SANITARY PRODUCT CARRYING LACTOFERRIN
20230001041 · 2023-01-05
Assignee
Inventors
- Yoshiyuki Sakuraba (Tokyo, JP)
- Yoko Nagai (Tokyo, JP)
- Tatsuo Hoshino (Kanagawa, JP)
- Megumi Ohno (Kanagawa, JP)
Cpc classification
A61K38/40
HUMAN NECESSITIES
A61K9/0036
HUMAN NECESSITIES
A61F13/2074
HUMAN NECESSITIES
A61F13/8405
HUMAN NECESSITIES
A61L15/32
HUMAN NECESSITIES
A61F13/51113
HUMAN NECESSITIES
A61L2300/252
HUMAN NECESSITIES
A61L2300/404
HUMAN NECESSITIES
International classification
Abstract
Provided is a method for preventing the disturbance of vaginal bacterial flora during the menstrual period and improving the vaginal bacterial flora. One aspect of the present invention is a sanitary product carrying lactoferrin or a composition comprising lactoferrin and an auxiliary substance. Also provided is a kit comprising a sanitary product, and lactoferrin or the composition comprising lactoferrin and an auxiliary substance.
Claims
1. A sanitary product carrying lactoferrin or a composition comprising lactoferrin and an auxiliary substance.
2. The sanitary product according to claim 1, wherein the sanitary product is a tampon or a napkin.
3. The sanitary product according to claim 1, wherein the composition is in the form of a powdery preparation, an oily liquid preparation, or an oily semi-solid preparation.
4. The sanitary product according to claim 1, characterized in that the amount of lactoferrin in the composition is 0.1 to 99.9% by weight based on the weight of the composition.
5. The sanitary product according to claim 1, characterized in that the amount of lactoferrin in the composition is 1 to 99% by weight based on the weight of the composition.
6. The sanitary product according to claim 1, characterized in that the amount of lactoferrin in the composition is 10 to 90% by weight based on the weight of the composition.
7. The sanitary product according to claim 1, characterized in that the amount of lactoferrin carried by the sanitary product is 5 to 1,000 mg/product.
8. The sanitary product according to claim 1, characterized in that the amount of lactoferrin carried by the sanitary product is 10 to 500 mg/product.
9. The sanitary product according to claim 1, characterized in that the amount of lactoferrin carried by the sanitary product is 20 to 200 mg/product.
10. A kit comprising a sanitary product, and lactoferrin or a composition comprising lactoferrin and an auxiliary substance.
11. The kit according to claim 10, wherein the sanitary product is a tampon or a napkin.
12. A method for improving the disturbance of vaginal bacterial flora during menstruation by using the sanitary product according to claim 1.
Description
BRIEF DESCRIPTION OF THE DRAWINGS
[0026]
[0027]
[0028]
[0029]
[0030]
[0031]
[0032]
[0033]
[0034]
MODE FOR CARRYING OUT THE INVENTION
[0035] As lactoferrin which is used in the present invention, any lactoferrin can be used as long as it exhibits an improving effect on the vaginal bacterial flora. Lactoferrin is a macromolecule having a molecular weight of about 80,000 and has a property of forming a chelate with two trivalent iron ions; however, the “lactoferrin” as used in the present invention includes all types including an iron ion-free type to a completely iron-ion saturated type. Further, in the present invention, any lactoferrin can be used regardless of its origin. For example, lactoferrin derived from a living body which is extracted from milk and the like of mammals such as human being and cow and genetically modified lactoferrin produced by genetic engineering or a salt thereof can be used. Commercially available lactoferrin which is purified from milk is available from vendors such as Morinaga Milk (Japan), Tatura (Australia), Tatua (New Zealand), and the like. A process for purifying lactoferrin from milk is disclosed in detail in, for example, U.S. Pat. No. 9,115,211 (issued on Aug. 25, 2015), and lactoferrin can be easily purified, basically through steps of adsorbing and desorbing lactoferrin contained in nonfat milk or whey on a cation exchange resin, followed by desalting, freeze-drying or spray drying, and the like.
[0036] In the present invention, only 1 kind of lactoferrin may be used, or 2 or more kinds of lactoferrin may be used in combination.
[0037] The sanitary product of the present invention carries lactoferrin, or a composition comprising lactoferrin and an auxiliary substance. In any case, the content of lactoferrin per 1 sanitary product can be any amount within the range in which the disturbance of vaginal bacterial flora during menstruation is speedily normalized, and can be preferably 5 to 1,000 mg/product, more preferably 10 to 500 mg/product, and particularly preferably 20 to 200 mg/product.
[0038] The amount of lactoferrin in the composition which is carried by the sanitary product of the present invention can be arbitrarily chosen within the range in which the disturbance of vaginal bacterial flora during menstruation is speedily normalized, and can be preferably 0.1 to 99.9% by weight based on the weight of the composition, more preferably 1 to 99% by weight based on the weight of the composition, and particularly preferably 10 to 90% by weight based on the weight of the composition.
[0039] As the auxiliary substance contained in the composition which is carried by the sanitary product of the present invention, an auxiliary substance in the form of powder, granule, oily solid, oily semi-solid, oily liquid, and the like can be used, and as such an auxiliary substance, ingredients or additives as exemplified below can be arbitrarily chosen and used in combination as long as the effect of the present invention is not adversely affected.
(1) Various Fats and Oils
[0040] Avocado oil, almond oil, fennel oil, perilla oil, olive oil, orange oil, orange roughy oil, sesame oil, cacao butter, chamomile oil, carrot oil, cucumber oil, beef tallow fatty acid, kukui nut oil, safflower oil, shea butter, liquid shea butter, soybean oil, camellia oil, corn oil, rape seed oil, persic oil, castor oil, cotton seed oil, peanut oil, turtle oil, mink oil, egg-yolk oil, palm oil, palm kernel oil, Japan wax, coconut oil, beef tallow, lard, squalene, squalane, pristane, hydrogenated products of these fats and oils (such as hardened oil), and the like.
(2) Waxes
[0041] Beeswax, carnauba wax, whale wax, lanolin, liquid lanolin, reduced lanolin, hard lanolin, candelilla wax, montan wax, shellac wax, rice wax, and the like.
(3) Mineral Oils
[0042] Liquid paraffine, vaseline, paraffine, ozocerite, ceresin, microcrystalline wax, and the like.
(4) Fatty Acids
[0043] Natural fatty acids such as lauric acid, myristic acid, palmitic acid, stearic acid, behenic acid, oleic acid, linolic acid, linolenic acid, docosahexaenoic acid, eicosapentaenoic acid, 12-hydroxystearic acid, undecylenic acid, tall oil, and lanolin fatty acid; and synthetic fatty acids such as isononanoic acid, caproic acid, 2-ethylbutanoic acid, isopentanoic acid, 2-methyl pentanoic acid, 2-ethyl hexanoic acid, and isopentanoic acid.
(5) Alcohols
[0044] Natural alcohols such as ethanol, isopropanol, lauryl alcohol, cetanol, stearyl alcohol, oleyl alcohol, lanolin alcohol, cholesterol, phytosterol, and phenoxyethanol; and synthetic alcohols such as 2-hexyl decanol, isostearyl alcohol, and 2-octyl dodecanol.
(6) Polyhydric Alcohols
[0045] Ethylene oxide, ethyleneglycol, diethyleneglycol, triethyleneglycol, ethyleneglycol monoethyl ether, ethyleneglycol monobutyl ether, diethyleneglycol monomethyl ether, diethyleneglycol monoethyl ether, polyethyleneglycol, propylene oxide, propyleneglycol, polypropyleneglycol, 1,3-butyleneglycol, pentylglycol, glycerol, pentaerythritol, threitol, arabitol, xylitol, ribitol, galactitol, sorbitol, mannitol, lactitol, maltitol, and the like.
(7) Esters
[0046] Isopropyl myristate, isopropyl palmitate, butyl stearate, hexyl laurate, myristyl myristate, oleyl oleate, decyl oleate, octyldodecyl myristate, hexyldexyl dimethyloctanoate, cetyl lactate, myristyl lactate, diethyl phthalate, dibutyl phthalate, lanolin acetate, ethyleneglycol monostearate, propyleneglycol monostearate, propyleneglycol dioleate, and the like.
(8) Gums, Saccharides, or High Molecular Compounds
[0047] Gum Arabic, xanthan gum, benzoin gum, dammar gum, gum guaicum, Irish moss, karaya gum, gum traganth, carob gum, quince seed, agar, casein, lactose, fructose, sucrose or esters thereof, trehalose or derivatives thereof, dextrin, gelatin, pectin, starch, carrageenan, carboxymethylchitin or chitosan, hydroxyalkyl(C2-C4)chitin or chitosan in which alkylene(C2-C4)oxide such as ethylene oxide is added, low molecular chitin or chitosan, chitosan salts, sulfated chitin or chitosan, phosphorylated chitin or chitosan, alginic acid or salts thereof, hyaluronic acid or salts thereof, chondroitin sulfate or salts thereof, heparin, ethyl cellulose, methyl cellulose, carboxymethyl cellulose, sodium carboxymethyl cellulose, carboxyethyl cellulose, sodium carboxyethyl cellulose, hydroxyethyl cellulose, hydroxypropyl cellulose, hydroxypropylmethyl cellulose, nitrocellulose, crystalline cellulose, polyethylene, polyvinyl alcohol, polyvinyl methyl ether, polyvinylpyrrolidone, polyvinyl methacrylate, polyacrylates, polyalkylene oxide such as polyethylene oxide and polypropylene oxide or crosslinked polymers thereof, carboxyvinyl polymer, polyethyleneimine, silicone, polysiloxane, and the like.
[0048] As described above, while the composition which is carried by the sanitary product of the present invention can comprise lactoferrin and an auxiliary substance, various solvents, preservatives, solubilizing agents, stabilizers and the like which are usually used in pharmaceuticals or cosmetics can be further arbitrarily added as necessary in an amount within the range in which the disturbance of vaginal bacterial flora during menstruation is speedily normalized. Further, another pharmaceutical agent can be added as necessary.
[0049] The composition which is carried by the sanitary product of the present invention is preferably in a form which is convenient for intravaginal administration, for example, a powdery preparation, an oily liquid preparation, or an oily semi-solid preparation, and can be prepared by, e.g., mixing or stirring the above described lactoferrin and an auxiliary substance. Since lactoferrin is unstable at a high temperature or a high humidity, the composition is preferably prepared under a dry condition.
[0050] The sanitary product of the present invention can be a sanitary product having an arbitrary form which enables the delivery of lactoferrin into the vagina, and a tampon and a napkin can be exemplified. In the case where the sanitary product of the present invention is a tampon or a napkin, the content of lactoferrin can be an arbitrary amount within the range in which the disturbance of vaginal bacterial flora during menstruation is speedily normalized, and can be preferably 5 to 1,000 mg/product, more preferably 10 to 500 mg/product, and particularly preferably 20 to 200 mg/product.
[0051] The sanitary product of the present invention can be prepared by making a sanitary product such as a tampon or a napkin to carry lactoferrin or a composition comprising lactoferrin and an auxiliary substance. As a process for carrying, the following processes can be exemplified. The following processes are for explanation of the present invention, and do not limit the present invention at all.
[0052] 1. Lactoferrin alone, for example, 0.2 g of lactoferrin is airtightly included between thin layers of an absorber part of a sanitary product during a step of forming the sanitary product. (
[0053] 2. A composition comprising lactoferrin and an auxiliary substance, for example, 0.1 g of a powdery preparation comprising 90% by weight of lactoferrin is airtightly included between thin layers of an absorber part of a sanitary product during a step of forming the sanitary product. (
[0054] 3. A composition comprising lactoferrin and an auxiliary substance, for example, 0.5 g of an oily liquid preparation comprising 20% by weight of lactoferrin is water-tightly included between thin layers of an absorber part of a sanitary product during a step of forming the sanitary product. (
[0055] 4. A composition comprising lactoferrin and an auxiliary substance, for example, 1 g of an oily liquid preparation comprising 10% by weight of lactoferrin is impregnated by dropping or spraying it onto an absorber part of a formed sanitary product. (
[0056] 5. A composition comprising lactoferrin and an auxiliary substance, for example, 0.2 g of an oily liquid preparation comprising 20% by weight of lactoferrin is impregnated into an absorber immediately before use of the sanitary product. (
[0057] 6. A composition comprising lactoferrin and an auxiliary substance, for example, 0.4 g of an oily semi-solid preparation comprising 10% by weight of lactoferrin is applied to an absorber immediately before use of the sanitary product. (
[0058] 7. A composition comprising lactoferrin and an auxiliary substance, for example, 0.2 g of an oily liquid preparation or an oily semi-solid preparation comprising 20% by weight of lactoferrin is injected into a gap between an applicator which is an assisting tool for insertion of a sanitary product and an absorber immediately before use of the sanitary product. (
[0059] The sanitary product of the present invention which carries lactoferrin or a composition comprising lactoferrin and an auxiliary substance can be used depending on the condition of menstruation. For example, 4 to 5 tampons per day or 7 to 18 napkins per day can be used throughout the menstrual period.
EXAMPLES
[0060] Hereinafter, the present invention will be more specifically described by way of Examples.
Example 1
[0061] <Composition Comprising Lactoferrin and an Auxiliary Substance>
[0062] Various compositions that were carried by the sanitary product of the present invention were prepared. The formulation examples are shown below, but since the compositions were prepared by a process of mixing and stirring, only the amounts are shown.
[0063] Appropriate amounts of lactoferrin (produced by Tatura Co., Australia) and an auxiliary substance(s) (various oils and fats, waxes, mineral oils, fatty acids, alcohols, polyhydric alcohols, esters, gums, saccharides, or high molecular compounds, and the like) were mixed. Lactoferrin was in the range of 0.1 to 90% by weight. Specific formulation examples are shown as follows.
(Formulation Example 1) Oily Semi-Solid Preparation
[0064]
TABLE-US-00001 Lactoferrin 10% Liquid paraffin 75% Sodium carboxymethyl cellulose 8% Polyethylene 6% Pectin 1%
(Formulation Example 2) Oily Semi-Solid Preparation
[0065]
TABLE-US-00002 Lactoferrin 40% Vaseline 60%
(Formulation Example 3) Oily Liquid Preparation
[0066]
TABLE-US-00003 Lactoferrin 0.1% Liquid paraffine 99.9%
(Formulation Example 4) Oily Liquid Preparation
[0067]
TABLE-US-00004 Lactoferrin 20% Butyleneglycol 8% Glycerol 72%
(Formulation Example 5) Oily Liquid Preparation
[0068]
TABLE-US-00005 Lactoferrin 30% Squalane 70%
(Formulation Example 6) Powdery Preparation
[0069]
TABLE-US-00006 Lactoferrin 80% Hydroxypropylmethyl cellulose 20%
(Formulation Example 7) Powdery Preparation
[0070]
TABLE-US-00007 Lactoferrin 90% Xanthan gum 10%
Example 2
[0071] <Carrying of Lactoferrin or a Composition Comprising Lactoferrin and an Auxiliary Substance on a Sanitary Product>
(Lactoferrin)
[0072] Lactoferrin (Tatura Co., Australia), 0.1 g, was added between the thin layers of an absorber part of a tampon during a step of forming the tampon, then the absorber part was formed into a cylindrical shape and compressed, thus obtaining the tampon of the present invention. (
(Lactoferrin)
[0073] Lactoferrin (Tatura Co., Australia), 0.2 g, was added between thin layers of an absorber part of a napkin during a step of forming the napkin, then the napkin was formed to obtain the napkin of the present invention. (
(Oily Liquid Preparation)
[0074] Lactoferrin (Tatura Co., Australia), 20 g, was added to 80 g of squalane, followed by stirring to prepare a composition. The composition, 0.5 g, was dropped or sprayed onto an absorber part of a tampon which had been formed, thus obtaining the tampon of the present invention. (
(Oily Liquid Preparation)
[0075] Lactoferrin (Tatura Co., Australia), 10 g, was added to 90 g of liquid paraffin, followed by stirring to prepare a composition. The composition, 2 g, was dropped or sprayed onto an absorber part of a napkin which had been formed, thus obtaining the napkin of the present invention. (
(Oily Semi-Solid Preparation)
[0076] 10 g of lactoferrin (Tatura Co., Australia), 8 g of cellulose gum, 6 g of polyethylene, and 1 g of pectin were added to 75 g of liquid paraffin, followed by mixing to prepare a composition. The composition, 0.38 g, was injected into a gap between an applicator and an absorber of a tampon (an applicator was attached) immediately before use of the tampon to obtain the tampon of the present invention. (
Example 3
[0077] Clinical Study
[0078] In the clinical study, for 9 weeks including 3 menstrual cycles in subjects who had agreed with the research, a method in which the vaginal bacterial flora was compared before and after the use of lactoferrin-injected tampon within the same menstrual cycle was employed.
[0079] The lactoferrin-injected tampon was prepared by injecting 0.38 g of the oily semi-solid preparation of Formulation example 1 comprising 10% by weight of lactoferrin (Tatura Co., Australia) (corresponding to 38 mg of lactoferrin) into the gap between the applicator and the absorber of Sofy Soft Tampon Regular (Unicharm Co.).
[0080] The subjects started the use of the lactoferrin-injected tampons from the 2nd or 3rd menstrual cycle, and changed the tampon every 4 hours.
[0081] The sampling method of the specimens was such that each subject collected the specimens by using the swab brushs of an intravaginal flora DNA sampling kit (product name: “OMNIgene VAGINAL” (DNA Genotek Inc., Canada)) by herself. The collected vaginal mucus was transferred into 1 ml of a preservation liquid (product name: “MMB collection tube” (DNA Genotek Inc., Canada)) for inactivation and stabilization of the bacteria and stored at an ordinary temperature.
[0082] Subject 1 avoided the intake of lactic acid bacteria-containing foods, fermented foods and the like to the utmost from the start of the first menstruation which was before the intervention, and the specimen was collected on the 7th day after the start of menstruation. After that, Subject 1 used the lactoferrin-injected tampons during the 2nd menstruation cycle and the 3rd menstruation cycle, and the respective specimen was collected on the 7th day after the start of menstruation. As a result, by using the lactoferrin-injected tampons, an increase in the vaginal Lactobacillus % was found in the 3rd menstrual cycle (Table 1).
TABLE-US-00008 TABLE 1 Vaginal Lactobacillus % in Subject 1 Whether the tampons were used Vaginal in the latest menstruation or not Lactobacillus % 7th day of the Not used 35.7% 1st cycle 7th day of the Used 37.7% 2nd cycle 7th day of the Used 61.2% 3rd cycle
[0083] In Subject 2, the long-term effect was further investigated. Subject 2 used the lactoferrin-injected tampons from the 1st cycle of menstruation, and the specimens were collected for 3 cycles on the 7th day after the start of menstruation. As a result, by using the lactoferrin-injected tampons for 3 cycles, an increase in the vaginal Lactobacillus % was found (Table 2).
TABLE-US-00009 TABLE 2 Vaginal Lactobacillus % in Subject 2 Whether the tampons were used Vaginal in the latest menstruation or not Lactobacillus % 7th day of the Used 81.5% 1st cycle 7th day of the Used 95.7% 2nd cycle 7th day of the Used 98.1% 3rd cycle
[0084] In Example 3, the vaginal bacterial flora analysis was carried out as follows.
[0085] The vaginal mucus which had been collected by the subject herself was transferred into 1 ml of a preservation liquid (product name: “MMB collection tube” (DNA Genotek Inc., Canada)) for inactivation and stabilization of the bacteria. In order to extract the bacterial genome DNA, proteinase K and lysozyme were added to the preservation liquid to dissolve the bacteria. The genome DNA was extracted by using a DNA extraction kit (product name: “Agencourt Genfind v2 Blood & Serum DNA Isolation Kit” (Beckman Coulter Inc. USA)). The concentration of the extracted DNA was determined by using a kit of the product name “Qubit dsDNA HS Assay Kit” (ThermoFisher Scientific K.K.)
[0086] Bacterial flora analysis was carried out by a 16S amplicon sequence method using a next generation sequencer. Based on the protocol of “Earth Microbiome Project” (Non-Patent Document 6), the bacterial DNA was amplified by using primers which had been ligated with a sequence for amplifying the V4 region of 16S rRNA gene and the Illumina Nextera XT adaptor sequence (Non-Patent Document 7). A mixture containing 25 ng/μL of DNA, each 200 μmol/L of deoxyribonucleotide triphosphates, 400 nmol/L of each primer, 2.5 U of product name: “FastStart Hifi polymerase”, 20 mg/mL of BSA (Sigma), 0.5 mol/L of betaine (Sigma), and MgCl.sub.2-containing buffer (Roche) was prepared for PCR. The PCR was carried out by using a thermal cycler (product name: “SimpliAmp Thermal Cycler” (Thermo Fisher)) in which degeneration at 94° C. for 2 minutes, followed by 30 cycles of 94° C. for 20 seconds, 50° C. for 30 seconds, and 72° C. for 1 minute, and finally a reaction at 72° C. for 5 minutes were carried out. The PCR product was purified with a product named “A gencourt AMPure XP” (Beckman Coulter Inc, USA). Then, a library was prepared by using a kit of the product name “Nextera XT Index kit” (Illumina Inc., USA) based on “llumina 16S Metagenomic Sequencing Library Preparation protocol” (https://support.illumina.com/documents/documentation/chemistry_documentation/16s/16s-metagenomic-library-prep-guide-15044223-b.pdf). The sequence of the prepared library was determined with pair end sequence of 2×200-bp by using a kit of the product name “MiSeq Reagent Kit v3” (Illumina K.K.). For the data analysis, the quality check of whole sequence was carried out by using “fastqQC” (https://www.bioinformatics.babraham.ac.uk/projects/fastqc/), and the bacteria were identified by using “USEARCH” (https://www.drive5.com/usearch/) and “QIIME” (http://qiime.org/) at their genus levels.
[0087] The present application is based on the Japanese Patent Application No. 2020-013871 filed on Jan. 30, 2020, and the subject matters described in the specification and the scope of the claims for patent of Japanese Patent Application No. 2020-013871 are all incorporated in this specification.