver skin was from the back of a human male, 46 years old.









TABLE 29







Ibuprofen with Isopropyl Myristate and Brij 58 Spray Compositions









Composition, wt. %












Ingredients
Ibu30
Ibu32
Ibu33















Ibuprofen
5
5
5



Propylene glycol
10
10
10



Isopropyl myristate
3
0
3



Lauryl lactate
3
3
3



Lactic acid
1.5
1.5
1.5



Brij 581

3
3



Glyceryl monolaurate
3
3
3



Ethanol
39.5
28
31.5



Water
35
46.5
40



TOTAL
100
100
100
















TABLE 30







Ibuprofen Permeation Data









Cumulative Amount in Receptor, μg/cm2















Time, hours
Ibu30
±SD
Ibu32
±SD
Ibu33
±SD
Ibuleve ®
±SD


















2
58.28
27.72
47.79
10.56
33.70
17.05
7.06
3.27


4
127.23
21.44
117.41
18.49
93.08
25.68
50.52
17.68


6
193.89
9.97
187.01
36.12
159.15
43.60
106.53
28.78









The above data show that addition of Brij 58 helped to increase the level of water in the formulation; however, the addition of isopropyl myristate and Brij 58 in the spray composition did not further enhance the skin permeation of ibuprofen.


The effects of two types of diclofenac were investigated. The experimental results obtained with a diclofenac cream composition using diclofenac sodium and diclofenac diethylamine are presented in Tables 31 and 32, below, and in FIG. 16. The dermatomed cadaver skin was from the back of a human male, 79 years old.









TABLE 31







Diclofenac Cream Composition










Composition, wt. %












Ingredients
Dc-05
Dc-07














Diclofenac Na
1




Diclofenac diethylamine

1



Carbopol 980 NF10
0.5
0.5



Ultrez 1011
1
1



Deionized water
63.95
63.95



Disodium EDTA
0.05
0.05



Isopropyl myristate
3
3



Ethanol
10
10



Propylene glycol
10
10



Isopropanol
9
9



Triethanolamine, NF
1.5
1.5



TOTAL
100
100






10acrylic acid homopolymer



11cross-linked polyacrylic acid polymer













TABLE 32







Diclofenac Permeation Data








Time,
Cumulative Amount in Receptor, μg/cm2













hours
Dc-05
±SD
Dc-07
±SD
Voltaren 1%
±SD
















2
1.94
1.95
1.70
2.95
0.00
0.00


4
6.28
2.27
6.62
4.46
3.70
0.70


6
10.10
2.85
10.60
5.96
6.13
1.14









The above data show that skin permeation for diclofenac sodium and diclofenac diethylamine cream formulations was similar.


The experimental results obtained with a diclofenac spray composition using diclofenac sodium and diclofenac diethylamine are presented in Tables 33 and 34, below, and in FIG. 17. The experimental procedure was the same as that for the previous spray compositions, except that the dermatomed cadaver skin was from the back of a human male, 79 years old.









TABLE 33







Diclofenac Spray Composition










Composition, wt. %












Ingredients
DcS02
DcS03














Diclofenac Na
1




Diclofenac diethylamine

1



Propylene glycol
10
10



Lauryl lactate
3
3



Lactic acid
1.5
1.5



Glyceryl monolaurate
3
3



Ethanol
48.5
48.5



Water
33
33



TOTAL
100
100
















TABLE 34







Diclofenac Permeation Data









Cumulative Amount in Receptor, μg/cm2













Time,




Swiss Relief ™



hours
DcS-02
±SD
DcS-03
±SD
spray gel
±SD
















2
9.29
1.06
9.98
4.16
0
0


4
17.69
1.30
18.91
6.47
2.57
0.93


6
23.43
1.38
25.33
7.99
4.31
1.44









The above data show that a diclofenac containing spray composition provided better skin permeation for diclofenac than a spray gel composition that has a relatively larger concentration of diclofenac.


The effects of propylene glycol, Brij 58 and lactic acid on diclofenac skin permeation were investigated. The experimental results obtained with a diclofenac spray composition using diclofenac sodium, Brij 58, and different levels of propylene glycol and lactic acid are presented in Tables 35 and 36, below, and in FIG. 18. The experimental procedure was the same as that for the previous spray compositions, except that the dermatomed cadaver skin was from the thigh of a human male, 79 years old.









TABLE 35







Diclofenac Spray Composition









Composition, wt. %













Ingredients
DcS02
DcS12
DcS12a
DcS14
















Diclofenac Na
1
1
1
1



Propylene glycol
10
15
10
10



Lauryl lactate
3
3
3
3



Lactic acid
1.5
1.5
1.5
0.5



Brij 581

3
3
3



Glyceryl
3
3
3
3



monolaurate







Ethanol
48.5
25
43.5
34.5



Water
33
53.5
35
45



TOTAL
100
100
100
100









Composition DcS12 was cloudy.









TABLE 36







Diclofenac Permeation Data









Cumulative Amount in Receptor, μg/cm2















Time hours,
DcS02
±SD
DcS12a
±SD
DcS14
±SD
Voltaren 1%
±SD


















2
5.98
2.94
5.97
3.42
2.47
2.17
0.00
0.00


4
16.33
6.10
14.68
5.39
7.24
6.34
3.36
1.11


6
25.37
8.82
22.33
6.67
11.52
10.23
7.10
1.33









Addition of a higher level of propylene glycol enhanced the water content but caused formulation DcS12 to precipitate. The above data show that a diclofenac spray composition with a lower level of lactic acid showed a lower level of skin permeation of diclofenac.


The effects of propylene glycol, Brij 58 and lactic acid on diclofenac skin permeation were investigated. The experimental results obtained with a diclofenac spray composition using diclofenac diethylamine, Brij 58, and different levels of propylene glycol and lactic acid are presented in Tables 37 and 38, below, and in FIG. 19. The experimental procedure was the same as that for the previous spray compositions, except that the dermatomed cadaver skin was from the thigh of a human male, 79 years old.









TABLE 37







Diclofenac Spray Composition









Composition, wt. %













Ingredients
DcS03
DcS13
DcS13a
DcS13a-2
DcS15
DcS15a
















Diclofenac
1
1
1
1
1
1


diethylamine


Propylene
10
15
10
15
10
10


glycol


Lauryl
3
3
3
3
3
3


lactate


Lactic acid
1.5
1.5
1.5
1.5
0.5
0.5


Brij 581
0
3
3
3
3
3


Glyceryl
3
3
3
3
3
3


monolaurate


Ethanol
48.5
23
38
45
26
39.5


Water
33
55.5
40.5
28.5
53.5
40


TOTAL
100
105
100
100
100
100









Compositions DcS13, DcS13a and DCS15 were cloudy.









TABLE 38







Diclofenac Permeation Data









Cumulative Amount in Receptor, μg/cm2















Time, hours
DcS03
±SD
DcS13a-2
±SD
DcS15a
±SD
Voltaren 1%
±SD


















2
5.99
2.58
4.84
3.56
3.42
0.79
0.00
0.00


4
14.39
6.54
11.65
5.16
10.00
1.87
3.36
1.11


6
21.60
9.52
17.61
6.29
16.14
3.04
7.10
1.33









Formulations DcS13, DcS13a, and DcS15 were cloudy. The above data show that incorporation of Brij 58 reduced skin permeation of diclofenac.


The effects of propylene glycol and thickeners on ketoprofen skin permeation were investigated. The experimental results obtained with a ketoprofen spray formulation using ketoprofen, different levels of propylene glycol, and thickeners hydroxypropyl cellulose (100 cps) and hydroxypropyl cellulose (150-400 cps) are presented in Tables 39 and 40, below and in FIG. 20. The experimental procedure was the same as that for the previous spray compositions, except that the dermatomed cadaver skin was from the thigh of a human male, 79 years old.









TABLE 39







Ketoprofen and Thickeners Spray Composition









Composition, wt. %












Ingredients
KeS47
KeS84
KeS85
KeS86
KeS89















Ketoprofen
5
5
5
5
5


Propylene glycol
10
20
20
10
10


Lauryl lactate
3
3
3
3
3


Lactic acid
1.5
1.5
1.5
1.5
1.5


HPC HY11712
0
0
0.5
0.5
0


HPC HY11913
0
0
0
0
0.25


Glyceryl monolaurate
3
3
3
3
3


Ethanol
37.5
27.5
27.5
32.5
32.25


Water
40
40
39.5
44.5
45


TOTAL
100
100
100
100
100






12hydroxypropyl cellulose (100 cps)



13hydroxypropyl cellulose (150-400 cps)













TABLE 40







Permeation Data









Cumulative Amount in Receptor, μg/cm2



















Time,










Profenid



hours
KeS47
±SD
KeS84
±SD
KeS85
±SD
KeS86
±SD
KeS89
±SD
2.5%
±SD






















2
82.63
27.60
94.36
51.62
104.05
13.26
80.82
22.75
117.71
21.55
12.75
3.00


4
167.45
34.34
221.64
118.40
213.69
37.65
157.90
42.69
221.11
6.86
42.43
5.90


6
232.80
42.90
309.28
144.22
311.38
48.99
214.48
57.66
290.61
25.07
71.36
8.79









All formulations above gave clear solutions. The above data show that KeS84, KeS85, and KeS89 all exhibited significant permeation enhancement compared to KeS47. KeS86, with lower propylene glycol, showed similar permeation to KeS47.


The foregoing discussion and the examples are to be taken as illustrative, but not limiting. Still other variants within the spirit and scope of the invention are possible, and will readily present themselves to those skilled in the art.

Claims
  • 1. A sprayable solution which comprises a nonsteroidal anti-inflammatory drug (NSAID); lauryl lactate; lactic acid; glyceryl monolaurate; ethanol; and water.
  • 2. The sprayable solution in accordance with claim 1 wherein the NSAID is a propionic acid derivative.
  • 3. The sprayable solution in accordance with claim 1 wherein the NSAID is a propionic acid derivative selected from the group consisting of ketoprofen, ibuprofen, naproxen, and pharmaceutically acceptable salts thereof.
  • 4. The sprayable solution in accordance with claim 1 wherein the NSAID is an acetic acid derivative.
  • 5. The sprayable solution in accordance with claim 1 wherein the NSAID is an acetic acid derivative selected from the group consisting of diclofenac, indomethacin, etodolac, and pharmaceutically acceptable salts thereof.
  • 6. The sprayable solution in accordance with claim 1 further comprising a non-ionic surfactant having an HLB value of at least 12.
  • 7. The sprayable solution in accordance with claim 6 wherein the non-ionic surfactant is an alkoxylated alcohol.
  • 8. The sprayable solution in accordance with claim 1 wherein the NSAID is ketoprofen.
  • 9. The sprayable solution in accordance with claim 1 wherein the water:ethanol weight ratio is in the range of about 0.3:1 to about 2.6:1.
  • 10. The sprayable solution in accordance with claim 1 wherein the lauryl lactate is present in an amount in the range of about 1 to about 5 weight percent, based on the total weight of the solution.
  • 11. A sprayable clear solution which comprises, based on total weight of the solution, a nonsteroidal anti-inflammatory drug (NSAID) in an amount in the range of about 1 to about 10 weight percent, lauryl lactate in an amount in the range of about 1 to about 5 weight percent,lactic acid in an amount in the range of about 0.5 to about 5 weight percent;glyceryl monolaurate in an amount in the range of about 2 to about 5 weight percent;propylene glycol in an amount in the range of about 5 to about 30 weight percent;alkoxylated alcohol having a HLB value of at least 12 in an amount in the range of 0 to about 7 percent; andthe remainder a mixture of water and ethanol in a respective weight ratio in the range of about 0.3:1 to about2.6:1.
  • 12. The sprayable clear solution in accordance with claim 11 which comprises about 5 weight percent ketoprofen; about 3 weight percent lauryl lactate;about 1.5 weight percent lactic acid;about 3 weight percent glyceryl monolaurate;about 3 weight percent polyethylene glycol ether of cetyl alcohol having a HLB value of about 15.7 and represented by the formula CH3(CH2)14CH2(OCH2CH2)nOH where n has an average value 20;about 10 weight percent propylene glycol; and the remainder a water-ethanol mixture in a respective weight ratio of about 1.7.
CROSS-REFERENCE TO RELATED APPLICATION

This application claims the benefit of U.S. Provisional Application No. 62/077,581, filed on Nov. 10, 2014, which is incorporated herein by reference in its entirety.

PCT Information
Filing Document Filing Date Country Kind
PCT/US2015/058927 11/4/2015 WO 00
Provisional Applications (1)
Number Date Country
62077581 Nov 2014 US