KR102230753B1 - Liposomal cosmetics and manufacturing method thereof - Google Patents

Abstract

Provided is liposome cosmetics, comprising: madecassoside; liposomes composed of hydrogenated lecithin for encapsulating the madecassoside inside the membrane and delivering the same to skin cells; and a coating layer coated on the membrane surface of the liposomes and composed of vegetable oil, wherein the liposome cosmetics include 0.1% or more and 1% or less of the madecassoside, 1% or more and 5% or less of the hydrogenated lecithin, and 25% or more and 50% or less of the vegetable oil.

Description

Liposomal cosmetics and manufacturing method thereof TECHNICAL FIELD

The present invention relates to a liposomal cosmetic product and a method for manufacturing the same, and more specifically, to a cosmetic product in which a coating layer is formed on the surface of a film of a liposome that captures madecassoside, and a method for manufacturing the same.

The liposome membrane may have a structure similar to that of a cell membrane.

More specifically, the outermost layer of the skin cell membrane may have a double lipid layer structure as a barrier system, and the membrane of the liposome may also have a double lipid layer structure similar to that of the skin barrier system.

Thus, the liposomal membrane and the skin cell membrane can have mutual compatibility due to the similar double lipid layer structure described above.

Accordingly, when a specific component is collected inside the liposome membrane and delivered to the skin cells, due to the mutual compatibility of the liposome membrane and the skin cell membrane, the specific component collected inside the liposome can be efficiently delivered to the skin cells.

Using this interchangeability between the liposome membrane and the skin cell membrane, in the conventional cosmetic field, certain cosmetic ingredients are collected inside the liposome membrane, and a specific cosmetic ingredient collected inside the liposome is delivered to the skin cells, thereby manufacturing liposomal cosmetics. .

However, there is a problem that the membrane structure of a liposome used in conventional liposome cosmetics is physicochemically unstable.

Accordingly, in the conventional liposome cosmetics, certain cosmetic ingredients cannot be properly collected inside the liposome, and there is a problem of leaking before delivery to skin cells.

Accordingly, there is a need for a liposome cosmetic product with improved drug delivery system (DDS) efficiency by reinforcing the structure of the liposome membrane.

One technical problem to be solved by the present invention is to provide a liposomal cosmetic product having a reinforced structure of a liposome membrane and a method for producing the same.

Another technical problem to be solved by the present invention is to provide a liposomal cosmetic product that effectively delivers madecassoside to skin cells and a method for manufacturing the same.

Another technical problem to be solved by the present invention is to provide a liposomal cosmetic and a method for producing the same, which effectively delivers a centella asiatica extract containing a poorly soluble component to skin cells.

Another technical problem to be solved by the present invention is to provide a liposomal cosmetic product having an anti-aging or antioxidant effect and a method for producing the same.

Another technical problem to be solved by the present invention is to provide a liposomal cosmetic product that can be stored at room temperature and a method for manufacturing the same.

The technical problem to be solved by the present invention is not limited to the above.

In order to solve the above technical problem, the present invention provides a liposome cosmetic.

According to an embodiment, the liposome cosmetic comprises madecassoside, the madecassoside, and the madecassoside collected inside the membrane and delivered to skin cells, but a liposome composed of hydrogenated lecithin, and the liposome Doedoe coated on the surface of the membrane, including a coating layer composed of vegetable oil, the madecassoside 0.1% or more to 1% or less, the hydrogenated lecithin 1% or more to 5% or less, and the vegetable oil 25% or more to 50 It may contain a content of% or less.

According to an embodiment, the liposome cosmetic further includes a surfactant, and the surfactant is at least one of glycerin, polyglyceryl-4caprate, and tocopherol Including, but the glycerin 10% or more to 25% or less, the polyglyceryl-4 caprate 1% or more to 5% or less, and the tocopherol may include a content of 1% or more to 5% or less.

According to an embodiment, the liposomal cosmetic further includes a ?t amount of centellar extract 5% or more and 10% or less, and the vegetable oil may be grape seed oil.

According to an embodiment, in the case of a liposomal cosmetic test sample, in which the liposomal cosmetic is contained in an amount of more than 0% to 1% or less, the survival rate of Raw 264.7 cells is higher than that of a reference sample that does not contain the liposomal cosmetic. I can.

According to an embodiment, when a toxic substance is added to a liposomal cosmetic test sample containing the liposomal cosmetic in an amount of more than 0% to 1% or less, the toxic substance is added to a reference sample that does not contain the liposomal cosmetic. Compared to one case, the survival rate of Raw 264.7 cells may be higher.

According to an embodiment, the liposome cosmetic may have stability in a temperature range of 5°C or higher to 50°C or lower for 28 days, from the viewpoint of separation and aggregation.

In order to solve the above-described technical problem, the present invention provides a method of manufacturing a liposomal cosmetic.

According to an embodiment, the manufacturing method of the liposomal cosmetic comprises 0.1% or more to 1% or less of madecassoside, 1% or more to 5% or less of hydrogenated lecithin, and 25% or more to 50% or less of vegetable oil. By providing a cosmetic composition to prepare a cosmetic composition, and using a microfluidizer to apply a predetermined high pressure to the cosmetic composition, a liposomal cosmetic preparation step of preparing a liposomal cosmetic Including, wherein the step of preparing the liposome cosmetic may include forming a liposome composed of the hydrogenated lecithin, which collects the madecassoside therein, seals it with a membrane, and delivers it to skin cells.

According to an embodiment, the manufacturing step of the liposome cosmetic may further include a step of forming a coating layer consisting of the vegetable oil, forming a coating layer coated on the surface of the liposome film, and the vegetable oil may be grape seed oil.

According to an embodiment, the step of manufacturing the liposome cosmetic may include performing a process of applying a predetermined high pressure to the cosmetic composition using the microfluidizer only once.

According to an embodiment, the step of preparing the cosmetic composition comprises further providing a surfactant, and the surfactant comprises at least one of glycerin, polyglyceryl-4caprate, and tocopherol, the glycerin It may include a content of 10% or more to 25% or less, the polyglyceryl-4 caprate 1% to 5% or less, and the tocopherol 1% or more to 5% or less.

According to an embodiment, the step of preparing the cosmetic composition may further include providing a ?t amount of centellar extract 5% or more to 10% or less.

In order to solve the above-described technical problem, the present invention provides a liposome cosmetic.

According to an embodiment, the liposomal cosmetic comprises centella asiatica extract containing a poorly soluble component, the poorly soluble component is collected inside a membrane and delivered to skin cells, but a liposome composed of hydrogenated lecithin, and a membrane of the liposome Doedoe coated on the surface, including a coating layer composed of vegetable oil, the hydrogenated lecithin 1% or more to 5% or less, and the vegetable oil may include a content of 25% or more to 50% or less.

According to an embodiment of the present invention, madecassoside, the madecassoside is collected inside the membrane and delivered to skin cells, but a liposome composed of hydrogenated lecithin, and the membrane surface of the liposome Doedoe coated on, but including a coating layer composed of vegetable oil, the madecassoside 0.1% or more to 1% or less, the hydrogenated lecithin 1% or more to 5% or less, and the vegetable oil 25% or more to 50% or less Liposomal cosmetics, including content, can be provided.

Accordingly, madecassoside is collected inside the membrane of the liposome, but a coating layer is formed on the surface of the membrane of the liposome, so that a liposomal cosmetic product with a reinforced structure of the liposome membrane can be provided.

In addition, since the membrane structure of the liposome is reinforced by the coating layer, leakage of madecassoside collected inside the liposome is minimized, and a liposomal cosmetic product with improved drug delivery system (DDS) efficiency can be provided.

Further, when the liposomal cosmetic is applied to the skin cell membrane, at least a portion of the coating layer is absorbed by the skin cell membrane to provide a path for delivering the madecassoside collected inside the liposome to the skin cells. I can.

In addition, at least another portion of the coating layer may coat the surface of the skin cell membrane to minimize the outflow of madecassoside delivered to the skin cells to the outside of the skin cell membrane.

1 to 5 are views for explaining a liposomal cosmetic according to an embodiment of the present invention.
6 is a flowchart illustrating a method of manufacturing a liposomal cosmetic according to an embodiment of the present invention.
7 to 11 are diagrams for explaining evaluation of properties of liposomal cosmetics according to an embodiment of the present invention.

Hereinafter, exemplary embodiments of the present invention will be described in detail with reference to the accompanying drawings. However, the technical idea of the present invention is not limited to the embodiments described herein and may be embodied in other forms. Rather, the embodiments introduced herein are provided so that the disclosed contents may be thorough and complete, and the spirit of the present invention may be sufficiently conveyed to those skilled in the art.

In the present specification, when a component is referred to as being on another component, it means that it may be formed directly on the other component or that a third component may be placed between them. In addition, in the drawings, the shape and the thickness of the regions are exaggerated for effective explanation of the technical content.

In addition, in various embodiments of the present specification, terms such as first, second, and third are used to describe various elements, but these elements should not be limited by these terms. These terms are only used to distinguish one element from another element. Accordingly, what is referred to as a first component in one embodiment may be referred to as a second component in another embodiment. Each embodiment described and illustrated herein also includes its complementary embodiment. In addition, in the present specification,'and/or' has been used to mean including at least one of the elements listed before and after.

In the specification, expressions in the singular include plural expressions unless the context clearly indicates otherwise. In addition, terms such as "comprise" or "have" are intended to designate the presence of features, numbers, steps, components, or a combination thereof described in the specification, and one or more other features, numbers, steps, or configurations. It is not to be understood as excluding the possibility of the presence or addition of elements or combinations thereof. In addition, in the present specification, "connection" is used to include both indirectly connecting a plurality of constituent elements and direct connecting.

In addition, terms such as "... unit", "... group", and "module" described in the specification mean a unit that processes at least one function or operation, which can be implemented by hardware or software or a combination of hardware and software. have.

In addition, in the following description of the present invention, if it is determined that a detailed description of a related known function or configuration may unnecessarily obscure the subject matter of the present invention, a detailed description thereof will be omitted.

Hereinafter, with reference to the drawings, a liposome cosmetic according to an embodiment of the present invention and a method of manufacturing the same will be described.

1 to 5 are views for explaining a liposomal cosmetic according to an embodiment of the present invention.

The liposome membrane may have a structure similar to that of a cell membrane.

More specifically, the outermost layer of the skin cell membrane may have a double lipid layer structure as a barrier system, and the membrane of the liposome may also have a double lipid layer structure similar to that of the skin barrier system.

Thus, the liposomal membrane and the skin cell membrane can have mutual compatibility due to the similar double lipid layer structure described above.

Accordingly, when a specific component is collected inside the liposome and delivered to the skin cells, due to the mutual compatibility of the liposome membrane and the skin cell membrane, the specific component collected inside the liposome can be efficiently delivered to the skin cells.

Using the interchangeability of such a liposome membrane and a skin cell membrane, in the conventional cosmetic field, a specific cosmetic ingredient is collected inside the liposome, and a specific cosmetic ingredient collected inside the liposome is delivered to the skin cells, thereby manufacturing a liposomal cosmetic.

However, there is a problem that the membrane structure of a liposome used in conventional liposome cosmetics is physicochemically unstable.

Accordingly, in the conventional liposome cosmetic, there is a problem that certain cosmetic ingredients collected inside the liposome cannot be properly collected and leaked before delivery to skin cells.

Meanwhile, according to an embodiment of the present invention, a liposomal cosmetic product with improved drug delivery system (DDS) efficiency can be provided by minimizing leakage of specific cosmetic ingredients collected inside the liposome by enhancing the membrane structure of the liposome.

Further, the liposome cosmetics, when applied to the skin, deliver specific cosmetic ingredients collected inside the liposome to the skin cells, but in order to minimize the outflow of the specific cosmetic ingredients outside the outermost layer of the skin cell membrane, the skin cell membrane The surface of the outermost layer can be coated.

To this end, referring to FIG. 1, the liposome cosmetic 1000 may include a liposome 200 or a coating layer 300.

More specifically, the liposome 200 may be composed of a collection space 210 for collecting a specific cosmetic ingredient 100 therein, or a liposome membrane 220 surrounding the collection space 210.

Accordingly, the liposome 200 collects the specific cosmetic component 100 in the collection space 210, and through the liposome membrane 220 surrounding the collection space 210, the specific cosmetic component 100 ) Can be delivered to skin cells (SC).

According to an embodiment, the liposome membrane 220 may be formed of hydrogenated lecithin.

Hydrogenated lecithin is a phospholipid formed by adding hydrogen to lecithin obtained from beans and eggs.

The liposomal membrane 220 may have a double phospholipid layer (DL) structure, as shown in FIG. 2, by being composed of hydrogenated lecithin.

In this case, the phospholipid may include a head portion HP having hydrophilicity and a tail portion LP having lipophilicity.

Accordingly, the structure of the double phospholipid layer (DL) means that when the phospholipid is exposed to moisture, the hydrophilic head HP prefers to be in contact with moisture, as shown in FIG. 2. The lipophilic tails LP, which are arranged and preferring to be away from moisture, may be referred to as a double layer DL formed by being arranged so as to gather away from moisture but gather with each other.

The structure of the double phospholipid layer (DL) of the liposome membrane 220 may be similar to the structure of the double phospholipid layer of the skin cell membrane (SK).

Accordingly, according to an embodiment of the present invention, due to the similar double phospholipid layer structure of the liposomal membrane 220 and the skin cell membrane SK, mutual compatibility may be achieved.

Accordingly, when a specific cosmetic ingredient 100 is collected in the collection space 210 and the liposome 200 surrounded by the liposome membrane 220 is delivered to the skin cells SC, the liposome membrane 220 and Due to the mutual compatibility of the skin cell membrane SK, the specific cosmetic ingredient 100 collected in the collection space 210 can be efficiently delivered to the skin cells SC.

In contrast, in conventional liposome cosmetics, liposomes composed of lecithin are used. That is, the conventional liposome cosmetics use a liposome membrane composed of lecithin phospholipids, not phospholipids formed by adding hydrogen to lecithin.

In such conventional liposomal cosmetics, when a liposome membrane composed of lecithin phospholipid contacts oxygen, the membrane structure becomes unstable.

Accordingly, in the conventional liposome cosmetics, certain cosmetic ingredients cannot be properly collected inside the liposome, and there is a problem of leaking before delivery to skin cells.

However, according to an embodiment of the present invention, since the liposome film 220 is composed of hydrogenated lecithin phospholipid formed by adding hydrogen to lecithin, it may have stability in the membrane structure even when in contact with oxygen.

Accordingly, the specific cosmetic ingredient 100 collected in the collection space 210 can be efficiently delivered to the skin cells SC.

According to an embodiment, the hydrogenated lecithin constituting the liposome membrane 220 may be included in an amount of 1% or more to 5% or less of the total content of the liposome cosmetic 1000.

Furthermore, the liposomal cosmetic 1000 according to an embodiment of the present invention may include a coating layer 300 as shown in FIG. 3.

More specifically, the coating layer 300 may be coated on the surface of the liposome film 220.

Accordingly, as shown in FIG. 3, when the liposomal cosmetic 1000 is provided on and applied to the skin cell membrane SK, as shown in FIG. 4, at least a portion of the coating layer 300 is a skin cell membrane. (SK) may be contacted first, and since the temperature of the skin cell membrane SK is higher than the coating layer 300, at least a portion of the coating layer 300 first contacting the skin cell membrane SK, the It can be absorbed into the skin cell membrane (SK).

When at least a portion of the coating layer 300 is absorbed by the skin cell membrane SK, the liposomal membrane 220 in an area corresponding to the portion of the coating layer 300 absorbed by the skin cell membrane SK Can come into contact with (SK).

As described above, the liposomal membrane 220 may have a double phospholipid layer structure similar to that of the skin cell membrane SK, and thus, the liposomal membrane 220 and the skin cell membrane SK may have mutual compatibility. I can.

Accordingly, as shown in FIG. 5, due to the mutual compatibility described above, the specific cosmetic component 100 collected in the collection space 210 may be delivered to the skin cells SC.

In this case, as shown in FIG. 5, at least one portion of the coating layer 300 may be absorbed by the skin cell membrane SK as described above, and at least another portion of the coating layer 300 is the skin cell membrane ( SK) Surface can be coated.

Accordingly, the coating layer 300 is coated on the surface of the skin cell membrane (SK), and the specific cosmetic component 100 transferred from the collection space 210 to the skin cells (SC), the skin cell membrane (SK) It can minimize leakage to the outside.

According to an embodiment, the coating layer 300 may be made of vegetable oil.

More specifically, the coating layer 300 may be composed of grape seed oil.

In the embodiments described below, it is assumed that the vegetable oil is grape seed oil.

Grapeseed oil may contain about 20% of fat in the total content, and about 95% of neutral fat, about 3% of phospholipids, and about 3% of sugar lipids in the about 20% of fat content.

As described above, the grape seed oil contains a very small amount of phospholipids compared to the amount of phospholipids constituting most of the liposome membrane 200, and contains more fat components other than phospholipids.

Accordingly, the phospholipids of the grape seed oil have mutual compatibility with the phospholipids of the liposome membrane 200, but fat components other than the phospholipids of the grape seed oil may be coated on the surface of the liposome membrane 200.

Accordingly, the coating layer 300 composed of grape seed oil may be coated on the surface of the liposomal membrane 220, thereby reinforcing the structure of the liposomal membrane 220.

Therefore, unlike the structure of the weak liposome membrane of the conventional liposomal cosmetic, the structure of the liposome membrane 220 surrounding the specific cosmetic ingredient 100 collected in the collection space 210 is strengthened, so that the collection space 210 It is possible to minimize the leakage of the specific cosmetic ingredient 100 collected in.

That is, according to an embodiment of the present invention, by reinforcing the structure of the liposome film 220 through the coating layer 300, the specific cosmetic ingredient 100 collected in the collection space 210 is sealed, but leaks Can be minimized. Accordingly, the liposomal cosmetic 1000 may improve encapsulation efficiency.

Furthermore, when the liposomal cosmetic 1000 is provided on and applied to the skin cell membrane SK, at least a portion of the coating layer 300 is absorbed by the skin cell membrane SK, and is thus contained in the collection space 210. A path for delivering the collected specific cosmetic ingredient 100 to skin cells (SC) may be provided.

Further, at least another part of the coating layer 300 coats the surface of the skin cell membrane (SK), so that the specific cosmetic ingredient 100 delivered to the skin cell (SC) flows out of the skin cell membrane (SK). It can be minimized.

According to an embodiment, the grape seed oil constituting the coating layer 300 may be included in an amount of 25% or more to 50% or less of the total content of the liposomal cosmetic 1000.

Meanwhile, according to an embodiment of the present invention, the specific cosmetic ingredient 100 collected in the collection space 210 may be madecassoside or centella asiatica extract.

Centella asiatica belongs to a family of dicotyledons, umbel, and is a creeping plant that grows as a vine with a stem or root extending over the ground, and is a perennial.

Centella is a representative species, and its origin is the tropical regions of the Indian Ocean. Centella asiatica until now has been used as a medicinal plant in various regions of the world, and is also known in Korea under the name tiger grass.

Through various studies in the prior art, Centella asiatica has been reported to have various effects such as wound healing, skin tissue regeneration, scar prevention, anti-inflammatory effect, antibacterial effect, antioxidant effect, anticancer effect, and whitening effect.

This is because it contains components such as centella, madecassoside 100, and asiaticoside.

In more detail, looking at the effect of each component of centella asiatica, the madecassoside 100 has an effect of improving wrinkles, flexibility, elasticity, skin roughness, or skin moisturizing. In addition, the madecassoside 100 has the effect of improving the survival rate of cells by protecting cells from toxic substances and minimizing cell death.

On the other hand, asiaticoside has an antibacterial or antifungal effect, and is also effective in treating wounds or skin diseases. In addition, asiaticoside has the effect of improving the survival rate of cells by minimizing cell death.

However, among the components of Centella asiatica, a component having poorly soluble properties that is not well soluble in a solvent is contained. Therefore, centella extract is difficult to use as a cosmetic raw material has a problem.

Due to the characteristics of centella asiatica extract containing such a poorly soluble component, in the conventional cosmetic field, centella asiatica extract cosmetics are manufactured in an emulsion form in order to use the centella asiatica extract as a cosmetic raw material.

Here, the emulsion formulation means, in two or more types of liquids each composed of different particle sizes, relatively small particles constituting one liquid. It may refer to a formulation dispersed between relatively large particles constituting another liquid. Therefore, emulsions are also referred to as emulsions or emulsions.

As described above, conventionally, by preparing a cosmetic product of centella asiatica extract in an emulsion formulation, the problem of poor solubility in the use of the cosmetic material of the centella asiatica extract described above was seen to be solved.

However, since the emulsion formulation is in a thermodynamically unstable state, it is necessary to use an emulsifier, and there is a problem that a separation phenomenon easily occurs due to agglomeration, sedimentation, or adhesion due to a thermodynamic unstable state.

In addition, if the emulsifier is continuously used on the skin in large amounts, the skin barrier may collapse. When the skin barrier collapses, ingredients such as preservatives included in the cosmetics may penetrate to the base layer of the skin through the cracks in order to minimize spoilage of the cosmetics. Accordingly, skin diseases such as seborrheic dermatitis or atopy may be induced in the skin.

That is, the conventional centella asiatica extract cosmetics are provided in an emulsion formulation due to the poorly soluble components contained in the centella asiatica extract, but skin diseases may be caused by the emulsifier included in the emulsion formulation.

Meanwhile, according to an embodiment of the present invention, a liposomal cosmetic that effectively delivers madecassoside or centella asiatica extract to skin cells SC can be provided without causing skin disease.

That is, as described above, the liposomal cosmetic 1000 according to the embodiment of the present invention can collect madecassoside or centella asiatica extract as a specific cosmetic ingredient 100 in the collection space 210, and the collection The space 210 may be surrounded by a liposome film 220 composed of the hydrogenated lecithin, and the surface of the liposome film 220 may be coated with a coating layer 300 composed of the grape seed oil.

Accordingly, unlike conventional centella asiatica extract cosmetics, the liposome cosmetic product 1000 is capable of effectively delivering to skin cells (SC) by collecting centella asiatica extract containing a poorly soluble component without containing a large amount of an emulsifier. will be.

According to an embodiment, the madecassoside 100 may be included in an amount of 0.1% or more to 1% or less of the total content of the liposomal cosmetic 1000.

In the above-described embodiment, madecassoside or centella asiatica extract is exemplified as an example of the specific cosmetic ingredient 100, but is not limited thereto.

That is, in the present invention, not only a soluble component, but also a cosmetic material having poorly soluble properties, such as a poorly soluble component included in centella asiatica extract, is collected in the collection space 210 and surrounded by the liposome membrane 220, and the liposome membrane It is an object of the present invention to provide a liposomal cosmetic 1000 including a reinforced reforming structure by forming the coating layer 300 on the surface of the 220.

In addition, in the above-described embodiment, the liposomal cosmetic 1000 has been described as including at least one of the madecassoside 100 or centella asiatica extract, the liposome 200, and the coating layer 300, The present invention is not limited thereto, and a functional cosmetic ingredient that provides effects such as lubrication, moisturization, nutrition, and whitening to the skin may be additionally included.

Furthermore, the liposome cosmetic 1000 may further include a surfactant to improve stability in terms of separation and aggregation between the cosmetic raw material having hydrophilicity and the cosmetic raw material having lipophilicity.

However, the liposomal cosmetic 1000 of the present invention, as described above, collects a specific cosmetic ingredient 100 inside the structure of the liposome 200, surrounds the liposome film 220, and forms a coating layer 300 to form a skin Since it is provided to the cells (SC), it does not contain a large amount of emulsifier, as in conventional emulsion formulation cosmetics.

The functional cosmetic raw material, and the surfactant, which are additionally included in the liposomal cosmetic 1000, will be described in more detail in the method of manufacturing a liposomal cosmetic to be described later.

Hereinafter, a method of manufacturing a liposomal cosmetic according to an embodiment of the present invention will be described.

6 is a flowchart illustrating a method of manufacturing a liposomal cosmetic according to an embodiment of the present invention.

Referring to FIG. 6, the manufacturing method of the liposome cosmetic may include a cosmetic composition manufacturing step (S110) or a liposomal cosmetic manufacturing step (S120).

Hereinafter, each step will be described in more detail. In each step to be described below, a description overlapping with the above description will be omitted. In addition, hereinafter, the specific cosmetic ingredient 100 will be described on the assumption that it is madecassoside, and the vegetable oil is grape seed oil.

Step S110

In step S110, a cosmetic composition may be prepared.

More specifically, the cosmetic composition may be prepared by providing at least one of madecassoside 100, hydrogenated lecithin, and grape seed oil.

According to an embodiment, the madecassoside 100 may be provided in an amount of 0.1% or more to 1% or less. In addition, the hydrogenated lecithin may be provided in an amount of 1% or more to 5% or less. In addition, the grape seed oil may be provided in an amount of 25% or more to 50% or less.

Unlike the exemplary embodiment of the present invention, when the hydrogenated lecithin is provided in an amount of less than 1%, separation or aggregation may occur in cosmetics manufactured in the steps described below. On the other hand, when the hydrogenated lecithin is provided in an amount of more than 5%, the viscosity of the cosmetic composition increases, and it may be difficult to form liposomes in the steps described below.

Alternatively, when the grape seed oil is provided in an amount of more than 50%, separation or aggregation may occur in the cosmetic manufactured in the step described below.

However, according to an embodiment of the present invention, the hydrogenated lecithin may be provided in an amount of 1% or more to 5% or less, and the grape seed oil may be provided in an amount of 25% or more to 50% or less.

Accordingly, it is easy to form a liposome in a step to be described later, and further, the liposome cosmetic product 1000 prepared in a step to be described later may have stability in terms of separation and aggregation.

On the other hand, in the above-described embodiment, the reason that the madecassoside 100 is provided in an amount of 0.1% or more to 1% or less is because if the madecassoside component is contained in excess of 1%, it is classified as a medicine.

According to an embodiment, in step S110, a functional cosmetic raw material may be further provided.

For example, the functional cosmetic raw material may be at least one selected from centella asiatica extract, stearic acid, asiaticoside, and ethylhexylglycerin.

The centella extract may be effective in wound healing, skin tissue regeneration, scar prevention, anti-inflammatory, antibacterial, antioxidant, anti-cancer, or whitening, as described above.

Meanwhile, as described above, the centella asiatica extract may contain a poorly soluble component.

The stearic acid may have an effect of preventing water evaporation by forming an oil film on the skin.

The asiaticoside, as described above, has an antibacterial/antifungal, or wound/skin disease treatment effect, and may have an effect of improving cell survival.

The ethylhexyl glycerin is effective in lubricating or moisturizing, and may have a deodorizing effect because it inhibits the growth or reproduction of bacteria that cause a characteristic odor.

According to an embodiment, the centella asiatica extract may be provided in an amount of ?t of 5% or more to 10% or less. In addition, the stearic acid may be provided in an amount of ?t of 0.1% or more to 1% or less. In addition, the asiaticoside may be provided in an amount of ?t of 0.1% or more to 1% or less. In addition, the ethylhexyl glycerin may be provided in an amount of ?t of 0.01% or more to 0.1% or less.

According to an embodiment, in step S110, a surfactant may be further provided.

The surfactant may reduce the interfacial tension between the cosmetic ingredients having hydrophilicity and the cosmetic ingredients having lipophilicity in the cosmetic composition, thereby maintaining a mixed state between the cosmetic ingredients, thereby minimizing separation or aggregation.

For example, the surfactant may be at least one selected from glycerin, polyglyceryl-4caprate, and tocopherol.

The glycerin may not only lower the interfacial tension between cosmetic ingredients as described above, but also have a lubricating or moisturizing effect.

In addition to lowering the interfacial tension between the tocopherol and the cosmetic ingredients as described above, it may have an antioxidant effect by providing vitamin E.

According to an embodiment, the glycerin may be provided in an amount of ?t of 10% or more to 25% or less. In addition, the polyglyceryl-4 caprate may be provided in an amount of ?t of 1% or more to 5% or less. In addition, tocopherol may be provided in an amount of ?t of 1% or more and 5% or less.

In addition, in step S110, purified water or 1,2-hexanediol may be further provided.

The purified water may provide fluidity to the liposomal cosmetic 1000 prepared in a step described later. That is, the purified water may serve to deliver cosmetic ingredients included in the liposomal cosmetic 1000 to the skin.

In general, most cosmetic ingredients exist in a sticky state with high viscosity. Accordingly, cosmetic ingredients have low fluidity, and therefore, when the cosmetic ingredients themselves are applied to the skin, they are difficult to be absorbed into the skin.

For example, in the case of cosmetics containing honey as a cosmetic raw material, if clean water is not included, it is difficult to apply to the skin due to the stickiness of the honey, and it is difficult to be absorbed by the skin. However, when honey is dissolved in water, its fluidity improves, making it easier to apply to the skin and absorb it into the skin.

In this way, the purified water not only provides fluidity to the liposomal cosmetic 1000, but also improves the skin absorption rate of the liposomal cosmetic 1000.

Meanwhile, the 1,2-hexanediol may minimize deterioration of the liposome cosmetic 1000. That is, the 1,2-hexanediol may serve as an antiseptic so that cosmetic ingredients included in the liposomal cosmetic 1000 do not deteriorate for a predetermined period and maintain their function or shape.

According to an embodiment, the purified water may be provided in an amount of ?t of 25% or more and 50% or less. In addition, the 1,2-hexanediol may be provided in an amount of ?t of 1% or more and 5% or less.

Step S120

In step S120, a liposomal cosmetic 1000 may be manufactured.

More specifically, the liposomal cosmetic 1000 may be manufactured through a process of applying a predetermined high pressure to the cosmetic composition prepared in step S110 using a microfluidizer.

Accordingly, as described above, the madecassoside 100 is collected in the collection space 210 and surrounded by the liposome film 220, and the coating layer 300 is provided on the surface of the liposome film 220. This formed, liposomal cosmetic 1000 can be manufactured.

Alternatively, the centella extract is collected in the collection space 210, and surrounded by the liposome membrane 220, and the coating layer 300 is formed on the surface of the liposome membrane 220, and a liposomal cosmetic 1000 is prepared. Can be.

At this time, as described above, the liposome film 220 may be composed of hydrogenated lecithin, and the coating layer 300 may be composed of grape seed oil.

The liposomal cosmetic 1000 has been described above, and redundant descriptions will be omitted.

According to an embodiment of the present invention, in step S120, the process of applying a predetermined high pressure to the cosmetic composition using the microfluidizer may be performed only once.

In contrast, in the conventional method of manufacturing liposomal cosmetics using a microfluidizer, the process of applying high pressure to the cosmetic composition using a microfluidizer is more than once, for example, most of them are 3 or more to 5 times. It is carried out as follows.

Accordingly, the conventional method of manufacturing a liposomal cosmetic using a microfluidizer has a disadvantage in that it takes a long time and high cost.

However, in the method of manufacturing a liposomal cosmetic according to an embodiment of the present invention, since the process of applying a predetermined high pressure to the cosmetic composition using a microfluidizer is performed only once, it is possible to save time and cost, so it is efficient. to be.

This, as described above, the liposome cosmetic 1000 is composed of a liposome membrane 220 of hydrogenated lecithin, a phospholipid formed by adding hydrogen to lecithin, and the surface of the liposome membrane 220 is made of grape seed oil Since the configured coating layer 300 is formed, it may be because the collection efficiency is improved.

That is, in the manufacturing method of the liposome cosmetic 1000, unlike the conventional liposomal cosmetic, the collection efficiency is improved, so that the process of applying a predetermined high pressure to the cosmetic composition using a microfluidizer is performed only once. It can be.

Hereinafter, evaluation of the properties of a liposomal cosmetic according to an embodiment of the present invention will be described.

7 to 11 are diagrams for explaining evaluation of properties of liposomal cosmetics according to an embodiment of the present invention.

7 and 8, in order to evaluate the cell viability of the liposome cosmetic 1000, a liposomal cosmetic test sample a containing the liposomal cosmetic 1000 in an amount of 0.1%, and the A liposome cosmetic test sample b containing a liposomal cosmetic 1000 in an amount of 1% was prepared.

At this time, a reference sample that does not contain the liposomal cosmetic 1000 was prepared and referred to as a comparison object of the liposomal cosmetic test sample a and the test sample b.

Referring to FIG. 7, the prepared liposome cosmetic test sample a, test sample b, and reference sample were provided to Raw 264.7 cells, respectively, and the survival rate of Raw 264.7 cells was examined.

As shown in FIG. 7, looking at 100% of the cell viability when the reference sample is provided to Raw 264.7 cells, the cell viability is about 170% when the liposome cosmetic test sample a is provided to Raw 264.7 cells, When the liposome cosmetic test sample b is provided to Raw 264.7 cells, it can be confirmed that the cell viability is about 150%.

That is, according to an embodiment of the present invention, in the case of a liposomal cosmetic test sample, which contains the liposomal cosmetic 1000 in an amount greater than 0% to 1% or less, compared to a reference sample that does not contain the liposomal cosmetic, It can be seen that the survival rate of Raw 264.7 cells is high.

Meanwhile, referring to FIG. 8, the prepared liposome cosmetic test sample a, test sample b, and reference sample were provided to Raw 264.7 cells, respectively, and toxic substances were additionally provided to examine the survival rate of Raw 264.7 cells.

Here, the toxic substance may be hydrogen peroxide (H ₂ O ₂ ).

As shown in Figure 8, looking at 100% of the cell viability when the reference sample is provided to Raw 264.7 cells, the cell viability when the reference sample is provided to Raw 264.7 cells and the toxic substance is additionally provided. Is about 5%, and when the liposome cosmetic test sample a is provided to Raw 264.7 cells, and the toxic substance is additionally provided, the cell viability is about 60%, and the liposome cosmetic test sample b is provided to Raw 264.7 cells. , When the toxic substance is additionally provided, it can be confirmed that the cell viability is about 30%.

That is, according to an embodiment of the present invention, when a toxic substance is added to a liposomal cosmetic test sample, which contains the liposomal cosmetic in an amount of more than 0% to 1% or less, the reference sample does not contain the liposomal cosmetic. Compared to the case of adding toxic substances, it can be seen that the survival rate of Raw 264.7 cells is higher.

On the other hand, hydrogen peroxide provided as the toxic substance is also one kind of active oxygen.

Here, the active oxygen may be understood as a concept collectively referring to a highly reactive oxygen compound made inside the human body or an active oxygen floating in the air.

Since reactive oxygen damages cells, since it is a substance related to aging of the human body or oxidation of the skin, it has become an issue in the field of human health or skin beauty.

However, as described above with reference to FIG. 8, the liposomal cosmetic 1000 according to an embodiment of the present invention can improve cell viability even when hydrogen peroxide, that is, active oxygen, is provided, so that anti-aging or antioxidant effects are achieved. You can see that there is.

On the other hand, referring to FIGS. 9 to 11, stability of the liposomal cosmetic 1000 in terms of separation and aggregation over time according to temperature can be observed.

Referring to FIG. 9, it can be seen that the liposomal cosmetic 1000 has stability without being separated or agglomerated for 28 days at a high temperature of 50°C.

In addition, referring to FIG. 10, it can be seen that the liposome cosmetic 1000 is not separated or aggregated for 28 days even at a low temperature of 5° C. and has stability.

Furthermore, referring to FIG. 11, it is known that the liposome cosmetic 1000 has stability without separation or aggregation even in a mixed environment of high temperature (50° C.) and low temperature (5° C.) alternately provided every other day for 28 days. I can.

Accordingly, the liposomal cosmetic 1000 can be stored at room temperature regardless of seasons such as summer or winter due to excellent temperature stability in a temperature range of 5° C. or more to 50° C. or less, as described above, This has an excellent advantage.

As described above, the present invention has been described in detail using preferred embodiments, but the scope of the present invention is not limited to specific embodiments, and should be interpreted by the appended claims. In addition, those who have acquired ordinary knowledge in this technical field should understand that many modifications and variations are possible without departing from the scope of the present invention.

100: madecassoside
200: liposome
210: collection space
220: liposome membrane
300: coating layer

Claims (12)

Madecassoside;
A liposome comprising a liposome membrane composed of hydrogenated lecithin, a phospholipid having stability against oxygen, which traps the madecassoside inside the liposome membrane and delivers it to skin cells; And
Doedoe coated on the surface of the liposome membrane, a coating layer composed of vegetable oil; Including,
The madecassoside 0.1% by weight or more and 1% by weight or less, the hydrogenated lecithin 1% by weight or more and 5% by weight or less, and the vegetable oil 25% by weight or more to 50% by weight or less,
The coating layer,
The vegetable oil contains a phospholipid and a fat component in an amount less than 33 times greater than that of the phospholipid,
The vegetable oil is grape seed oil, liposomal cosmetics.
The method of claim 1,
Further comprising a surfactant,
The surfactant includes at least one of glycerin, polyglyceryl-4caprate, and tocopherol,
Liposomal cosmetics comprising a content of 10 wt% or more to 25 wt% or less of the glycerin, 1 wt% or more to 5 wt% or less of the polyglyceryl-4caprate, and 1 wt% or more to 5 wt% or less of the tocopherol .
The method of claim 1,
Centella asiatica extract 5% by weight or more to 10% by weight or less ?t amount further comprising, a liposome cosmetic.
The method of claim 1,
In the case of a liposome cosmetic test sample, wherein the liposomal cosmetic is contained in an amount of more than 0% by weight to 1% by weight or less, the survival rate of Raw 264.7 cells is higher than that of the reference sample, which does not contain the liposome cosmetic.
The method of claim 1,
When the toxic substance is added to the liposomal cosmetic test sample, which contains the liposomal cosmetic in an amount of more than 0% by weight to 1% by weight, compared to the case where the toxic substance is added to the reference sample without the liposomal cosmetic , Raw 264.7 Cell viability is high, liposome cosmetics.
The method of claim 1,
The liposome cosmetics,
Liposomal cosmetics having stability in terms of separation and aggregation for 28 days in a temperature range of 5° C. or more to 50° C. or less.
Madecassoside 0.1% by weight or more and 1% by weight or less, hydrogenated lecithin 1% by weight or more and 5% by weight or less, and vegetable oil 25% by weight or more and 50% by weight or less, to prepare a cosmetic composition , Cosmetic composition manufacturing step; And
Using a microfluidizer, a process of applying a predetermined high pressure to the cosmetic composition to prepare a liposomal cosmetic, a liposomal cosmetic manufacturing step; including,
The liposome cosmetic manufacturing step,
Including a liposome membrane composed of the hydrogenated lecithin, which is a phospholipid having stability against oxygen, trapping the madecassoside inside the liposome membrane and forming a liposome for delivery to skin cells, forming a liposome; And
Consisting of the vegetable oil, forming a coating layer coated on the surface of the liposome film, forming a coating layer; further comprising,
The liposome,
Even when in contact with oxygen, through hydrogenated lecithin constituting the liposomal membrane having stability against oxygen, madecassoside inside the liposome membrane is protected from oxygen to non-spill out of the liposome membrane,
The coating layer,
Phospholipid in the vegetable oil and a fat component in an amount less than 33 times greater than that of the phospholipid, but the phospholipid in the vegetable oil has mutual compatibility with the hydrogenated lecithin,
The fat component of the vegetable oil is coated on the surface of the liposome membrane, so that the madecassoside inside the liposome membrane is protected so that it non-spills out of the liposome membrane before the coating layer comes into contact with the skin cell membrane,
When the coating layer is in contact with the skin cell membrane, at least a portion of the coating layer is absorbed by the skin cell membrane so that the madecassoside inside the liposome membrane is transferred to the skin cells, and at least another portion of the coating layer is the madecassoside. Coats the surface of the skin cell membrane that has been transferred,
The method of manufacturing a liposomal cosmetic comprising that the vegetable oil is grape seed oil.
delete The method of claim 7,
The liposome cosmetic manufacturing step,
A method for producing a liposomal cosmetic comprising performing a process of applying a predetermined high pressure to the cosmetic composition using the microfluidizer only once.
The method of claim 7,
The manufacturing step of the cosmetic composition,
Including further providing a surfactant,
The surfactant includes at least any one of glycerin, polyglyceryl-4 caprate, and tocopherol,
Liposomal cosmetics comprising a content of 10 wt% or more to 25 wt% or less of the glycerin, 1 wt% or more to 5 wt% or less of the polyglyceryl-4caprate, and 1 wt% or more to 5 wt% or less of the tocopherol Manufacturing method.
The method of claim 7,
The manufacturing step of the cosmetic composition,
Centella asiatica extract comprising further providing a ?t amount of 5% by weight or more and 10% by weight or less, a method for producing a liposome cosmetic.
Centella asiatica extract containing poorly soluble ingredients;
A liposome comprising a liposome membrane composed of hydrogenated lecithin, which is a phospholipid having stability against oxygen, which traps the poorly soluble component inside the liposome membrane and delivers it to skin cells; And
Doedoe coated on the surface of the liposome membrane, a coating layer composed of vegetable oil; Including,
The hydrogenated lecithin 1% by weight or more and 5% by weight or less, and the vegetable oil 25% by weight or more and 50% by weight or less,
The coating layer,
The vegetable oil contains a phospholipid and a fat component in an amount less than 33 times greater than that of the phospholipid,
The vegetable oil is grape seed oil, liposomal cosmetics.

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