JPS6027648B2 - painkillers - Google Patents
painkillersInfo
- Publication number
- JPS6027648B2 JPS6027648B2 JP58012405A JP1240583A JPS6027648B2 JP S6027648 B2 JPS6027648 B2 JP S6027648B2 JP 58012405 A JP58012405 A JP 58012405A JP 1240583 A JP1240583 A JP 1240583A JP S6027648 B2 JPS6027648 B2 JP S6027648B2
- Authority
- JP
- Japan
- Prior art keywords
- kojic acid
- asbergillus
- acid
- analgesic
- strains
- 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
Links
Classifications
-
- Y—GENERAL TAGGING OF NEW TECHNOLOGICAL DEVELOPMENTS; GENERAL TAGGING OF CROSS-SECTIONAL TECHNOLOGIES SPANNING OVER SEVERAL SECTIONS OF THE IPC; TECHNICAL SUBJECTS COVERED BY FORMER USPC CROSS-REFERENCE ART COLLECTIONS [XRACs] AND DIGESTS
- Y02—TECHNOLOGIES OR APPLICATIONS FOR MITIGATION OR ADAPTATION AGAINST CLIMATE CHANGE
- Y02A—TECHNOLOGIES FOR ADAPTATION TO CLIMATE CHANGE
- Y02A50/00—TECHNOLOGIES FOR ADAPTATION TO CLIMATE CHANGE in human health protection, e.g. against extreme weather
- Y02A50/30—Against vector-borne diseases, e.g. mosquito-borne, fly-borne, tick-borne or waterborne diseases whose impact is exacerbated by climate change
Landscapes
- Pyrane Compounds (AREA)
- Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
Description
【発明の詳細な説明】 本発明は新規な鎮痛剤に関する。[Detailed description of the invention] The present invention relates to a novel analgesic agent.
さらに詳しくは、コウジ酸を有効成分とする鎮痛剤に関
する。コウジ酸はアスベルギルス属などのコウジ菌群に
よって生育される化合物であって、近時該コウジ酸の利
用に関して種々の報告がなされている。本出願人はさき
にコウジ酸が美白効果などにすぐれているという事実を
見出し、該コウジ酸を有効成分とする色白化粧料に関す
る特許出願を行なつた。その後さらに本発明者はかかる
コウジ酸の利用について鋭意研究を重ねた結果、コウジ
酸がきわめて強力な鎮痛作用を有しているというまった
く新たな事実を見出し、本発明を完成するにいたった。More specifically, the present invention relates to an analgesic containing kojic acid as an active ingredient. Kojic acid is a compound grown by the Aspergillus group such as Asbergillus, and recently various reports have been made regarding the use of kojic acid. The applicant has previously discovered that kojic acid has excellent whitening effects, and has filed a patent application for a skin-whitening cosmetic containing kojic acid as an active ingredient. After that, the present inventor conducted extensive research into the use of such kojic acid, and as a result discovered a completely new fact that kojic acid has an extremely strong analgesic effect, leading to the completion of the present invention.
すなわち本発明はコウジ酸を有効成分とする鎮痛剤を要
旨とするものである。That is, the gist of the present invention is an analgesic containing kojic acid as an active ingredient.
コウジ酸は1907年に斎藤賢道により発見され、味噌
、醤油、酒などの発酵食品中に星味成分として多く含有
されていることはよく知られているが、かかるコウジ酸
が食品以外の分野において利用された例は袷んどなく、
本発明において初めて医薬品としての新たな用途が見出
されたことは画期的なことである。Kojic acid was discovered by Kendo Saito in 1907, and it is well known that it is contained in large amounts as a star-tasting ingredient in fermented foods such as miso, soy sauce, and sake. There are countless examples of it being used in
It is groundbreaking that a new use as a pharmaceutical has been discovered for the first time in the present invention.
本発明におけるコウジ酸は、通常コウジ酸生産能を有す
る菌株を用いるいわゆるコウジ酸発酵によって生成する
ことができる。Kojic acid in the present invention can usually be produced by so-called kojic acid fermentation using a bacterial strain capable of producing kojic acid.
かかるコウジ酸生産能を有する菌株としては、たとえば
アスベルギルス属、ベニシリウム属、ェスカリキア属、
アセトバクター属、グルコノバクター属などのコウジ酸
生産能を有する菌株があげられる。Examples of such bacterial strains having the ability to produce kojic acid include Asbergillus spp., Benicillium spp., Aescalichia spp.
Examples include strains having the ability to produce kojic acid, such as those of the genus Acetobacter and Gluconobacter.
ここにコウジ酸生産能を有するアスベルギルス属の菌株
としては、たとえばアスベルギルス・アルバス、アスベ
ルギルス・カンジダス、アスベルギルス・オリゼー、ア
スベルギルス・ニデユランス、アスベルギルス‘/fラ
シテイカス、アスベルギルス・アワモリ、アスベルギル
ス・タマリ、アスベルギルス・ニービユース、アスベル
ギルス・フラ/ゞス、アスベルギルス・ウエンチ、アス
ベルギルス・グラウカス、アスベルギルス・クラベイタ
ス、アスベルギルス・フミガタス、アスベルギルス・ジ
ガンタスなどの菌株が、またべニシリウム属の菌株とし
てはたとえばべニシリウム・ダレーなどの菌株が、また
ェスカリキア属の菌株としてはたとえばェスカリキア・
コリなどの菌株が、またアセトバクター属の菌株として
はたとえばアセトバクター・アセチ、アセトバクター・
グルコニカス、アセトバクター・キシリナムなどの菌株
が、またグルコノバクター属の菌株としてはたとえばグ
ルコノバクター・ロシウス、グルコノバクター・グルコ
ニカスなどの菌株が好適に採用されうる。これらの菌株
の培地組成としては、通常ショ糖、果糖、ブドウ糖、デ
ンプン、麦芽糖、グリセリン、マンニツト、ラムノース
、キシロース、グルコン酸、アラビノース、ジヒドロキ
シアセトン、イノシツト、ラクトース、エタノールなど
の炭素源が約5〜15%、硫酸アンモニア、ベプトン、
硝酸ソーダ、パン酵母抽出物、ビール酵母抽出物などの
チッ素源が約0.5〜1.0%、硫酸マグネシウムなど
のマグネシウム源が約0.02〜0.07%、リン酸1
水素カリ、リン酸2水素カリなどのリンおよびカリウム
源が0.1〜0.3%、その他要すれば硫酸第二鉄、塩
化第二鉄、塩化ナトリウム、塩化カルシウムなどの無機
塩が約0.001〜0.005%のものが採用されうる
。Examples of strains of the genus Asbergillus having the ability to produce kojic acid include Asbergillus albus, Asbergillus candidus, Asbergillus oryzae, Asbergillus nidulans, Asbergillus'/f rashiteicus, Asbergillus awamori, and Asbergillus. Strains such as Asbergillus tamari, Asbergillus nebieus, Asbergillus fura/su, Asbergillus wench, Asbergillus glaucus, Asbergillus clavaitus, Asbergillus fumigatus, Asbergillus digitus, and Venicillium spp. Bacterial strains of the genus include Benicillium daleley, and strains of the genus Aescalichia include, for example, Aescalichia.
strains such as Acetobacter coli, and strains of the Acetobacter genus such as Acetobacter aceti and Acetobacter aceti.
Bacterial strains such as Gluconicus and Acetobacter xylinum can be suitably employed, and strains of the genus Gluconobacter such as Gluconobacter rosius and Gluconobacter gluconicus can be suitably employed. The medium composition for these strains usually contains about 5 to 50% of carbon sources such as sucrose, fructose, glucose, starch, maltose, glycerin, mannitrate, rhamnose, xylose, gluconic acid, arabinose, dihydroxyacetone, inosyte, lactose, and ethanol. 15%, ammonia sulfate, veptone,
Nitrogen sources such as sodium nitrate, baker's yeast extract, and brewer's yeast extract are approximately 0.5 to 1.0%, magnesium sources such as magnesium sulfate are approximately 0.02 to 0.07%, and phosphoric acid 1
Phosphorus and potassium sources such as potassium hydrogen and potassium dihydrogen phosphate are 0.1 to 0.3%, and if necessary, inorganic salts such as ferric sulfate, ferric chloride, sodium chloride, and calcium chloride are approximately 0. .001 to 0.005% may be employed.
さらに要すれば、これら培地組成にポリオキシヱチレン
アルキルェーテル、ショ糖ェステルなどの界面活性剤を
約0.05〜0.2%添加し、pH3〜4に調整される
。かくしてえられる培地に前述のごとき菌株を接種し、
温度25〜35qoで約5〜10日間静直培養または振
蝿培養したのち、培養液より常法により酢酸エチルェス
テルなどの溶媒にてコウジ酸を抽出し、再結晶して針状
結晶のコウジ酸がえられる。Furthermore, if necessary, about 0.05 to 0.2% of a surfactant such as polyoxyethylene alkyl ether or sucrose ester is added to the medium composition to adjust the pH to 3 to 4. Inoculating the above-mentioned bacterial strain into the thus obtained medium,
After static culture or shaking fly culture for about 5 to 10 days at a temperature of 25 to 35 qo, kojic acid is extracted from the culture solution using a solvent such as acetic acid ethyl ester by a conventional method, and recrystallized to obtain needle-shaped crystals of kojic acid. available.
かかるコウジ酸は発酵食品中に多く含有されていること
からも明らかなごとく、きわめて毒性が低く、たとえば
マウスやラツトを用いて行なった急性毒性試験では、経
口投与、腹腔内投与、皮下投与によるLD5。はいずれ
もこれら彼検動物の雄雌に関係なく、約2.5〜3.5
夕/k9であった。また皮膚に対しても、コウジ酸は一
次刺激および累積刺激がなく、アレルギー反応もまった
く認められなかった。本発明の鎮痛剤は、コウジ酸を有
効成分と十る注射剤(注射液)、内服剤(カプセル、錠
剤、内服液など)、外用剤(軟膏など)などの形態で好
適に使用せられる。As is clear from the fact that kojic acid is contained in large amounts in fermented foods, it has extremely low toxicity. . is approximately 2.5 to 3.5, regardless of the male or female of these animals.
It was evening/K9. Furthermore, kojic acid caused no primary or cumulative irritation to the skin, and no allergic reactions were observed at all. The analgesic of the present invention is suitably used in the form of injections (injection solutions), internal preparations (capsules, tablets, oral solutions, etc.), external preparations (ointments, etc.) containing kojic acid as an active ingredient.
しかして本発明の鎮痛剤は静脈内投与、皮下投与、経口
投与などによって投与されるか、あるいは患部に直接塗
布するなどして使用される。The analgesic of the present invention may be administered intravenously, subcutaneously, orally, or applied directly to the affected area.
注射剤または内服剤として用いるぱあし、、コウジ酸の
投与量は1日あたり約1〜10夕であるのがその薬理効
果のうえで好ましい。つぎに実施例および製剤例をあげ
て本発明の鎮痛剤を説明する。In view of its pharmacological effects, the dosage of kojic acid used as an injection or oral preparation is preferably about 1 to 10 minutes per day. Next, the analgesic of the present invention will be explained with reference to Examples and Formulation Examples.
実施例
酢酸法により、8匹のマウスを用いてコウジ酸の鎮痛作
用を調べた。EXAMPLE The analgesic effect of kojic acid was investigated using eight mice by the acetic acid method.
すなわち被検動物にあうかじめコウジ酸の250の‘/
k9を皮下注射し、ついで30分ごとに1%酢酸水溶液
を腹腔内注射した。酢酸水溶液を投与後、2粉ふ間にわ
たってラィジング回数を記録した。なお対照として同じ
8匹のマウスを用い、コウジ酸に代えて水(蒸留水)を
同量投与して試験を行なった。その結果、コウジ酸の鎮
痛抑制作用はきわめて顕著であり、抑制率はloo%で
あることが判明した。That is, 250'/ of kojic acid in the test animal.
K9 was injected subcutaneously, followed by intraperitoneal injections of 1% aqueous acetic acid every 30 minutes. After administering the acetic acid aqueous solution, the number of risings was recorded over two weeks. As a control, a test was conducted using the same eight mice and administering the same amount of water (distilled water) instead of kojic acid. As a result, it was found that the analgesic suppressing effect of kojic acid was extremely significant, and the suppression rate was loo%.
この試験結果を第1表に示す。The test results are shown in Table 1.
第1表
製剤例
〔注射液(静脈内投与用)〕
‘aー 生理食塩液(日本薬局方収載品)にコウジ酸を
3.5%濃度で加えた。Table 1 Preparation Example [Injection solution (for intravenous administration)] 'a- Kojic acid was added to a physiological saline solution (product listed in the Japanese Pharmacopoeia) at a concentration of 3.5%.
{b’生理食塩液(前記と同じ)にコウジ酸およびグリ
シルリチン酸をそれぞれ2.5%および0.1%濃度で
加えた。{b' Kojic acid and glycyrrhizic acid were added to physiological saline (same as above) at concentrations of 2.5% and 0.1%, respectively.
‘a}、【b}でえた各注射液は1回の投与量20泌で
静脈内投与される。Each of the injection solutions obtained in 'a} and [b} is administered intravenously at a single dose of 20 doses.
{aー コウジ酸200の9と微結晶セルロースの適量
とを含有する錠剤を調製し、糠衣をほどこした。{a- Tablets containing 200 parts of kojic acid and an appropriate amount of microcrystalline cellulose were prepared and coated with rice bran.
{b’コウジ酸200の9、グリシルリチン酸ジカリウ
ム10の9および微結晶セルロースの適量を含有する錠
剤を調製し、糖衣をほどこした。‘a’、‘b’でえた
各錠剤は1回の投与量5〜雌菱で使用される。{b' Tablets containing appropriate amounts of 200 parts of kojic acid, 10 parts of dipotassium glycyrrhizinate and microcrystalline cellulose were prepared and sugar-coated. Each tablet of 'a' and 'b' is used in a single dose of 5 to 50 mg.
‘a} コウジ酸(微粉末状) 20タ吸
水軟膏(日本薬局方収載品) 80タコウジ酸を
まず少量の吸水軟膏と充分に練り合わせ、ついで残った
吸水軟膏を徐々に加えて均一になるまで練り合わせて軟
膏をえた。'a} Kojic acid (fine powder) 20 Ta water-absorbing ointment (listed in the Japanese Pharmacopoeia) First, thoroughly knead 80 Takojic acid with a small amount of water-absorbing ointment, then gradually add the remaining water-absorbing ointment and mix until homogeneous. I got some ointment.
(bー コウジ酸 20タグ
リシルレチン酸 80夕吸水軟膏(日
本薬局方収載品) 79.5タコウジ酸とグリシル
レチン酸とを混和し、微粉末状としたものをまず少量の
吸水軟骨と充分に練り合わせ、ついで残った吸水軟骨を
徐々に加えて均一になるまで練り合わせ、軟膏をえた。(b-Kojic acid 20 Taglycyrrhetinic acid 80 Water-absorbing ointment (listed in the Japanese Pharmacopoeia) 79.5 Takojic acid and glycyrrhetinic acid are mixed and made into a fine powder, which is first thoroughly kneaded with a small amount of water-absorbing cartilage, and then The remaining water-absorbing cartilage was gradually added and kneaded until homogeneous to obtain an ointment.
‘a}、【bーでえた各軟膏は1日4〜5回患部に塗布
される。なお前記吸水軟膏に代えて日本薬局方収載品で
ある親水軟膏や親水ワセリンなどを用いてもよい。'a}, [b-Each ointment prepared is applied to the affected area 4 to 5 times a day. In place of the water-absorbing ointment, hydrophilic ointment, hydrophilic vaseline, etc. listed in the Japanese Pharmacopoeia may be used.
Claims (1)
剤。 3 内服剤形態にある特許請求の範囲第1項記載の鎮痛
剤。 4 外用剤形態にある特許請求の範囲第1項記載の鎮痛
剤。[Claims] 1. An analgesic containing kojic acid as an active ingredient. 2. The analgesic according to claim 1, which is in the form of an injection. 3. The analgesic according to claim 1, which is in the form of an internal medicine. 4. The analgesic according to claim 1, which is in the form of an external preparation.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP58012405A JPS6027648B2 (en) | 1983-01-27 | 1983-01-27 | painkillers |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP58012405A JPS6027648B2 (en) | 1983-01-27 | 1983-01-27 | painkillers |
Related Parent Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP6372279A Division JPS5834446B2 (en) | 1979-05-22 | 1979-05-22 | anti-inflammatory agent |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| JPS58131915A JPS58131915A (en) | 1983-08-06 |
| JPS6027648B2 true JPS6027648B2 (en) | 1985-06-29 |
Family
ID=11804347
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP58012405A Expired JPS6027648B2 (en) | 1983-01-27 | 1983-01-27 | painkillers |
Country Status (1)
| Country | Link |
|---|---|
| JP (1) | JPS6027648B2 (en) |
Families Citing this family (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| KR20150034247A (en) | 2012-07-31 | 2015-04-02 | 더블유.엘.고어 앤드 어소시에이츠 게엠베하 | Envelope for a laminar structure providing adaptive thermal insulation |
-
1983
- 1983-01-27 JP JP58012405A patent/JPS6027648B2/en not_active Expired
Also Published As
| Publication number | Publication date |
|---|---|
| JPS58131915A (en) | 1983-08-06 |
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