Creams containing vitamin D3 derivatives

Drug – bio-affecting and body treating compositions – Preparations characterized by special physical form – Cosmetic – antiperspirant – dentifrice

Reexamination Certificate

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Details

C514S167000, C514S168000, C424S078030

Reexamination Certificate

active

06432422

ABSTRACT:

FIELD OF THE INVENTION
The present invention relates to O/W type creams for skin application, which creams exhibit improved skin transfer and physical/chemical stability of maxacalcitol as an active ingredient, more specifically, the present invention relates to O/W type creams in which maxacalcitol as an active ingredient exists in the oil phase and/or water phase.
BACKGROUND ART
Some classes of vitamin D
3
derivatives such as 1&agr;,3&bgr;-dihydroxy-20&agr;-(3-hydroxy-3-methylbutyloxy)-9,10-seco-5,7,10(19)-pregnatriene (22-oxa-1&agr;,25-dihydroxitamin D
3
; herein also referred to as maxacalcitol) have been reported to have epidermal cell growth-inhibiting and differentiation-inducing effects and to be useful as antipsoriatics (JPA Nos. 267550/86 and 183534/88). In development of dosage forms of antipsoriatics, preparations for topical application are thought to be preferable because the target site of antipsoriatic therapy is epidermal cells.
However, no formulation for topical application containing maxacalcitol as an active ingredient and having excellent performance has been reported to date.
DISCLOSURE OF THE INVENTION
Preparations for topical application may be presented in such dosage forms as ointments, creams or lotions. Dosage forms vary with the application site. Ointments are applied on the whole body, especially under clothing, creams are applied on parts exposed to the air such as the face or the hands, and lotions are applied to the scalp or the like. Especially, creams which are exposed to the air are required to have benefits such as non-tackiness after application and inconspicuous appearance at the treated site.
In the development of creams as one dosage fom for topical application, O/W type creams containing a large amount of water in an outer water phase are thought to be most advantageous for seeking such benefits as non-tackiness after application and inconspicuous appearance at the treated site. O/W type creams containing maxacalcitol as an active ingredient may include two types depending on whether the active ingredient exists in the oil phase or the water phase.
Maxacalcitol is known to be scarcely soluble in water and to be unstable in aqueous solutions; it is also known to be highly soluble and have dramatically improved stability in organic solvents such as ethanol and chloroform and also to have very high stability in base materials such as petrolatum. Therefore, O/W type creams containing maxacalcitol in an inner oil phase have been supposed to be preferable for maintaining an advantageous creamy form and for stably containing the active ingredient maxacalcitol.
However, it is also important in development of creams to ensure chemical stability of the active ingredient, as well as physical stability of the emulsion. It is regarded that the physical stability of the emulsion depends on the concentrations of surfactants and co surfactants; as both concentrations become higher and as the ratio of the concentrations becomes closer to a proper value, more stable emulsification is achieved.
As for skin absorption of the active ingredient, the following are regarded as contributing to low skin absorption of the active ingredient:
1) high affinity of maxacalcitol for the oil phase base material, 2) low delivery or access rate of oil phase to skin, and 3) inhibition release of the maxacalcitol from the oil phase during transfer of maxacalcitol to skin. More specifically, transfer of maxacalcitol to skin may be inhibited by the presence of surfadctants and cosurfacatants at the oil/water interface or the presence of crystalline structures around oil-phase particles. Namely, when a drug is contained in the inner oil phase, the surfactant phase existing at the oil/water interface or the crystalline structures existing around the oil-phase particles during the release process may hinder the release of the drug.
In order to eliminate the above disadvantages and enhance skin transfer by removing rate-limiting factors during the release process, we tried to develop a cream containing the drug maxacalcitol in the outer water phase and concurrently a cream containing maxacalcitol in the oil phase.
As described above, an object of the present invention is to provide a cream maintaining a creamy form, showing high skin absorption of the active ingredient maxacalcitol and stably maintaining said active ingredient for a long time-period.
As a result of careful studies conducted to find a cream showing high skin absorption of the active ingredient maxacalcitol and stably maintaining said active ingredient for a long time-period, we obtained the following findings. In O/W type creams wherein maxacalcitol exists in the oil phase, stability of the emulsion dramatically improved, however the skin transfer rate of the active ingredient decreased when the concentrations of surfactants and cosurfactants increased. In order to increase the skin transfer rate, it seemed necessary to decrease those factors which are regarded to be responsible for the absorption inhibition, in other words, the amount of surfactants existing at the oil/water interface or the amount of crystalline structures produced around oil-phase particles. Thus, we attempted to decrease the loading of surfactants and cosurfactants in so far as a stable emulsion would be maintained. As a result, we found that an excellent cream is provided when the total concentration of surfactants and cosurfactants in the cream is within the range of from 2 to 7% by weight. We also found that absorption can be controlled by incorporation of maxacalcitol in the oil phase, whereby an optimal level in skin can be maintained. A part of the present invention was accomplished on the basis of these findings.
As a result of careful studies to improve the skin absorption and the storage stability of creams containing maxacalcitol in the water phase, we also found that a homogeneous dispersion of maxacalcitol in the outer water phase ensures the storage stability of maxacalcitol and also remarkably improves the skin absorption to approximately twice as compared with creams containing maxacalcitol in the inner oil phase. A part of the present invention was accomplished on the basis of these findings.
As described above, we accomplished the present invention on the basis of the findings that incorporating maxacalcitol in the water phase can remarkably improve absorption and that incorporating maxacalcitol in the oil phase can control absorption.
Moreover, we also found that the maxacalcitol level in skin can be controlled over a wide range, from low to high levels, by incorporation of maxacalcitol in both of oil and water phases.
Accordingly, the present invention provides an O/W type cream containing maxacalcitol in the oil phase and/or water phase.
According to an aspect of the present invention, there is provided an O/W type cream containing maxacalcitol and an emulsifier, wherein maxacalcitol exists in the oil phase.
In creams of the present invention, the emulsifier is preferably a mixture of a surfactant and a cosurfactant.
In creams of the present invention, the ratio between surfactants and cosurfactants is preferably within the range of from 1:1 to 1:11.
In creams of the present invention, the total concentration of surfactants and cosurfactants in a cream is preferably within the range of from 2 to 7% by weight.
In creams of the present invention, the surfactant is preferably an ether-type surfactant.
In creams of the present invention, the surfactant is more preferably a polyoxyethylene alkyl ether.
In creams of the present invention, the cosurfactant is preferably a higher alcohol.
In creams of the present invention, the cosurfactant is more preferably stearyl alcohol, cetyl alcohol or cetostearyl alcohol.
In creams of the present invention, the ratio of oil phase in an O/W type cream is preferably within the range of from 30 to 50% by weight.
According to another aspect of the present invention, there is provided an O/W type cream, wherein maxacalcitol exists in the water phase.
According to an embodiment of the O/W typ

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