JP2664699B2 - External preparation - Google Patents
External preparationInfo
- Publication number
- JP2664699B2 JP2664699B2 JP63024536A JP2453688A JP2664699B2 JP 2664699 B2 JP2664699 B2 JP 2664699B2 JP 63024536 A JP63024536 A JP 63024536A JP 2453688 A JP2453688 A JP 2453688A JP 2664699 B2 JP2664699 B2 JP 2664699B2
- Authority
- JP
- Japan
- Prior art keywords
- external preparation
- saponin
- active ingredient
- kojic acid
- water
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
- Expired - Lifetime
Links
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- Medicinal Preparation (AREA)
Description
【発明の詳細な説明】 [産業上の利用分野] 本発明は、経皮吸収促進性が高められた親水性の外用
剤に関するものであり、より詳しくは、コウジ酸、胎盤
エキス、ビタミンC、ハイドロキノンまたはそれらの誘
導体からなるメラニン生成抑制活性成分を含む親水性外
用剤における経皮吸収促進剤として、特定の植物から抽
出精製されたサポニンを配合した親水性外用剤に関す
る。DETAILED DESCRIPTION OF THE INVENTION [Industrial Application Field] The present invention relates to a hydrophilic external preparation having enhanced percutaneous absorption promotion properties, and more specifically, kojic acid, placental extract, vitamin C, The present invention relates to a hydrophilic external preparation containing a saponin extracted and purified from a specific plant as a percutaneous absorption enhancer in a hydrophilic external preparation containing a melanin production-inhibiting active ingredient composed of hydroquinone or a derivative thereof.
[従来の技術および課題] 医薬、医薬部外品、化粧料などの外用剤はいずれも、
薬理活性を有する有効成分が皮膚を透過して体内組織に
吸収されて初めて有効に作用するものであり、その効果
は有効成分の皮膚透過率によって大きく左右される。し
かし、皮膚組織は本来体内からの排出作用を主として有
しており、体外からの吸収に対しては抵抗性をもつもの
である。したがって、有効成分をいかに効率よく経皮吸
収させるかが外用剤の大きな課題である。[Conventional technology and problems] All external preparations such as pharmaceuticals, quasi-drugs, and cosmetics
An effective ingredient having a pharmacological activity is effective only when it penetrates the skin and is absorbed into a body tissue, and its effect largely depends on the skin permeability of the active ingredient. However, the skin tissue has an action of excreting mainly from the body, and is resistant to absorption from outside the body. Therefore, how to efficiently absorb the active ingredient through the skin is a major issue for external preparations.
そうした課題に対し、有効成分の経皮吸収性を高める
ために種々の検討が行なわれているが、そのうちの1つ
に有効成分の経皮吸収を補助・促進させる経皮吸収促進
剤の開発がある。To address such issues, various studies have been conducted to enhance the transdermal absorption of the active ingredient. One of them is the development of a transdermal absorption enhancer that assists and promotes the transdermal absorption of the active ingredient. is there.
現在知られている経皮吸収促進剤としてはジメチルス
ルホキシド(DMSO)、尿素、アルコール類、オレイン
酸、ピロリドン誘導体およびエイゾン(Azone)などが
知られているが、高濃度に配合しないとその効果が奏さ
れなかったり、皮膚刺激があるなど安全性に問題があ
り、未だ充分なものとはいえない。また、これらの経皮
吸収促進剤は数多くのスクリーニングにより経験的にし
か見出せないものであり、その開発には多大な労力を要
している。Currently known dermal absorption enhancers include dimethyl sulfoxide (DMSO), urea, alcohols, oleic acid, pyrrolidone derivatives, and Azone (Azone). There is a problem in safety such as not being played or skin irritation, and it is not yet sufficient. Further, these percutaneous absorption enhancers can only be found empirically by numerous screenings, and their development requires a great deal of effort.
[課題を解決するための手段] 本発明は、特定の植物から抽出精製されたサポニン
が、コウジ酸、胎盤エキス、ビタミンC、アルブチンま
たはそれらの誘導体からなるメラニン生成抑制活性成分
の経皮吸収性を著しく促進するという驚くべき発見に基
づくものである。[Means for Solving the Problems] The present invention relates to a transdermal absorbability of a melanin production-inhibiting active ingredient in which saponin extracted and purified from a specific plant is composed of kojic acid, placental extract, vitamin C, arbutin or a derivative thereof. Based on the surprising finding that it significantly promotes
すなわち、本発明によれば、 コウジ酸、胎盤エキス、ビタミンC、ハイドロキノン
またはそれらの誘導体からなる群より選ばれた1種また
は2種以上のメラニン生成抑制活性成分と、薬用ニンジ
ン、ヘチマ、大豆、キラヤ、カンゾウおよびキキョウか
らなる群より選ばれた植物の水または水−エタノール抽
出物を精製し得られたサポニンとを含有する親水性外用
剤が提供される。That is, according to the present invention, kojic acid, placenta extract, vitamin C, hydroquinone or a derivative thereof, one or more melanin production-inhibiting active ingredients selected from the group consisting of medicinal carrot, loofah, soybean, The present invention provides a hydrophilic external preparation containing saponin obtained by purifying a water or water-ethanol extract of a plant selected from the group consisting of Kiraya, liquorice and fennel.
[作用] 本発明において経皮吸収促進剤として用いられるサポ
ニンは、薬用ニンジン、ヘチマ、大豆、キラヤ、カンゾ
ウおよびキキョウからなる群より選ばれた植物の水また
はエタノール抽出物を精製し得られるものであり、なか
でも、薬用ニンジンの水または水−エタノール抽出物の
精製物が好ましく用いられる。これらの抽出物は、古
来、滋養強壮剤、消炎剤、血行促進剤、肉芽形成抑制
剤、細胞賦活剤、疲労、強心・強精剤、鎮痛剤として漢
方で使用されている。[Action] Saponin used as a transdermal absorption enhancer in the present invention is obtained by purifying a water or ethanol extract of a plant selected from the group consisting of medicinal carrot, loofah, soybean, quilla, liquorice and fennel. In particular, a purified water or water-ethanol extract of medicinal carrot is preferably used. These extracts have been used in Chinese medicine since ancient times as nutrient tonics, anti-inflammatory agents, blood circulation promoters, granulation formation inhibitors, cell activators, fatigue, inotropic / strong semen and analgesics.
また、本発明において用いられるメラニン生成抑制活
性成分は、コウジ酸、胎盤エキス、ビタミンC、ハイド
ロキノンまたはそれらの誘導体であり、後述する実施例
においては、その代表的なメラニン生成抑制活性成分で
ある、コウジ酸およびハイドロキノンの誘導体として知
られているアルブチンについての経皮吸収特性を開示し
ている。In addition, the melanin production-inhibiting active ingredient used in the present invention is kojic acid, placenta extract, vitamin C, hydroquinone or a derivative thereof, and in Examples described later, it is a typical melanin production-inhibiting active ingredient. It discloses the transdermal absorption properties of arbutin, which is known as a derivative of kojic acid and hydroquinone.
本発明の外用剤の剤形は特に限定されず、剤形として
はたとえば化粧水、乳液、クリーム、パックなどの化粧
料のほか、乳剤、リニメント剤、軟膏剤、パップ剤、ロ
ーション剤、育毛・養毛剤などの医薬、医薬部外品など
の種々の外用形態の製剤があげられる。本発明の経皮吸
収促進剤の配合割合は、メラニン生成抑制活性成分の種
類や量、剤形、pH、使用方法などにより異なるが、通
常、有効成分1gに対して0.01〜10g、好ましくは0.1〜3.
0gである。また、外用剤自体は通常の処方が採用され
る。The dosage form of the external preparation of the present invention is not particularly limited. Examples of the dosage form include cosmetics such as lotion, emulsion, cream, pack, emulsion, liniment, ointment, cataplasm, lotion, hair growth, Examples include various external preparations such as a medicament such as a hair restorer and a quasi-drug. The blending ratio of the transdermal absorption enhancer of the present invention varies depending on the type and amount of the melanin production-inhibiting active ingredient, the dosage form, the pH, the method of use, etc., but is usually 0.01 to 10 g, preferably 0.1 to 1 g of the active ingredient. ~ 3.
It is 0g. The external preparation itself is usually formulated.
サポニンは皮膚に対して安全であり、本発明の親水性
外用剤に配合することに何ら問題はない。Saponin is safe for the skin and there is no problem in blending it with the hydrophilic external preparation of the present invention.
実施例 つぎに本発明の親水性の外用剤を製造例、試験例、処
方例をあげて説明するが、本発明はそれらのみに限定さ
れるものではない。EXAMPLES Next, the hydrophilic external preparation of the present invention will be described with reference to Production Examples, Test Examples, and Formulation Examples, but the present invention is not limited thereto.
製造例 [ニンジンサポニン] ニンジン(局方)10kgを細切し、これに30容量%エタ
ノール30を加え、2日間室温に放置したのち布ごしし
た。残渣に30容量%エタノール30を加え、同様に操作
した。これを計3回繰返し、ロ液を合せ減圧濃縮し、褐
色のエキス約4kgをえた。Production Example [Carrot saponin] 10 kg of carrot (pharmacopoeia) was finely chopped, 30% by volume of ethanol 30 was added thereto, left at room temperature for 2 days, and then clothed. To the residue, 30% by volume of ethanol 30 was added, and the same operation was performed. This was repeated three times in total, and the combined solutions were concentrated and concentrated under reduced pressure to obtain about 4 kg of a brown extract.
これに水飽和n−ブタノール12を加え溶解したの
ち、さらに水10を加え、よく振とうし、静置後n−ブ
タノール層を分取した。n−ブタノールを減圧留去し、
粗サポニン約300gをえた(粗サポニン含量85.0〜95.0
%)。After water-saturated n-butanol 12 was added and dissolved therein, water 10 was further added, and the mixture was shaken well. After standing, the n-butanol layer was separated. n-Butanol was distilled off under reduced pressure,
About 300 g of crude saponin (crude saponin content 85.0-95.0
%).
なお、ヘチマ(全草)、大豆(胚芽)、キラヤ(樹
皮)、カンゾウ(根)、キキョウ(全草)などからも同
様にしてサポニンを抽出することができた。In addition, saponin could be similarly extracted from loofah (whole plant), soybean (germ), quilla (bark), liquorice (root), kikyo (whole plant) and the like.
試験例1 コウジ酸の1%水溶液(エタノール5%含有)にニン
ジンサポニン(トキワ漢方製薬(株)製)を濃度が0.02
%、0.2%および1.0%となるように添加して試料を調製
し、つぎのin vitro透過試験を行なった。結果を第1表
に示す。Test Example 1 The concentration of carrot saponin (manufactured by Tokiwa Kampo Pharmaceutical Co., Ltd.) in a 1% aqueous solution of kojic acid (containing 5% ethanol) was 0.02.
%, 0.2% and 1.0% to prepare samples, and the following in vitro permeation test was performed. The results are shown in Table 1.
(試験方法) フランツ型セル(クラウンガラス社製のFDC−400)に
7〜8週令(体重約30g)の雄性ヘアレスマウスから採
取した背部皮膚をセットし、前記試料(100ml)をドナ
ー側に入れ、pH7.4リン酸緩衝液と生理食塩水を等量混
合した液に、防腐剤として硫酸カナマイシンを20μg/ml
添加したものをレセプター液とし、レセプター液中に透
過してくるコウジ酸の量を経時的にHPLC法により定量す
る。各濃度につき3回試験を行ない。その平均値をデー
タとした。(Test method) The back skin collected from a male hairless mouse of 7 to 8 weeks of age (weight about 30 g) was set in a Franz cell (FDC-400 manufactured by Crown Glass), and the sample (100 ml) was placed on the donor side. Put, pH 7.4 phosphate buffer and a mixture of physiological saline in equal amounts, kanamycin sulfate as a preservative 20μg / ml
The added solution is used as a receptor solution, and the amount of kojic acid permeating into the receptor solution is quantified over time by the HPLC method. Test three times for each concentration. The average value was used as data.
第1表から明らかなように、サポニンの濃度が増加す
るにしたがってコウジ酸の透過量も増大する。サポニン
濃度0.02%(試料3)ですでに促進作用が認められ、0.
2%(試料2)では24時間後に試料中のコウジ酸の約60
%が透過した。また1.0%(試料1)では10時間後にす
でにコントロール(試料4)の約13倍の透過量となっ
た。また、コウジ酸の皮膚透過のラグタイムはコントロ
ール(試料4)では8時間であるのに対し、0.2%(試
料2)で4時間、1.0%(試料1)では3時間と短く、
即効性が向上することもわかる。 As is clear from Table 1, the permeation amount of kojic acid increases as the concentration of saponin increases. A promoting effect was already observed at a saponin concentration of 0.02% (sample 3),
At 2% (sample 2), after about 24 hours, about 60% of kojic acid
% Transmitted. At 1.0% (sample 1), the permeation amount was about 13 times that of the control (sample 4) after 10 hours. The lag time of kojic acid permeation through the skin was 8 hours in the control (sample 4), 4 hours in 0.2% (sample 2) and 3 hours in 1.0% (sample 1).
It can also be seen that the immediate effect is improved.
試験例2 ハイドロキノンの誘導体であるアルブチンの1%水溶
液にニンジンサポニン(トキワ漢方製薬(株)製)を濃
度が0.1%、1.0%および3.0%となるように添加して調
整した試料を用いたほかは試験例1と同様にして経皮吸
収促進作用を調べた。Test Example 2 In addition to using a sample prepared by adding carrot saponin (manufactured by Tokiwa Kampo Pharmaceutical Co., Ltd.) to a 1% aqueous solution of arbutin, which is a derivative of hydroquinone, so that the concentrations would be 0.1%, 1.0%, and 3.0%. In the same manner as in Test Example 1, the effect of promoting percutaneous absorption was examined.
結果を第2表に示す。 The results are shown in Table 2.
処方例1(軟膏剤) A モノステアリン酸ソルビタン 1.5% 自己乳化型モノステアリン酸グリセリン 3.5% セタノール 2.0% サラシミツロウ 3.0% ラノリン 5.0% 流動パラフィン 30.0% 防腐剤 適量 B プロピレングリコール 5.0% 精製水 〜100 % C 胎盤エキス 3.0% D キラヤサポニン 0.5% (製法) Aに属する成分を加熱溶解する(油相)。別に、Bに
属する成分を加熱溶解する(水相)。油相に水相を添加
して撹拌乳化後、冷却する。途中、C、Dを加え軟膏剤
をえた。 Formulation Example 1 (Ointment) A Sorbitan monostearate 1.5% Self-emulsifying glyceryl monostearate 3.5% Cetanol 2.0% Salami beeswax 3.0% Lanolin 5.0% Liquid paraffin 30.0% Preservatives proper amount B Propylene glycol 5.0% Purified water -100% C Placental extract 3.0% D Kirayasaponin 0.5% (Preparation method) Heat and dissolve the components belonging to A (oil phase). Separately, the components belonging to B are dissolved by heating (aqueous phase). The aqueous phase is added to the oil phase, and the mixture is emulsified with stirring and then cooled. On the way, C and D were added to obtain an ointment.
処方例2(クリーム) A モノステアリン酸ソルビタン 2.0% 親油型モノステアリン酸グリセリン 3.0% ステアリン酸 5.0% ベヘニルアルコール 5.0% スクワラン 5.0% ホホバ油 1.0% 流動パラフィン 12.0% B 1,3ブチレングリコール 5.0% 精製水 〜100 % C コウジ酸 1.0% ニンジンサポニン 0.2% 精製水 8.0% (製法) Aに属する成分を加熱溶解する(油相)。Bに属する
成分を加熱溶解する(水相)。油相に水相を添加して乳
化する。撹拌冷却後、Cを添加してクリームをえた。Formulation Example 2 (Cream) A Sorbitan monostearate 2.0% Lipophilic glyceryl monostearate 3.0% Stearic acid 5.0% Behenyl alcohol 5.0% Squalane 5.0% Jojoba oil 1.0% Liquid paraffin 12.0% B 1,3 butylene glycol 5.0% Purified water -100% C Kojic acid 1.0% Carrot saponin 0.2% Purified water 8.0% (Production method) Heat and dissolve components belonging to A (oil phase). The components belonging to B are dissolved by heating (aqueous phase). The aqueous phase is added to the oil phase and emulsified. After cooling with stirring, C was added to obtain a cream.
処方例3(パック剤)(クリーム状パック) A POE(20)ベヘニルエーテル 1.0% テトラオレイン酸POE(40)ソルビット 2.0% 親油型モノステアリン酸グリセリン 2.0% ベヘニルアルコール 3.0% スクワラン 25.0% オクタン酸グリセリン 10.0% 防腐剤 適量 B 1.3−ブチレングリコール 5.0% 精製水 〜100 % C アスコルビン酸 1.0% ヘチマサポニン 1.0% 精製水 8.0% (製法) Aに属する成分を加熱溶解する(油相)。別に、Bに
属する成分を加熱溶解する(水相)。油相に水相を添加
して撹拌乳化後、冷却途中にCを加えクリーム状パック
をえた。Formulation Example 3 (pack) (cream pack) A POE (20) behenyl ether 1.0% POE (40) sorbitol tetraoleate 2.0% lipophilic glyceryl monostearate 2.0% behenyl alcohol 3.0% squalane 25.0% glycerin octoate 10.0 % Preservatives Appropriate amount B 1.3-butylene glycol 5.0% Purified water -100% C Ascorbic acid 1.0% Hetimasaponin 1.0% Purified water 8.0% (Production method) Heat and dissolve components belonging to A (oil phase). Separately, the components belonging to B are dissolved by heating (aqueous phase). After the aqueous phase was added to the oil phase and stirred and emulsified, C was added during cooling to obtain a creamy pack.
処方例4(乳剤) A モノステアリン酸POE(20)ソルビタン 2.0% 親油型モノステアリン酸グリセリン 1.5% ステアリン酸 5.0% スクワラン 15.0% アボカド油 3.0% 流動パラフィン 5.0% B 1,3−ブチレングリコール 5.0% グリセリン 5.0% 精製水 〜100 % C アルブチン 1.0% カンゾウサポニン 0.5% エタノール 5.0% (製法) Aに属する成分を加熱溶解する(油相)。Bに属する
成分を加熱溶解する(水相)。油相を添加し乳化する。
撹拌冷却後、Cを添加して乳液をえた。Formulation Example 4 (emulsion) A POE (20) sorbitan monostearate 2.0% Lipophilic glyceryl monostearate 1.5% Stearic acid 5.0% Squalane 15.0% Avocado oil 3.0% Liquid paraffin 5.0% B 1,3-butylene glycol 5.0% Glycerin 5.0% Purified water -100% C Arbutin 1.0% Licorice saponin 0.5% Ethanol 5.0% (Production method) Heat and dissolve components belonging to A (oil phase). The components belonging to B are dissolved by heating (aqueous phase). Add oil phase and emulsify.
After cooling with stirring, C was added to obtain an emulsion.
[発明の効果] 本発明の親水性の外用剤は薬理活性成分の経皮吸収性
を大きく促進し、メラニン生成抑制活性成分の薬理作用
を増大させ、さらに即効性をも向上させる効果を奏す
る。[Effects of the Invention] The hydrophilic external preparation of the present invention greatly enhances the percutaneous absorption of a pharmacologically active ingredient, increases the pharmacological action of a melanin production-inhibiting active ingredient, and further improves the immediate effect.
Claims (1)
ドロキノンまたはそれらの誘導体からなる群より選ばれ
た1種または2種以上のメラニン生成抑制活性成分と、
薬用ニンジン、ヘチマ、大豆、キラヤ、カンゾウおよび
キキョウからなる群より選ばれた植物の水または水−エ
タノール抽出物を精製し得られたサポニンとを含有する
親水性外用剤。(1) one or more melanin production-inhibiting active ingredients selected from the group consisting of kojic acid, placental extract, vitamin C, hydroquinone or a derivative thereof;
A hydrophilic external preparation containing saponin obtained by purifying a water or water-ethanol extract of a plant selected from the group consisting of medicinal carrot, loofah, soybean, quilla, liquorice and fennel.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP63024536A JP2664699B2 (en) | 1988-02-04 | 1988-02-04 | External preparation |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP63024536A JP2664699B2 (en) | 1988-02-04 | 1988-02-04 | External preparation |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| JPH01199908A JPH01199908A (en) | 1989-08-11 |
| JP2664699B2 true JP2664699B2 (en) | 1997-10-15 |
Family
ID=12140875
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP63024536A Expired - Lifetime JP2664699B2 (en) | 1988-02-04 | 1988-02-04 | External preparation |
Country Status (1)
| Country | Link |
|---|---|
| JP (1) | JP2664699B2 (en) |
Families Citing this family (4)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| KR100197543B1 (en) * | 1990-09-14 | 1999-06-15 | 오쓰까 아끼히꼬 | Detergent composition |
| JP5475419B2 (en) * | 2009-12-03 | 2014-04-16 | 花王株式会社 | Redness unevenness improver |
| JP2012031132A (en) * | 2010-07-02 | 2012-02-16 | Fancl Corp | Composition for ameliorating fatigue |
| CN114651075A (en) * | 2019-11-11 | 2022-06-21 | 马福特克有限公司 | Annealing furnace, method for constructing annealing furnace, and prefabricated structure |
Family Cites Families (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| JPS5846016A (en) * | 1981-09-10 | 1983-03-17 | Nitto Electric Ind Co Ltd | External preparation |
-
1988
- 1988-02-04 JP JP63024536A patent/JP2664699B2/en not_active Expired - Lifetime
Non-Patent Citations (1)
| Title |
|---|
| 刈込達夫著「世界の民間薬」(株)廣川書店、昭和48−1−15、初版、P96 |
Also Published As
| Publication number | Publication date |
|---|---|
| JPH01199908A (en) | 1989-08-11 |
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