CN106619588A - Self-microemulsion nutrient composition containing coenzyme Q10 and preparation method and application - Google Patents
Self-microemulsion nutrient composition containing coenzyme Q10 and preparation method and application Download PDFInfo
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- CN106619588A CN106619588A CN201611245883.8A CN201611245883A CN106619588A CN 106619588 A CN106619588 A CN 106619588A CN 201611245883 A CN201611245883 A CN 201611245883A CN 106619588 A CN106619588 A CN 106619588A
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- ubidecarenone
- self
- parts
- microemulsion
- curcumin
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- 239000004006 olive oil Substances 0.000 description 1
- 235000008390 olive oil Nutrition 0.000 description 1
- 210000000056 organ Anatomy 0.000 description 1
- 239000007800 oxidant agent Substances 0.000 description 1
- 230000001590 oxidative effect Effects 0.000 description 1
- 230000036542 oxidative stress Effects 0.000 description 1
- 229920002866 paraformaldehyde Polymers 0.000 description 1
- 230000008506 pathogenesis Effects 0.000 description 1
- 230000010412 perfusion Effects 0.000 description 1
- 230000035699 permeability Effects 0.000 description 1
- 230000000144 pharmacologic effect Effects 0.000 description 1
- 239000012071 phase Substances 0.000 description 1
- 239000006187 pill Substances 0.000 description 1
- 229940044519 poloxamer 188 Drugs 0.000 description 1
- 235000010482 polyoxyethylene sorbitan monooleate Nutrition 0.000 description 1
- 229920001451 polypropylene glycol Polymers 0.000 description 1
- 229920000136 polysorbate Polymers 0.000 description 1
- 229920000053 polysorbate 80 Polymers 0.000 description 1
- 230000008092 positive effect Effects 0.000 description 1
- 238000001556 precipitation Methods 0.000 description 1
- 238000004321 preservation Methods 0.000 description 1
- 208000018290 primary dysautonomia Diseases 0.000 description 1
- RUOJZAUFBMNUDX-UHFFFAOYSA-N propylene carbonate Chemical compound CC1COC(=O)O1 RUOJZAUFBMNUDX-UHFFFAOYSA-N 0.000 description 1
- 230000001681 protective effect Effects 0.000 description 1
- 238000001671 psychotherapy Methods 0.000 description 1
- UMJSCPRVCHMLSP-UHFFFAOYSA-N pyridine Natural products COC1=CC=CN=C1 UMJSCPRVCHMLSP-UHFFFAOYSA-N 0.000 description 1
- 150000003233 pyrroles Chemical class 0.000 description 1
- 125000004151 quinonyl group Chemical group 0.000 description 1
- 230000008439 repair process Effects 0.000 description 1
- 239000003813 safflower oil Substances 0.000 description 1
- 235000005713 safflower oil Nutrition 0.000 description 1
- 238000005070 sampling Methods 0.000 description 1
- 210000000582 semen Anatomy 0.000 description 1
- 239000002002 slurry Substances 0.000 description 1
- 239000011780 sodium chloride Substances 0.000 description 1
- 239000007787 solid Substances 0.000 description 1
- 239000003549 soybean oil Substances 0.000 description 1
- 235000012424 soybean oil Nutrition 0.000 description 1
- 241000894007 species Species 0.000 description 1
- 239000007921 spray Substances 0.000 description 1
- 239000001334 starch sodium octenyl succinate Substances 0.000 description 1
- 235000013826 starch sodium octenyl succinate Nutrition 0.000 description 1
- 230000000638 stimulation Effects 0.000 description 1
- 238000003860 storage Methods 0.000 description 1
- 239000007929 subcutaneous injection Substances 0.000 description 1
- 238000010254 subcutaneous injection Methods 0.000 description 1
- 150000003900 succinic acid esters Chemical class 0.000 description 1
- 239000005720 sucrose Substances 0.000 description 1
- 235000000346 sugar Nutrition 0.000 description 1
- 150000008163 sugars Chemical class 0.000 description 1
- 230000001629 suppression Effects 0.000 description 1
- 239000000725 suspension Substances 0.000 description 1
- 238000002560 therapeutic procedure Methods 0.000 description 1
- 210000001519 tissue Anatomy 0.000 description 1
- 231100000331 toxic Toxicity 0.000 description 1
- 230000002588 toxic effect Effects 0.000 description 1
- 230000001988 toxicity Effects 0.000 description 1
- 231100000419 toxicity Toxicity 0.000 description 1
- UFTFJSFQGQCHQW-UHFFFAOYSA-N triformin Chemical compound O=COCC(OC=O)COC=O UFTFJSFQGQCHQW-UHFFFAOYSA-N 0.000 description 1
Classifications
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K31/00—Medicinal preparations containing organic active ingredients
- A61K31/12—Ketones
- A61K31/122—Ketones having the oxygen directly attached to a ring, e.g. quinones, vitamin K1, anthralin
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K31/00—Medicinal preparations containing organic active ingredients
- A61K31/12—Ketones
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K47/00—Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
- A61K47/06—Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite
- A61K47/08—Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite containing oxygen, e.g. ethers, acetals, ketones, quinones, aldehydes, peroxides
- A61K47/14—Esters of carboxylic acids, e.g. fatty acid monoglycerides, medium-chain triglycerides, parabens or PEG fatty acid esters
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K47/00—Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
- A61K47/44—Oils, fats or waxes according to two or more groups of A61K47/02-A61K47/42; Natural or modified natural oils, fats or waxes, e.g. castor oil, polyethoxylated castor oil, montan wax, lignite, shellac, rosin, beeswax or lanolin
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K9/00—Medicinal preparations characterised by special physical form
- A61K9/10—Dispersions; Emulsions
- A61K9/107—Emulsions ; Emulsion preconcentrates; Micelles
- A61K9/1075—Microemulsions or submicron emulsions; Preconcentrates or solids thereof; Micelles, e.g. made of phospholipids or block copolymers
-
- A—HUMAN NECESSITIES
- A23—FOODS OR FOODSTUFFS; TREATMENT THEREOF, NOT COVERED BY OTHER CLASSES
- A23V—INDEXING SCHEME RELATING TO FOODS, FOODSTUFFS OR NON-ALCOHOLIC BEVERAGES AND LACTIC OR PROPIONIC ACID BACTERIA USED IN FOODSTUFFS OR FOOD PREPARATION
- A23V2002/00—Food compositions, function of food ingredients or processes for food or foodstuffs
Landscapes
- Health & Medical Sciences (AREA)
- Chemical & Material Sciences (AREA)
- Life Sciences & Earth Sciences (AREA)
- Epidemiology (AREA)
- General Health & Medical Sciences (AREA)
- Veterinary Medicine (AREA)
- Medicinal Chemistry (AREA)
- Pharmacology & Pharmacy (AREA)
- Public Health (AREA)
- Animal Behavior & Ethology (AREA)
- Oil, Petroleum & Natural Gas (AREA)
- Molecular Biology (AREA)
- Biophysics (AREA)
- Dispersion Chemistry (AREA)
- Engineering & Computer Science (AREA)
- Chemical Kinetics & Catalysis (AREA)
- General Chemical & Material Sciences (AREA)
- Acyclic And Carbocyclic Compounds In Medicinal Compositions (AREA)
Abstract
The invention discloses a self-microemulsion nutrient composition containing coenzyme Q10 and a preparation method and application. The self-microemulsion nutrient composition comprises the following components in parts by weight: 1-15 parts of coenzyme Q10, 1-15 parts of curcumin, 10-50 parts of carrier oil, 15-75 parts of a nonionic surfactant, 1-5 parts of a cationic gemini surfactant, 5-30 parts of a cosurfactant and 0-2 parts of an antioxidant, wherein the components are prepared into a uniform, stable, clear and transparent solution. The self-microemulsion nutrient composition has good stability, crystallization of coenzyme Q10 is remarkably inhibited, and the product shelf life is prolonged. In the application process, the composition can be simply and conveniently added into systems of water-phase food, medicines and the like according to demand amounts, and is safe and effective. Meanwhile, the whole preparation process is green, environmental-friendly, low in energy consumption and easy in industrial production.
Description
Technical field
The present invention relates to compositions field, more particularly to a kind of self-microemulsion type alimentation composition, preparation side containing Ubidecarenone
Method and purposes.
Background technology
Parkinson disease (Parkinson disease, PD) are that one kind is mainly in middle-aged and elderly people, the nervous system of chronic progression
Degenerative disease, typical performance is static tremor, bradykinesia, myotonia and posture abnormal gait etc., while also with compared with
Serious non-motor symptoms, such as cognitive disorder, sleep disorder, depressive symptom and dysautonomia, this is not only
The quality of life of patient is seriously reduced, and white elephant is brought to family and society.With China human mortality structure it is old
Yearization problem it is increasingly serious, Parkinsonian sickness rate is also increasing considerably year by year, and it is old that parkinson disease have become impact
The primary killers of year people health.Therefore, active development to go out safely and effectively prevent or treat Parkinsonian medicine and its preparation
The arduous and urgent task of medical scientific research worker is become.
The pathogenesis of PD are extremely complex, and the cause of disease does not still understand so far.Inherited genetic factorss, oxidative stress, mitochondrial function barrier
Hinder, immunologic dysfunction and environmental factorss etc. all may induction PD.Currently for the different clinical symptoms of PD, Therapeutic Method has medicine
Thing treatment, operative treatment, rehabilitation and psychotherapy etc..Drug therapy is still occupied an leading position, although medicine can be obviously improved patient
Symptom, but have the shortcomings that toxic side effects are big, bioavailability is low.Thus, it is pre- from small toxicity, natural active matter
Demand that is anti-or treating PD is increasing.
Ubidecarenone (Coenzyme Q10, CoQ10) is the fat-soluble quinoness that a kind of biology is widely present in vivo,
Chemical name is 2,3- dimethoxy -5- methyl -6- last of the ten Heavenly stems isopentene group -1,4- benzoquinone.Ubidecarenone is a kind of good biological medicament
Thing, is the key element that energy is produced in human body, in being present in each cells of organs film, can improve myocardial metabolism, strengthen cardiac function;
And its strong anti-oxidation function can protect body cell from the destruction of free radical, improve the immunity of body.With coenzyme
Critical functions and health-care effect of the Q10 in terms of biology it is continuous revealed, along with its avirulence, without teratogenesis and nothing
It is the characteristics of apparent side effect, interior at the international level in recent years, have been widely used for all kinds of heart diseases, diabetes, cancer, acute and chronic
The treatment of the diseases such as hepatitis, Parkinson's disease, and can prevention of arterial hardening, apoplexy and hypertension, have good to heart, liver and kidney
Good health-care effect, the practical ranges of Ubidecarenone are constantly expanded.Ubidecarenone is widely used in food in American-European countries
Product, cosmetics, supplementary etc., the soft gel products for also having various correlations on China's market today.
Substantial amounts of research shows that Ubidecarenone has important protective effect in the damage and reparation of nervous system.The U.S.
The neurosurgeon Shults in University of California San Diego branch school has carried out 16 months to the Q10 that PD patient's packet imposes 3 kinds of dosage
Clinical trial, research finds that the development process of Parkinson's disease is delayed in the experimental group for applying maximum dose level Q10
44%.Liu Fei of Shandong University et al. has found that Q10 has improvement to make the cognitive function of PD patient, anxiety and sleep disorder
With.Mischley has found that PD patient's Q10 contents are significantly low compared with normal population.The above is true to be illustrated Q10 in the prevention of PD or controls
There is certain positive effect in treatment.
Ubidecarenone is liposoluble substance, and its water-insoluble makes it have difficulties at the aspect of digesting and assimilating of human body.And it is auxiliary
There is quinonyl in enzyme Q10 structures, quite sensitive to light and oxygen, it is given birth to make conventional tablet, hard capsule and suspension type soft capsule
Thing utilization rate is extremely low.
Curcumin is a kind of xanthein extracted from the dry rhizome of Zingiberaceae curcumin platymiscium, there is important Jing
Ji value and extensive pharmacological action (antitumor, antioxidation, antiinflammatory, blood fat reducing etc.).Because curcumin is safe and malicious pair
Effect is little, and in modern medicine, curcumin is because of itself and the connection between neuranagenesis (especially parkinson disease) and carcinogen
It is and receives special attention.Recent studies indicate that, curcumin can be used for controlling for neurodegenerative diseases such as PD and AD
Treat.But curcumin is as Q10, water is practically insoluble in, oral administration biaavailability is very low.
Therefore, Ubidecarenone and curcumin dissolubility in an aqueous medium and storage-stable how to be improved, become its
Key technical problem during production and consumption.
Self-microemulsion drug-supplying system (self-microemulsifying drug delivery system, SMEDDS) be by
Homogeneous, Thermodynamically stable, isotropic liquid oral that medicine, oil phase, surfactant and cosurfactant are constituted
Dosage form or solid dosage formss.The basic feature of the drug-supplying system is, it is oral after spontaneously form particle diameter < in the case where gastrointestinal is wriggled
The oil in water emulsion of 100nm.SMEDDS can improve the dissolubility and bioavailability of poorly water-soluble or fat-soluble medicine, while can
The pessimal stimulation of the degraded of labile drugs and medicine to gastrointestinal in avoid water.It promotes the mechanism and advantage of drug absorption
It is mainly reflected in the following aspects:(1) free energy needed for emulsifying is very low, spontaneously forms in the case where gastrointestinal is slightly wriggled
The emulsion droplet of particle diameter very little has larger surface area, increased the permeability of medicine chrotoplast on the gastrointestinal tract;(2) medicine is improved
Dissolubility and improve the dissolution of medicine;(3) small microemulsion is dripped because of the parent with less surface tension and microemulsion surface
Aqueouss so as to be easy to the hydrated sheath by gastrointestinal tract wall, increase penetrance, promote to absorb and improve bioavailability;(4) it is relative
Emulsion, with higher physical stability;(5) preparation process is simple, is appropriate to industrialized production.
Correlational study shows that the gastrointestinal tract epithelial cell of body is electronegative.Thus sun can be introduced in microemulsion
Ionic species so as to gastrointestinal tract epithelial cell because electrostatic attraction is acted on, so as to further promote the absorption of insoluble medicine, improve
Bioavailability.Gemini is a kind of gemini surfactant, and it is in respective ion head by two monomcric surfactants
The Ji Chu class surfactants that chemical bonding gets up by connection base.This special dimeric structure imparts Shuangzi surface
It is the more superior performance of the more corresponding conventional single-ended base of activating agent, single alkane chain surfactant, such as high surface, low
The water solublity that Krafft points are become reconciled, shows higher efficiency and ability, itself and monomer table in terms of the surface tension of water is reduced
The compounding of face activating agent, especially nonionic surfactant can produce higher cooperative effect, to oil solubilising power more
By force.
The content of the invention
It is an object of the invention to provide a kind of water solublity is good, excellent in stability, bioavailability are high containing Ubidecarenone
Self-microemulsion type alimentation composition.
For achieving the above object, the present invention provides a kind of self-microemulsion type alimentation composition containing Ubidecarenone, and its feature exists
In, it is prepared by each composition of following weight portion,
1~15 part of Ubidecarenone, 1~15 part of curcumin, 10~50 parts of carrier oils, 15~75 parts of non-ionic surfactants
Agent, 1~5 portion of cationic Gemini surfactants, 5~30 portions of cosurfactants, 0-2 part antioxidants.
Further, it is prepared by each composition of following weight portion, 2~12 parts of Ubidecarenone, 2~12 parts of curcumins, 15
~45 parts of carrier oils, 25~60 parts of nonionic surfactant, 1.5~4.5 parts of cationic Gemini surfactants, 10
~25 portions of cosurfactants, 0-2 part antioxidants.
Further, it is prepared by each composition of following weight portion, 5~10 parts of Ubidecarenone, 5~10 parts of curcumins, 20
~30 parts of carrier oils, 30~45 parts of nonionic surfactant, 2~3 parts of cationic Gemini surfactants, 12~20
Part cosurfactant, 0-1 part antioxidants;
Preferably, it is prepared by each composition of following weight portion, 8 parts of Ubidecarenone, 7 parts of curcumins, 28 parts of carriers
Oil, 40 portions of nonionic surfactant, 2 portions of cationic Gemini surfactants, 15 portions of cosurfactants, 1 part resists
Oxidant.
Further, the Ubidecarenone is at least one in CoQ10, reduced coenzyme Q 10;Preferably, it is auxiliary
At least one in Native Oxide type Ubidecarenone and reduced coenzyme Q 10 that enzyme Q10 is prepared for microbe fermentation method;
It is optional, the carrier oil be crude vegetal or it is strong to key component solvability, through structure of modification, water
Vegetable oil or fatty acid ester after solution;Preferably, crude vegetal is soybean oil, Oleum Arachidis hypogaeae semen, olive oil, Oleum Ricini, safflower oil
In one or more;Vegetable oil strong to key component solvability, after structure of modification, hydrolysis or fatty acid ester are
Almond oil Oleic acid PEG-6 glyceride, isopropyl myristate, ethyl oleate, medium chain length fatty acid triglyceride, Oleic acid Polyethylene Glycol are sweet
One or more in grease, Masine 35-1 and polypropylene glycol caprylate;
Optional, the nonionic surfactant is selected from the dihydroxy stearic acid ester of Polyethylene oxide ten, the poly- second of caprylic capric
Glycol glyceride, Polyoxyl 40 Hydrogenated Castor Oil, the sucrose ester of HLB value 13~16, Pluronic F68,
One or more in vitamin E polyethylene glycol succinic acid ester, tween 85, tween 80, Poloxamer 188, lecithin;
Optional, the cosurfactant is selected from glycerol, ethanol, ethylene glycol, PEG200-600, diethylene glycol mono-ethyl
One or more in ether, propylene carbonate and Propylene Glycol;
Optional, the antioxidant is extracted selected from sodium ascorbate, natural Vitamin E and its ester derivant, Herba Rosmarini Officinalis
One or more in thing.
Further, the self-microemulsion type alimentation composition containing Ubidecarenone of the present invention also contains antibacterial, stabilizer, helps
One or more in stream agent and coloring agent.
Further, preparation method is,
Each component is weighed in proportion, by remaining each component mix homogeneously outside Ubidecarenone and curcumin, adds coenzyme
Q10 and curcumin, are heated to 50-65 DEG C of stirring up to whole system transparent and homogeneous, then are incubated 15-60min, are cooled to room temperature i.e.
Can.Insulated and stirred therein advantageously forms stable oil preparation, and Ubidecarenone is difficult crystallize.
Further, the preparation process and the preservation after preparing are in inert atmosphere or vacuum state;It is preferred that nitrogen or
Helium atmosphere atmosphere.
Further, microcapsule, soft capsule, hard capsule, tablet, powder, pill, Emulsion or suspensoid can be prepared into.
The present invention also provides the self-microemulsion type alimentation composition containing Ubidecarenone for preparing prevention and/or treating handkerchief
The purposes of the gloomy medicine of gold.
The present invention also provides the self-microemulsion type alimentation composition containing Ubidecarenone for preparing prevention and/or treating handkerchief
The dietary supplement of the gloomy disease of gold or the purposes of health food.
The self-microemulsion type alimentation composition good stability containing Ubidecarenone that the present invention is prepared, it is existing without oil slick, aggregation
As.When not in the amount ranges of the present invention, the self-microemulsion type alimentation composition oil preparation containing Ubidecarenone has oil slick, clustering phenomena.
Ubidecarenone of the present invention and curcumin have antioxidation, the function of eliminating free radical, repair injured nerve, send out
A person of good sense has found that the two carries out by a certain percentage compatibility and can play the effect of Synergistic, and Ubidecarenone is stablized with the compatibility of curcumin,
There is no chemical reaction, have no adverse reaction, it is safe and feasible.
The antioxidant does not have special restriction, can be sodium ascorbate, natural Vitamin E and its ester derivant,
One or more in Herba Rosmarini Officinalis extract etc.;To the antibacterial, stabilizer, fluidizer, coloring agent etc., other adjuvants do not have
It is special to limit, but should can be the composition for allowing to be added in food, medicine etc..
Self-microemulsion type alimentation composition containing Ubidecarenone of the present invention or its preparation, by oral administration after, in vivo by stomach
The wriggling of intestinal spontaneously forms microemulsion of the oil droplet mean diameter less than 100nm.
Positively charged microemulsion is formed in the present invention by introducing the cationic Gemini surfactants of recipe quantity
Drop, the effective absorption by electrostatic interaction with enhancing body to Ubidecarenone and curcumin.
The invention has the beneficial effects as follows:
1st, after the self-microemulsion type alimentation composition containing Ubidecarenone prepared by the present invention mixes with water, can form uniform, steady
The fixed, solution of clear.In application process, simply and easily can on demand be added to the bodies such as water phase food, medicine
In the middle of system.
2nd, the self-microemulsion type alimentation composition containing Ubidecarenone prepared by the present invention has the stability of height, significantly suppression
The crystallize of Ubidecarenone has been made, shelf life has been extended.
2nd, the emulsion droplet size that the self-microemulsion type alimentation composition containing Ubidecarenone prepared by the present invention is formed is up to 10-100
Nanometer, belongs to nanometer formulation category, and body absorption effect is good.By the cationic Gemini surfactants for adding recipe quantity
Drip to form positively charged microemulsion, the effective absorption by electrostatic interaction with enhancing body to Ubidecarenone and curcumin,
Further improve the bioavailability of medicine.
3rd, after taking the self-microemulsion type alimentation composition containing Ubidecarenone of the present invention, Ubidecarenone is with curcumin in blood plasma
The ratio of release is substantially constant, is not arbitrarily release, but slow, stable in blood plasma according to the ratio in formula
Middle release, so as to ensure the safety and effectiveness taken.
4th, the Ubidecarenone and curcumin that have potential using value in prevention or treatment PD are carried out science by the present invention
Compatibility, both at all-natural product, with obvious synergistic function.
5th, the present invention directly can add water solublity wall material solution on the basis of obtained self-emulsifying microemulsion oil preparation, stir
Afterwards, it is spray-dried and the good self-emulsifying microemulsion microcapsule of water solublity is obtained, or is prepared into various desired dosage forms.
6th, there is no chemical change in the preparation process is simple of the self-microemulsion type alimentation composition containing Ubidecarenone of the present invention
Change, do not change Ubidecarenone and curcumin chemical constitution, whole preparation process environmental protection, low energy consumption, it is easy to accomplish industrial metaplasia
Produce.
Specific embodiment
Embodiments of the invention are described below in detail, the example of the embodiment is being intended to for explaining the present invention, and not
It is understood that as limitation of the present invention.Unreceipted particular technique or condition person in embodiment, are retouched according to document in the art
The technology stated or condition are carried out according to product description.Agents useful for same or the unreceipted production firm person of instrument, being can be with
By city available from conventional products.
Embodiment 1:
The each Ingredient Amount table of embodiment 1-6 of table 1
The each Ingredient Amount table of embodiment 7-13 of table 2
Preparation method:Each composition is weighed by listed mass fraction in table 1, by remaining each group outside Ubidecarenone and curcumin
Divide mix homogeneously, add Ubidecarenone and curcumin, be heated to 55 DEG C of stirrings up to whole system transparent and homogeneous, then be incubated
30min, is down to after room temperature and obtains orange-yellow transparent homogeneous self-emulsifying microemulsion oil preparation.
Take gained self-emulsifying microemulsion oil preparation about 1g to be added in 100ml deionized waters, slightly shake, obtain orange-yellow transparent water
Emulsion, it is therefore seen that this product water dispersible is good.
(1) gained self-emulsifying microemulsion oil preparation is obtained into Ubidecarenone-Rhizoma-curcumae-longae element-soft cap sule by soft capsule production equipment.
(2) water of 200 mass parts, stirring is added to be formed and put into after uniform solution 56 mass in gained self-emulsifying microemulsion oil preparation
Part starch sodium octenyl succinate, 35 mass parts maltodextrins, 9 mass parts white sugars, stirring and dissolving, the homogenizing under 30Mpa, most
Microemulsion is spray-dried afterwards, at 170 DEG C, air outlet temperature is controlled at 80 DEG C the control of spray tower intake air temperature, atomization
Device rotating speed 1200r/min, is spray-dried to obtain self-emulsifying microemulsion microcapsule.
Embodiment 2
Raw material:It is shown in Table 1.
Preparation method:Each composition is weighed by listed mass fraction in table 1, by remaining each group outside Ubidecarenone and curcumin
Divide mix homogeneously, add Ubidecarenone and curcumin, be heated to 50 DEG C of stirrings up to whole system transparent and homogeneous, then be incubated
40min, is down to after room temperature and obtains orange-yellow transparent homogeneous self-emulsifying microemulsion oil preparation.
Take gained self-emulsifying microemulsion oil preparation about 1g to be added in 100ml deionized waters, slightly shake, obtain orange-yellow transparent water
Emulsion, it is therefore seen that this product water dispersible is good.
(1) Ubidecarenone-Rhizoma-curcumae-longae element-soft cap sule is obtained by soft capsule production equipment.
(2) self-emulsifying microemulsion microcapsule is prepared by the microcapsule preparation process of embodiment 1.
Embodiment 3
Raw material:It is shown in Table 1.
Preparation method:Each composition is weighed by listed mass fraction in table 1, by remaining each group outside Ubidecarenone and curcumin
Divide mix homogeneously, add Ubidecarenone and curcumin, be heated to 60 DEG C of stirrings up to whole system transparent and homogeneous, then be incubated
50min, is down to after room temperature and obtains orange-yellow transparent homogeneous self-emulsifying microemulsion oil preparation.
Take gained self-emulsifying microemulsion oil preparation about 1g to be added in 100ml deionized waters, slightly shake, obtain orange-yellow transparent water
Emulsion, it is therefore seen that this product water dispersible is good.
(1) Ubidecarenone-Rhizoma-curcumae-longae element-soft cap sule is obtained by soft capsule production equipment.
(2) self-emulsifying microemulsion microcapsule is prepared by the microcapsule preparation process of embodiment 1.
Embodiment 4
Raw material:It is shown in Table 1.
Preparation method:Each composition is weighed by listed mass fraction in table 1, by remaining each group outside Ubidecarenone and curcumin
Divide mix homogeneously, add Ubidecarenone and curcumin, be heated to 65 DEG C of stirrings up to whole system transparent and homogeneous, then be incubated
60min, is down to after room temperature and obtains orange-yellow transparent homogeneous self-emulsifying microemulsion oil preparation.
Take gained self-emulsifying microemulsion oil preparation about 1g to be added in 100ml deionized waters, slightly shake, obtain orange-yellow transparent water
Emulsion, it is therefore seen that this product water dispersible is good.
(1) Ubidecarenone-Rhizoma-curcumae-longae element-soft cap sule is obtained by soft capsule production equipment.
(2) self-emulsifying microemulsion microcapsule is prepared by the microcapsule preparation process of embodiment 1.
Embodiment 5:
Raw material:It is shown in Table 1.
Preparation method:Each composition is weighed by listed mass fraction in table 1, by remaining each group outside Ubidecarenone and curcumin
Divide mix homogeneously, add Ubidecarenone and curcumin, be heated to 52 DEG C of stirrings up to whole system transparent and homogeneous, then be incubated
35min, is down to after room temperature and obtains orange-yellow transparent homogeneous self-emulsifying microemulsion oil preparation.
Embodiment 6:
Raw material:It is shown in Table 1.
Preparation method:Each composition is weighed by listed mass fraction in table 1, by remaining each group outside Ubidecarenone and curcumin
Divide mix homogeneously, add Ubidecarenone and curcumin, be heated to 62 DEG C of stirrings up to whole system transparent and homogeneous, then be incubated
45min, is down to after room temperature and obtains orange-yellow transparent homogeneous self-emulsifying microemulsion oil preparation.
Embodiment 7:
Raw material:It is shown in Table 2.
Preparation method:Each composition is weighed by listed mass fraction in table 1, by remaining each group outside Ubidecarenone and curcumin
Divide mix homogeneously, add Ubidecarenone and curcumin, be heated to 54 DEG C of stirrings up to whole system transparent and homogeneous, then be incubated
55min, is down to after room temperature and obtains orange-yellow transparent homogeneous self-emulsifying microemulsion oil preparation.
Embodiment 8:
Raw material:It is shown in Table 2.
Preparation method:Each composition is weighed by listed mass fraction in table 1, by remaining each group outside Ubidecarenone and curcumin
Divide mix homogeneously, add Ubidecarenone and curcumin, be heated to 56 DEG C of stirrings up to whole system transparent and homogeneous, then be incubated
32min, is down to after room temperature and obtains orange-yellow transparent homogeneous self-emulsifying microemulsion oil preparation.
Embodiment 9:
Raw material:It is shown in Table 2.
Preparation method:Each composition is weighed by listed mass fraction in table 1, by remaining each group outside Ubidecarenone and curcumin
Divide mix homogeneously, add Ubidecarenone and curcumin, be heated to 58 DEG C of stirrings up to whole system transparent and homogeneous, then be incubated
15min, is down to after room temperature and obtains orange-yellow transparent homogeneous self-emulsifying microemulsion oil preparation.
Embodiment 10:
Raw material:It is shown in Table 2.
Preparation method:Each composition is weighed by listed mass fraction in table 1, by remaining each group outside Ubidecarenone and curcumin
Divide mix homogeneously, add Ubidecarenone and curcumin, be heated to 59 DEG C of stirrings up to whole system transparent and homogeneous, then be incubated
20min, is down to after room temperature and obtains orange-yellow transparent homogeneous self-emulsifying microemulsion oil preparation.
Embodiment 11:
Raw material:It is shown in Table 2.
Preparation method:Each composition is weighed by listed mass fraction in table 1, by remaining each group outside Ubidecarenone and curcumin
Divide mix homogeneously, add Ubidecarenone and curcumin, be heated to 61 DEG C of stirrings up to whole system transparent and homogeneous, then be incubated
25min, is down to after room temperature and obtains orange-yellow transparent homogeneous self-emulsifying microemulsion oil preparation.
Embodiment 12:
Raw material:It is shown in Table 2.
Preparation method:Each composition is weighed by listed mass fraction in table 1, by remaining each group outside Ubidecarenone and curcumin
Divide mix homogeneously, add Ubidecarenone and curcumin, be heated to 63 DEG C of stirrings up to whole system transparent and homogeneous, then be incubated
52min, is down to after room temperature and obtains orange-yellow transparent homogeneous self-emulsifying microemulsion oil preparation.
Embodiment 13:
Raw material:It is shown in Table 2.
Preparation method:Each composition is weighed by listed mass fraction in table 1, by remaining each group outside Ubidecarenone and curcumin
Divide mix homogeneously, add Ubidecarenone and curcumin, be heated to 64 DEG C of stirrings up to whole system transparent and homogeneous, then be incubated
57min, is down to after room temperature and obtains orange-yellow transparent homogeneous self-emulsifying microemulsion oil preparation.
Embodiment 14:Droplet measurement, the experiment of self-emulsifying microemulsion time
Droplet measurement:
Self-emulsifying microemulsion oil preparation prepared by case study on implementation and self-emulsifying microemulsion microcapsule sample distilled water are with 1:20 ratio
Dilute, gently shake up, that is, form the microemulsion of clarification.Then emulsion is determined with laser fineness gage (Malvern companies of Britain)
Particle diameter distribution, temperature of the measurement be 25 DEG C.
Self-microemulsion speed:
According to《Pharmacopoeia of People's Republic of China》(2005 editions) annex leaching slurry processes are measured, Example 1-4's
Self-emulsifying microemulsion oil preparation and self-emulsifying microemulsion microcapsule (each 100mg) are dissolved in 37 DEG C of simulated gastric fluids, record each case study on implementation self-microemulsion
The change time.
The particle diameter of the self-micro emulsion formulation of table 1, self emulsifying time data table
Experimental result shows that emulsion mean diameter is respectively less than 100nm, and solution clear illustrates to define stable uniform
Microemulsion;The emulsion dispersion uniform time completely is respectively less than 3 minutes, with self-emulsifying microemulsion speed faster, i.e., by slight
Stirring, it becomes possible to form the homogeneous Emulsion of appearance transparent.
The result of embodiment 5-13 is herewith.
Embodiment 15:Stability experiment:
Self-emulsifying microemulsion oil preparation, self-emulsifying microemulsion microcapsule and the Ubidecarenone raw material that Example 1 is prepared is respectively placed in
The irradiation of 4500Lx intensities of illumination, oxygenation fill (25 DEG C), 60 DEG C (calorstat) place 15 days, respectively at 0 day, 5 days, 10 days, 15
Its sampling and measuring, with HPLC methods Ubidecarenone content is determined, and investigates illumination, oxygen, temperature conditionss to Ubidecarenone sign content
(%) impact.As a result it is as shown in table 2:
Impact table of the illumination of table 2 to stability
Impact of the oxygen of table 3 to stability
Impact table of the temperature of table 4 to stability
Influence factor test result indicate that, the self-emulsifying microemulsion oil preparation and the self-emulsifying microemulsion that further prepares of the present invention is micro-
Under illumination, oxygenation, hot conditionss, Ubidecarenone sign content and face shaping are not changed in capsule.Face shaping aspect,
Self-emulsifying microemulsion oil preparation is in yellow clear solution, does not crystallize precipitation;Self-emulsifying microemulsion microcapsule is yellow powder, not bright in color
It is aobvious to change.Ubidecarenone sign content aspect, As time goes on (5 days, 10 days, 15 days), its Ubidecarenone sign contains quantitative change
Change less, it is more more stable than the Ubidecarenone sign content in Ubidecarenone raw material.Illustrate the self-emulsifying microemulsion oil preparation of the present invention and enter one
The self-emulsifying microemulsion microcapsule that step is prepared has preferable stability, reduces the shadow of illumination, oxygen, temperature to its property
Ring, extend product storage life.
The result of embodiment 2-13 is herewith.
Embodiment 16:Internal pharmacokinetic studies:
16.1 samples:
(code name is Ubidecarenone-Rhizoma-curcumae-longae element-soft cap sule prepared by embodiment 1~4:Sample 1, sample 2, sample 3, sample 4);
The configuration of Ubidecarenone-curcumin raw material medicine solution agent:Precision weighs 50g Ubidecarenone, 10g curcumins (the two weight
Amount ratio 5:1, consistent with the ratio of sample 1), be dissolved in 800ml ethanol-PEG400 solution (v/v, 1:1) (code name is:Raw material
Sample).
Total of five sample carries out animality experiment.
16.2 experiment conditions:25 ± 3 DEG C of laboratory rearing ambient temperature, relative humidity 55%~70% is freely drunk daily
Water is ingested (deionized water and standard feed), its fasting 12h before experiment, free water.
16.3 laboratory animals and packet:By Changsha Kaifu District Dong Chuan Animal Sciences service department, (laboratory animal is used
Credit number be SYXK (Hunan) 2010-0010) provide SPF levels Kunming kind female mice, 3 months Mus ages, 18~22g of body weight.
Animal is operated according to International Laboratory Animal experiment criterion, to reduce pain of the laboratory animal in experimentation.Using
The mice of fasting 12h is divided into one group by completely randomized design per 10 at random, totally five groups.
16.4 oral administrations and sample collecting, process:Mouse stomach same dose (35mg/kg is given respectively:Ubidecarenone
With curcumin total content) self-microemulsion drug-supplying system sample (i.e. sample 1-4) and crude drug (i.e. raw material sample), after administration respectively at
5th, 15,30min and 1,2,4,6,12h collections blood plasma extremely contain in the anticoagulant centrifuge tube of heparin, mix, 3000r/min centrifugal treating
After 10min, separated plasma detects plasma drug level after process with HPLC methods.
16.5 pharmacokinetic studies
According to blood drug level result, applied statistics analysis software carries out statistics Fitting Analysis to experimental result, calculates blood
Concentration data, are as a result represented (table 5) with means standard deviation.
Its mouse oral of table 5 clothes are administered sample average blood concentration-time (mean ± SD, n=10) (mg/L) table
As a result show after oral administration, self-microemulsion type preparation (i.e. Ubidecarenone-the Rhizoma-curcumae-longae element-soft cap sule of embodiment 1-4)
Peak concentration cmax value is significantly higher than the cmax value (P < 0.05) of crude drug, AUC also greater than crude drug AUC, Ubidecarenone
Accelerate and can reach higher plasma concentration, the bioavailability of body in mice body absorption Jing after self-emulsifying microemulsion with curcumin
Also dramatically increase.Self-micro emulsion formulation belongs to nanometer formulation category, is conducive to improving the uniformity of drug absorption, shown self-microemulsion system
The fluctuation of agent peak concentration is less than crude drug, so as to improve the safety of medication.
Its mouse oral of table 6 clothes administration Ubidecarenone and ratio table of the curcumin in plasma concentration under each detection time
From table 6 according to contrast each sample, the concentration ratio of raw material sample Ubidecarenone and curcumin in different test period blood plasma
Value, it can be seen that the ratio that self-micro emulsion formulation Ubidecarenone and curcumin prepared by the present invention discharges in blood plasma is substantially perseverance
Fixed, it is slowly, smoothly to discharge according to the ratio in formula.
Relative bioavailability F is to weigh bioavailability of a certain medicine compared to other prescriptions of same medicine,
That is the ratio of the lower area of blood concentration-time curve AUC of test agent and reference reagent, with regard to the important of drug absorption performance
Parameter.The results are shown in Table 7.
Its mouse oral of table 7 clothes administration sample medicine kinetic parameter table
As known from Table 7 the F values of sample 1 are 206.9% (72.88/35.22), the i.e. bioavailability of self microemulsifying preparation
It it is 2.07 times of crude drug, sample 2 is 217.9%, sample 3 is 226.8%, sample 4 is 202.5%.Illustrate to change dosage form pair
In vivo absorption process is substantially improved medicine.Illustrate the self-microemulsion type alimentation composition containing Ubidecarenone that the present invention is prepared
Different dosage form substantially improve the body absorption process of medicine.
The biological half-life t of self-micro emulsion formulation1/2It is not significantly different from crude drug, illustrates that self microemulsifying preparation does not affect
Medicine elimination in vivo.
The result of embodiment 5-13 is herewith.
Embodiment 17:Animal behavioral study and test:
17.1 samples:
Sample 1:Self-emulsifying microemulsion oil preparation prepared by embodiment 1.
Reference substance 1:Curcumin in the formula of embodiment 1 is substituted for the MCT of equal quality number, remaining component and preparation side
Method is consistent with embodiment 1, prepares self-emulsifying microemulsion oil preparation reference substance 1.
Reference substance 2:Ubidecarenone in the formula of embodiment 1 is substituted for the MCT of equal quality number, remaining component and preparation
Method is consistent with embodiment 1, prepares self-emulsifying microemulsion oil preparation reference substance 2.
17.2 experiment conditions:25 ± 3 DEG C of laboratory rearing ambient temperature, relative humidity 55%~70% is freely drunk daily
Water is ingested (deionized water and standard feed), its fasting 12h before experiment, free water.
17.3 laboratory animals and packet:By Changsha Kaifu District Dong Chuan Animal Sciences service department, (laboratory animal is used
Credit number be SYXK (Hunan) 2010-0010) provide SPF levels Kunming kind female mice, 3 months Mus ages, 18~22g of body weight.
Animal is operated according to International Laboratory Animal experiment criterion, to reduce pain of the laboratory animal in experimentation.Using
Mice is divided into one group by completely randomized design per 10 at random, totally 6 groups.Each matched group lumbar injection volume is consistent, daily injection
Time point is similar.
Normal group:Continuous intraperitoneal injection of saline 24 days;
Solvent control group:Continuous 5 days lumbar injections 30mg/kg MPTP (1- methyl 4-phenyl -1,2,3,6- tetrahydrochysene pyrroles
Pyridine), subsequent continuous 19 days lumbar injection DMSO (dimethyl sulfoxide);
Treat 1 group:Sample 1+MPTP groups, i.e., continuous 5 days lumbar injections 30mg/kg MPTP, then use 30mg/kg samples 1 instead
Continuous injection 19 days;
Treat 2 groups:Reference substance 1+MPTP groups, i.e., continuous 5 days lumbar injections 30mg/kg MPTP, then use 30mg/kg pair instead
Continuously inject 19 days according to product 1;
Treat 3 groups:Reference substance 2+MPTP groups, i.e., continuous 5 days lumbar injections 30mg/kg MPTP, then use 30mg/kg pair instead
Continuously inject 19 days according to product 2;
Prevention group:Inject 30mg/kg samples 1 within continuous 7 days before MPTP models treated is carried out, then continuous 5 days abdominal cavities note
30mg/kg MPTP are penetrated, subsequently continuous 19 days lumbar injection DMSO;
17.4 apomorphines induce rotation test:In each point observing time in mouse subcutaneous injection dosage for 0.3mg/kg's
Apomorphine, induces the circling behavior of mice, it is stipulated that be rotated by 360 ° as one turn, records the rotation revolution in mice 30min.If receiving
Examination thing group rotation revolution is significantly less than solvent control group rotation revolution, and difference has significance (P<0.05), can determine that this is tested
Thing has prevention or alleviates Parkinsonian effect.Result of the test is shown in Table 8.
The apomorphine of table 8 induces rotation test revolution (X ± S, n=10) table
As can be seen from Table 8, the apomorphine induction rotation test revolution for the treatment of group 1-3 groups and prevention group is significantly lower than molten
Agent matched group, and difference has significance (P<0.05), illustrate that the self-emulsifying microemulsion oil preparation of the present invention has and prevent or alleviate parkinson
The effect of disease.Simultaneously visible, Ubidecarenone has obvious synergistic function (the test effect of 1 group for the treatment of with the compatibility of curcumin
Fruit is significantly better than 3 groups of 2 groups for the treatment of and treatment).
The asymmetrically placed experiment of 17.5 triggerings:Hold mice trunk and leave ground, by its side antenna touching table angle.When
Placement action of the homonymy forelimb to table angle can be induced during the antenna touching table angle of mice side, impaired forelimb can not be by forelimb into power amplifier
It is placed in table angle.During scoring, both sides forelimb is tested respectively 10 times, calculates the asymmetrically placed experiment score of triggering.The data obtained is meter
Amount data, if the asymmetrically placed experiment score of tested material group triggering is significantly lower than solvent control group, and difference has significance (P<
0.05), can determine that the tested material has prevention or alleviates Parkinsonian effect.Result of the test is shown in Table 9.
Table 9 triggers asymmetrically placed experiment score (X ± S, n=10) table
As can be seen from Table 9,1-3 groups are treated and the asymmetrically placed experiment score of prevention group triggering is significantly lower than solvent control
Group, and difference has significance (P<0.05) the self-emulsifying microemulsion oil preparation for, illustrating the present invention has prevention or alleviates Parkinsonian work
With.Simultaneously visible, Ubidecarenone has obvious synergistic function with the compatibility of curcumin, and (test effect of 1 group for the treatment of is notable
Better than 3 groups of 2 groups for the treatment of and treatment).
17.6 immunohistochemical analysis:
After the detection of each group mice behavior, under urethane deep anaesthesia, with the fixed brain of (4 DEG C) perfusions of 4% paraformaldehyde
Tissue, takes Mus brain midbrain sections, 24 hours in immersion fixative.Select midbrain black after Mus brain midbrain sections after fixation is processed
Matter, striatum position, carry out immunohistochemical staining process, are placed in after mounting under laser confocal microscope and are observed, will be each
The black substance TH Positive Cell Counts of group mice, it is as a result as shown in table 10 below:
The black substance TH Positive Cell Counts and P value tables of the mice of table 10
As can be seen from Table 10, treat 1-3 groups, the TH positive cell numbers of prevention group substantially increases (P < compared with solvent control group
0.05), it can be seen that, Ubidecarenone and curcumin can promote the expression of TH, reduce neurotoxin Dui -matter TH damage, enter
And preventing or to treat have on PD potential using value.Simultaneously visible, Ubidecarenone has obvious with the compatibility of curcumin
Synergistic function (1 group of test effect for the treatment of is significantly better than 3 groups of 2 groups for the treatment of and treatment), and have no adverse reaction, safety
High, good stability.
The result of embodiment 2-13 is herewith.
Although embodiments of the invention have been shown and described above, it is to be understood that above-described embodiment is example
Property, it is impossible to limitation of the present invention is interpreted as, one of ordinary skill in the art is in the principle and objective without departing from the present invention
In the case of above-described embodiment can be changed within the scope of the invention, change, replace and modification.
Claims (10)
1. a kind of self-microemulsion type alimentation composition containing Ubidecarenone, it is characterised in that it is prepared by each composition of following weight portion
Obtain,
1~15 part of Ubidecarenone, 1~15 part of curcumin, 10~50 parts of carrier oils, 15~75 parts of nonionic surfactant, 1
~5 portions of cationic Gemini surfactants, 5~30 portions of cosurfactants, 0-2 part antioxidants.
2. the self-microemulsion type alimentation composition of Ubidecarenone is contained described in claim 1, it is characterised in that it is by following weight portion
Each composition is prepared, 2~12 parts of Ubidecarenone, 2~12 parts of curcumins, 15~45 parts of carrier oils, 25~60 parts of nonionic tables
Face activating agent, 1.5~4.5 portions of cationic Gemini surfactants, 10~25 portions of cosurfactants, 0-2 part antioxidation
Agent.
3. the self-microemulsion type alimentation composition of Ubidecarenone is contained described in claim 2, it is characterised in that it is by following weight portion
Each composition is prepared, 5~10 parts of Ubidecarenone, 5~10 parts of curcumins, 20~30 parts of carrier oils, 30~45 parts of nonionic tables
Face activating agent, 2~3 portions of cationic Gemini surfactants, 12~20 portions of cosurfactants, 0-1 part antioxidants;
Preferably, it is prepared by each composition of following weight portion, 8 parts of Ubidecarenone, 7 parts of curcumins, 28 parts of carrier oils, 40
Part nonionic surfactant, 2 portions of cationic Gemini surfactants, 15 portions of cosurfactants, 1 part of antioxidation
Agent.
4. the self-microemulsion type alimentation composition of Ubidecarenone is contained described in any one of claim 1-3, it is characterised in that the coenzyme
Q10 is at least one in CoQ10, reduced coenzyme Q 10;Preferably, Ubidecarenone is microbe fermentation method preparation
Obtained by least one in Native Oxide type Ubidecarenone and reduced coenzyme Q 10;
It is optional, the carrier oil be crude vegetal or it is strong to key component solvability, after structure of modification, hydrolysis
Vegetable oil or fatty acid ester;Preferably, crude vegetal is in soybean oil, Oleum Arachidis hypogaeae semen, olive oil, Oleum Ricini, safflower oil
One or more;Vegetable oil strong to key component solvability, after structure of modification, hydrolysis or fatty acid ester are Semen Armeniacae Amarum
Oleic acid PEG-6 glyceride, isopropyl myristate, ethyl oleate, medium chain length fatty acid triglyceride, Oleic acid polyethylene glycol glycerol
One or more in ester, Masine 35-1 and polypropylene glycol caprylate;
Optional, the nonionic surfactant is selected from the dihydroxy stearic acid ester of Polyethylene oxide ten, caprylic capric Polyethylene Glycol
Glyceride, Polyoxyl 40 Hydrogenated Castor Oil, the sucrose ester of HLB value 13~16, Pluronic F68, dimension life
One or more in plain E polyethanediol succinates, tween 85, tween 80, Poloxamer 188, lecithin;
It is optional, the cosurfactant selected from glycerol, ethanol, ethylene glycol, PEG200-600, TC,
One or more in propylene carbonate and Propylene Glycol;
Optional, the antioxidant is in sodium ascorbate, natural Vitamin E and its ester derivant, Herba Rosmarini Officinalis extract
One or more.
5. the self-microemulsion type alimentation composition of Ubidecarenone is contained described in any one of claim 1-4, it is characterised in that also containing suppression
One or more in microbial inoculum, stabilizer, fluidizer and coloring agent.
6. the self-microemulsion type alimentation composition of Ubidecarenone is contained described in any one of claim 1-4, it is characterised in that preparation method
For,
Weigh each component in proportion, by remaining each component mix homogeneously outside Ubidecarenone and curcumin, add Ubidecarenone and
Curcumin, is heated to 50-65 DEG C of stirring up to whole system transparent and homogeneous, then is incubated 15-60min, is cooled to room temperature.
7. the self-microemulsion type alimentation composition of Ubidecarenone is contained described in claim 6, it is characterised in that the preparation process and system
Preservation after standby is in inert atmosphere or vacuum state;It is preferred that nitrogen or helium atmosphere atmosphere.
8. the self-microemulsion type alimentation composition of Ubidecarenone is contained described in any one of claim 1-4, it is characterised in that can be prepared into
Microcapsule, soft capsule, hard capsule, tablet, powder, pill, Emulsion or suspensoid.
9. described in a kind of any one of claim 1-4 containing Ubidecarenone self-microemulsion type alimentation composition be used for prepare prevention and/or
The purposes for the treatment of anti-parkinson drug.
10. described in a kind of any one of claim 1-4 containing Ubidecarenone self-microemulsion type alimentation composition be used for prepare prevention and/
Or the dietary supplement or the purposes of health food for the treatment of Parkinson's disease.
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| CN111201041A (en) * | 2017-07-11 | 2020-05-26 | 阿奎诺瓦股份公司 | Solubilizer with curcumin and optionally at least one other active substance |
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