Method of treating onychomycosis

Description

FIELD OF THE INVENTION

The present invention relates to methods of treating onychomycosis employing compositions with urea as the active ingredient. The present invention also finds new uses for urea as an antifungal agent. Onychomycosis refers to a fungal infection of the nail unit, defined as the nail matrix, bed or plate.

BACKGROUND OF THE INVENTION

Urea has been long recognized as a cosmetic ingredient in formulations acting as a humectant and moisturizer. High concentrations of urea, such as 40%, are also known to have mild, antibacterial effect. At these strengths the antibacterial effects are said to be similar to those of antibiotics, with the further advantage that all the common organisms are susceptible and the possibility of resistant strains need not be seriously considered. There have been reports of keratolytic activity attributed to urea with the ability at high concentrations to solubilize and denature protein. Dermatological compositions containing from 21 to 40 wt-% urea for treating dry scaly skin have been described in U.S. Pat. No. 5,919,470.

Concentrated solutions of urea can change the conformation of protein molecules. A striking effect is upon the water-binding capacity of the horny layer of the skin: pieces of normal horny layer, or scales from ichthyotic or psoriatic skin that have been soaked in 30% urea solution take up much more water. This is important because in maintaining the flexibility of the horny layer and the softness of the skin, the water content of the horny layer matters much more than its oil content.

Fungal infections of the nail are notoriously difficult to treat. Traditional, topical therapies cannot penetrate the nail plate, and eradicate the infection in and under the nail bed; they are useful only in milder forms of the disease. Systemic antifungal drug therapy is associated with potentially harmful side effects. Since oral antifungals are distributed throughout the entire body, systemic side effects such as elevated liver enzymes, gastrointestinal disorders and skin rashes are not uncommon and may require expensive medical intervention and laboratory tests.

Topical formulations for treating fungal infections, such as onychomycosis, have recently been described in U.S. Pat. No. 6,281,239B1. The method employs the use of a combination of a known antifungal agent and a tissue softening composition containing 30 to 60 wt-% urea.

SUMMARY OF THE INVENTION

The present invention relates to methods of treating onychomycosis employing compositions containing urea as the antifungal agent. The present invention relates to methods for treating onychomycosis in humans with urea. These methods include topically administrating to the nail area of a human a safe and effective amount of urea. Onychomycosis refers to a fungal infection of the nail unit, defined as the nail matrix, bed or plate.

Accordingly, the present invention is a method for treating onychomycosis by topically administering a safe and effect amount of urea in a pharmaceutically acceptable carrier.

DETAILED DESCRIPTION OF THE INVENTION

The present invention is a method for treating or preventing onychomycosis. Such method includes administering to the nail area of a human in need of such treatment or prevention, a safe and effective amount of urea, for example, from about 10 to 60 wt-%, preferably about 30-50 wt-%, and particularly about 40 wt-%.

The term “administering” as needed herein refers to any method which, in sound medical practice delivers the urea, e.g., 40% urea, to be treated in such a manner so as to be effective in the treatment of onychomycosis. Preferably, the urea is administered topically in a single composition.

The phrase “safe and effective amount”, as used herein, means an amount of urea sufficient enough to significantly and positively modify the condition to be treated but low enough to avoid serious side effects, within the scope of sound medical advice. The safe and effective amount of the urea of the present invention will vary with the particular condition being treated, the severity of the condition, the duration of treatment, the particular pharmaceutically acceptable carriers utilized, and the like factors within the knowledge and expertise of the attending physician.

The method of the present invention typically involve administering the urea in an amount to cover the affected area. The specific preferred quantity of the urea depends upon the nature of the fungus and other skin or nail conditions also present.

The method of the present invention typically involves administering urea in an amount to cover the affected area.

Thus for example, the dosing of the agents includes up to 720 days of administration of a pharmaceutical composition of the present invention.

For the method of the present invention, the duration of administration of the urea will vary according to the specific extent of the onychomycosis being treated, but typically is within the range of 90 to 210 days.

Topical Antifungal Agents

Typically, a topical antifungal agent consists of known naturally-occurring, synthetic or semi-synthetic composition, or mixture thereof, which is safe for use in the methods of the present invention, and is effective in killing or substantially inhibiting the growth of fungi, including but not limited to dermatophytes or yeast, Epidermophyton, Microsporum, Trichophyton and

Candida albicans,

and others.

Antifungal agents known to be useful for the treatment of onychomycosis include but are not limited to: topical creams, ointments, solutions, lacquers and gels containing as active agents, for example, amoroline, betadine, bifonazole, butenafine, clotrimazole, econazole nitrate, isoconazole, ketoconazole, miconazole nitrate, naftifine hydrochloride, oxiconazole, sulfanazole, terbinafine, ticonazole, tolnaftate, undecenoates and ciclopirox. The above antifungal topical compositions are known to those skilled in the art.

We have now surprisingly found urea to be an antifungal agent of equal potency to known antifungal agents. Urea was previously known as mentioned in the above Background section for its effectiveness for tissue softening and treating dry skin, without the need of traditional preservatives. Although there may have been some belief that urea had a mild antibacterial effect, nothing would have suggested that urea was an effective antifungal agent.

Thus, the present invention provides a method of treating onychomycosis in a topical composition containing urea as the sole active ingredient.

In addition to containing a therapeutically antifungal effective amount of urea, the composition includes dermatologically acceptable excipients as described in U.S. Pat. No. 5,919,470, which patent is incorporated herein by reference. The excipients particularly include skin protectants which include a combination of semi-solid and liquid petroleum fractions. The semi-solid skin protectant is contained in about 5.5 to about 20 wt-% and includes petrolatum or a synthetic or semi-synthetic hydrocarbon of the same nature as petrolatum. Mixtures of such ingredients can also be used. The preferred semi-solid material is petrolatum, commercially available from a wide variety of sources.

The liquid portion skin protectant is a liquid petrolatum and contained in the composition in about 10 to about 20 wt-%. This material can include any synthetic or semi-synthetic oleaginous liquid fraction. A preferred embodiment is mineral oil, which is a liquid mixture of hydrocarbons obtained from petroleum.

Another preferred ingredient encompassed in the composition of the present invention is propylene glycol which may be contained up to about 5 wt-% in the composition, preferably in the range of from about 1 to about 5 wt-%.

Various compositions, e.g. creams, lotions, and gels, containing urea as the sole active ingredient at various concentrations were tested against

Trychophyton rubrum

, a fungus typically implicated in

Moccasin tinea pedis

and onychomycosis, and compared to traditional antifungal compositions. A solution of the individual or combination products were inoculated with a known starting concentration of

T. rubrum

. These solutions were then retested at the specific time intervals to determine the residual microbial content. The decrease in observed microbial content was measured by standard serial dilution methods. The decrease in the residual microbial content calculated as a percentage of its initial starting concentration is the percent kill rate reported in the following table.

PERCENT KILL RATE

AT TIME INDICATED

“ACTIVE”

2

6

24

3

PRODUCT(S)

INGREDIENT(S)

HRS

HRS

HRS

DAYS

Carmol 40 Cream

40% Urea

93.6

99.5

98.2

>99.9

Loprox

0.77% Ciclopirox

No kill

No kill

91.0 >99.9

Loprox + Carmol 40

0.77% Ciclopirox +

99.8

>99.9

>99.9

>99.9

40% Urea

Carmol 40 Cream

40% Urea

Not tested

99.9

99.9

99.9

40% Urea

62.1

93.0

91.7

>99.9

40% Urea

99.7

>99.9

>99.9

>99.9

40% Urea

97.6

98.3

>99.9

>99.9

Carmol 40 Lotion

40% Urea

25.0

98.1

98.3

>99.9

Carmol 40 Gel

40% Urea

62.1

87.9

>99.9

>99.9

Carmol 20 Cream

20% Urea

69.2

68.7

91.2

>99.9

Carmol 10 Lotion

10% Urea

80.4

82.1

83.3

>99.9

Carmol Scalp

10% Sulfacetamide,

78.3

82.9

98.0

>99.9

Lotion

10% Urea

Miconazole

2% Miconazole

Not tested

>99.9

>99.9

>99.9

Nitrate

Miconazole &

2% Miconazole +

Not tested

>99.9

>99.9

>99.9

Carmol 40

40% Urea

Nizoral

2% Ketoconazole

40.0

No Kill

No Kill

75.0

Nizoral + Carmol 40

2% Ketoconazole +

79.0

55.0

83.0

98.1

40% Urea

Lotrimin

1% Clotrimazole

10.0

No Kill

No Kill

No Kill

Lotrimin + Carmol 40

1% Clotrimazole +

51.0

60.0

83.0

>99.9

40% Urea

Oxistat

1% Oxiconazole

88.0

96.0

99.0

>99.9

Oxistat + Carmol 40

1% Oxiconazole +

99.5

97.0

>99.9

>99.9

40% Urea

Mentax

1% Butenafine

99.6

99.9

>99.9

>99.9

Mentax + Carmol 40

1% Butenafine +

99.5

98.8

>99.9

>99.9

40% Urea

Spectazol

1% Econazole

No Kill

No Kill

85.0

>99.9

Spectazol + Carmol 40

1% Econazole +

No Kill

99.2

99.9

>99.9

40% Urea

The above tests indicate that urea is an effective antifungal agent.

Typical compositions employed in the present invention are for example:

Ingredient

Approximate Wt %

urea

40

petrolatum or a synthetic or semi-synthetic

5.5-20

hydrocarbon, or a semi-solid mixture thereof

liquid petrolatum or synthetic or semi-synthetic

10-20

oleaginous liquid fraction, or a mixture thereof

C

16-18

aliphatic straight or branched chain fatty

0.25-2

alcohol or fatty acid, or a mixture thereof

propylene glycol

1-5

glyceryl stearate

1-3

xanthan gum

0.01-0.5

water

balance

urea

30

petrolatum or a synthetic or semi-synthetic

5.5-20

hydrocarbon, or a semi-solid mixture thereof

liquid petrolatum or a synthetic or semi-synthetic

10-20

oleaginous liquid fraction, or a mixture thereof

C

16-18

aliphatic straight or branched chain fatty

0.25-2

alcohol or fatty acid, or a mixture thereof

propylene glycol

1-5

glyceryl stearate

1-3

xanthan gum

0.01-0.5

mixture of a carbomer and triethanolamine

0.05-30

water

balance

A typical formulation representing the particular and most preferred embodiment of the present invention is illustrated as follows:

Ingredient

% W/W

Purified water

36.149

Urea USP

40.000

Carbopol 940

0.150

Petrolatum

5.940

Mineral oil

12.060

Glyceryl stearate

1.875

Cetyl alcohol

0.626

Propylene glycol

3.000

Xanthan gum

0.050

Trolamine NF

0.150

TOTAL

100.000

Claims

1. A method of treating onychomycosis, comprising:administering to a nail area of a patient a composition consisting essentially of urea as the sole active ingredient and a dermatologically acceptable excipient selected from the group consisting of petrolatum or a synthetic or semi-synthetic hydrocarbon, or a semi-solid mixture thereof; a liquid petrolatum or a synthetic or semi-synthetic oleaginous liquid fraction, or a mixture thereof; a C16-18 aliphatic or branched chain fatty alcohol or fatty acid, or a mixture thereof; glyceryl stearate; xanthan gum; water; and optionally a mixture of a carbomer and triethanolamine, wherein the urea is present in an amount therapeutically effective for treating onychomycosis.
2. The method of claim 1, wherein the administering step is carried out by topically applying the composition.
3. The method of claim 1, wherein the urea is present from about 10 to about 60 wt-% urea.
4. The method of claim 1, wherein the urea is present from about 30 to about 50 wt-% urea.
5. The method of claim 1, wherein the urea is present from about 10 to about 40 wt-% urea.
6. The method of claim 1, wherein the composition is in a topical form selected from the group consisting of cream, ointment, solution, lacquer, gel, and foam.
7. The method of claim 3, wherein the composition is a gel.
8. The method of claim 1, wherein the urea is present in an amount of about 40 wt-% urea.
9. The method of claim 8, wherein the composition is a gel.

US Referenced Citations (8)

Number	Name	Date	Kind
4295567	Knudsen	Oct 1981	A
4581351	Berke et al.	Apr 1986	A
5340836	Reinhard et al.	Aug 1994	A
5407958	Heath et al.	Apr 1995	A
5573765	Reinhard et al.	Nov 1996	A
5853732	Munden	Dec 1998	A
5919470	Valdez et al.	Jul 1999	A
6281239	Glassman	Aug 2001	B1

Foreign Referenced Citations (1)

Number	Date	Country
WO 9619186	Jun 1996	WO

Non-Patent Literature Citations (2)

Entry
Aguado et al, Reaggrefation and binding of cell wall proteins from . . . , Database Caplus, AN:1998:463776, abstract, Research Microbiologia, 1998, Vol 149(5), 327-338.*
Friedman-Birnbaum et al., International Journal of Dermatology, 36(1), p 67-69 (abstract), 1977.

Method of treating onychomycosis

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Inventors

Original Assignees

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Agents

CPC

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US

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Abstract

Description

Claims

US Referenced Citations (8)

Foreign Referenced Citations (1)

Non-Patent Literature Citations (2)