JPS6045614B2 - Diyne polyprenyl alcohol and antihypertensive agents containing it - Google Patents
Diyne polyprenyl alcohol and antihypertensive agents containing itInfo
- Publication number
- JPS6045614B2 JPS6045614B2 JP9496477A JP9496477A JPS6045614B2 JP S6045614 B2 JPS6045614 B2 JP S6045614B2 JP 9496477 A JP9496477 A JP 9496477A JP 9496477 A JP9496477 A JP 9496477A JP S6045614 B2 JPS6045614 B2 JP S6045614B2
- Authority
- JP
- Japan
- Prior art keywords
- diyne
- compound
- administration
- blood pressure
- polyprenyl alcohol
- 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.)
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- Acyclic And Carbocyclic Compounds In Medicinal Compositions (AREA)
- Organic Low-Molecular-Weight Compounds And Preparation Thereof (AREA)
Description
【発明の詳細な説明】 本発明は次の一般式(I) 〔式中Aは 。[Detailed description of the invention] The present invention relates to the following general formula (I) [In the formula, A is .
,,,,,上 ,,, 鎖を、nは整数3または4を表
わす。で表わされるジイン系ポリプレニルアルコールお
よびそれを含有する血圧降下剤に関するものである。, , , , upper , , , chain, and n represents an integer 3 or 4. The present invention relates to a diyne polyprenyl alcohol represented by the following formula and an antihypertensive agent containing the diyne polyprenyl alcohol.
本発明の目的を達成させるために使用される化合物(1
)は新規化合物であり、その化学構造上合成方法として
は種々の方法があるが、次に述べる方法もその一方法で
ある。Compound (1) used to achieve the object of the present invention
) is a new compound, and there are various methods for synthesizing it due to its chemical structure, one of which is the method described below.
即ち、1,4ジクロローブチンー2と次の一般式(■)
〔式中Aおよびnは前記の意味を表わす。That is, 1,4 dichlorobetin-2 and the following general formula (■)
[In the formula, A and n represent the above meanings.
で表わされるポリプレニルアセトンを液体アンモニア中
、−50リC位の低温において、金属ナトリウムを触媒
として使用して反応させることにより得ることができる
〔Armita?,J.B等J.Chem.SOC.4
4(1951)〕。It can be obtained by reacting polyprenylacetone represented by [Armita? , J. B et al. J. Chem. SOC. 4
4 (1951)].
従来、高血圧症の治療の目的で、各種の血圧降下剤が使
用されているが、これら薬剤は種々の副作用を伴い、投
与上、特に大量投与および長期連続投与において、問題
がある。Conventionally, various antihypertensive agents have been used for the purpose of treating hypertension, but these drugs are accompanied by various side effects and pose problems in administration, particularly in large doses and long-term continuous administration.
例えば、スルホンアミド製剤およびサイアザイド製剤で
代表される利尿降圧剤ては、高尿酸血症、低カリウム血
症等の重篤な副作用を、レセルピン製剤、メチルドパ製
剤等の交感神経抑制剤では口渇、意識障害、起立性低血
圧等の副作用を、アプレゾリン等の血管拡張剤では頭痛
、頻脈、狭心症等の副作用を伴うことが多い。これらの
欠点がない、より安全な血圧降下剤を探索し、本発明の
化合物(1)を見出した。本発明の化合物の動物実験で
明らかになつた薬理作用および毒性(急性毒性)は次の
如くである。For example, diuretic antihypertensive drugs such as sulfonamides and thiazide preparations cause serious side effects such as hyperuricemia and hypokalemia, while sympatholytic drugs such as reserpine and methyldopa preparations cause dry mouth and Vasodilators such as apresolin often have side effects such as headache, tachycardia, and angina pectoris, while vasodilators such as apresoline often have side effects such as disturbance of consciousness and orthostatic hypotension. We searched for a safer antihypertensive agent that does not have these drawbacks, and found the compound (1) of the present invention. The pharmacological action and toxicity (acute toxicity) of the compound of the present invention revealed in animal experiments are as follows.
薬理試験
O岡本と青木の自然発症高血圧ラット(以下一SHRと
略す)に対する血圧降下作用〔方 法〕
岡本と青木のSHRに対する試験化合物の血圧降下作用
を測定した。Pharmacological Test O Blood Pressure Lowering Effect of Okamoto and Aoki on Spontaneous Hypertensive Rats (hereinafter abbreviated as 1SHR) [Method] The blood pressure lowering effect of the test compound on SHR of Okamoto and Aoki was measured.
SHRは生後約40週令の慢性的高血?HRを使用した
。血圧は最高血圧で0240mHy前後であつた。血圧
測定方法は島津式連続血圧測定装置SCS−301〔島
津製作所(株)製品〕を使用し、ラット尾部の動脈より
収縮期血圧を非観血的に測定した。試験化合物はアラビ
アゴムにより懸濁液とし、5実験動物は、試験化合物の
投与量により50m91k9投与群とし、更にアラビア
ゴム水溶液のみを投与するコントロール群をもうけた。Is SHR chronic hyperemia at about 40 weeks old? HR was used. The systolic blood pressure was around 0,240 mHy. Blood pressure was measured using a Shimadzu continuous blood pressure measuring device SCS-301 (manufactured by Shimadzu Corporation), and systolic blood pressure was measured non-invasively from the rat's tail artery. The test compound was made into a suspension with gum arabic, and five experimental animals were divided into 50m91k9 administration groups depending on the dose of the test compound, and a control group was also administered with only an aqueous solution of gum arabic.
各群とも実験動物4匹を使用した。投与は1日1回を3
日間、連続的に経口投与した。血圧測定は投与前、第1
回投与6時間後、同24時間後(第2回投与時)、同指
時間後(第3回投与時)および同7時間後に行い、血圧
の変化を観察した。Four experimental animals were used in each group. Administration: once a day for 3
It was orally administered continuously for 1 day. Blood pressure was measured before administration and at the first
Changes in blood pressure were observed at 6 hours, 24 hours (second administration), 7 hours (third administration), and 7 hours after each administration.
2,6,10.14,19,23,27,31−オクタ
メチルー2,6,10,22,26,30−ドトリアコ
ンタヘキセンー15,17ージインー14,19−ジオ
ール(以下化合物Aと称する)〔結 果〕
岡本と青木のSHRにおいて、化合物A5O7yl9l
kgを3日間連続的に経口投与した実験動物群に、第1
図に示される如く明確な血圧降下作用が認められた。2,6,10.14,19,23,27,31-octamethyl-2,6,10,22,26,30-dotriacontahexene-15,17-diyne-14,19-diol (hereinafter referred to as compound A) [Results] In Okamoto and Aoki's SHR, compound A5O7yl9l
kg was administered orally for 3 consecutive days to a group of experimental animals.
As shown in the figure, a clear blood pressure lowering effect was observed.
即ち、コントロール群(試験開始時の血圧240Tn!
NHg)では実験期間の3日後においても246717
7!Hyの血圧を示し、殆ど血圧に変化がみられなかつ
たのに対し、投与群(試験開始の血圧239?Hy)で
は第1回投与6時間後には210TIr!NHyl同2
4n間後(第2回投与時)には223順Hyl同3時間
後(第3回投与時)には210wunHyの血圧を示し
、持続的な血圧降下作用があることが認められた。以上
の薬理試験および毒性試験の結果より明らかなように、
化合物Aで代表される本発明の化合物(1)は、優れた
血圧降下作用を有し、毒性も殆ど認められないことから
安全性も非常に高いものである。That is, the control group (blood pressure at the start of the test 240Tn!
NHg), 246,717 even after 3 days of the experimental period.
7! In contrast, in the administration group (blood pressure at the start of the test 239?Hy), the blood pressure was 210 TIr!6 hours after the first administration. NHyl same 2
After 4 hours (at the time of the second administration), the blood pressure was 223 wunHy, and after the same 3 hours (at the time of the third administration), the blood pressure was 210 wunHy, indicating that it had a sustained blood pressure lowering effect. As is clear from the results of the above pharmacological and toxicity tests,
The compound (1) of the present invention, represented by Compound A, has an excellent antihypertensive effect and exhibits almost no toxicity, so it is extremely safe.
従つて、本発明の化合物(1)は、腎性、内分泌性、心
臓血管性、神経性、本態性等の各種の高血圧症の予防お
よび治療に有効な化合物である。本発明の化合物(1)
の投与方法および投与量は、治療すべき症状によつて、
適宜選択、調整され得るが、成人における経口投与で、
1日10〜200m9、好ましくは50〜100m9で
ある。本発明の化合物(1)は、通常の製剤技術を用い
て投与用に調製することができる。 」従
つて、この発明は人体医薬として好適な、少なくとも一
種の一般式(1)で表わされる化合物を含有する製剤組
成物をも包含するものである。このような組成物は任意
所要の製薬用担体あるいは賦形剤により慣用の方法で使
用に供される。この組成物は胃腸管からの吸収に好適な
形態で提供されるのが望ましい。経口投与用の錠剤およ
びカプセルは単位置投与形態であり、結合剤例えばシロ
ツプ、アラビアゴム、ゼラチン、ソルビツト、トンガカ
ント、またはポリビニルピロリドン、賦形薬例えば乳糖
、砂糖、とうもろこし澱粉、りん酸カルシウム、ソルビ
ツトまたはグリシン、潤滑剤例えばステアリン酸マグネ
シウム、タルク、ポリエチレングリコールまたはシリカ
、崩壊剤例えば馬鈴薯澱粉あるいは許容し得る湿潤剤例
えばラウリル硫酸ナトリウムのような慣用の賦形剤を含
有していてもよい。錠剤は当業界において周知の方法で
コーティングしてもよい。経口用液体製剤は水性または
油性懸濁液、溶液、シロツプ、エリキシル剤その他であ
つてもよく、あるいは使用する前に水または他の適当な
ビヒクルで再溶解させる乾燥生成物てあつてもよい。こ
のような液体製剤は普通に用いられる添加剤例えば懸濁
化剤例えばソルビツトシロツプ、メチルセルロース、グ
ルコース/糖シロツプ、ゼラチン、ヒドロキシエチルセ
ルロース、ヒドロキシプロピルセルローズ、カルボキシ
メチルセルロース、ステアリン酸アルミニウムゲルまた
は水素化食用脂、乳化剤例えばレシチン、モクオレイン
酸ゾルビタンまたはアラビアゴム、非水性ビヒクル例え
ばアーモンド油、分別ココナツト油、油性エステル、プ
ロピレングリコールまたはエチルアルコール、防腐剤例
えばp−ヒドロキシ安息香酸メチル、p−ヒドロキシ安
息香酸プロピルまたはソルピン酸を含有してもよい。注
射用組成物は単位投与量アンプルあるいは添加防腐剤と
共に多投与量容器中に提供される。Therefore, the compound (1) of the present invention is an effective compound for the prevention and treatment of various types of hypertension, including renal, endocrine, cardiovascular, neurological, and essential hypertension. Compound (1) of the present invention
The administration method and dosage depend on the symptoms to be treated.
Although it can be selected and adjusted as appropriate, for oral administration in adults,
10 to 200 m9 per day, preferably 50 to 100 m9. Compound (1) of the invention can be prepared for administration using conventional formulation techniques. Therefore, the present invention also includes a pharmaceutical composition containing at least one compound represented by formula (1), which is suitable as a human medicine. Such compositions are provided for use in a conventional manner with any required pharmaceutical carriers or excipients. Desirably, the composition is provided in a form suitable for absorption from the gastrointestinal tract. Tablets and capsules for oral administration are single-position dosage forms, with binders such as syrup, acacia, gelatin, sorbitol, tongacanth, or polyvinylpyrrolidone, excipients such as lactose, sugar, corn starch, calcium phosphate, sorbitol, or It may contain conventional excipients such as glycine, lubricants such as magnesium stearate, talc, polyethylene glycol or silica, disintegrants such as potato starch, or acceptable wetting agents such as sodium lauryl sulfate. Tablets may be coated by methods well known in the art. Oral liquid preparations may be aqueous or oily suspensions, solutions, syrups, elixirs, etc., or they may be a dry product for reconstitution with water or other suitable vehicle before use. Such liquid preparations may contain commonly used excipients such as suspending agents such as sorbitol syrup, methylcellulose, glucose/sugar syrup, gelatin, hydroxyethylcellulose, hydroxypropylcellulose, carboxymethylcellulose, aluminum stearate gel or hydrogenated Edible fats, emulsifiers such as lecithin, zorbitan moqualate or gum arabic, non-aqueous vehicles such as almond oil, fractionated coconut oil, oily esters, propylene glycol or ethyl alcohol, preservatives such as methyl p-hydroxybenzoate, propyl p-hydroxybenzoate. Alternatively, it may contain sorbic acid. Compositions for injection may be presented in unit-dose ampoules or in multi-dose containers with an added preservative.
組成物は懸濁液、溶液、油性または水性ビヒクル中の乳
液のような形態であつてもよく、懸濁化剤、安定化剤お
よび(または)分散剤のような処方剤を含んでいてもよ
い。一方、活性成分は使用する前に適当なビヒクル例え
ば発熱物質不含の滅菌した水で再溶解させる粉末であつ
てもよい。次に実施例により本発明を説明する。The compositions may take such forms as suspensions, solutions, emulsions in oily or aqueous vehicles, and may contain formulating agents such as suspending, stabilizing, and/or dispersing agents. good. Alternatively, the active ingredient may be in powder form for reconstitution with a suitable vehicle, eg sterile pyrogen-free water, before use. Next, the present invention will be explained with reference to examples.
実施例1〕2,6,10,14,19,23,27,3
1−オクタメチルー2,6,10,22,26,30−
ドトリアコンタヘキセンー15,17ージインー14,
19−ジオーノレ液体アンモニア250m1を−50℃
に冷却下、金属ナトリウム4.6yを加え1時間攪拌す
る。Example 1] 2, 6, 10, 14, 19, 23, 27, 3
1-octamethyl-2,6,10,22,26,30-
dotriacontahexene-15,17-diyne-14,
19-Dionole 250ml of liquid ammonia at -50℃
While cooling, add 4.6y of sodium metal and stir for 1 hour.
次いで6.2yの1,4−ジクロローブチンー2を3紛
を要して滴下し、更に同条件下で1紛間攪拌を継続する
。フアルネシルアセトン27gを乾燥エチルエーテル3
0m1に溶解して先に調整した溶液に滴下する。滴下終
了後、反応混合物を一夜−50゜Cにて保ち、次いでア
ンモニアを留去する。残渣をn−ヘキサン200mLに
溶解し、次いで水洗する。有機溶媒層を分取し、減圧濃
縮して得られる橙黄色油状物質を、エーテル・n−ヘキ
サン混合溶媒を溶出溶媒とするシリカゲルクロマトによ
り精製し、目的物を淡黄色油状物質として得る。収量9
f元素分析値:C4OH62O2MASスペクトル測定
値:M+574
IRスペクトル測定値: (Crn−1)3350(0
H),2950,2200,1640,1450,″1
378,1128,1030,900NMRスペクトル
測定値:(CDCl3,ppm)実施例2〕2,6,1
0,14,18,23,27,31,35,39−デカ
メチルー2,6,10,14,26,30,34,38
−テトラコンタオクタエンー19,21−ジインー18
,23−ジオール1,4−ジクロルーブチンー2とゲラ
ニルゲラニルアセトンとを実施例1〕に従つて反応処理
する。Next, 6.2y of 1,4-dichlorobutin-2 was added dropwise in 3 powders, and stirring was continued for 1 powder under the same conditions. 27g of phalnesyl acetone and 33g of dry ethyl ether
Dissolve in 0ml and drop into the solution prepared earlier. After the addition was complete, the reaction mixture was kept overnight at -50°C, and then the ammonia was distilled off. The residue is dissolved in 200 mL of n-hexane and then washed with water. The organic solvent layer is separated and concentrated under reduced pressure to obtain an orange-yellow oily substance, which is purified by silica gel chromatography using a mixed solvent of ether/n-hexane as an eluent to obtain the desired product as a pale yellow oily substance. Yield 9
f elemental analysis value: C4OH62O2MAS spectrum measurement value: M+574 IR spectrum measurement value: (Crn-1) 3350 (0
H), 2950, 2200, 1640, 1450, ″1
378,1128,1030,900 NMR spectrum measurement value: (CDCl3, ppm) Example 2] 2,6,1
0,14,18,23,27,31,35,39-decamethyl-2,6,10,14,26,30,34,38
-tetracontaoctaene-19,21-diyne-18
, 23-diol 1,4-dichlororubutin-2 and geranylgeranylacetone are reacted according to Example 1].
目的物を淡黄色油状物として得る。元素分析値:C5O
H76O2
′〜Vl4lU=◆〜Rv′ν皐?VA蕃v●●t′M
ASスペクトル測定値:M+708IRスペクトル測定
値; (C77!−1)3350(0H),2950,
2200,1640,1450,1378,1128,
1030,900NMRスペクトル測定値:(CDCl
3,ppm)次に、2,6,10,14,1S23,2
7,31−オクタメチルー2,6,10,22,26,
30−ドトリアコンタヘキサエンー15,17ージイン
ー14,19−ジオール(以下、主薬と称する)を使用
した処方を実施例として配す。The desired product is obtained as a pale yellow oil. Elemental analysis value: C5O
H76O2'~Vl4lU=◆~Rv'ν甐? VA 蕃v●●t'M
AS spectrum measurement value: M+708IR spectrum measurement value; (C77!-1) 3350 (0H), 2950,
2200, 1640, 1450, 1378, 1128,
1030,900 NMR spectrum measurements: (CDCl
3, ppm) Next, 2, 6, 10, 14, 1S23, 2
7,31-octamethyl-2,6,10,22,26,
A formulation using 30-dotriacontahexaene-15,17-diyne-14,19-diol (hereinafter referred to as the main drug) is provided as an example.
実施例3 カプセル剤
上記成分をi法により顆粒化したのち、セ2;;ン硬カ
プセル1000カプセルに充填した。Example 3 Capsules The above ingredients were granulated by method I, and then filled into 1000 hard capsules.
1カプセル中に主薬5mgを含有する。One capsule contains 5mg of the main drug.
実施例4 散 剤
主薬をアセトンに溶解し、次いでこれを微結晶セルロー
ズに吸着させたのち、乾燥した。Example 4 Powder The main ingredient was dissolved in acetone, then adsorbed onto microcrystalline cellulose, and then dried.
これをトウモロコシデンプンと混合し、常法により散剤
として、主薬の2皓散を調製した。実施例5 錠
剤
主薬;アセ7ンに溶解し、次いでこれを微結晶セルロー
ズに吸着させたのち、乾燥した。This was mixed with corn starch and a powder was prepared as the main drug, 2 Kosan, by a conventional method. Example 5 Tablet
The main agent of the agent was dissolved in acetate, and then adsorbed onto microcrystalline cellulose, followed by drying.
これにトウモロコシデンプン、乳糖、カルボキシメチル
セルローズカルシウムを混合し、次いでポリビニ7ルピ
ロリドンの水溶液を結合剤として加えて常法により顆粒
化した。これに滑沢剤としてタルクを加えて混合したの
ち、1錠100m9の錠剤に打錠した。1錠中には主薬
5mgを含有する。Corn starch, lactose, and carboxymethylcellulose calcium were mixed therein, and then an aqueous solution of polyvinyl-7-lpyrrolidone was added as a binder and granulated by a conventional method. After adding talc as a lubricant and mixing, the mixture was compressed into tablets of 100 m9 each. One tablet contains 5mg of the main drug.
実施例6 注射剤
主薬,NikkOlHCO−60,ゴマ油および半量の
プロピレングリコールを混合して約80℃で加温溶解し
、これにリン酸緩衝液および塩化ナトリウムとプロピレ
ングリコールを予め溶解した蒸留水を約80′Cに加温
して加え、全量1000m1の水溶液とした。Example 6 The main drug for injection, NikkOlHCO-60, sesame oil, and half the amount of propylene glycol were mixed and dissolved by heating at about 80°C. To this was added distilled water in which phosphate buffer, sodium chloride, and propylene glycol had been dissolved in advance. The mixture was heated to 80'C and added to make an aqueous solution with a total volume of 1000ml.
この水溶液を2ntのアンプルに分注して熔閉したのち
、加熱滅菌した。1管中、主薬20m9を含有する。This aqueous solution was dispensed into 2 nt ampoules, which were melted and sterilized by heating. One tube contains 20m9 of the active ingredient.
図面1)自然発症高血圧ラットに、本発明の化合物2,
6,10,1.4,19,23,27,31−オクタメ
チルー2,6,10,22,26,30−ドトリアコン
タヘキセンー15,17ージインー14,19−ジオー
ル(以下化合物Aと称する)を投与した時の血圧降下作
用を示したものである。Figure 1) Compound 2 of the present invention was administered to spontaneously hypertensive rats.
6,10,1.4,19,23,27,31-octamethyl-2,6,10,22,26,30-dotriacontahexene-15,17-diyne-14,19-diol (hereinafter referred to as compound A) This shows the blood pressure lowering effect when administered.
Claims (1)
は整数3または4を表わす。 で表わされるジイン系ポリプレニルアルコール2 2,
6,10,14,19,23,27,31−オクタメチ
ル−2,6,10,22,26,30−ドトリアコンタ
ヘキセン−15,17−ジイン−14,19−ジオール
である特許請求の範囲第1項記載のジイン系ポリプレニ
ルアルコール。 3 2,6,10,14,18,23,27,31,3
5,39−デカメチル−2,6,10,14,26,3
0,34,38−テトラコンタオクタエン−19,21
−ジイン−18,23−ジオールである特許請求の範囲
第1項記載のジイン系ポリプレニルアルコール。 4 次の一般式 ▲数式、化学式、表等があります▼ 〔式中Aは▲数式、化学式、表等があります▼鎖を、n
は整数3または4を表わす。 で表わされるジイン系ポリプレニルアルコールを含有す
る血圧降下剤。[Claims] 1 The following general formula▲There are mathematical formulas, chemical formulas, tables, etc.▼ [In the formula, A is ▲There are mathematical formulas, chemical formulas, tables, etc.▼The chain is n
represents an integer 3 or 4. Diyne polyprenyl alcohol 2 2,
6,10,14,19,23,27,31-octamethyl-2,6,10,22,26,30-dotriacontahexene-15,17-diyne-14,19-diol Diyne polyprenyl alcohol according to item 1. 3 2, 6, 10, 14, 18, 23, 27, 31, 3
5,39-decamethyl-2,6,10,14,26,3
0,34,38-tetracontaoctaene-19,21
The diyne-based polyprenyl alcohol according to claim 1, which is -diyne-18,23-diol. 4 The following general formula ▲ There are mathematical formulas, chemical formulas, tables, etc. ▼ [In the formula, A is ▲ There are mathematical formulas, chemical formulas, tables, etc. ▼ The chain is n
represents an integer 3 or 4. A hypotensive agent containing diyne polyprenyl alcohol represented by:
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP9496477A JPS6045614B2 (en) | 1977-08-10 | 1977-08-10 | Diyne polyprenyl alcohol and antihypertensive agents containing it |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP9496477A JPS6045614B2 (en) | 1977-08-10 | 1977-08-10 | Diyne polyprenyl alcohol and antihypertensive agents containing it |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| JPS5430108A JPS5430108A (en) | 1979-03-06 |
| JPS6045614B2 true JPS6045614B2 (en) | 1985-10-11 |
Family
ID=14124601
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP9496477A Expired JPS6045614B2 (en) | 1977-08-10 | 1977-08-10 | Diyne polyprenyl alcohol and antihypertensive agents containing it |
Country Status (1)
| Country | Link |
|---|---|
| JP (1) | JPS6045614B2 (en) |
-
1977
- 1977-08-10 JP JP9496477A patent/JPS6045614B2/en not_active Expired
Also Published As
| Publication number | Publication date |
|---|---|
| JPS5430108A (en) | 1979-03-06 |
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