KR20000015793A - Immunopotentiators - Google Patents

Abstract

PURPOSE: An improving and preventing agent for the depression of a skin immune function is provided to prevent the lowering of skin immune function caused by an ultraviolet ray by an external use. CONSTITUTION: Skin immunopotentiators containing glutathione or a scutellaria root extract for preventing skin immune depression caused by ultraviolet light or drugs for ameliorating or preventing skin immune depression caused by ultraviolet light; and immunopotentiators or drugs containing an extract of Tiliaceae, cloves, Geranium thunbergii or rosemary for ameliorating or preventing immune depression. These drugs can prevent skin immune depression caused by ultraviolet light.

Description

Immunopotentiator

The skin is the organ that is located in the outermost layer of the living body, the body that wears the strongest and direct physical, chemical and biological invasion, but in recent years skin has been found to be the most developed immune organ.

The skin is composed of keratinocytes of the epidermis, Langerhans cells, dermal dendritic cells, vascular endothelial cells, and macrophages, but Langerhans cells play a central role in skin immune function by antigen treatment and antigen presentation ability. It is thought that a rapid contact with the antigen entry as a foreign substance from the outside is processed, it moves to the phagocytes, presents it to T cells, and subsequent series of immune response reactions are considered.

In recent years, it has been pointed out that in addition to the carcinogenicity of ultraviolet light itself, the skin immune response is reduced by ultraviolet light, thereby promoting cancer. Protecting UV rays with sunburn anti-cosmetic cosmetics such as sunscreen is extremely important for the prevention of UV carcinogenesis, but there is a possibility of immunosuppressive effects by continuously receiving UV rays every day even when the sunscreen is not used daily. Various adverse effects on living organisms other than carcinogenesis are also concerned.

It is also known that skin immune function is lowered by various causes other than ultraviolet rays, such as skin immune function is lowered, for example.

For the above reasons, the development of a medicament having an action of improving the skin immune enhancer or reducing the skin immune function which can be used on a daily basis is urgently needed.

However, no detailed elucidation of the interrelationship between the lowering of skin immune function by various causes has been made, and for example, a substance which inhibits the skin immunosuppressive effect by, for example, can suppress the skin immunosuppressive effect by other causes. There is no guarantee that it can.

In addition, conventionally, for example, studies on the prevention of skin immune function deterioration by ultraviolet rays have not been sufficiently performed, compared to studies on the prevention of skin immune function deterioration due to aging.

For example, it is known to take glutathion by oral as a substance which inhibits the decrease in skin immune function by, for example (see, for example, Fragrance Journal No. 82, 1987, 65). Whether glutathione can suppress skin immune function deterioration due to external use also has not been studied at all.

Therefore, the inventors of the present invention, in particular, investigated the effect of preventing skin immune action by ultraviolet light, as a result, the glutathione, which has the effect of preventing the immune function deterioration by oral by the oral, the external effect of the immune function caused by ultraviolet By discovering a new knowledge that it can be prevented even by this, it came to complete this invention based on this knowledge.

Until now, there have been no reports on the immune strengthening effect and the immune lowering effect of inhibiting the immune lowering effect of ultraviolet glutathione by the ultraviolet ray. The invention is completed as a result of discovering a new effect unpredictable to those skilled in the art that it can be improved and prevented.

On the other hand, for golden extract, it is known that Baikallein, one of its components, has a cell-reinforcing effect (see, for example, Japanese Patent Application Laid-Open No. 64-50877). Has not been studied at all.

Therefore, the inventors of the present invention, in particular, investigated the effect of inhibiting the skin immune effect by ultraviolet light on a variety of substances, as a result of discovering a new knowledge that the golden extract can prevent the immune function lowering effect of ultraviolet light, based on this knowledge Thus, the present invention has been completed.

There has been no report on the immunopotentiation effect of inhibiting the immunosuppressive effect of the golden extract by the ultraviolet ray and the improvement and prevention of the immune function, and the present invention shows that the golden extract significantly improves the decrease of the immune function caused by the ultraviolet ray. The invention is completed as a result of discovering a new effect unforeseen to those skilled in the art that it can be prevented.

In addition, whether bark extract, cloves extract, algae extract, or rosemary extract has suppressed immune function has not been studied at all.

Thus, the present inventors have investigated the effect of preventing the immune suppression effect on various substances as a solution to these problems, the bark extract, cloves extract, algae extract, rosemary extract has a significant immune strengthening effect and immune function deterioration The present inventors have found that they have an effect of improving and preventing the present invention.

There have been no reports on the immunity strengthening effect and the improvement and prevention of immune function of basswood extract, cloves extract, algae extract, and rosemary extract. The invention was completed as a result of discovering a new effect of improving and preventing the problem.

The present invention relates to a skin immune enhancing agent or an external preparation for improving / preventing UV-immunity lowering of function for preventing the decrease in immune function of the skin caused by ultraviolet rays by external application.

1 is a view showing the protective action of Langerhans cell antigen presentation function and glutathione (GSH) by UV irradiation,

2 is a diagram showing the inhibition of the intercellular adhesion molecule ICAM-1 expression of the Langerhans cells and UV extract protection by UV irradiation,

3 is a diagram showing the inhibitory effect of ICAM-1 expression of intercellular adhesion molecules of Langerhans cells and the protective effect of basswood extract by UV irradiation,

4 is a diagram showing the inhibitory effect of ICAM-1 expression of intercellular adhesion molecules of Langerhans cells and the protective effect of clove extract by UV irradiation.

5 is a diagram showing the inhibition of intercellular adhesion molecule ICAM-1 expression of Langerhans cells by UV irradiation and the protective effect of the extract

6 is a diagram showing the inhibition of intercellular adhesion molecule ICAM-1 expression of Langerhans cells and the protective effect of rosemary extracts by UV irradiation.

Disclosure of the Invention

The present invention provides an immunopotentiator for preventing the reduction of ultraviolet skin immune function, which comprises glutathione.

Moreover, this invention provides the ultraviolet-ray skin immune function fall improvement improvement agent characterized by containing glutathione.

Moreover, this invention provides the immune strengthening external preparation for ultraviolet-ray skin immune function fall prevention characterized by containing glutathione.

Moreover, this invention provides glutathione containing external preparation for the ultraviolet-ray skin immune function fall improvement and prevention characterized by the above-mentioned.

In addition, the present invention is to provide an immunopotentiator for preventing the reduction of ultraviolet skin immune function, characterized in that it contains a golden extract.

The present invention also provides a UV skin immune function lowering improvement / prevention agent comprising golden extract.

In addition, the present invention is to provide an immune enhancer characterized by containing a basswood extract.

In addition, the present invention provides an agent for improving and preventing immunity lowering, which comprises a bark extract.

In addition, the present invention is to provide an immunopotentiator, characterized in that it contains a clove extract.

The present invention also provides an agent for improving / preventing a decrease in immune function, which comprises clove extract.

In addition, the present invention is to provide an immunopotentiator, characterized in that it contains an extract of algae.

In addition, the present invention provides an agent for improving / preventing a decrease in immune function, which contains an extract of the herbaceous herb.

In addition, the present invention provides an immunopotentiator characterized by containing a rosemary extract.

The present invention also provides an agent for improving and preventing immune function degradation, comprising a rosemary extract.

Best Mode for Carrying Out the Invention

Hereinafter, the structure of this invention is explained in full detail.

Glutathione used in the skin immune enhancer or the skin impairment improving / preventive agent of the present invention is the most frequently present SH compound in the body, and reacts enzymatically and non-enzymatically with proteins and other disulfides to maintain the SH. It has a function and is converted into oxidized glutathione by this reaction.

Golden extract used in the skin immune enhancer or skin immune function improvement and prevention agent of the present invention, the Jasaceae (紫 蘇科) plant is a golden organic solvent extract of the root of Scutellaria baicalensis Georgi, specifically For example, the golden dry powder or the non-dried golden gold cutting is extracted with stirring such as methanol, ethanol, 1,3-butylene glycol under heating at 30 to 70 ° C. for 1 to 10 hours, or at room temperature for 1 day. The extract can be extracted for 20 days, filtered, the filtrate is concentrated, and the concentrated powder is stirred with purified water to precipitate a yellow powder that can be dried. In the present invention, the golden extract can be used in the step of the concentrate, it can also be used in the step of drying.

Basswood extract used in the immunopotentiator or immune improving and preventing agent of the present invention is a barley tree (Tilia platyphyllos Scop), or winter barley tree (Tilia cordaca Mill), or Tilia europaea L. As an extract of water or an organic solvent, specifically, for example, dry powder or non-dried cuttings of flowers or leaves of winter barley, water or methanol, ethanol, propylene glycol, 1,3-butylene glycol, etc. The alcohol may be extracted by stirring under heating at 30 to 70 ° C. for 1 to 10 hours or by extraction at room temperature for 1 to 20 days, filtering, concentrating the filtrate, and concentrating under reduced pressure to dryness. In the present invention, basswood extract can be used in the step of concentrate, and can also be used in the step of dry matter.

Clove extract used in the immunopotentiator or immune improving and preventing agent of the present invention is an extract of water or an organic solvent of Syzygium aromticum Merrill et Perry, which is a plated sheep and a plant. For example, clove buds, leaves, seeds, ground or starch dry powder or undried clove bud cuttings can be water or methanol, ethanol, propylene glycol, 1,3-butylene glycol. , Butanol, chloroform, dichloromethane, carbon tetrachloride, ethyl acetate, ether or the like, or a mixture thereof, and the mixture is stirred for 1 to 10 hours under heating at 30 to 70 ° C, or extracted at room temperature for 1 to 20 days, and filtered The filtrate can be concentrated and concentrated under reduced pressure and dried. In the present invention, the clove extract can be used at the stage of the concentrate, and can also be used at the stage of the dry matter.

Heterogeneous herb extract used in the immunopotentiator or immune-improving agent of the present invention is an extract of water or organic solvent of Geranium thunbergii Siebold et Zuccarini, which is a rat handiwork and a plant, and specifically, for example, the ground part of the herbaceous herb. Dry powder or non-dried dry grass cuttings of flowers, or seeds or fruits, or leaves, or roots, or outposts, with water or methanol, ethanol, propylene glycol, 1,3-butylene glycol, butanol, chloroform, dichloroethane , Carbon tetrachloride, ethyl acetate, ether or the like, or a mixture thereof and the mixture is stirred for 1 to 10 hours under heating at 30 to 70 ° C, or for 1 to 20 days at room temperature, filtered, and the filtrate is concentrated and concentrated under reduced pressure. Dry can be used. In the present invention, the algae extract can be used in the step of concentrate, and can also be used in the step of dry matter.

The amount of glutathione blended in the skin immune enhancer or the skin immune function deterioration improving / preventing agent of the present invention is 0.005 to 20.0% by weight, preferably 0.01 to 10.0% by weight, as the total amount of the skin immune enhancer or skin immune deterioration improving / preventing agent. to be. If it is less than 0.005% by weight, the effect of improving or preventing immunity deterioration by ultraviolet rays is not sufficiently exhibited. If it exceeds 20.0% by weight, it is difficult to formulate. Moreover, even if it mix | blends 10.0 weight% or more, the improvement of a very big effect is not seen.

The compounding amount of the golden extract, basswood extract, cloves extract, algae extract, or rosemary extract in the immunopotentiator or immune suppression improving / preventing agent is a dry matter of the whole immunopotentiator or immune suppression improving / preventing agent. It is 0.0005-10.0 weight%, Preferably it is 0.001-5.0 weight%. If it is less than 0.0005 weight%, the immunopotentiator or immune function lowering improvement / prevention effect of this invention is not fully exhibited, and when it exceeds 10.0 weight%, it is difficult to formulate and it is unpreferable. Moreover, even if it mix | blends 5.0 weight% or more, the improvement of a very big effect is not acquired.

Skin immune enhancer or skin immune function improvement / preventive agent of the present invention, in addition to the above essential ingredients, ingredients commonly used in skin external preparations such as cosmetics and pharmaceuticals, for example, whitening agent, moisturizing agent, antioxidant, oily ingredient, ultraviolet absorber, anti-inflammatory agent , Surfactants, thickeners, alcohols, powder components, colorants, aqueous components, water, various skin nutrients and the like can be appropriately blended as necessary.

The skin immunity enhancer or skin immunity improving / preventive agent of the present invention is used, for example, in the form of external skin preparations such as ointments, creams, emulsions, lotions, packs, bath solvents, and the formulation thereof is not particularly defined. The skin immunity enhancer or skin immunity deterioration improving / preventing agent of the present invention has high use value as an immunostimulating agent or skin immunity improving / preventive cosmetic for preventing immunity lowering by ultraviolet rays.

Next, the present invention will be described in more detail with reference to Examples. In addition, this invention is not limited to this. The compounding quantity is weight%.

[1] Embodiments of Claims 1 to 4

The immune potentiating effect of glutathione and the improvement / prevention of immune deterioration by ultraviolet light were examined as a protective effect against inhibition of intercellular adhesion molecule-1 (ICAM-1) expression in Langerhans cells by UV irradiation.

`` Test Methods and Results ''

Antigen (trinitrobenzenesulfonic acid, 1mg / ml) was added to the Langerhans cells, and the cultured cells were mixed and cultured with T cells obtained by purification of nylon cell column (Wako). As a result, Langerhans cells present antigens to T cells and increase T cells. However, when Langerhans cells are irradiated with UV light, antigens are added and mixed culture with T cells inhibits antigen presentation of Langerhans cells. Reduced proliferation of T cells is observed. We investigated the protective effect of glutathione against UV-induced inhibitory activity of Langerhans cells by adding 3 mM glutathione (GSH) during UV irradiation. The result is shown in FIG. The vertical axis of FIG. 1 indicates the proliferation of T cells, and indicates that immune function is working when the T cells increase. The horizontal axis indicates the presence or absence of antigen addition, UV irradiation and glutathione (GSH) with + and-(+ indicates addition or irradiation, and-indicates no addition and non-irradiation). In FIG. 1, only T cells proliferate when the antigen is added (17500), and T cells decrease when irradiated with UV rays (5000). At this time, it can be seen that the proliferation of T cells is restored (11000) while adding glutathione. Therefore, it was confirmed that glutathione exerts an excellent immune strengthening action and skin immune function improving action.

Below, the Example which used glutathione as an external skin strengthening agent or skin immune function prevention / improvement agent for the purpose of preventing the immune function lowering by ultraviolet-ray by external use is shown.

"Example 1 cream"

(Prescription)

Stearic acid 5.0 wt%

Stearyl Alcohol 4.0

Isopropyl myristate 18.0

Glycerine Monostearic Acid Ester 3.0

Propylene Glycol 10.0

Glutathione 0.01

Paraaminobenzoic acid0.5

Potassium Hydroxide 0.2

Preservative

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol, glutathione, and potassium hydroxide are added to the ion-exchanged water, dissolved, and heated to 70 ° C (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is slowly added to the aqueous phase and the addition is complete and held at that temperature for a while to cause the reaction. Thereafter, the mixture is emulsified uniformly with a homomixer and cooled to 30 ° C while stirring well.

`` Example 2 Cream ''

(Prescription)

Stearic acid 2.0% by weight

Stearyl Alcohol 7.0

Water added Lanolin 2.0

Squalane 5.0

2-octyldodecyl alcohol 6.0

Polyoxyethylene (25 mol) cetyl alcohol ether 3.0

Glycerin Monostearic Acid Ester 2.0

Propylene Glycol 5.0

Glutathione 0.05

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol is added to ion-exchanged water, and it heats and maintains at 70 degreeC (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is added to the aqueous phase, pre-emulsification is carried out, and it is emulsified uniformly with a homomixer, and it cools to 30 degreeC, stirring well.

`` Example 3 Cream ''

(Prescription)

5.0% by weight of solid paraffin

Beeswax 10.0

Waselin 15.0

Liquid Paraffin 41.0

Glycerin Monostearic Acid Ester 2.0

Polyoxyethylene (20 mol) sorbitan monolauline ester 2.0

Soap Powder 0.1

Borax 0.2

Glutathione 0.05

Ascorbic acid 2.0

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Soap powder and borax are added to the ion-exchanged water, dissolved in heat and maintained at 70 ° C (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). It adds gradually, mixing an oil phase to an aqueous phase, and reacts. After completion of the reaction, the mixture was emulsified uniformly with a homomixer, and then cooled to 30 ° C while stirring well.

Example 4 Latex

(Prescription)

Stearic acid 2.5% by weight

Cetyl Alcohol 1.5

Waselin 5.0

Liquid Paraffin 10.0

Polyoxyethylene (10 mol) monooleic acid ester 2.0

Polyethylene Glycol 1500 3.0

Triethanolamine 1.0

Carboxy vinyl polymer 0.05

(Brand name: Carbopol 941, B.F.Goodrich Chemical company)

Glutathione 0.01

Octyl dimethylaminobenzoate 1.0

Sodium hydrogen sulfite 0.01

Arbutin 3.5

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

The carboxyvinyl polymer is dissolved in a small amount of ion exchanged water (phase A). Polyethylene glycol 1500 and triethanolamine were added to the remaining ion-exchanged water, and the mixture was heated and dissolved at 70 ° C. (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is added to the aqueous phase, pre-emulsification is performed, A phase is added, and it is emulsified uniformly with a homomixer, and it cools to 30 degreeC, stirring well after emulsification.

Example 5 Latex

(Prescription)

1.0% by weight of microcrystalline wax

Beeswax 2.0

Lanolin 20.0

Liquid Paraffin 10.0

Octyl dimethylaminobenzoate 3.0

Squalane 5.0

Sorbanthesquiolefin acid ester 4.0

Polyoxyethylene (20 mol) sorbitan monooleic acid ester 1.0

Propylene Glycol 7.0

Glutathione 10.0

Ascorbic Magnesium Phosphate 3.0

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol is added to ion-exchanged water and heated to maintain it at 70 캜 (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). Slowly add the aqueous phase to the oil phase while uniformly emulsifying it with a homomixer. After emulsification, the mixture is cooled to 30 ° C while stirring well.

"Example 6 jelly"

(Prescription)

95% ethyl alcohol 10.0% by weight

Dipropylene Glycol 15.0

Polyoxyethylene (50 mol) oleyl alcohol ether 2.0

Carboxy Vinyl Polymer 1.0

(Brand name: Carbopol 940, B.F.Goodrich Chemical company)

Sodium hydroxide 0.15

L-arginine 0.1

Paramethoxy Cinnamic Acid Isopropyl 0.1

Titanium Oxide 5.0

Glutathione 7.0

Sodium 2-hydroxy-4-methoxybenzophenonesulfonate 0.05

Ethylenediaminetetraacetate, trisodium, 2-water 0.05

Methylparaben 0.2

Spices

Ion Exchange Water Residue

(quite)

Carbopol 940 is uniformly dissolved in ion-exchanged water, while glutathione and polyoxyethylene (50 mole) oleyl alcohol ether are dissolved in 95% ethanol and added to the aqueous phase. Subsequently, other ingredients are added and then neutralized with sodium hydroxide and L-arginine to thicken.

"Example 7 serum"

(Prescription)

(A phase)

10% by weight of ethyl alcohol (95%)

Polyoxyethylene (20 mol) octyldodecanol 1.0

Pantothenylethyl Ether 0.1

Glutathione 1.5

Methylparaben 0.15

(B phase)

Potassium Hydroxide 0.1

(C phase)

Glycerin 5.0

Dipropylene Glycol 10.0

Carboxy Vinyl Polymer 0.2

(Brand name: Carbopol 940, B.F.Goodrich Chemical company)

Purified water residual

(quite)

A phase and C phase are melt | dissolved uniformly, respectively, and a solubilization is carried out by adding A phase to C phase. Subsequently, after adding B phase, a container is filled.

`` Example 8 Pack ''

(Prescription)

(A phase)

Dipropylene glycol 5.0 wt%

Polyoxyethylene (60 mol) hardened castor oil 5.0

(B phase)

Glutathione 0.01

Olive oil 5.0

Tocopherol Acetate 0.2

Ethylparaben 0.2

Spices 0.2

(C phase)

Polyvinyl Alcohol 13.0

(90 degree of soap, degree of polymerization 2,000)

Ethanol 7.0

Purified water residual

(quite)

A phase, B phase, and C phase are melt | dissolved uniformly, respectively, and B phase is added and solubilized. Subsequently, this is added to phase C, and then the container is filled.

`` Example 9 solid foundation ''

(Prescription)

Talc 43.1% by weight

Kaolin 15.0

Serisite 10.0

Zinc Oxide 7.0

Titanium Dioxide 3.8

Yellow Iron Oxide 2.9

Black Iron Oxide 0.2

Squalane 8.0

Isostearic acid 4.0

Monoolefinic Acid POE Solbitan 3.0

Isobutyl octane 2.0

Glutathione 1.0

Preservative

Spices

(quite)

Powder components of talc to black iron oxide are sufficiently mixed with a blender, and the oil component, glutathione, preservative, and fragrance of squalane-isotanyl is added thereto, kneaded well, and then filled and molded into a container.

`` Example 10 emulsification type foundation (cream type) ''

(Prescription)

(Powder part)

Titanium Dioxide 10.3% by weight

Serisite 5.4

Kaolin 3.0

Yellow Iron Oxide 0.8

Red Iron (III) Oxide 0.3

Black Iron Oxide 0.2

(Charged)

Decamethylcyclopentasiloxane 11.5

Liquid Paraffin 4.5

Polyoxyethylene Modified Dimethyl Polysiloxane 4.0

(Awards)

Purified water 50.0

1,3-butyleneglucol 4.5

Glutathione 1.5

Ascorbic Acid Glucoside 1.0

Sorbanthesquioleic Acid Ester 3.0

Preservative

Spices

(quite)

After heating and stirring the aqueous phase, a sufficiently mixed powder portion is added to the homomixer. After heat-mixed oil phase is added and the homomixer is processed, the fragrance is added while stirring and cooled to room temperature.

[2] Examples of claims 5 to 6

Immune potentiation of gold extract and improvement and prevention of immunosuppression by UV rays were examined as a bare effect on the inhibition of expression of intercellular adhesion molecule-1 (ICAM-1) in Langerhans cells by UV irradiation.

`` Golden Extract ''

The golden extract used in the examples below was added to water and the water was removed from the roots of the roots of Scutellaria baicalensis Geogi, heated to 50 ° C., and then ethanol was extracted for 5 hours. The filtrate was then used to concentrate the filtrate solvent.

`` Test Methods and Results: Protective Effects Against Inhibition of Intercellular Adhesion Molecule-1 (ICAM-1) Expression in Langerhans Cells by UV Irradiation ''

Langerhans cells obtained by 0.5% tripsin treatment of human skin epidermis were irradiated with UVA (5J / cm ² , BLB lamp), and then cultured in a CO ₂ incubator at 37 ° C. for 24 hours at RPMI 1640/10% FBS. After incubation, the cells were treated with FITC-labeled anti-MHC class II antibody (manufactured by Pamigen) and FE-labeled anti-ICAM-1 antibody (manufactured by Pamigen) to 3x10 ⁴ cells with proscimeter (XL: Epix) ICAM-1 expression intensity of Langerhans cells expressing MHC class II antigen was measured. This result is shown in FIG. 2. The vertical axis of FIG. 2 shows the expression rate (%) of ICAM-1, and the horizontal axis shows the presence or absence of the addition of the golden extract (final concentration: wt%). The addition of the golden extract in Figure 2 can be seen that the intercellular adhesion molecule-1 (ICAM-1) expression suppression action in Langerhans cells according to UVA is clearly protected.

Below, the Example which used the golden extract as a skin immunity strengthening agent or skin immune function prevention / improvement agent for the purpose of preventing the immune function lowering by ultraviolet-ray by external use is shown.

"Example 1 cream"

(Prescription)

Stearic acid 5.0 wt%

Stearyl Alcohol 4.0

Isopropyl myristate 18.0

Glycerine Monostearic Acid Ester 3.0

Propylene Glycol 10.0

Golden Extract 0.01

Paraaminobenzoic acid0.5

Potassium Hydroxide 0.2

2-ethylhexyl paramethoxy cinnamic acid 3.0

Preservative

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol, golden extract and potassium hydroxide are added to ion-exchanged water, dissolved, and heated to 70 ° C. (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is slowly added to the aqueous phase and the addition is complete and held at that temperature for a while to cause the reaction. Thereafter, the mixture is emulsified uniformly with a homomixer and cooled to 30 ° C while stirring well.

`` Example 2 Cream ''

(Prescription)

Stearic acid 2.0% by weight

Stearyl Alcohol 7.0

Water added Lanolin 2.0

Squalane 5.0

2-octyldodecyl alcohol 6.0

Polyoxyethylene (25 mol) cetyl alcohol ether 3.0

Glycerin Monostearic Acid Ester 2.0

Propylene Glycol 5.0

2-ethylhexyl paramethoxy cinnamic acid 10.0

Golden Extract 0.05

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol is added to ion-exchanged water and heated to maintain it at 70 캜 (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is added to the aqueous phase, preliminary dropping is performed, and the resultant is uniformly emulsified with a homomixer, and then cooled to 30 ° C while stirring well.

`` Example 3 Cream ''

(Prescription)

5.0% by weight of solid paraffin

Beeswax 10.0

Waselin 15.0

Liquid Paraffin 41.0

Glycerine Monostearic Acid Ester 2.0

Polyoxyethylene (20 mol) sorbitan monolauric acid ester 2.0

Soap Powder 0.1

2-ethylhexyl paramethoxy cinnamic acid 3.0

Borax 0.2

Golden Extract 0.05

Ascorbic acid 2.0

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Soap powder and borax are added to the ion-exchanged water and dissolved by heating to maintain the temperature at 70 ° C (water phase). The other components are mixed, dissolved in heat, and kept at 70 ° C (oil phase). It adds gradually, mixing an oil phase to an aqueous phase, and reacts. After completion of the reaction, the mixture was emulsified uniformly with a homomixer, and then emulsified and cooled to 30 ° C while stirring well.

Example 4 Latex

(Prescription)

Stearic acid 2.5% by weight

Cetyl Alcohol 1.5

Waselin 5.0

Liquid Paraffin 10.0

Polyoxyethylene (10 mol) monooleic acid ester 2.0

Polyethylene Glycol 1500 3.0

Triethanolamine 1.0

Carboxy vinyl polymer 0.05

(Brand name: Carbopol 941, B.F.Goodrich Chemical company)

Golden Extract 0.01

Octyl dimethylaminobenzoate 1.0

Sodium hydrogen sulfite 0.01

Arbutin 3.5

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

The carboxyvinyl polymer is dissolved in a small amount of ion exchanged water (phase A). Polyethyleneglycol 1500 and triethanolamine were added to the remaining ion-exchanged water and dissolved by heating to maintain the temperature at 70 ° C (water phase). The other ingredients are mixed, soluble, and kept at 70 ° C (oil phase). The oil phase is added to the aqueous phase, pre-emulsification is carried out, phase A is added, and the emulsion is uniformly emulsified with a homomixer, and then cooled to 30 ° C while stirring well.

Example 5 Latex

(Prescription)

1.0% by weight of microcrystalline wax

Beeswax 2.0

Lanolin 20.0

Liquid Paraffin 10.0

Octyl dimethylaminobenzoate 3.0

2-ethylhexyl paramethoxy cinnamic acid 4.0

Squalane 5.0

Sorbanthesquioleic acid ester 4.0

Polyoxyethylene (20 mol) sorbitan monooleic acid ester 1.0

Propylene Glycol 7.0

Golden Extract 10.0

Ascorbic Magnesium Phosphate 3.0

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol is added to ion-exchanged water and heated to maintain it at 70 캜 (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The water phase is gradually added thereto while stirring the oil phase, and the oil phase is uniformly emulsified. After emulsification, the mixture is cooled to 30 ° C while stirring well.

"Example 6 jelly"

(Prescription)

95% ethyl alcohol 10.0% by weight

Dipropylene Glycol 15.0

Polyoxyethylene (50 mol) oleyl alcohol ether 2.0

Carboxy Vinyl Polymer 1.0

(Brand name: Carbopol 940, B.F.Goodrich Chemical company)

Sodium hydroxide 0.15

L-arginine 0.1

Paramethoxy Cinnamic Acid Isopropyl 0.1

Titanium Oxide 5.0

Golden Extract 7.0

Sodium 2-hydroxy-4-methoxybenzophenonesulfonate 0.05

Ethylenediaminetetraacetate, trisodium, 2-water 0.05

Methylparaben 0.2

Spices

Ion Exchange Water Residue

(quite)

Carbopol 940 is uniformly dissolved in ion-exchanged water, while golden extract and polyoxyethylene (50 mole) oleyl alcohol ether are dissolved in 95% ethanol and added to the aqueous phase. Subsequently, other components are added and then neutralized with sodium hydroxide and L-arginine to thicken.

"Example 7 serum"

(Prescription)

(A phase)

Ethyl alcohol (95%) 10.0 wt%

Polyoxyethylene (20 mol) octyldodecanol 1.0

Pantothenylethyl Ether 0.1

Golden Extract 1.5

Methylparaben 0.15

(B phase)

Potassium Hydroxide 0.1

(C phase)

Glycerin 5.0

Dipropylene Glycol 10.0

Carboxy Vinyl Polymer 0.2

(Brand name: Carbopol 940, B.F.Goodrich Chemical company)

Purified water residual

(quite)

A phase and C phase are melt | dissolved uniformly, respectively, and a solubilization is carried out by adding A phase to C phase. Subsequently, after adding B phase, a container is filled.

`` Example 8 Pack ''

(Prescription)

(A phase)

Dipropylene glycol 5.0 wt%

Polyoxyethylene (60 mol) hardened castor oil 5.0

(B phase)

Golden Extract 0.01

Olive oil 5.0

Tocopherol Acetate 0.2

Ethylparaben 0.2

Spices 0.2

(C phase)

Polyvinyl Alcohol 13.0

(90 degree of soap, degree of polymerization 2,000)

Ethanol 7.0

Purified water residual

(quite)

A phase, B phase, and C phase are melt | dissolved uniformly, respectively, and B phase is added and solubilized. Subsequently, this is added to phase C, and then the container is filled.

`` Example 9 solid foundation ''

(Prescription)

Talc 43.1% by weight

Kaolin 15.1

Serisite 10.0

Zinc Oxide 7.0

Titanium Dioxide 3.8

Yellow Iron Oxide 2.9

Black Iron Oxide 0.2

Squalane 8.0

Isostearic acid 4.0

Monooleic acid POE sorbitan 3.0

Isobutyl octane 2.0

Golden Extract 1.0

Preservative

Spices

(quite)

The talc to black iron oxide powder component is sufficiently mixed with a blender, and the oil component, squash extract, preservative, and fragrance of squalane-isotanyl octanoate is added thereto, kneaded well, and then filled and molded into a container.

`` Example 10 emulsification type foundation (cream type) ''

(Prescription)

(Powder part)

Titanium Dioxide 10.3% by weight

Serisite 5.4

Kaoli 3.0

Iron Oxide 0.8

Red Iron (III) Oxide 0.3

Black Iron Oxide 0.2

(Charged)

Decamethylcyclopentasiloxane 11.5

Liquid Paraffin 4.5

Polyoxyethylene Modified Dimethyl Polysiloxane 4.0

(Awards)

Purified water 50.0

1,3-butylene glycol 4.5

Golden Extract 1.5

Ascorbic Acid Glucoside 1.0

Solbitan sesquioleic acid ester 3.0

Preservative

Spices

(quite)

After heating and stirring the aqueous phase, a sufficiently mixed powder portion is added to the homomixer. After heat-mixing the oil phase is added, the homomixer is treated, the fragrance is added while stirring, and cooled to room temperature.

[3] Examples of claims 7 to 8

Immunopotentiation and improvement and prevention of immune function deterioration by UV light were investigated as a protective effect against inhibition of intercellular adhesion molecule-1 (ICAM-1) expression in Langerhans cells by UV irradiation.

Basswood Extract

Basilwood extract used in the following examples were extracted from the flowers and leaves of winter barley (Tillia cordatamill) in 50% ethanol, heated at 50 ° C. for 5 hours, filtered, and the filtrate was used as a concentrate distilling off the solvent. .

`` Test Methods and Results: Protective Effects Against Inhibition of Intercellular Adhesion Molecule-1 (ICAM-1) Expression in Langerhans Cells by UV Irradiation ''

Langerhans cells obtained by 0.5% trypsin treatment of human skin were irradiated with UVA (5J / cm ² , BLB lamp), and then cultured in a CO ₂ incubator at 37 ° C for 24 hours with RPMI 1640/10% FBS. After incubation, the cells were treated with a FITC-labeled anti-MHC class II antibody (made by Pharmagene) and a PE-labeled anti-ICAM-1 antibody (made by Pharmazen), and then 3 x 10 ⁴ cells were treated with a flowitem (XL: Epix). ICAM-1 expression intensity of Langerhans cells expressing MHC class II antigen was measured. This result is shown in FIG. 3 shows the ICAM-1 expression rate (%), the horizontal axis shows the presence or absence of the addition of basswood extract (final concentration: wt%). It can be seen from FIG. 3 that the intercellular adhesion molecule-1 (ICAM-1) expression inhibitory effect in Langerhans cells by UVA is clearly defended while adding the basswood extract.

Below, the Example which used the extract of basswood as an immunopotentiator or an immune suppression prevention / improvement agent is shown.

"Example 1 cream"

(Prescription)

Stearic acid 5.0 wt%

Stearyl Alcohol 4.0

Isopropyl myristate 18.0

Glycerine Monostearic Acid Ester 3.0

Propylene Glycol 10.0

Basswood Extract 0.01

Paraaminobenzoic acid0.5

2-ethylhexyl paramethoxy cinnamic acid 5.0

Potassium Hydroxide 0.2

Preservative

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol, basswood extract, and potassium hydroxide are added to the ion-exchanged water, dissolved, and heated to 70 ° C (water phase). The other ingredients are mixed, soluble, and kept at 70 ° C (oil phase). The oil phase is slowly added to the aqueous phase and the addition is complete and held at that temperature for a while to cause the reaction. Thereafter, the mixture is emulsified uniformly with a homomixer and cooled to 30 ° C while stirring well.

`` Example 2 Cream ''

(Prescription)

Stearic acid 2.0% by weight

Stearyl Alcohol 7.0

Water added Lanolin 2.0

Squalane 5.0

2-octyldodecyl alcohol 6.0

Polyoxyethylene (25 mol) cetyl alcohol ether 3.0

Glycerin Monostearic Acid Ester 2.0

Propylene Glycol 5.0

2-ethylhexyl paramethoxy cinnamic acid 10.0

Basswood Extract 0.05

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol is added to ion-exchanged water and heated to maintain it at 70 캜 (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). Pre-emulsion is performed by adding an oil phase to the aqueous phase, and it is emulsified uniformly with a homomixer, and it cools to 30 degreeC, stirring well.

`` Example 3 Cream ''

(Prescription)

5.0% by weight of solid paraffin

Beeswax 10.0

Waselin 15.0

Liquid Paraffin 41.0

Glycerin Monostearic Acid Ester 2.0

Polyoxyethylene (20 mol) sorbitan monolauric acid ester 2.0

Soap Powder 0.1

2-ethylhexyl paramethoxy cinnamic acid 1.0

Borax 0.2

Basswood Extract 0.05

Ascorbic acid 2.0

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Soap powder and borax are added to ion-exchanged water, dissolved in heat and maintained at 70 ° C (water phase). The other components are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The reaction is carried out by gradually adding the oil phase to the aqueous phase. After completion of the reaction, the mixture was emulsified uniformly with a homomixer, and then emulsified and cooled to 30 ° C while stirring well.

Example 4 Latex

(Prescription)

Stearic acid 2.5% by weight

Cetyl Alcohol 1.5

Waselin 5.0

Liquid Paraffin 10.0

Polyoxyethylene (10 mol) monooleic acid ester 2.0

Polyethylene Glycol 1500 3.0

Triethanolamine 1.0

Carboxy vinyl polymer 0.05

(Brand name: Carbopol 940, B.F.Goodrich Chemical company)

Basswood Extract 0.01

Octyl Dimethylaminobenzoate 1.0

Sodium hydrogen sulfite 0.01

Arbutin 3.5

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

The carboxyvinyl polymer is dissolved in a small amount of ion exchanged water (phase A). Polyethyleneglycol 1500 and triethanolamine are added to the remaining ion-exchanged water, and it is dissolved by heating and kept at 70 ° C (water phase). The other components are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is added to the aqueous phase to pre-emulsify, A phase is added to emulsify uniformly with a homomixer, and then cooled to 30 ° C while stirring well after emulsification.

Example 5 Latex

(Prescription)

1.0% by weight of microcrystalline wax

Beeswax 2.0

Lanolin 20.0

Liquid Paraffin 10.0

Octyl dimethylaminobenzoate 3.0

2-ethylhexyl paramethoxy cinnamic acid 5.0

Squalane 5.0

Sorbanthesquioleic acid ester 4.0

Polyoxyethylene (20 mol) sorbitan monooleic acid ester 1.0

Propylene Glycol 7.0

Basswood Extract 10.0

Ascorbic Magnesium Phosphate 3.0

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol is added to ion-exchanged water and heated to maintain it at 70 캜 (water phase). The other components are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The water phase is gradually added thereto while stirring the oil phase, and the oil phase is uniformly emulsified. After emulsification, the mixture is cooled to 30 ° C while stirring well.

"Example 6 jelly"

(Prescription)

95% ethyl alcohol 10.0% by weight

Dipropylene Glycol 15.0

Polyoxyethylene (50 mol) oleyl alcohol ether 2.0

Carboxy Vinyl Polymer 1.0

(Brand name: Carbopol 940, B.F.Goodrich Chemical company)

Sodium hydroxide 0.15

L-arginine 0.1

Paramethoxy Cinnamic Acid Isopropyl 0.1

2-ethylhexyl paramethoxy cinnamic acid 0.5

Titanium Oxide 5.0

Basswood Extract 7.0

Sodium 2-hydroxy-4-methoxybenzophenonesulfonate 0.05

Ethylenediaminetetraacetate, trisodium, 2-water 0.05

Methylparaben 0.2

Spices

Ion Exchange Water Residue

(quite)

Carbopol 940 is uniformly dissolved in ion-exchanged water, while basswood extract and polyoxyethylene (50 mole) oleyl alcohol ether are dissolved in 95% ethanol and added to the aqueous phase. Then, other ingredients are added, followed by neutralization with sodium hydroxide and L-arginine for thickening.

"Example 7 serum"

(Prescription)

(A phase)

Ethyl alcohol (95%) 10.0 wt%

Polyoxyethylene (20 mol) octyldodecanol 1.0

Pantothenylethyl Ether 0.1

Basswood Extract 1.5

Methylparaben 0.15

(B phase)

Potassium Hydroxide 0.1

(C phase)

Glycerin 5.0

Dipropylene Glycol 10.0

Carboxy Vinyl Polymer 0.2

(Brand name: Carbopol 940, B.F.Goodrich Chemical company)

Purified water residual

(quite)

A phase and C phase are melt | dissolved uniformly, respectively, and a solubilization is carried out by adding A phase to C phase. Subsequently, after adding B phase, a container is filled.

`` Example 8 Pack ''

(Prescription)

(A phase)

Dipropylene glycol 5.0 wt%

Polyoxyethylene (60 mol) hardened castor oil 5.0

(B phase)

Basswood Extract 0.01

Olive oil 5.0

Tocopherol Acetate 0.2

Ethylparaben 0.2

Spices 0.2

(C phase)

Polyvinyl Alcohol 13.0

(90 degree of soap, degree of polymerization 2,000)

Ethanol 7.0

Purified water residual

(quite)

A phase, B phase, and C phase are melt | dissolved uniformly, respectively, and B phase is added and solubilized. Subsequently, this is added to phase C, and then the container is filled.

`` Example 9 solid foundation ''

(Prescription)

Talc 43.1% by weight

Kaolin 15.0

Serisite 10.0

Zinc Oxide 7.0

Titanium Dioxide 3.8

Yellow Iron Oxide 2.9

Black Iron Oxide 0.2

Squalane 8.0

Isostearic acid 4.0

Monooleic acid POE sorbitan 3.0

Isobutyl octane 2.0

Basswood Extract 1.0

Preservative

Spices

(quite)

The talc to black iron oxide powder components are sufficiently mixed with a blender, and oily components of squalane to isocyanate isocetyl, basswood extract, preservatives, and fragrance are added and kneaded well, then filled and molded into a container.

`` Example 10 emulsification type foundation (cream type) ''

(Prescription)

(Powder part)

Titanium Dioxide 10.3% by weight

Serisite 5.4

Kaolin 3.0

Iron Oxide 0.8

Red Iron (III) Oxide 0.3

Black Iron Oxide 0.2

(Charged)

Decamethylcyclopentasiloxane 11.5

Liquid Paraffin 4.5

Polyoxyethylene Modified Dimethyl Polysiloxane 4.0

(Awards)

Purified water 50.0

1,3-butylene glycol 4.5

Basswood Extract 1.5

Ascorbic Acid Glucoside 1.0

Solbitan sesquioleic acid ester 3.0

Preservative

Spices

(quite)

After heating and stirring the aqueous phase, a sufficiently mixed powder portion is added to the homomixer. After heat-mixing the oil phase is added, the homomixer is treated, the fragrance is added while stirring, and cooled to room temperature.

[4] Embodiments of Claims 9 to 10

Immune potentiation of Clove extract and improvement and prevention of immune function deterioration by UV light were examined as a protective effect against inhibition of intercellular adhesion molecule-1 (ICMA-1) expression in Langerhans cells by UV irradiation.

Clove Extract

The clove extract used in the following examples was dried at 50 ℃ in 50% ethanol, dried for 5 hours after extracting dried flowers of the clove (Syzygium aromaticum Merrill et Perry) and filtered to concentrate the filtrate solvent Used.

`` Test Methods and Results: Protective Effects Against Inhibition of Intercellular Adhesion Molecule-1 (ICAM-1) Expression in Langerhans Cells by UV Irradiation ''

UVA (5J / cm ² , BLB lamp) was irradiated to Langerhans cells obtained by 0.5% trypsin treatment of the epidermis of human skin, and then cultured in a CO ₂ incubator at 37 ° C for 24 hours with RPMI 1640/10% FBS. After incubation, the cells were treated with a FITC-labeled anti-MHC class II antibody (made by Pharmagene) and a PE-labeled anti-ICAM-1 antibody (made by Pharmazen), and then 3 x 10 ⁴ cells were treated with a flowitem (XL: Epix). ICAM-1 expression intensity of Langerhans cells expressing MHC class II antigen was measured. This result is shown in FIG. 4 shows the ICAM-1 expression rate (%), and the horizontal axis shows the presence or absence of clove extract (final concentration: wt%). 4, it can be seen that the intercellular adhesion molecule-1 (ICAM-1) expression inhibitory action in Langerhans cells by UVA is clearly protected.

Below, the Example which used the clove extract as an immunopotentiator or an immune suppression prevention / improvement agent is shown.

"Example 1 cream"

(Prescription)

Stearic acid 5.0 wt%

Stearyl Alcohol 4.0

Isopropyl myristate 18.0

Glycerine Monostearic Acid Ester 3.0

Propylene Glycol 10.0

Clove Extract 0.01

Paraaminobenzoic acid0.5

2-ethylhexyl paramethoxy cinnamic acid 5.0

Potassium Hydroxide 0.2

Preservative

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol, cloves extract and potassium hydroxide are added to the ion-exchanged water, dissolved, and heated to 70 캜 (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is slowly added to the aqueous phase and the addition is complete and held at that temperature for a while to cause the reaction. Thereafter, the mixture is emulsified uniformly with a homomixer and cooled to 30 ° C while stirring well.

`` Example 2 Cream ''

(Prescription)

Stearic acid 2.0% by weight

Stearyl Alcohol 7.0

Water added Lanolin 2.0

Squalane 5.0

2-octyldodecyl alcohol 6.0

Polyoxyethylene (25 mol) cetyl alcohol ether 3.0

Glycerin Monostearic Acid Ester 2.0

Propylene Glycol 5.0

2-ethylhexyl paramethoxy cinnamic acid 10.0

Clove Extract 0.05

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol is added to ion-exchanged water and heated to maintain it at 70 캜 (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). Pre-emulsion is performed by adding an oil phase to the aqueous phase, and it is emulsified uniformly with a homomixer, and it cools to 30 degreeC, stirring well.

`` Example 3 Cream ''

(Prescription)

5.0% by weight of solid paraffin

Beeswax 10.0

Waselin 15.0

Liquid Paraffin 41.0

Glycerin Monostearic Acid Ester 2.0

Polyoxyethylene (20 mol) sorbitan monolauric acid ester 2.0

Soap Powder 0.1

2-ethylhexyl paramethoxy cinnamic acid 1.0

Borax 0.2

Clove Extract 0.05

Ascorbic Acid 2.0

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Soap powder and borax are added to ion-exchanged water, dissolved in heat and maintained at 70 ° C (water phase). The other components are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is gradually added to the aqueous phase while stirring to carry out the reaction. After completion of the reaction, the mixture is emulsified uniformly with a homomixer and cooled to 30 ° C while stirring well after emulsification.

Example 4 Latex

(Prescription)

Stearic acid 2.5% by weight

Cetyl Alcohol 1.5

Waselin 5.0

Liquid Paraffin 10.0

Polyoxyethylene (10 mol) monooleic acid ester 2.0

Polyethylene Glycol 1500 3.0

Triethanolamine 1.0

Carboxy vinyl polymer 0.05

(Brand name: Carbopol 941, B.F.Goodrich Chemical company)

Clove Extract 0.01

Octyl dimethylaminobenzoate 1.0

Arbutin 3.5

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

The carboxyvinyl polymer is dissolved in a small amount of ion exchanged water (phase A). Polyethyleneglycol 1500 and triethanolamine are added to the remaining ion-exchanged water, and it is dissolved by heating and kept at 70 ° C (water phase). The other components are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is added to the aqueous phase to pre-emulsify, A phase is added to emulsify uniformly with a homomixer, and then cooled to 30 ° C while stirring well after emulsification.

Example 5 Latex

(Prescription)

1.0% by weight of microcrystalline wax

Glutathione 1.0

Beeswax 2.0

Lanolin 20.0

Liquid Paraffin 10.0

Octyl dimethylaminobenzoate 3.0

2-ethylhexyl paramethoxy cinnamic acid 5.0

Squalane 5.0

Sorbanthesquioleic acid ester 4.0

Polyoxyethylene (20 mol) sorbitan monooleic acid ester 1.0

Propylene Glycol 7.0

Clove Extract 10.0

Ascorbic Magnesium Phosphate 3.0

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol is added to ion-exchanged water and heated to maintain it at 70 캜 (water phase). The other components are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The aqueous phase is slowly added to it while the oil phase is mixed and emulsified uniformly with a homomixer. After emulsification, the mixture is cooled to 30 ° C while stirring well.

"Example 6 jelly"

(Prescription)

95% ethyl alcohol 10.0% by weight

Dipropylene Glycol 15.0

Polyoxyethylene (50 mol) oleyl alcohol ether 2.0

Carboxy Vinyl Polymer 1.0

(Brand name: Carbopol 940, B.F.Goodrich Chemical company)

Sodium hydroxide 0.15

L-arginine 0.1

Paramethoxy Cinnamic Acid Isopropyl 0.1

2-ethylhexyl paramethoxy cinnamic acid 0.5

Titanium Oxide 5.0

Clove Extract 7.0

Sodium 2-hydroxy-4-methoxybenzophenonesulfonate 0.05

Ethylenediaminetetraacetate, trisodium, 2-water 0.05

Methylparaben 0.2

Spices

Ion Exchange Water Residue

(quite)

Carbopol 940 is uniformly dissolved in ion-exchanged water, while clove extract and polyoxyethylene (50 mole) oleyl alcohol ether are dissolved in 95% ethanol and added to the aqueous phase. Then, other ingredients are added, followed by neutralization with sodium hydroxide and L-arginine for thickening.

"Example 7 serum"

(Prescription)

(A phase)

Ethyl alcohol (95%) 10.0 wt%

Polyoxyethylene (20 mol) octyldodecanol 1.0

Pantothenylethyl Ether 0.1

Clove Extract 1.5

Methylparaben 0.15

(B phase)

Potassium Hydroxide 0.1

(C phase)

Glycerin 5.0

Dipropylene Glycol 10.0

Carboxy Vinyl Polymer 0.2

(Brand name: Carbopol 940, B.F.Goodrich Chemical company)

Purified water residual

(quite)

A phase and C phase are melt | dissolved uniformly, respectively, and a solubilization is carried out by adding A phase to C phase. Subsequently, after adding B phase, a container is filled.

`` Example 8 Pack ''

(Prescription)

(A phase)

Dipropylene glycol 5.0 wt%

Polyoxyethylene (60 mol) hardened castor oil 5.0

(B phase)

Clove Extract 0.01

Olive oil 5.0

Tocopherol Acetate 0.2

Ethylparaben 0.2

Spices 0.2

(C phase)

Polyvinyl Alcohol 13.0

(90 degree of soap, degree of polymerization 2,000)

Ethanol 7.0

Purified water residual

(quite)

A phase, B phase, and C phase are melt | dissolved uniformly, respectively, and B phase is added and solubilized. Subsequently, this is added to phase C, and then the container is filled.

`` Example 9 solid foundation ''

(Prescription)

Talc 43.1% by weight

Kaolin 15.0

Serisite 10.0

Zinc Oxide 7.0

Titanium Dioxide 3.8

Yellow Iron Oxide 2.9

Black Iron Oxide 0.2

Squalane 8.0

Isostearic acid 4.0

Monooleic acid POE sorbitan 3.0

Isobutyl octane 2.0

Clove Extract 1.0

Preservative

Spices

(quite)

The talc to black iron oxide powder component is sufficiently mixed with a blender, and the oil component, squash extract, preservative, and fragrance of squalane to isocyanate is added thereto, kneaded well, and then filled and molded into a container.

`` Example 10 emulsification type foundation (cream type) ''

(Prescription)

(Powder part)

Titanium Dioxide 10.3% by weight

Celsite 5.4

Kaolin 3.0

Iron Oxide 0.8

Red Iron (III) Oxide 0.3

Black Iron Oxide 0.2

(Charged)

Decamethylcyclopentasiloxane 11.5

Liquid Paraffin 4.5

Polyoxyethylene Modified Dimethyl Polysiloxane 4.0

(Awards)

Purified water 50.0

1,3-butylene glycol 4.5

Clove Extract 1.5

Ascorbic Acid Glucoside 1.0

Solbitan sesquioleic acid ester 3.0

Preservative

Spices

(quite)

After heating and stirring the aqueous phase, a sufficiently mixed powder portion is added to the homomixer. After heat-mixing the oil phase is added, the homomixer is treated, the fragrance is added while stirring, and cooled to room temperature.

[5] Examples of claims 11 to 12

Immunopotentiation and improvement and prevention of immunosuppression by UV irradiation were investigated as a protective effect against inhibition of intercellular adhesion molecule-1 (ICMA-1) expression in Langerhans cells by UV irradiation.

`` Shellweed Extract ''

In the following example, the extract of the genus herb was used to extract the ground section of the genus herb (Geranium thunbergii Siebold et Zuccarini) under 50% warming in 50% ethanol for 5 hours, followed by filtration and distilling off the solvent of the filtrate. .

`` Test Methods and Results: Protective Effects Against Inhibition of Intercellular Adhesion Molecule-1 (ICAM-1) Expression in Langerhans Cells by UV Irradiation ''

UVA (5J / cm ² , BLB lamp) was irradiated to Langerhans cells obtained by 0.5% trypsin treatment of the epidermis of human skin, and then cultured in a CO ₂ incubator at 37 ° C for 24 hours with RPMI 1640/10% FBS. After incubation, the cells were treated with FITC-labeled anti-MHC class II antibody (manufactured by Pamigen) and PE-labeled anti-ICAM-1 antibody (manufactured by Pamigen) to 3x10 ⁴ cells with flocite meta (XL: Epix). ICAM-1 expression intensity of Langerhans cells expressing MHC class II antigen was measured. This result is shown in FIG. 5 shows the ICAM-1 expression rate (%), the horizontal axis shows the presence or absence of the extract of the heterogeneous grass (final concentration: wt%). 5, it can be seen that the addition of the extract of the herbaceous grass clearly inhibits the intercellular adhesion molecule-1 (ICAM-1) expression inhibition activity in Langerhans cells by UVA.

Below, the Example which used the heterogeneous herb extract as an immunopotentiator or immune suppression prevention / improvement agent is shown.

"Example 1 cream"

(Prescription)

Stearic acid 5.0 wt%

Stearyl Alcohol 4.0

Isopropyl myristate 18.0

Glycerine Monostearic Acid Ester 3.0

Propylene Glycol 10.0

Cranberry Extract 0.01

Paraaminobenzoic acid0.5

2-ethylhexyl paramethoxy cinnamic acid 5.0

Potassium Hydroxide 0.2

Preservative

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol, distilled grass extract, and potassium hydroxide are added to the ion-exchanged water, dissolved, and heated to 70 ° C. (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is slowly added to the aqueous phase and the addition is complete and held at that temperature for a while to cause the reaction. Thereafter, the mixture is emulsified uniformly with a homomixer and cooled to 30 ° C while stirring well.

`` Example 2 Cream ''

(Prescription)

Stearic acid 2.0% by weight

Stearyl Alcohol 7.0

Water added Lanolin 2.0

Squalane 5.0

2-octyldodecyl alcohol 6.0

Polyoxyethylene (25 mol) cetyl alcohol ether 3.0

Glycerin Monostearic Acid Ester 2.0

Propylene Glycol 5.0

2-ethylhexyl paramethoxy cinnamic acid 10.0

Cranberry Extract 0.05

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol is added to ion-exchanged water and heated to maintain it at 70 캜 (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). Pre-emulsion is performed by adding an oil phase to the aqueous phase, and it is emulsified uniformly with a homomixer, and it cools to 30 degreeC, stirring well.

`` Example 3 Cream ''

(Prescription)

5.0% by weight of solid paraffin

Beeswax 10.0

Waselin 15.0

Liquid Paraffin 41.0

Glycerin Monostearic Acid Ester 2.0

Polyoxyethylene (20 mol) sorbitan monolauric acid ester 2.0

Soap Powder 0.1

2-ethylhexyl paramethoxy cinnamic acid 1.0

Borax 0.2

Cranberry Extract 0.05

Ascorbic acid 2.0

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Soap powder and borax are added to ion-exchanged water, dissolved in heat and maintained at 70 ° C (water phase). The other components are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is gradually added to the aqueous phase while stirring to carry out the reaction. After completion of the reaction, the mixture is emulsified uniformly with a homomixer and cooled to 30 ° C while stirring well after emulsification.

Example 4 Latex

(Prescription)

Stearic acid 2.5% by weight

Cetyl Alcohol 1.5

Waselin 5.0

Liquid Paraffin 10.0

Polyoxyethylene (10 mol) monooleic acid ester 2.0

Polyethylene Glycol 1500 3.0

Triethanolamine 1.0

Carboxy vinyl polymer 0.05

(Brand name: Carbopol 941, B.F.Goodrich Chemical company)

Cranberry Extract 0.01

Octyl Dimethylaminobenzoate 1.0

Sodium hydrogen sulfite 0.01

Arbutin 3.5

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

The carboxyvinyl polymer is dissolved in a small amount of ion exchanged water (phase A). Polyethyleneglycol 1500 and triethanolamine are added to the remaining ion-exchanged water, and it is dissolved by heating and kept at 70 ° C (water phase). The other components are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is added to the aqueous phase to pre-emulsify, A phase is added to emulsify uniformly with a homomixer, and then cooled to 30 ° C while stirring well after emulsification.

Example 5 Latex

(Prescription)

1.0% by weight of microcrystalline wax

Glutathione 1.0

Beeswax 2.0

Lanolin 20.0

Liquid Paraffin 10.0

Octyl dimethylaminobenzoate 3.0

2-ethylhexyl paramethoxy cinnamic acid 5.0

Squalane 5.0

Sorbanthesquioleic acid ester 4.0

Polyoxyethylene (20 mol) sorbitan monooleic acid ester 1.0

Propylene Glycol 7.0

Cranberry Extract 10.0

Ascorbic Magnesium Phosphate 3.0

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol is added to ion-exchanged water and heated to maintain it at 70 캜 (water phase). The other components are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The aqueous phase is slowly added thereto while mixing the oil phase and emulsified uniformly with a homomixer. After emulsification, the mixture is cooled to 30 ° C while stirring well.

"Example 6 jelly"

(Prescription)

95% ethyl alcohol 10.0% by weight

Dipropylene Glycol 15.0

Polyoxyethylene (50 mol) oleyl alcohol ether 2.0

Carboxy Vinyl Polymer 1.0

(Brand name: Carbopol 940, B.F.Goodrich Chemical company)

Sodium hydroxide 0.15

L-arginine 0.1

Paramethoxy Cinnamic Acid Isopropyl 0.1

2-ethylhexyl paramethoxy cinnamic acid 0.5

Titanium Oxide 5.0

Cranberry Extract 7.0

Sodium 2-hydroxy-4-methoxybenzophenonesulfonate 0.05

Ethylenediaminetetraacetate, trisodium, 2-water 0.05

Methylparaben 0.2

Spices

Ion Exchange Water Residue

(quite)

Carbopol 940 is uniformly dissolved in ion-exchanged water, while heterozygous extract and polyoxyethylene (50 mol) oleyl alcohol ether are dissolved in 95% ethanol and added to the aqueous phase. Then, other ingredients are added, followed by neutralization with sodium hydroxide and L-arginine for thickening.

"Example 7 serum"

(Prescription)

(A phase)

Ethyl alcohol (95%) 10.0 wt%

Polyoxyethylene (20 mol) octyldodecanol 1.0

Pantothenylethyl Ether 0.1

Cranberry Extract 1.5

Methylparaben 0.15

(B phase)

Potassium Hydroxide 0.1

(C phase)

Glycerin 5.0

Dipropylene Glycol 10.0

Carboxy Vinyl Polymer 0.2

(Brand name: Carbopol 940, B.F.Goodrich Chemical company)

Purified water residual

(quite)

A phase and C phase are melt | dissolved uniformly, respectively, and a solubilization is carried out by adding A phase to C phase. Subsequently, after adding B phase, a container is filled.

`` Example 8 Pack ''

(Prescription)

(A phase)

Dipropylene glycol 5.0 wt%

Polyoxyethylene (60 mol) hardened castor oil 5.0

(B phase)

Cranberry Extract 0.01

Olive oil 5.0

Tocopherol Acetate 0.2

Ethylparaben 0.2

Spices 0.2

(C phase)

Polyvinyl Alcohol 13.0

(90 degree of soap, degree of polymerization 2,000)

Ethanol 7.0

Purified water residual

(quite)

A phase, B phase, and C phase are melt | dissolved uniformly, respectively, and B phase is added and solubilized. Subsequently, this is added to phase C, and then the container is filled.

`` Example 9 solid foundation ''

(Prescription)

Talc 43.1% by weight

Kaolin 15.0

Serisite 10.0

Zinc Oxide 7.0

Titanium Dioxide 3.8

Yellow Iron Oxide 2.9

Black Iron Oxide 0.2

Squalane 8.0

Isostearic acid 4.0

Monooleic acid POE sorbitan 3.0

Isobutyl octane 2.0

Cranberry Extract 1.0

Preservative

Spices

(quite)

The talc to black iron oxide powder components are sufficiently mixed with a blender, and the oil component, squash extract, preservative, and fragrance of squalane to isocyanate is added thereto, kneaded well, and then filled and molded into a container.

`` Example 10 emulsification type foundation (cream type) ''

(Prescription)

(Powder part)

Titanium Dioxide 10.3% by weight

Serisite 5.4

Kaolin 3.0

Iron Oxide 0.8

Red Iron (III) Oxide 0.3

Black Iron Oxide 0.2

(Charged)

Decamethylcyclopentasiloxane 11.5

Liquid Paraffin 4.5

Polyoxyethylene Modified Dimethyl Polysiloxane 4.0

(Awards)

Purified water 50.0

1,3-butylene glycol 4.5

Cranberry Extract 1.5

Ascorbic Acid Glucoside 1.0

Solbitan sesquioleic acid ester 3.0

Preservative

Spices

(quite)

After heating and stirring the aqueous phase, a sufficiently mixed powder portion is added to the homomixer. After heat-mixed oil phase is added and the homomixer is processed, the fragrance is added while stirring and cooled to room temperature.

[6] Embodiments of the Claims 13 to 14

The immune potentiating effect of rosemary extract and the improvement and prevention of immune function deterioration by ultraviolet rays were examined as a protective effect against inhibition of intercellular adhesion molecule-1 (ICMA-1) expression in Langerhans cells by UV irradiation.

`` Rosemary Extract ''

The rosemary extract used in the following examples was extracted in 50% ethanol of rosemary flowers in 50% ethanol, heated at 50 ° C. for 5 hours, and then filtered and used to concentrate the filtrate.

`` Test Methods and Results: Protective Effects Against Inhibition of Intercellular Adhesion Molecule-1 (ICAM-1) Expression in Langerhans Cells by UV Irradiation ''

Langerhans cells obtained by 0.5% trypsin treatment of human skin were irradiated with UVA (5J / cm ² , BLB lamp), and then cultured in a CO ₂ incubator at 37 ° C for 24 hours with RPMI 1640/10% FBS. After incubation, the cells were treated with a FITC-labeled anti-MHC class II antibody (made by Pharmagene) and a PE-labeled anti-ICAM-1 antibody (made by Pharmazen), and then 3 x 10 ⁴ cells were treated with a flowitem (XL: Epix). ICAM-1 expression intensity of Langerhans cells expressing MHC class II antigen was measured. This result is shown in FIG. 6, the vertical axis represents the ICAM-1 expression rate (%), and the horizontal axis represents the presence or absence of rosemary extract addition (final concentration: wt%). When the rosemary extract is added in FIG. 6, it can be seen that the intercellular adhesion molecule-1 (ICAM-1) expression inhibition effect in Langerhans cells by UVA is clearly defended.

Below, the Example which used rosemary extract as an immunopotentiator or immune suppression prevention / improvement agent is shown.

"Example 1 cream"

(Prescription)

Stearic acid 5.0 wt%

Stearyl Alcohol 4.0

Isopropyl myristate 18.0

Glycerine Monostearic Acid Ester 3.0

Propylene Glycol 10.0

Rosemary Extract 0.01

Paraaminobenzoic acid0.5

2-ethylhexyl paramethoxy cinnamic acid 5.0

Potassium Hydroxide 0.2

Preservative

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol, rosemary extract, and potassium hydroxide are added to the ion-exchanged water, dissolved, and heated to 70 ° C (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is slowly added to the aqueous phase and the addition is complete and held at that temperature for a while to cause the reaction. Thereafter, the mixture is emulsified uniformly with a homomixer and cooled to 30 ° C while stirring well.

`` Example 2 Cream ''

(Prescription)

Stearic acid 2.0% by weight

Stearyl Alcohol 7.0

Water added Lanolin 2.0

Squalane 5.0

2-octyldodecyl alcohol 6.0

Polyoxyethylene (25 mol) cetyl alcohol ether 3.0

Glycerin Monostearic Acid Ester 2.0

Propylene Glycol 5.0

2-ethylhexyl paramethoxy cinnamic acid 10.0

Rosemary Extract 0.05

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol is added to ion-exchanged water and heated to maintain it at 70 캜 (water phase). The other ingredients are mixed, dissolved in heat, and kept at 70 ° C (oil phase). Pre-emulsion is performed by adding an oil phase to the aqueous phase, and it is emulsified uniformly with a homomixer, and it cools to 30 degreeC, stirring well.

`` Example 3 Cream ''

(Prescription)

5.0% by weight of solid paraffin

Beeswax 10.0

Waserin 15.0

Liquid Paraffin 41.0

Glycerin Monostearic Acid Ester 2.0

Polyoxyethylene (20 mol) sorbitan monolauric acid ester 2.0

Soap Powder 0.1

2-ethylhexyl paramethoxy cinnamic acid 1.0

Borax 0.2

Rosemary Extract 0.05

Ascorbic acid 2.0

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Soap powder and borax are added to ion-exchanged water, dissolved in heat and maintained at 70 ° C (water phase). The other components are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is gradually added to the aqueous phase while stirring to carry out the reaction. After completion of the reaction, the mixture is emulsified uniformly with a homomixer, and then cooled to 30 ° C while stirring well after emulsification.

Example 4 Latex

(Prescription)

Stearic acid 2.5% by weight

Cetyl Alcohol 1.5

Waselin 5.0

Liquid Paraffin 10.0

Polyoxyethylene (10 mol) monooleic acid ester 2.0

Polyethylene Glycol 1500 3.0

Triethanolamine 1.0

Carboxy vinyl polymer 0.05

(Brand name: Carbopol 941, B.F.Goodrich Chemical company)

Rosemary Extract 0.01

Octyl Dimethylaminobenzoate 1.0

Sodium hydrogen sulfite 0.01

Arbutin 3.5

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

The carboxyvinyl polymer is dissolved in a small amount of ion exchanged water (phase A). Polyethyleneglycol 1500 and triethanolamine are added to the remaining ion-exchanged water, and it is dissolved by heating and kept at 70 ° C (water phase). The other components are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The oil phase is added to the aqueous phase to pre-emulsify, A phase is added to emulsify uniformly with a homomixer, and then cooled to 30 ° C while stirring well after emulsification.

Example 5 Latex

(Prescription)

1.0% by weight of microcrystalline wax

Glutathione 1.0

Beeswax 2.0

Lanolin 20.0

Liquid Paraffin 10.0

Octyl dimethylaminobenzoate 3.0

2-ethylhexyl paramethoxy cinnamic acid 5.0

Squalane 5.0

Sorbanthesquioleic acid ester 4.0

Polyoxyethylene (20 mol) sorbitan monooleic acid ester 1.0

Propylene Glycol 7.0

Rosemary Extract 10.0

Ascorbic Magnesium Phosphate 3.0

Ethylparaben 0.3

Spices

Ion Exchange Water Residue

(quite)

Propylene glycol is added to ion-exchanged water and heated to maintain it at 70 캜 (water phase). The other components are mixed, dissolved in heat, and kept at 70 ° C (oil phase). The aqueous phase is slowly added thereto while mixing the oil phase and emulsified uniformly with a homomixer. After emulsification, the mixture is cooled to 30 ° C while stirring well.

"Example 6 jelly"

(Prescription)

95% ethyl alcohol 10.0% by weight

Dipropylene Glycol 15.0

Polyoxyethylene (50 mol) oleyl alcohol ether 2.0

Carboxy Vinyl Polymer 1.0

(Brand name: Carbopol 940, B.F.Goodrich Chemical company)

Sodium hydroxide 0.15

L-arginine 0.1

Paramethoxy Cinnamic Acid Isopropyl 0.1

2-ethylhexyl paramethoxy cinnamic acid 0.5

Titanium Oxide 5.0

Rosemary Extract 7.0

Sodium 2-hydroxy-4-methoxybenzophenonesulfonate 0.05

Ethylenediaminetetraacetate, trisodium, 2-water 0.05

Methylparaben 0.2

Spices

Ion Exchange Water Residue

(quite)

Carbopol 940 is uniformly dissolved in ion-exchanged water, while rosemary extract and polyoxyethylene (50 mole) oleyl alcohol ether are dissolved in 95% ethanol and added to the aqueous phase. Then, other ingredients are added, followed by neutralization with sodium hydroxide and L-arginine for thickening.

"Example 7 serum"

(Prescription)

(A phase)

Ethyl alcohol (95%) 10.0 wt%

Polyoxyethylene (20 mol) octyldodecanol 1.0

Pantothenylethyl Ether 0.1

Rosemary Extract 1.5

Methylparaben 0.15

(B phase)

Potassium Hydroxide 0.1

(C phase)

Glycerin 5.0

Dipropylene Glycol 10.0

Carboxy Vinyl Polymer 0.2

(Brand name: Carbopol 940, B.F.Goodrich Chemical company)

Purified water residual

(quite)

A phase and C phase are melt | dissolved uniformly, respectively, and a solubilization is carried out by adding A phase to C phase. Subsequently, after adding B phase, a container is filled.

`` Example 8 Pack ''

(Prescription)

(A phase)

Dipropylene glycol 5.0 wt%

Polyoxyethylene (60 mol) hardened castor oil 5.0

(B phase)

Rosemary Extract 0.01

Olive oil 5.0

Tocopherol Acetate 0.2

Ethylparaben 0.2

Spices 0.2

(C phase)

Polyvinyl Alcohol 13.0

(90 degree of soap, degree of polymerization 2,000)

Ethanol 7.0

Purified water residual

(quite)

A phase, B phase, and C phase are melt | dissolved uniformly, respectively, and B phase is added and solubilized. Subsequently, this is added to phase C, and then the container is filled.

`` Example 9 solid foundation ''

(Prescription)

Talc 43.1% by weight

Kaolin 15.0

Serisite 10.0

Zinc Oxide 7.0

Titanium Dioxide 3.8

Yellow Iron Oxide 2.9

Black Iron Oxide 0.2

Squalane 8.0

Isostearic acid 4.0

Monooleic acid POE sorbitan 3.0

Isobutyl octane 2.0

Rosemary Extract 1.0

Preservative

Spices

(quite)

The talc to black iron oxide powder component is sufficiently mixed with a blender, and the oil component of squalane to isocyanate isocetyl, rosemary extract, preservative, and fragrance are kneaded well, followed by filling and molding into a container.

`` Example 10 emulsification type foundation (cream type) ''

(Prescription)

(Powder part)

Titanium Dioxide 10.3% by weight

Serisite 5.4

Kaolin 3.0

Iron Oxide 0.8

Red Iron (III) Oxide 0.3

Black Iron Oxide 0.2

(Charged)

Decamethylcyclopentasiloxane 11.5

Liquid Paraffin 4.5

Polyoxyethylene Modified Dimethyl Polysiloxane 4.0

(Awards)

Purified water 50.0

1,3-butylene glycol 4.5

Rosemary Extract 1.5

Ascorbic Acid Glucoside 1.0

Solbitan sesquioleic acid ester 3.0

Preservative

Spices

(quite)

After heating and stirring the aqueous phase, a sufficiently mixed powder portion is added to the homomixer. After heat-mixing the oil phase is added, the homomixer is treated, the fragrance is added while stirring, and cooled to room temperature.

As described above, it is possible to provide an excellent skin immunity enhancer or skin immune function improvement / preventive agent which prevents the decrease in skin immune function caused by ultraviolet rays by external use.

Claims (14)

An immunopotentiator for preventing the reduction of ultraviolet skin immune function, comprising glutathione. Ultraviolet ray immune function improvement and prevention agent containing glutathione. An immunopotentiated external preparation for preventing ultraviolet light immune function deterioration, comprising glutathione. An external preparation for improving and preventing ultraviolet skin immune function deterioration, comprising glutathione. Ultraviolet skin immune function lowering immune booster, characterized in that it contains golden extract. Ultraviolet skin immune function improvement improvement prevention agent characterized by containing golden extract. An immunopotentiator, comprising basswood extract. Immune function improvement and prevention agent containing basswood extract. An immunopotentiator, comprising clove extract. Immune function improvement and prevention agent containing clove extract. Immunopotentiator, characterized in that it contains algae extract. Immune function improvement and prevention agent characterized by containing the algae extract. An immunopotentiator, comprising a rosemary extract. Immune function improvement and prevention agent containing rosemary extract.