KR20190122561A - Lymphatic circulation promotor - Google Patents

Abstract

Disclosed is a lymphatic circulation promoter which promotes lymph circulation in the body to improve an environment around cells and to help a cell metabolism recovered normally. The lymphatic circulation promoter according to the present invention contains Cnidium officinale, maple syrup, Citrus aurantium, Phllostachys nigra, Kalopanax pictus, and Coix lacryma-jobi var. mayuen in a form of powder, liquid or extract.

Description

Lymphatic circulation promoter and its use {LYMPHATIC CIRCULATION PROMOTOR}

The present invention relates to a lymph circulation promoting agent and its use, and more particularly, to a lymph circulation promoting agent and its use which can promote the lymph circulation in the body to improve the environment around the cell and help the cell metabolism to be restored normally.

The inventors of the present invention have learned from numerous clinical experiences that smooth lymph circulation plays an important role in maintaining a healthy body condition and rapidly recovering a diseased body.

Body fluid circulation involves both blood and lymphatic circulation and is responsible for the physical material circulation in the body. Blood circulation plays a pivotal role in the body's material circulation, and lymph circulation plays a secondary role in helping cardiovascular material circulation.

Lymphatic system is composed of lymph, lymphatic vessels, lymph nodes. They are responsible for returning the body fluids that may be present between the tissues of the body to the heart. In addition, after metabolism from the tissue and the remaining waste and cell metabolites such as high molecular weight fat or protein that can not pass through the capillaries, it serves to send blood through the vena cava. Capillary lymphatic vessels exist adjacent to capillaries and are distributed throughout the body. Tissue fluid in the tissue enters the capillary lymphatic vessel and becomes lymphatic fluid. When the fluid enters the lymphatic vessels, unlike capillaries, they do not pass through the membrane, but through the small holes at the ends of the capillary lymphatic vessels. Therefore, even a large molecular weight that can not pass through the membrane of the capillaries can easily pass through, most of the components of the tissue fluid is contained in the lymph. The distal end of the capillary lymphatic vessel has a structure that is difficult for fluid to enter the lymphatic vessel. Lymphatic fluid is similar to tissue fluid and consists of water, dead cells, fats and proteins, salts, sugars, urea, and lymphocytes. Lymphatic vessels are the channels that carry lymph from the tissues to the vena cava. Lymphatic vessels are divided into perforated lymphatic vessels between the skin and fascia and deep lymphatic vessels located under the fascia. Therefore, the lymphatic vessels play an important role in lymph circulation, and it is possible to promote lymph circulation through lymph massage, which physically stimulates the skin in position. Lymphatic fluid movement is caused mainly by the small forces produced by the contraction and relaxation of the valves and muscles in the lymphatic vessels. When the muscles contract, the lymphatic vessels are pressed by the partially thickened muscles, reducing the volume inside the lymphatic vessels. Lymphatic fluid does not go in the direction blocked by the valve by the volume of the reduced lymphatic vessels, but moves in the heart direction. On the contrary, when the muscle is relaxed, the lymphatic vessel, which was partially pressed down, recovers and the volume inside the lymphatic vessel increases. In this case, the lymphatic fluid must be replenished by the increased volume, but it does not come from the heart blocked by the valve, but moves away from the heart to fill. Thus, one segment of the valve acts as a small heart-like pump that assists in lymph circulation as the muscles move. In addition, many of these small pumps are connected in series, so long-term muscle movement such as arms and legs is a powerful power source for promoting lymphatic movement. Capillary lymphatic vessels, which are closer to the skin than capillaries, are susceptible to pathogenic microorganisms such as bacteria and viruses even when the skin is lightly damaged. To compensate for this, lymph nodes are present before the lymphatic vessels reach the vena cava. Lymph nodes have a network structure and the internal network structure can be blocked well, so it is distributed mainly in the ears, under the tongue, under the armpits, the groin, etc., where there are many muscle movements or large parts. Lymph nodes produce lymphocytes to protect the body from invasion by pathogens, and filter and disintegrate and remove pathogens, such as bacteria and viruses, and dead cells and waste products from the lymph before returning to the blood. Lymphatic flow begins when tissue fluid enters the capillary lymphatic vessels. Capillary lymphatic vessels join the lymphatic vessels, and the lymphatic vessels have lymphatic valves that prevent the backflow of lymphatic fluid and create a circulating power of the lymphatic fluid, like the venous valve. Lymph fluid, in turn, passes through the lymph nodes, which block the invasion of microorganisms, and merges with blood in the vena cava. Thus, the lymphatic circulation begins at the fingertips, toes and heads and proceeds toward the heart, passing through the lymph nodes in the armpits, groin, under the ear and under the tongue, filtering out pathogenic microorganisms and wastes, entering the vena cava as they merge with the vena cava This is the circulation of the body fluid.

As such, the lymphatic system is a secondary circulatory system that is closely related to the cardiovascular system and aids in fluid circulation. When material is exchanged between capillaries and tissues, the amount of fluid that is structurally released from capillaries to tissues is always greater than the amount that enters capillaries from tissues. At this time, if the remaining fluid accumulates as it is, edema occurs in the tissue and hydrostatic pressure increases. Blood also loses moisture due to lack of fluids, making it dry and sticky. If these symptoms do not improve and continue to cause serious fluid circulation disorders, many problems occur. The lymphatic system improves this imbalance by allowing fluids accumulated in tissues to travel to the vena cava through lymphatic vessels, which are the channels through which fluid flows from the tissue to the vena cava. Thus, edema in the human body means a disorder of humoral circulation, and humoral circulation disorder means a lymph circulation disorder. In addition, improvement of edema in the human body, whether improvement of systemic edema or improvement of local edema, means improvement of humoral circulation disorder, and improvement of humoral circulation disorder means improvement of lymph circulation disorder.

Lymphatic circulation is the process of collecting stagnant body fluids throughout the body and returning them through the vena cava into the blood, which promotes the discharge of waste and recycles what is needed. Blood circulation is more important than lymph circulation in terms of body circulation, but lymph circulation, which is directly involved in the circulation of tissue fluid, is more important than blood circulation in terms of the tissue environment that affects cell metabolism. Lymph circulation first aids blood circulation in the cardiovascular system, promoting the supply of nutrients, moisture, oxygen, and hormones, which are needed for cells, and at the same time, quickly removing wastes, toxic substances, and inflammatory substances accumulated in tissues and cells. Helps create an optimal environment for cells to function normally. It also helps the absorption and movement of ingested medicines and nutrients and delivers them quickly to the area they need to increase their effectiveness. As such, lymph circulation plays an important role in creating optimal conditions for cells to work, and thus, it can be said to be an important factor for healthy operation of the human body.

Lymphatic circulatory disorders are systemic edema or local edema because fluids accumulated in tissues remain in the tissues rather than return to the blood through the lymphatic circulation. That is, systemic edema or local edema of the body can be concluded that all are lymph circulation disorders. If this edema is not a big problem in the short term, but if it lasts for a long time, it lowers the metabolic function of the affected part, causing many diseases. Considering that muscle exercise is the only power of lymph circulation, all the symptoms that can occur due to lack of exercise are symptoms of lymphatic circulation disorder, and all the effects that can be improved by exercise are the effects that can be obtained by promoting lymph circulation. Lymph circulation is obtained only by muscle movement, the reality is that the modern man has less need for movement for survival because the lymph circulation is not smoothly performed because of the lack of opportunities for muscle movement. Therefore, it is urgent to find a way to promote lymph circulation to the modern man who is absolutely lacking in exercise and lack of fluid circulation. Nevertheless, although a lot of discussions and methods have been developed for blood circulation, it is true that there is a lack of discussion regarding the importance of lymph circulation. This concept of lymph circulation is not yet medically significant compared to the actual importance and the development of medicines is insufficient.

SUMMARY OF THE INVENTION An object of the present invention is to provide a lymph circulation promoter that can promote lymph circulation in the body to improve the environment around cells and help the cell metabolism to be restored normally.

Another object of the present invention to provide a lymph circulation promoter that can improve various symptoms that may occur due to lymph circulation disorder.

The problems of the present invention described above, can be solved by the lymph circulation promoter including cheongung, maple syrup, crust, bamboo, thawed blood and Euiin in powder, liquid or extract form.

The lymph circulation promoter may be mixed with maple syrup and mortality in a mixed powder of uterus, crust, thawed blood, and uiyiin to make pills for internal use, granules, or powders.

The lymph circulation promoter is a powder, granules, powders for oral use by mixing maple syrup and mortality with water, ethanol, or liquid or powdered extracts extracted with water and ethanol from a mixed powder of cheongung, crust, thawed blood, and Euiin. Can be made liquid.

The lymph circulation promoting agent, a mixture of cheongung, maple syrup, crust, mortality, thaw blood and uiyiin in a constant ratio of water, or ethanol, or extracts extracted with water and ethanol as an active ingredient, oral tablets, granules, powder or Can be made liquid.

Lymphatic circulation promoter according to the present invention, basically, to facilitate the lymph circulation in the body to improve the environment around the cells, to help the cell metabolism normal recovery, to create an environment for the cells in the body to work normally give. Directly, it promotes lymph circulation in the body, thereby improving edema, improving inflammation and pain, removing bruises, controlling body temperature, improving cellular environment, and promoting drug delivery.

1) Improved edema effect: Lymphatic circulation promotion according to the present invention basically circulates fluids accumulated in the tissues through the lymphatic vessels to be combined with blood in the vena cava, through which the body fluids are included in the systemic circulation is the first direct The effect is the improvement of edema. Edema occurs due to stagnation of body fluids. The stagnation of body fluids in the human body can only be resolved by lymph circulation. Because the circulation of body fluids is done through the lymphatic circulation, stagnation of body fluids means a disorder of the lymphatic circulation. When you eliminate the stagnation of fluid, the edema disappears. Therefore, it can be directly confirmed that lymph circulation was improved from the improvement of edema by the present invention. The following effects are of course physiologically predicted when lymph circulation is promoted.

2) Improvement of inflammation and pain: Muscle pain is mainly caused by excessive use of muscles. Muscle fibers are loosely wound like coils. Therefore, when the muscle fibers are excessively contracted or edema occurs due to accumulation of lactic acid, inflammatory substances, etc., the muscle fibers become thicker than a certain degree, so that the sensory nerves are physically taut to be pulled to show pain. This structure is intended to prevent damage to muscles, ligaments, joints, and bones, which are likely to occur due to excessive contraction or edema of muscles. Clinically, pain is caused in two ways: when there is no pain when not moving or moving lightly, but when pain is strengthened when exercise is strengthened, when pain is caused even when not moving. When you do not move or move lightly, there is no pain, but when you exercise hard, the pain comes when there is a slight swelling of muscle fibers. When you do not move or move lightly, the muscles are relaxed or contracted properly, so the sensory nerve fibers are not pulled tight, so there is no pain. However, if the muscle contraction occurs greatly due to the strong exercise, the muscle fiber becomes thick with swelling and the muscle fiber becomes thick with contraction, so the sensory nerve fibers of the muscle fiber are pulled tight, causing pain. If the pain is induced even if the movement does not move, the swelling of the muscle fibers is severe, even if there is no contraction of the muscles, the sensory nerve fibers surrounding the muscle fibers are pulled tight, causing pain. In both cases, the rapid improvement of muscle fiber swelling by promoting lymph circulation according to the present invention reduces pain and at the same time, the inflammatory substances causing edema are also removed, thereby improving the inflammatory state. Tendon pain is also primarily caused by excessive muscle use. Sensory nerve fibers are loosely attached to the tendon like a spider's web. Therefore, when swelling occurs in the tendon due to accumulation of lactic acid, inflammatory substances, or the like, the tendon is stretched more than necessary due to excessive contraction of muscle fibers, and the sensory nerve is physically stretched to show pain. This structure is intended to prevent damage to muscles, tendons, ligaments, joints, bones, etc., which are likely to occur due to excessive contraction of muscles. Clinically, pain in the tendon is not pain when not moving or lightly moving, but if you exercise severe pain, and pain even if you do not move. If you do not move or move lightly pain, but if you exercise severe pain comes tendon swelling of the tendon. If you do not move or move lightly, the sensory nerve fibers attached to the tendon is not pulled tight, there is no pain. However, when more muscle contraction occurs due to severe exercise, the tendon becomes thicker due to edema, and at the same time, the tendon is stretched by the contraction of muscle fibers, so that the sensory nerve fibers of the muscle fibers are pulled tight, causing pain. Pain may be caused even when not moved because tendon swelling is so severe that even if there is no contraction of muscles, the nerve fibers that are wrapped tendons are pulled tight and pain is caused. In both cases, improving the tendon swelling by promoting lymph circulation according to the present invention reduces pain and at the same time reduces the inflammatory substances that caused edema, thereby reducing inflammation. Lymphatic circulation helps circulate fluids and improves pain in muscles and tendons. This can happen not only in muscles and tendons, but also in other areas of inflammation.

3) cell environment improvement effect: promote lymph circulation, improve the surrounding environment of body tissue and help the cell metabolism to be restored normally. Lymph circulation first aids blood circulation in the cardiovascular system, promoting the supply of nutrients, moisture, oxygen, and hormones, which are needed for cells, and at the same time, rapidly removing wastes, toxic substances, and inflammatory substances accumulated in tissues or cells. To create an optimal environment in which to function normally. This is an immediate effect that allows cells to efficiently utilize the nutrients and oxygen in the body.

4) Removal of bruises: Bruises are blood vessels ruptured due to bruises or other causes, causing blood to come out of the vessels and form a bruise under the skin and appear red or dark red due to red blood cells in the blood. The red blood cells in the blood don't penetrate the walls of the capillaries because they have a high molecular weight and must be degraded in place or removed by lymph circulation. Lymphatic circulation promotion according to the present invention promotes the movement of a material having a high molecular weight that does not pass through the capillary wall, thereby rapidly removing blood.

5) Thermoregulation effect: The promotion of lymph circulation according to the present invention promotes the circulation of body heat through the circulation of body fluids. Lymph circulation promotes body heat transfer and dispersion and improves cell metabolism to normalize locally low body temperature, and when body temperature is high, it helps normalize by lowering body temperature.

6) Drug Delivery Promoting Effect: In the case of taking a medicine prescribed by a specific disease or injecting an injection, when the lymphatic circulation is promoted according to the present invention, the drug moves quickly and reliably to the lesion so that the administered drug effectively acts on the lesion. do.

These various effects can be explained only by anatomical physiology or pathologically by the lymph circulation promoting effect. Therefore, by confirming these individual effects it is possible to confirm the lymph circulation promoting effect of the present invention.

As such, the lymph circulation promoter according to the present invention can be widely applied to improve various pathological symptoms.

1 is a photograph of the product contents of the lymph circulation promoter according to the present invention.
Figure 2 is a photograph of the product packaging of the lymph circulation promoter according to the present invention.
Figure 3 is a chart showing the results of the measurement of lymph flow rate changes of the lymph circulation promoter according to the present invention.
4 to 8 are diagrams showing the results of the edema improvement test of the lymph circulation promoter according to the present invention.
9 and 10 are diagrams showing the pain improvement test results of the lymph circulation promoter according to the present invention.

Lymphatic circulation promoters according to the present invention include cheongung, maple syrup, crust, mortality, thawed blood and uiyiin in powder, liquid or extract form.

Lymphatic circulation promoter according to the present invention is composed of the following components and composition ratio.

i) 20-50% by weight of uterus known to be good for blood circulation (based on the total weight, less than);

ii) 20-50% by weight of maple syrup, which is used as a sugar substitute or sweetener for its sweet taste, but its pharmacological action is unknown;

iii) 10 to 30% by weight of crust known to turn stagnant groups

iv) 10-30% by weight of death known to lower heat and sputum;

v) 5-25% by weight thawed skin known to be well-permeated;

vi) 1 to 20% by weight, which is known to be effective for edema.

If the amount of archery is added less than 20% by weight, the effect of promoting lymphatic circulation by the arch is insignificant, and if the amount of archery is added more than 50% by weight, the increase in the effect of promoting lymphatic circulation by the archery does not reach the increase in the amount of the archery.

If maple syrup is added in less than 20% by weight, the effect of promoting the lymphatic circulation by maple syrup is insignificant, and adding maple syrup in excess of 50% by weight increases the lymph circulation-promoting effect by maple syrup. Falls short of

If the crust is added less than 10% by weight, the lymph circulation promoting effect by the crust is insignificant, and when the crust is added more than 30% by weight, the increase in the lymph circulation-promoting effect by the crust does not reach the increase in the amount of the crust.

When the killing force is added less than 10% by weight, the lymph circulation promoting effect by the killing force is insignificant, and when the killing force is added more than 30% by weight, the increase in the lymphatic circulation promoting effect by the killing force does not reach the increase in the amount of killing.

If the thawed blood is added at less than 5% by weight, the lymphatic circulation promoting effect by the thawed blood is insignificant. If the thawed blood is added more than 25% by weight, the increase of the lymphatic circulation promoting effect by the thawed blood does not reach the increase in the amount of thawed blood.

Addition of less than 1% by weight of the righteous person has a slight effect on promoting lymphatic circulation, and more than 20% by weight of the righteous person does not increase the effect of promoting the lymphatic circulation by the righteous person does not reach an increase in the amount of the righteous person.

The lymph circulation promoter according to the present invention may be mixed with maple syrup and mortality in a mixed powder of celestial organs, crust, thawed blood, and Euiin, to make an oral pill, granule, or powder.

Lymphatic circulation promoting agent according to the present invention, in the mixed powder of cheongung, crust, thaw and uiyiin water, ethanol, or liquid or powdery extract extracted with water and ethanol, maple syrup and mortar by mixing oral medicine, granules, It can be made into powder or liquid.

Lymphatic circulation promoter according to the present invention, by mixing the uterus, maple syrup, crust, mortality, thaw blood and Euiin in a constant ratio of water, or ethanol, or extracts extracted with water and ethanol as an active ingredient pill, granules, It can be made into powder or liquid.

Cheonggung is dried root stems of the Apiaceae, Gungung and Sangung.

Maple syrup is a concentrated collection of Canadian maple sap and is widely used as a substitute for sugar.

Crust is known to turn stagnant phases into mature fruits of tangerines and improve dyspepsia.

The killing force, In the process of making charcoal from bamboo, the sap of bamboo that is evaporated by strong heat is collected.

Thawed blood is dried bark of the oakpiaceae.

The Ui-in is a dried seed of Yulmu, a rice plant. Yulmu is planted in various parts of Korea. After the seeds are ripe in the fall, they are cut and dried, beaten, and the seeds are peeled off.

Among these, bamboo, thawed blood and maple syrup have the most direct and powerful effect on promoting lymph circulation, irrespective of its composition ratio. Therefore, if one of the components of the killing power and thawed blood and maple syrup, the lymph circulation promoting effect is significantly reduced. Cheongung, crust and Ui-in supplement and strengthen the lymph circulation-stimulating effects of bamboo and thawed blood and maple syrup. Lymphatic circulation promoter according to the present invention to exhibit a variety of effects, such as edema improvement, inflammation and pain improvement, elimination of bruises, body temperature regulation, cellular environment improvement, drug delivery promotion, the addition of the archery and perception and righteous person exhibits a synergistic effect Because.

Lymph circulation promotion is to create an optimal environment for the metabolic activity of the cell, so the lymph circulation promoter according to the present invention can be used for almost all symptoms caused by inappropriate cell metabolic environment. In a narrow range, it can be used to improve edema, improve pain, improve inflammation, control body temperature, remove bruises, and promote drug delivery, while widening can be used for all symptoms that can be caused by lack of exercise, which is a cause of poor lymph circulation. have. In addition, the lymph circulation promoter according to the present invention can be used in almost all fields for disease prevention, for symptom improvement of disease, and for treatment of disease.

When mixed with drugs or functional foods with other functions does not cause problems, but rather helps the absorption and delivery of the active ingredient, and also helps to improve the cellular environment of the area causing the symptoms increase the efficacy effect of the active ingredient. For example, when the lymph circulation promoter according to the present invention is taken together with vitamin C or a fat-soluble blood circulation agent, the effect is reliably increased.

<Example 1: C4U-1>

In order to confirm the clinical experiment and efficacy of the lymph circulation promoter according to the present invention, an oral therapeutic lymph circulation ring was prepared several times in the following amounts.

Make a mixed powder of 2,700g of cheongung powder, 1,400g of crust powder, 1,100g of thawed blood powder, and 800g of Euiin powder.Add 2,600g of maple syrup and 1,400g of maple syrup. Made and packed in 4.8 g units.

<Example 2: C4U-2>

220g of thawed blood extract, 500g of maple syrup, and 280g of bamboo powder were mixed to make about 1,000g of syrup, and they were packed in units of 4.8g.

<Example 3: C4U-3>

A total of 540 g of cheongung extract, 300 g of crust extract, and 160 g of Euiin extract were mixed to make about 1,000 g of syrup, and they were packed in units of 4.8 g.

[Evaluation of Lymphatic Fluid Flow Rate through Lymphatic Sampling in the Mesenteric Lymphatic Tube of Rat]

1) Objectives: To evaluate the lymphatic flow in rats' mesenteric lymphatic vessels to evaluate the increase in lymph flow in C4U-1, C4U-2, and C4U-3 samples. The purpose of this study was to evaluate the effects of lymph circulation.

2) Experiment Method

(1) animal treatment and sample administration

To identify lymphatic vessels, 1.5 ml of peanut oil was orally administered 1 hour prior to lymph collection to rats fasted for 24 hours (Male, Sprague-Dawley Rat, weight 240 g). After 30 minutes of Peanut oil administration, C4U-1 was powdered in an amount corresponding to 1,666 mg and dispersed in a small amount of purified water. C4U-2 and C4U-3 were orally administered in 3 divided doses of 3,636 mg. As a control, the same amount of purified water as C4U-2 and C4U-3 was orally administered. Rats were anesthetized by administering 1 ml of urethane intraperitoneally 30 minutes after sample administration.

(2) Collection of lymph and measurement of lymph flow

As shown in FIG. 3, the peritoneum of the anesthetized rat was incised 3-4 cm. At this time, the small intestine was moved to the side of the abdominal cavity slightly and protected with gauze soaked in warm saline. Polyethylene tubes (0.5 mm inner diameter, 0.9 mm outer diameter) were inserted into the white and shiny lymphatic vessels (see FIG. 3) located perpendicular to the vena cava below the liver, and lymph fluid was collected for 1 hour. After 1 hour the microtubes were removed and the weight of lymph flow rate introduced into the microtubes was measured on a microbalance.

3) Experiment result

The test results are shown graphically in FIG. 4. As can be seen with reference to FIG. The flow rate of lymphatic fluid collected for 1 hour without any administration to the rats was 1.1 mg by weight. However, after the administration of C4U-1, C4U-2, and C4U-3, the flow rates increased significantly to 1.8 mg (63.6% increase), 1.6 mg (45.4% increase), and 1.3 mg (18.2% increase). It was found that the 1, C4U-2, and C4U-3 samples can significantly increase the flow of lymph. This change in flow rate was noticeable even during lymphatic collection. It can be seen that the circulation of lymph fluid is promoted when C4U-1, C4U-2, and C4U-3 are administered. In particular, it can be seen that the increase rate of lymph circulation promotion of C4U-2 is more than two times the increase rate of lymph circulation promotion of C4U-3, and the increase rate of lymph circulation promotion of C4U-1 is more than three times the increase rate of lymph circulation promotion of C4U-3. Able to know. That is, it was confirmed that the extracts of thawed blood, maple syrup, and bamboo power had a greater lymph circulation promoting effect than the extracts of celestial, perceptual, and Euiin, and synergistically showed a synergistic effect of lymph circulation.

[Carrageenan-Induced Foot Edema Test Using Sprague-Dawley Rat]

1) Test purpose

The easiest way to see the effects of lymph circulation is the edema test. This is because almost all conditions that cause edema are accompanied by stagnation of lymph. Therefore, the lymph circulation effect can be confirmed by confirming the improvement of edema.

2) test substance

C4U-1, C4U-2 and C4U-3 were used as test materials, and Diclofenac Sodium was used as a positive control. As excipient 1, sterile injectable water (Korean sterile distilled water-source: Korea Pharmaceutical Industry Co., Ltd.) was used, and excipient 2 (0.9% saline (sterile physiological saline-source: Korea Pharmaceutical Industry Co., Ltd.)) was used.

3) test method

(1) Exam preparation

Specific pathogen free (SPF) rats, Hsd: Sprague Dawley® ™ SD® ™ (producer and source: Coatech Co., Ltd. (181-21, Jinwi-myeon, Pyeongtaek-si, Gyeonggi-do), 30 males, 30 males, were used. The rats were chosen because they are widely used in various drug efficacy and toxicity tests, have accumulated abundant test basis data, and use these data for easy interpretation and evaluation of test results. During the administration and observation periods (red), they were identified using the unlabeling method, with a color-coded individual identification card attached to the breeding box, and an animal room record sheet attached to the entrance to the breeding room. Nortus Rodent Breeding Zone 1 with 3 ℃, relative humidity 55 ± 15%, ventilation frequency 10-20 times / hr, lighting time 12 hours (lighting 8 am-8 pm off) and illuminance 150-300 Lux number During the breeding period, the environmental conditions such as temperature / humidity, ventilation frequency and illuminance of the animal room were regularly measured.For feed, the feed for experimental animals produced by Cargill Agripurina Co., Ltd. was used in Gwangnaru, Gwangjin-gu, Seoul. 507), and freely ingested water, and purified water can be freely ingested using polycarbonate drinking bottle .. The rug was used from Koatech Co., Ltd. (406, Dongcheon-ri, Jinwi-myeon, Pyeongtaek-si, Gyeonggi-do, Korea). During the period of acclimation and testing, no more than 5 animals / cage were raised in a rodent polycarbonate cage (W 235 x L 380 x H 175 mm) The cage, rug and water bottle were replaced at least once a week. Measure the weight of the animals determined to be healthy and distribute the average weight of each group as uniformly as possible according to the ranked weight. Less it was isolated group illegally.

(2) Composition of test group

The composition and dosage of the test group was determined as follows. Test substance 1 represents C4U-1, test substance 2 represents C4U-2, and test substance 4 represents C4U-3. As mentioned above, the positive control is Diclofenac Sodium.

(3) Preparation of administration test substance

In case of Carrageenan, the required amount was weighed and dissolved in sterile physiological saline as an excipient at a concentration of 1% (10mg / mL) and used as a edema causing substance.

In the case of test substances, at the request of the sponsor, the required amount is weighed according to the information provided by the sponsor, and then, sterilized water is added to prepare a concentration of 400 mg (based on the main ingredient) / 10 mL, which is then used for the test. It was.

Test substance 1 (C4U-1)

Formulation: Pill

Prescription: 240 mg of drug, 1000 mg of excipient

Dosage: 400 mpk as main ingredient (approximately 1666 mg as powder)

Test substance 2 (C4U-2)

Formulation: Syrup

Prescription: 110 mg of syrup, 1000 mg of excipient, 890 mg of excipient

Dosage: 400 mpk as main ingredient (about 3636 mg as syrup)

Test substance 3 (C4U-3)

Formulation: Syrup

Prescription: 110 mg of syrup, 1000 mg of excipient, 890 mg of excipient

Dosage: 400 mpk as main ingredient (about 3636 mg as syrup)

In the case of a positive control, the required amount was taken, and then, sterilized water was added to prepare a concentration of 30 mg / 10 mL, and then used for the test.

(4) administration

For the test substance, oral administration, which is a planned clinical route, was selected. Carrageenan, an edema-causing substance, was selected for intradermal administration to the plantar area. In the case of the test substance, a single dose was administered 2 hours before the Carrageenan administration, and the trigger was also administered once. In the case of test substance and positive control substance, it shall be administered by calculating 10 mL / kg based on the weight measured on the day of the test. In the case of Carrageenan, 50 μL was administered intradermally to the sole of the right hind leg. In the case of oral administration, the animals were fixed by transcutaneous skin fixation method and administered directly into the stomach using sonde for oral administration. In the case of Carrageenan, 50 μL was administered intradermally to the sole of the right hind leg. Animals for test substance administration were fasted for at least 16 hours prior to test substance administration.

(5) observation and inspection items

The volume of the hind limbs was measured prior to Carrageenan and 3 hours after injection.

Edema inhibition (%) was calculated using the formula given below.

* Edema rate (%) and edema inhibition rate (%) of each test group were calculated.

Edema rate (%) = {(Vt-Vn) / Vn} X 100

Vt: Foot volume after a certain time after Carrageenan injection,

Vn: Foot volume before Carrageenan injection

Edema inhibition rate (%) = (average edema rate of induced controls. Edema rate of each individual) / (edema rate of induced controls) x 100

4) Test result

Test results are shown graphically in Figures 5-8.

Figure 5 is the result of measuring only the test substance and the volume of the hind legs before the Carrageenan administration using the edema meter. It can be seen that the volume is about 1 mL in all groups (G1-G6). 6 is a result of measuring the volume of the hind limb after 3 hours after administration of Carrageenan to the G2-G6 group using a leg edema meter, and FIG. 7 is a difference value between the measurement result of FIG. 6 and the measurement result of FIG. Increased volume). FIG. 8 is a result table of calculating the edema rate using the measured value of FIG. 7 and calculating the edema inhibition force (%) using this edema rate.

As can be seen in Figure 8, the edema inhibition of G4 (C4U-1) is a positive control material can be confirmed that close to 17% of the edema inhibition of Diclofenac Sodium. Edema inhibition of G5 (C4U-2) is around 8%, G6 (C4U-3) can be confirmed that the edema suppression of about 4%. It can be seen that C4U-1, in which C4U-2 and C4U-3 components are combined, exhibits a synergistic edema improvement effect. In addition, it is possible to confirm the lymphatic promoting effect of the present invention through this edema improvement effect.

[PBQ-Induced Twist Test Using Sprague-Dawley Rat]

1) Test purpose

Pain is the result of the accumulation of pain-causing substances in muscles and the like. Promoting lymph circulation promotes the release of pain-causing substances. This study was performed to evaluate the effect of treatment of test substance in pain-induced model using Sprague Dawley rat. The effect of lymph circulation can be checked by checking for improvement in pain.

2) test substance

C4U-1, C4U-2 and C4U-3 were used as test materials, and Diclofenac Sodium was used as a positive control. As excipient 1, sterile injectable water (Korean sterile distilled water-source: Korea Pharmaceutical Industry Co., Ltd.) was used, and excipient 2 (0.9% saline (sterile physiological saline-source: Korea Pharmaceutical Industry Co., Ltd.)) was used.

3) test method

(1) Exam preparation

Specific pathogen free (SPF) rats, Hsd: Sprague Dawley® ™ SD® ™ (producer and source: Coatech Co., Ltd. (181-21, Jinwi-myeon, Pyeongtaek-si, Gyeonggi-do), 30 males, 30 males, were used. The rats were chosen because they are widely used in various drug efficacy and toxicity tests, have accumulated abundant test basis data, and use these data for easy interpretation and evaluation of test results. During the administration and observation periods (red), they were identified using the unlabeling method, with a color-coded individual identification card attached to the breeding box, and an animal room record sheet attached to the entrance to the breeding room. Nortus Rodent Breeding Zone 1 with 3 ℃, relative humidity 55 ± 15%, ventilation frequency 10-20 times / hr, lighting time 12 hours (lighting 8 am-8 pm off) and illuminance 150-300 Lux number During the breeding period, the environmental conditions such as temperature / humidity, ventilation frequency and illuminance of the animal room were regularly measured.For feed, the feed for experimental animals produced by Cargill Agripurina Co., Ltd. was used in Gwangnaru, Gwangjin-gu, Seoul. 507), and freely ingested water, and purified water can be freely ingested using polycarbonate drinking bottle .. The rug was used from Koatech Co., Ltd. (406, Dongcheon-ri, Jinwi-myeon, Pyeongtaek-si, Gyeonggi-do, Korea). During the period of acclimation and testing, no more than 5 animals / cage were raised in a rodent polycarbonate cage (W 235 x L 380 x H 175 mm) The cage, rug and water bottle were replaced at least once a week. Measure the weight of the animals determined to be healthy and distribute the average weight of each group as uniformly as possible according to the ranked weight. Less it was isolated group illegally.

(2) Composition of test group

The composition and dosage of the test group was determined as follows. Test substance 1 represents C4U-1, test substance 2 represents C4U-2, and test substance 4 represents C4U-3. As mentioned above, the positive control is Diclofenac Sodium.

(3) Preparation of administration test substance

In the case of PBQ, the required amount is weighed and then in a concentration of 2 mg / 10 mL in an excipient sterile saline solution

It was prepared by dissolving it and using it as a pain-causing substance.

In the case of test substances, at the request of the sponsor, the required amount is weighed according to the information provided by the sponsor, and then, sterilized water is added to prepare a concentration of 400 mg (based on the main ingredient) / 10 mL, which is then used for the test. It was.

Test substance 1 (C4U-1)

Formulation: Pill

Prescription: 240 mg of drug, 1000 mg of excipient

Dosage: 400 mpk as main ingredient (approximately 1666 mg as powder)

Test substance 2 (C4U-2)

Formulation: Syrup

Prescription: 110 mg of syrup, 1000 mg of excipient, 890 mg of excipient

Dosage: 400 mpk as main ingredient (about 3636 mg as syrup)

Test substance 3 (C4U-3)

Formulation: Syrup

Prescription: 110 mg of syrup, 1000 mg of excipient, 890 mg of excipient

Dosage: 400 mpk as main ingredient (about 3636 mg as syrup)

In the case of a positive control, the required amount was taken, and then, sterilized water was added to prepare a concentration of 30 mg / 10 mL, and then used for the test.

(4) administration

For PBQ, intraperitoneal administration was chosen based on the references. In the case of PBQ, the dose was calculated at 10 mL / kg based on the weight measured on the test day. In the case of test substances, a single dose was administered 2 hours before the administration of the trigger (PBQ), and the trigger was also administered once. In the case of test substance and positive control substance, it shall be administered by calculating 10 mL / kg based on the weight measured on the day of the test. In the case of oral administration, the animals were fixed by transcutaneous skin fixation method and administered directly into the stomach using sonde for oral administration. For PBQ, animals are fixed by transdermal skin fixation and administered intraperitoneally using a syringe equipped with a 26 gauge needle. Animals for test substance administration were fasted for at least 16 hours prior to test substance administration.

(5) observation and inspection items

The total number of twists was measured for 30 minutes for each subject 10 minutes after PBQ administration, and the pain inhibition (%) was calculated using the formula given below.

% Pain suppression = (number of twists in the control group; number of twists in the drug group) / (number of twists in the group) x 100

4) Test result

Test results are shown graphically in FIGS. 9 and 10.

FIG. 9 is a result table of measuring the total number of twists for 30 minutes for each individual from 10 minutes after PBQ administration, and FIG. 10 is a chart showing pain inhibition force (%) calculated using the results of FIG. 9.

As can be seen in Figure 10, the edema suppression of G4 (C4U-1) is a positive control can be confirmed that close to 42% of the edema suppression of Diclofenac Sodium. G5 (C4U-2) edema suppression of about 39%, G6 (C4U-3) can be confirmed that the edema suppression of about 8%. It can be seen that the components of C4U-2 have a great effect on pain suppression, in particular, and when combined with the components of C4U-3, have a greater pain inhibitory effect, as the result of C4U-1.

Through such a pain inhibitory effect it can be confirmed the lymphatic promoting effect of the present invention.

[Evaluation of Viscosity of Lymphatic Fluid Collected from Mesenteric Lymphatic Vessels in Rats]

1) When the administration of C4U-1, C4U-2, and C4U-3 is expected to change the viscosity of the lymph fluid, the viscosity of the lymph fluid collected after the administration of the sample to the rat was evaluated.

2. Experimental method

1) Animal Treatment and Sample Administration

(1) To 40 rats fasted for 24 hours (Sprague-Dawley rat, male, weight 190-200g), using the TPA (12-O-tetradecanoylphorbol-13-acetate) to 4 points of the ear and lower extremity of the rat Caused skin inflammation.

(2) After 6 hours of induction of inflammation, 40 rats were divided into four groups of 10, A, B, C, and D, and then powdered for groups B, C, and D, except for group A (control group), respectively. 1,666 mg of C4U-1, C4U-2, C4U-3 was dispersed in purified water (4.5 ml) and orally administered.

(4) The rats were anesthetized with chloroform 30 minutes after the administration of C4U-1, C4U-2, and C4U-3 as above, and then an additional 1 ml of urethane was administered intraperitoneally to maintain the anesthesia of the rat during the experiment. It was.

2) collection of lymph

(1) After anesthesia, the rat peritoneum was incised 3-4 cm. After this, the small intestine was placed out of the abdominal cavity and covered with gauze soaked in warm saline to prevent drying.

(2) Insert polyethylene microtubes (ID 0.5 mm, OD 0.9 mm) into the lymphatic vessel located perpendicular to the vena cava below the liver and drain the lymph fluid from each group of A, B, C, and D groups. Not much gathered.

3) measuring the viscosity of lymph

(1) A rheometer (model name: HAAKE RheoStress 1, Thermo Fisher Scientific Co. Ltd.) equipped with a 35 mm diameter parallel plate (P TiL 30, Thermo Fisher Scientific Co. Ltd., USA) was taken in each group with 2,000 μl of lymph fluid. , USA) was used to measure the viscosity of lymphatic fluid. At this time, the gap between the two plates was set to 1.0 mm, the temperature of the lower plate to 20 ℃.

(3) After putting about 2,000 μl of sample between two plates, the sample was stabilized for 5 minutes.

(4) The strain value of the sample was measured while applying a shear stress of 0.1 Pa for 500 seconds.

Measured.

(5) After the measurement was completed, the zero shear viscosity was calculated.

3. Experimental Results

As shown in FIG. 11, in the case of the control group (Group A), the zero shear viscosity was measured as an average of 2.21 mPa · s, and C4U-1 (Group B), C4U-1 (Group C), and C4U-3 (Group D) ), The zero shear viscosity averaged 1.78 mPa · s (about 19.5% viscosity drop), 1.85 mPa · s (about 16.3% viscosity drop), and 1.93 mPa · s (about 12.7% viscosity drop) Was measured.

[Measurement of Drug Delivery Promoting Effect]

1) Test purpose

Lymphatic circulation can lead to accelerated drug delivery. Therefore, if the drug delivery effect is confirmed in addition to the edema improvement effect and pain improvement effect, the lymph circulation effect can be confirmed through these.

2) test method

One head of 10 hairless mice was infected with Staphylococcus aureus, Candida albicans, Microsporium canis and yeast to cause erythema and inflammation.

Five hairless mice selected for the test group were ground with 0.5 mg of C4U-1 in powder form immediately after erythema and inflammation, mixed with warm water and continuously administered orally every 6 hours. Was injected. Five hairless mice selected for comparison were injected with 30 mg of vancomycin in the lower extremity of the hairless mice immediately after erythema and inflammation. For the test and control groups, skin conditions were observed for 84 hours every 12 hours after the initial injection.

3) Test result

As a result of the above experiments, it was observed that in the mice in the test group, the inflammation subsided and the erythema was alleviated after 12 hours. In one remaining mouse, inflammation subsided and erythema was relieved after 24 hours. After 72 hours, erythema and inflammation were no longer observed in three mice. After 84 years, erythema and inflammation were no longer observed in all mice. In addition, no toxicity was seen in hairless mice during the test.

On the other hand, in the comparison mice, erythema tended to relieve after 48 hours in two mice, and erythema tended to relieve after 72 hours in the other three mice. The mice in the control group were still observed to have inflammation after 84 hours.

Through the test results, the drug delivery promoting effect of the present invention can be confirmed, and through the drug delivery promoting effect, the lymph circulation effect of the present invention can be confirmed.

[Clinical test]

Hereinafter, unless otherwise stated, the lymph circulation promoter according to the present invention is C4U-1 according to Example 1.

<Measurement of Edema Improvement Effect>

Edema refers to a condition in which excess fluid, such as lymph fluid or exudates of tissues, is present in tissues due to lymph circulation disorders. Edema in the skin and soft tissues causes clinical swelling, a sloppy feeling, and when pressed, the skin temporarily dents. These symptoms disappear when the circulation of lymph flows smoothly. Thus, improvement of edema means improvement of lymph circulation. If edema is confirmed, it can be concluded that there is an improvement in lymph circulation.

At the age of 50 or more, 50 female patients with swelling of the lower limbs were selected, and these patients were taken to take the lymph circulation promoter according to the present invention twice a day, twice a packet, and after 7 consecutive days, Each patient was measured for i) weight change (weight scale), ii) thigh, calf, instep circumferential length change (using plastic tape) and iii) edema (visual observation). The results are shown in Table 3 below.

From the measurement results below, 45 (90%) of the 50 patients showed a decrease in the circumferential length of the most severe area of the lower limb edema, and 40 (80%) patients lost weight. In 46 patients (92%), edema was alleviated. Edema circumference was confirmed to decrease in the range of 1.0% ~ 10.0% of the circumference before taking. Body weight was confirmed to decrease in the range 0.5% ~ 4.0% of body weight before taking. Body fluids (lymph fluid or tissue exudate) stagnated in the lower limb tissue are excreted in the feces through urine or bile, resulting in weight changes. Improved edema usually involves significant weight loss.

From these results, it is possible to confirm the improvement of the edema of the present invention, that is, the improvement of lymph circulation.

Measurement item

Number of patients
Patient rate


Changes in the circumference of the thigh, calf, or instep where the swelling is most severe
The circumference of the edema is reduced

45
90%
No circumference in edema area

4
8%

Increased circumference of edema area

One
2%



Weight change
I lost weight.

40
80%
No change in weight

9
18%
Gained weight

One
2%



Edema
Edema is relieved

46
92%
No change in edema status

4
8%
Edema worsened

0
0%

<Measurement of pain relief effect>

As mentioned above, lymph circulation promotion relieves pain through anatomically physiological or pathological fast release of pain-causing substances. Thus, of the present invention Through the pain relief effect confirmation can be confirmed the lymph circulation promoting effect of the present invention.

Ten patients with low back pain who feel back pain without movement were selected, and five patients (M1-M5) were asked to take C4U-1 three times a day for 28 days, and the remaining five patients (m1-m5) The effect was measured by taking C4U-3 once a day for 28 days three times a day.

After taking 28 days, the pain was not felt even when moving, 3 points, the pain was not felt when not moving, but the pain was felt when moving, 1 point, 0 points if the pain is still felt without moving.

The measurement results were shown in Table 4 below.

From the measurement results below, it can be seen that the degree of pain improvement of patients taking C4U-1 is better than that of patients taking C4U-3.

Patients Taking C4U-1

Patients Taking C4U-3

M1

M2
M3
M4
M5

m1
m2
m3
m4
m5
3

3
3
2
3
2
0
2
2
0

Through this can be confirmed the lymph circulation promoting effect of the present invention.

<Measurement of Bruising Effect 1>

The extinction of bruises is directly related to lymphatic circulation anatomically or pathologically. Therefore, the rapid disappearance of the bruise can be said to promote the lymph circulation.

For 10 female patients who had blood vessels around the eyes due to the rupture procedure, 5 patients (M1 ~ M5) were to continuously take the lymph circulation promoter according to the present invention once a day and 2 times 3 times a day, and the remaining 5 Myeong (m1 ~ m5) was asked to massage the egg around the dogs 6 times a day for at least 5 minutes. The length of time it took for the bruise to no longer be observed with the naked eye was measured.

The measurement results were shown in Table 5 below.

Patients taking C4U-1

Egg Massage Patient
M1

M2
M3
M4
M5
m1
m2
m3
m4
m5
15th

17 days
13th
18 days
11th
55 days
45 days
60 days
75 days
70 days

From the measurement results, it was confirmed that the blood removal rate of the patient taking the embodiment of the present invention is egg massaging, but three times faster than the blood removal rate of the patient.

<Measurement of Bruising Effect 2>

For 10 male patients with bruises with similar bruises around the eyes, five (M1-M5) patients were given a pill according to the invention three times a day, three times a day, and the remaining five (m1). ~ m5) was asked to massage the eggs more than 5 minutes once a day, 6 times a day. The length of time it took for the bruise to no longer be observed with the naked eye was measured.

The measurement results were shown in Table 6 below.

Patients taking C4U-1

Egg Massage Patient
M1

M2
M3
M4
M5
m1
m2
m3
m4
m5
5 days

4 days
7 days
3 days
6 days
14 days
18 days
20 days
15th
16th

In the case of bruises due to bruises, it was confirmed from the measurement result that the blood removal rate of the patient taking the embodiment of the present invention was egg-flavored, but it was 2 to 3 times faster than the blood removal rate of the patient.

Through this can be confirmed the lymph circulation promoting effect of the present invention.

Minimum Masking Level (MML) Measurement for Tinnitus Patients

Five relatively severe male tinnitus patients and five female tinnitus patients were selected, and the lymph circulation promoter according to Example 1 was inhaled for 1 month with tid once a month, and minimal occlusion before starting dose and after 1 month was taken. Threshold (MML) was measured. The minimum shielding threshold (MML) is a minimum value in which the noise including tinnitus frequency is gradually increased by 1 dB in the ear where tinnitus is heard, and the tinnitus is not heard. In general, decreasing the minimum shielding threshold translates to improved tinnitus. Lower minimum shielding means that tinnitus is less intense.

First, tinnitus frequency was obtained by pitch matching test for selected tinnitus patients. Increasing the narrowband noise frequency including the tinnitus frequency found in the tinnitus frequency test by 1 dB, giving the shielding sound to the ear with tinnitus, obtaining the minimum intensity value (minimum shielding threshold) of the shielding sound without tinnitus, and detecting the Sensation Level ( dB SL) (difference from sound threshold). The measurement results are shown in Table 7 below. The results below show that tinnitus patients had a reduced minimum shielding threshold in 9 of 10 patients after taking the lymph circulation promoter according to the present invention. This means that the degree of tinnitus was relieved in 9 of 10 patients. The magnitude of the improvement is 1dBSL-4dBSL, although there is a personal variation, but overall it shows significance for tinnitus improvement.

patient

M1
M2
M3

M4
M5
W1
W2
W3
W4
W5
tinnitus
frequency
(Hz)


4,000

3,000

4,000

4,000

5,000

3,000

4,000

4,000

4,000

5,000
Before taking
MML
(dBSL)


5

7

8

8

6

8

8

7

7

7
After 1 month
MML
(dBSL)

5


4

4

6

5

6

5

3

4

4

The causes of tinnitus vary, but finally, tinnitus develops as it affects the lymphatic fluid in the cochlea. If for any reason the amount of lymph fluid in the cochlea is too high or too low, changes in the concentration, pressure or temperature of the lamp fluid, changes in the composition of the lymph fluid, or problems with the circulation of the lamp fluid, This ideally stimulates the hair cells, and the stimulus is transmitted to the brain through the auditory nerve. Lymphatic circulation promoter according to the present invention, basically, to facilitate the lymph circulation in the body to improve the environment around the cells, to help the cell metabolism normal recovery, to make the environment for the cells in the body to work normally give. Directly, lymphatic circulation in the cochlea is promoted to restore the insufficient or excessive amount of lymphatic fluid in the cochlea to an appropriate level, and to quickly discharge impurities and wastes entrained in the lymphatic fluid in the cochlea. As a result, the amount, composition and circulation of lymphatic fluid in the cochlea is quickly restored to a normal state, and the environment and function of the auditory cells (hair cells) are also normally restored to rapidly improve tinnitus symptoms. In addition, it promotes the circulation of substances by promoting the circulation of lymph, which facilitates the supply of nutrients, oxygen, and water required for hair cells, improves nutritional imbalance, and facilitates metabolism by mobilizing cell metabolites. This prevents hair cells from hypersensitivity in response to changes in lymphatic fluid.

Clinical Cases for Individual Patients

The following clinical trial results are, of course, physiologically predicted when lymph circulation is promoted and have been confirmed clinically.

Clinical trial 1-Edema improvement (43 years old, female)

After thyroid cancer surgery, he continued to take thyroid drug Synthroid for a long period of time and suffered from swollen symptoms of swollen face and fingers as well as whole body in the morning. Lymphatic circulation promoting agent according to the present invention was started to eat one by one bid, the facial swelling in seven days, the whole body swelling in five days could be observed visually. Weight was also reduced 2.0kg. The patient himself stated that her body became lighter, her face smaller and her skin better. Treatment of edema generally limits salt intake or administers diuretics but does not have a satisfactory effect. According to the present invention, it was confirmed that a very rapid edema improvement effect appeared. Because edema occurs due to stagnation of body fluids, and stagnation of body fluids is caused by lymphatic circulation disorders, improved edema means improved lymph circulation.

2) Clinical Trial 2-Edema Improvement (54 years old, female)

This patient, a 54-year-old female pharmacist with allergies and frequent edema. There was always swelling in the knee due to degenerative arthritis. A few days ago, I was bitten by mosquitoes, but when I left it, two days later, my wrists became swollen and itchy. I applied steroid ointment, but rather swelled and had a fever. Two circulatory lymphocyte promoters according to the present invention were to be taken, and two vesicles were taken again after 5 hours. The next morning, little swelling of the wrist was observed. After one more dose of 5 days by bid, and no more swelling of the knee was observed. Because edema occurs due to stagnation of body fluids, and stagnation of body fluids is caused by lymphatic circulation disorders, improved edema means improved lymph circulation.

3) Clinical Trial 3-Edema Improvement (40 years old, female)

A 40-year-old plump female patient who had swollen instep and soles of the foot, and pain in the back neck and shoulders. The patient was asked to take two doses of the lymph circulation promoter according to the present invention in tid for 5 days. Five days after taking it, the instep and sole swelling disappeared completely, and he said that he felt a little loose. It was judged that the whole body waste was discharged by the promotion of lymph circulation.

4) Clinical Trial 4-Edema Improvement (72 years old, female)

A female patient with cracked skin due to swelling of the leg for more than 10 years. The skin was so sensitive that even when I touched it, I felt pain. Entelon Tab (150 mg), which is marketed as a circulatory drug, was taken for several years but did not improve. The patient was inoculated with a three-pack dose of lymph circulation promoter according to the present invention for 20 days. After 20 days, the swelling was reduced to the extent that wrinkles occurred on the calf skin.

5) Trial 5-Pain Improvement (48 years old, female)

She is a female pharmacist and complained that her wrist was so severe that she could not lift a box of 500g medicine. One packet of lymph circulation promoter according to the present invention was taken 3 days as tid. Wrist pain was alleviated from the first dose of 1 packet, and on day 3, wrist pain was completely cleared. Lymphatic circulation promotion facilitates the discharge of pain-causing substances, which can confirm the lymphatic circulation effect of the present invention.

6) Clinical Trial 6-Pain Improvement (50 years old, female)

30 years of business in the market was a strange patient. He suffered severe ankle and heel pain and had been on acupuncture and pain medication for a long time. Lymphatic circulation promoter according to the present invention was allowed to take two packs of tid for 5 days, and then to take one more pack bid for 10 days. About two weeks later, the patient stated that she no longer felt ankle and heel pain. Lymphatic circulation promotion facilitates the discharge of pain-causing substances, which can confirm the lymphatic circulation effect of the present invention.

7) Clinical Trial 7-Pain Improvement (80 years old, female)

She was a grandmother patient who performed waist and knee surgery and carried a cane on her body. After taking the lymph circulation promoter according to the present invention for 10 days with two bags of tid, and then to take one more by bid for three months from 10 days. The patient stated that after about two days the pain in the lower back and knee had been alleviated, and after three months all the pain in the whole body had disappeared. Lymphatic circulation promotion facilitates the discharge of pain-causing substances, which can confirm the lymphatic circulation effect of the present invention.

Clinical Trial 8-Pain Improvement (61 years old, female)

She was a 60-year-old woman from China. Hearing back pain was young. The patients had worsened back pain, which he described as pulling and hurting the hips and thighs. When the lymphatic circulation promoter according to the present invention was taken in tids for 10 days, the patient stated that after 10 days, the pain was alleviated much. After 10 days, three more months of bids were taken in bids, and after 3 months, not only lower back pain but also thigh pain was stated. Lymphatic circulation promotion facilitates the discharge of pain-causing substances, which can confirm the lymphatic circulation effect of the present invention.

9) Clinical Trial 9-Pain Improvement (31 years old, female)

This patient was a 31 year old female athlete. The patient was injured in the Achilles tendon during training. The patient received hospital treatment for a period of time but had no improvement in symptoms. Not only could this patient not run, but it was also difficult to walk. The entire Achilles tendon is swollen and complains of severe pain, even if you touch it with your fingertips. Looking closely, the entire Achilles tendon was swelled with inflammation and severe pain caused by severe edema.

When intensively taking the lymph circulation promoter according to the present invention for 3 days in three packs of tid, the pain was improved so that there was no pain in touching and massaging the Achilles tendon and no problem in walking. Since the lymph circulation promoter according to the present invention to take two more packs of tid for 7 days, it was possible to jog by morning exercise. After 7 days after taking the lymph circulation promoter according to the present invention in two more tids, it is possible to exercise by increasing the intensity of exercise by 90% and there was almost no pain in the Achilles tendon. It is a good example of a tendon recovery. Lymphatic circulation promotion facilitates the discharge of pain-causing substances, which can confirm the lymphatic circulation effect of the present invention.

10) Clinical Trial 10-Inflammation Improvement (42 years old, male)

This patient Achilles tendon was broken in an accident while riding a motorcycle, and after surgery, the surgical site became inflamed. Since then, the inflammation has worsened almost every year, with dozens of reoperations and treatments, but the inflammation has not cleared up. Seoul National University Hospital confirmed the infection of the superbacteria and virus on the wound and said that it is no longer possible to cure it with surgery and medication. If the inflammation worsens, there is a risk of systemic infection. In this state, the lymph circulation promoter according to the present invention was intensively taken for 4 days with four bags of tid, and first, pus came out, and immediately after the dark black blood, a large amount of inflammation greatly decreased in size. After that, the lymph circulation promoter according to the present invention was further taken for 3 days with three packets of tid, so that the inflammation subsided cleanly and there was no discomfort due to the affected area. Naturally, there was no ankle amputation and when examined again in the hospital, the superbacteria or virus were no longer identified. In this case, it was thought that the lymph circulation promoting agent according to the present invention promoted the circulating discharge of the inflammatory substance, strengthened the immune function, and helped the movement of the immune cells, thereby removing the superbacteria and the virus in the inflammatory site.

Clinical Example 11 Skin Cell Regeneration Promotion (45 years old, male)

Patients of clinical example 1 shown in Table 7 below were damaged to the dermis layer by a hand-clamping accident, and were diagnosed as a very large wound of more than 5 centimeters in all directions in the hospital, which is impossible to regenerate and requires skin transplantation.

                      Photo a) Before treatment               Photo b) Twice weekly patch replacement 2 months after treatment

      Photo c) Twice weekly patch replacement 4 months after treatment      Photo d) Twice weekly patch replacement 6 months after treatment

As can be seen in the photograph in Table 8, in this patient or in patients with similar lesions, if no treatment or only massage treatment is applied, internal damage such as muscles, blood vessels and nerves as well as skin tissue damage is applied. It can also cause serious damage to tissue. In addition, such severe burns are accompanied by complex pathological and physiological changes. The patch was applied using Example 1 and the pill was taken two times by tid. As seen in photograph b of Table 8, the dermal layer recovered in most burned areas after 2 months of treatment. In addition, as shown in the photograph c of Table 8, it was observed that after 4 months of treatment, a substantial portion of the epidermal layer was recovered in most burned areas. In addition, as confirmed in the photograph d of Table 8, it was observed that all of the epidermal layers were recovered in most burned areas after 6 months of treatment. In addition, keloids were also observed finely.

Reducing scars by reducing keloids that have already occurred is a long and time-consuming and difficult task.However, reducing the production of keloids before the keloids do not cause scars is simpler than improving keloids that have already been formed. It's an easy task. If the skin is damaged enough to develop keloids, it may be caused by damage to the dermis and normal skin regeneration. At this time, if you actively help the body fluid circulation by using the lymph circulation promoter according to the present invention to quickly discharge the inflammatory or toxic substances of the damaged skin to prevent inflammation, improve pain, help the movement of immune cells immune function of the damaged area It improves the inflammation caused by the infection of microorganisms and helps the skin regeneration by smoothly supplying the nutrients, oxygen and moisture necessary for skin regeneration. The patch and the ring using the lymph circulation promoter in the present invention help to restore the damaged skin with the above functions and thus do not provide a fundamental cause of keloid production.

<Clinical example 12> Skin cell regeneration promotion (35 years old, male)

               Photo a) After 1 time management       Photo b) Twice weekly patch replacement 4 months after treatment

The patient was sent to check whether it is possible that the scar caused by the burn from the 00 surgeon, a specialist in burns in Incheon can be removed by the patch of Example 1. A patient who had been damaged for more than a year after burned the skin and had already completed keloid formation, it was impossible to reduce the scars. The skin graft showed thickening of the scar layer.

To this patient, the patch using the lymph circulation promoter of Example 1 was affixed, and the pill was taken twice by tid. As confirmed in the photograph a of Table 9, it was observed that the keloid disappeared by 95% or more after 4 months (approximately 30 times of patch replacement).

The principle of removing scars is not to get rid of keloids directly, but to promote lymph circulation to improve the environment of damaged dermal tissues to help normal skin cells develop. The keloid no longer occurs, and the keloid that has already been formed will peel off over time and slowly disappear. The scars that have already occurred need to be recovered from the dermal layer, which takes a lot of time. Especially, the scar management is a difficult field due to the formation of keloids. The improvement of the burn scar gives new hope not only to the burn scar but also to the general scar improvement. In the case of the transplanter, when the skin was transplanted, there was a pain as if the needle was sticking the skin with nerve damage, so I had to live with pressure socks at all times, but after 2 months, the pain was reduced and after 4 months, I did not have to wear pressure socks. This is thought to be the case that not only the skin cell recovery but also the nerve cell damage is recovered, and the effect of cell regeneration when the cell environment is normalized by promoting lymph circulation is known.

Clinical Example 13 Skin Cell Regeneration Promotion (48 Years Old, Female)

              Photo a) Before treatment        Photo b) Patch replacement once daily 14 days after treatment

      Photo c) Patch replacement once daily 28 days after treatment      D) Patch replacement once daily 40 days after treatment

As shown in Table 10, a female patient suffering from ankle burns in hot water was given tid three times a round of Example 1.

After 14 days of treatment, as can be seen in the photograph b) of Table 3, it was observed that not only the dermal cells but also the epidermal cells were partially regenerated in the entire burn area.

After 28 days of treatment, as can be seen in photograph c) of Table 3, it was observed that the epidermal cells were regenerated to a considerable extent in the entire burn area.

After 40 days of treatment, as confirmed in the photographic d) of Table 3, it was observed that the skin cells of the entire burn area were regenerated. In addition, burn scars (keloids) were hardly observed even in severe burns.

As such, the composition according to the present invention basically improves the environment around the skin cells by smoothly circulating the lymph in the skin, helps the metabolism of the skin cells to be restored normally, and enables the skin cells to function normally. Makes damaged skin cells regenerate.

14) Clinical Trial 14-Removal of Bruising (48 Years, Female)

The patient had a dark red color due to a rupture of blood vessels under the eye during the procedure. The patient was diagnosed with severe bruising in the hospital and it would take three to six months to remove the bruise. After taking the lymph circulation promoter according to the present invention for 2 days with two packets of tid, the bruise was removed to the extent that it is hardly observed with the naked eye. According to the lymph circulation principle, the bruise easily disappears when the lymph circulation is promoted.

15) Clinical Trial 15-Removal of Bruising (32 Years, Female)

She was a bruised woman patient with bruises all around her eyes. The blood-removing lymph circulation promoter according to the present invention was to be taken once every two bags of tid for 5 days. It was observed with the naked eye that all the remaining blood disappeared, leaving only traces of small spots that could not be seen in detail. Since bruises from bruises disappear due to the circulation of body fluids (lymph fluid), rapid removal of the bruises confirms the effect of promoting lymph circulation.

16) Clinical Trial 16-Temperature Control (50 years old, female)

This is a middle-aged woman with menopausal symptoms who are very tired for no reason but very tired for no reason, butt and stomach are cold, and the back feels hot from time to time, and in the morning wakes. Lymphatic circulation promoters according to the present invention were to be taken for 1 month by bid. After January, the hips and tummy were less cold, the back sensation was gone, and in the morning, the cold was no longer felt. Above all, he stated that he no longer felt tired and found vitality in his body. Anatomically physiologically, it can be explained that local cold air disappears when the lymph circulation is promoted, and it can confirm the lymph circulation promoting effect of the present invention through this clinical example.

Clinical Trials 17-Promote Drug Delivery (45, Female)

This patient had chronic cystitis. For severe cystitis, I took Septrin Tab (an antibiotic for treating acute cystitis, pyelonephritis, urethritis, and prostatitis). However, even when taking Septrin Tab, the effect was not frequent. The patient was asked to take the lymph circulation promoter according to the present invention together with the Septrin Tab. Later, the patient stated that the effect of taking Septrin Tab was rapid, and that the improvement in symptoms was clearer and clearer than before. Lymph circulation was promoted by the present invention, the active ingredient of the Septrin Tab to the bladder was quickly and surely determined that the Septrin Tab effectively acted on the lesion of the bladder.

18) Clinical Trials 18-Drug Delivery (68 years old, male)

She had relatively widespread shingles around her mouth. Aciclovir ointment was prescribed in the hospital and applied for a week, but there was no improvement. Again, I was prescribed Famclean Tab at the hospital and took one tablet every day for a week, but the symptoms did not improve. Lymphatic circulation promoter according to the present invention was to be taken together with two sachets every time Famclean Tab. Two days later, the shingles disappeared cleanly, leaving only traces. These results can be predicted through the lymph circulation promoting effect of the present invention.

As mentioned above, these various effects can only be explained by anatomical physiology or pathologically by the lymph circulation promoting effect. Therefore, by confirming these individual effects it is possible to confirm the lymph circulation promoting effect of the present invention.

<Manufacturing and marketing>

Lymphatic circulation promoter according to the present invention was prepared in the following composition ratios and packaging units.

27% by weight of Cheongung powder, 14% by weight of crust powder, 11% by weight of thawed skin powder, and 8% by weight of Euiin powder were made, and 26% by weight of maple syrup and 14% by weight of bamboo powder were further mixed. After making lyophilized rings, they were packed with sticks of 4.8 g units.

1 is a photograph of the product contents of the lymph circulation promoter according to the present invention, Figure 2 is a photograph of the product packaging of the lymph circulation promoter according to the present invention.

The product has sold more than 6,000,000 stick packaging (4.8g per stick packaging) from 2017.5.1 to 2018.3.31 through more than 2,000 pharmacies in Korea. The pharmacist participating in the marketing followed the administration of 2,000 patients with edema. As a result, 1,960 patients (about 98%) relieved edema with weight loss of 1.0% ~ 5.0%.

As described above, the edema-improving effect is directly related to the lymph circulation promoting effect anatomically and pathologically. Also, since edema occurs due to stagnation of body fluids and stagnation of body fluids is caused by lymphatic circulation disorders, improved edema means improved lymph circulation. Therefore, it is possible to confirm the lymph circulation promoting effect of the present invention by confirming the effect of improving the edema.

Claims (9)

Lymphatic circulation promoter comprising cheongung, maple syrup, crust, bamboo, thawed blood, and uiyiin in powder, liquid or extract form.
Lymphatic circulation promoting agent comprising maple syrup, bamboo and thawed blood in powder, liquid or extract form.
Lymphatic circulatory accelerator, characterized in that the cheongung, crust and uiyiin in powder, liquid or extract form.
Food use for edema improvement of the lymph circulation promoter of any one of Claims 1-3.
Food use for pain improvement of the lymph circulation promoter of any one of Claims 1-3.
Food use for the degumming of the lymph circulation promoter of any one of Claims 1-3.
Food use for skin cell regeneration of any one of claims 1 to 3 lymph circulation promoter.
A food use for promoting drug delivery of the lymph circulation promoter according to any one of claims 1 to 3.
Food use for tinnitus improvement of any one of Claims 1-3.

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