JP2720176B2 - Method for producing panaxacols - Google Patents

Method for producing panaxacols

Info

Publication number
JP2720176B2
JP2720176B2 JP63225048A JP22504888A JP2720176B2 JP 2720176 B2 JP2720176 B2 JP 2720176B2 JP 63225048 A JP63225048 A JP 63225048A JP 22504888 A JP22504888 A JP 22504888A JP 2720176 B2 JP2720176 B2 JP 2720176B2
Authority
JP
Japan
Prior art keywords
compound
group
mixture
ethyl acetate
added
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
Application number
JP63225048A
Other languages
Japanese (ja)
Other versions
JPH0273026A (en
Inventor
康雄 藤本
美鶴 佐藤
直樹 竹内
敬一 牛山
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Nitto Denko Corp
RIKEN Institute of Physical and Chemical Research
Original Assignee
Nitto Denko Corp
RIKEN Institute of Physical and Chemical Research
Priority date (The priority date 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 date listed.)
Filing date
Publication date
Application filed by Nitto Denko Corp, RIKEN Institute of Physical and Chemical Research filed Critical Nitto Denko Corp
Priority to JP63225048A priority Critical patent/JP2720176B2/en
Publication of JPH0273026A publication Critical patent/JPH0273026A/en
Application granted granted Critical
Publication of JP2720176B2 publication Critical patent/JP2720176B2/en
Anticipated expiration legal-status Critical
Expired - Lifetime legal-status Critical Current

Links

Classifications

    • YGENERAL 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
    • Y02TECHNOLOGIES OR APPLICATIONS FOR MITIGATION OR ADAPTATION AGAINST CLIMATE CHANGE
    • Y02PCLIMATE CHANGE MITIGATION TECHNOLOGIES IN THE PRODUCTION OR PROCESSING OF GOODS
    • Y02P20/00Technologies relating to chemical industry
    • Y02P20/50Improvements relating to the production of bulk chemicals
    • Y02P20/52Improvements relating to the production of bulk chemicals using catalysts, e.g. selective catalysts

Landscapes

  • Low-Molecular Organic Synthesis Reactions Using Catalysts (AREA)
  • Organic Low-Molecular-Weight Compounds And Preparation Thereof (AREA)

Description

【発明の詳細な説明】 (技術分野) 本発明は、オタネニンジン(Panax.ginseng C.A.Meye
r)の根又はカルスより抽出されるジイン化合物ジヒド
ロパナキサコール(dihydropanaxacol)及びその類縁化
合物の新規合成方法に関するものである。Description: TECHNICAL FIELD The present invention relates to panax ginseng (Panax.ginseng CAMeye).
The present invention relates to a novel method for synthesizing a diyne compound dihydropanaxacol extracted from the root or callus of r) and related compounds.

(従来の技術) 従来、癌化学療法剤として、アルキル化剤(ナイトロ
ジェンマスタード類、エチレンイミン類、スルホン酸エ
ステル類)、代謝拮抗物質、(葉酸拮抗剤、プリン拮抗
剤、ピリミジン拮抗剤)、植物性核分裂毒(コルセミ
ド、ビンブラスチン等)、抗生物質(ザルコマイシン、
カルチノフィリン、マイトマイシン等)、ホルモン類
(副腎ステロイド、男性ホルモン、女性ホルモン)及び
ポルフィリン錯塩(マーフィリン、COPP)等が用いられ
ている。(Prior art) Conventionally, as cancer chemotherapeutic agents, alkylating agents (nitrogen mustards, ethyleneimines, sulfonic esters), antimetabolites, (folate antagonists, purine antagonists, pyrimidine antagonists), Plant fission toxins (colcemid, vinblastine, etc.), antibiotics (sarcomycin,
Cartinophilin, mitomycin, etc., hormones (adrenal steroids, male hormones, female hormones), porphyrin complex salts (murphyrin, COPP) and the like are used.

しかしながら、その殆んどは、細胞毒型の物質であ
り、重大な副作用を呈するため、低毒性で優れた制癌活
性を有する制癌剤の開発が望まれている。However, most of them are cytotoxic substances and exhibit serious side effects. Therefore, development of anticancer agents having low toxicity and excellent anticancer activity has been desired.

本発明者らは、上記趣旨に鑑み、低毒性で制癌活性を
有する物質を動・植物、微生物界の広い生物範囲から探
索を行った結果、オタネニンジンの根又はそのカルスよ
り抽出された新規なジイン化合物が、優れた制癌活性を
有し、且つ毒性の極めて少いことを見出し、該発明につ
き特許出願を行った(特願昭61−50067号)。In view of the above, the present inventors have conducted a search for a substance having a low toxicity and an anticancer activity from a wide range of animals, plants and microorganisms, and as a result, a novel substance extracted from the roots of Panax ginseng or its callus. The diyne compound was found to have excellent anticancer activity and extremely low toxicity, and a patent application was filed for this invention (Japanese Patent Application No. 61-50067).

しかし、カルス中のポリアセチレン誘導体の含量が低
いために、in vivoでの活性試験を行うことができない
という問題があった。However, there is a problem that the in vivo activity test cannot be performed because the content of the polyacetylene derivative in the callus is low.

(発明が解決しようとする課題) 従って本発明は、化学合成により大量のポリアセチレ
ン誘導体の供給を可能にすることを目的とする。(Problems to be Solved by the Invention) Accordingly, an object of the present invention is to enable supply of a large amount of a polyacetylene derivative by chemical synthesis.

(課題を解決するための手段) 本発明者は、酒石酒エステルを合成原料として選択す
ることにより、目的とするジヒドロパナキサコール及び
その類縁化合物を立体選択的に、かつ収率よく合成でき
ることを見い出し、上記課題を解決することができた。(Means for Solving the Problems) The inventor of the present invention is able to synthesize the desired dihydropanaxacol and its analogous compounds in a stereoselective and high-yield manner by selecting tartar tartrate as a raw material for synthesis. And solved the above problem.

すなわち、本発明は 化合物(A) (式中R1は、テトラヒドロピラニル基、トリアルキルシ
リル基のいずれかを示す。) と化合物(B) (式中R2は、テトラヒドロピラニル基、トリアルキルシ
リル基のいずれかを示し、R3はエチル基を示す。) を塩基の存在下に反応させて、化合物(C) (式中、R1及びR2は、それぞれテトラヒドロピラニル
基、トリアルキルシリル基のいずれかを示し、R3はエチ
ル基を示す。) を製造した後、酸で処理することにより化合物(1) を製造する方法を提供することを目的とする。That is, the present invention relates to the compound (A) (Wherein R 1 represents one of a tetrahydropyranyl group and a trialkylsilyl group) and the compound (B) (Wherein R 2 represents any one of a tetrahydropyranyl group and a trialkylsilyl group, and R 3 represents an ethyl group.) In the presence of a base to give a compound (C) (Wherein R 1 and R 2 each represent either a tetrahydropyranyl group or a trialkylsilyl group, and R 3 represents an ethyl group.). ) An object of the present invention is to provide a method for producing the same.

本発明の方法で合成される代表的な化合物であるジヒ
ドロパナキサコールは、特開昭62−207234号公報中、第
223頁の実施例に記載される化合物であり、以下の式 で示される化合物(1)(4,6−ヘプタデカジイン−3,
9,10−トリオール)であり、以下の物理化学的性質を有
する。Dihydropanaxacol, a typical compound synthesized by the method of the present invention, is described in JP-A-62-207234.
Compounds described in Examples on page 223, having the following formula Compound (1) represented by the formula (4,6-heptadecadiin-3,
9,10-triol) and has the following physicochemical properties.

(a)物質の形態:無色油状物質 本発明はかかる特徴的なジイン構造を有するジヒドロ
パナキサコール及びその類縁化合物を、2つのコンポネ
ートより合成することを特徴とする。(A) Form of substance: colorless oily substance The present invention is characterized in that dihydropanaxacol having such a characteristic diyne structure and its analogous compound are synthesized from two components.

すなわち、 例えばジヒドロパナキサコール(I)において説明す
れば、 プロパノール部とジイン部より得られる部、及
びグリコール部とヘキシル部より得られる部のコ
ンポーネントより合成することを特徴とする。That is, for example, in the case of dihydropanaxacol (I), It is characterized by being synthesized from components obtained from a propanol part and a diyne part, and components obtained from a glycol part and a hexyl part.

ジヒドロパナキサコールの合成法を例にとり、L−酒
石酸ジエチルエステルを原料とした本発明の合成方法の
好ましい1態様を、以下のスキームに示す。Taking the synthesis method of dihydropanaxacol as an example, a preferred embodiment of the synthesis method of the present invention using L-tartaric acid diethyl ester as a raw material is shown in the following scheme.

以上のスキームに示される各反応につき以下に詳細に
説明する。 Each reaction shown in the above scheme will be described in detail below.

(イ)ケタール(2)の合成 原料物質として用いる酒石酸エステルは、L−酒石酸
のエステル若しくはD−酒石酸のエステルのいずれでも
よく、用いる酒石酸エステルの立体配置により最後のジ
ヒドロパナキサコールの立体配置により最終のジヒドロ
パナキサコールの立体配置が定まる。D−酒石酸のエス
テルを用いた場合には、得られるジヒドロパナキサコー
ルのグリコール部分の立体配置は、天然型のパナキサコ
ールと同一となる。エステルとしてはアルキルエステル
の他、ベンジル等のエステルでも良く、ジエステルは、
同一のアルコール由来のエステルでなくてもよい。すな
わち非対称の酒石酸エステルを用いることもできる。特
にL−(+)−酒石酸ジエチルエステル若しくは、D−
(−)−酒石酸ジエチルエステルを用いることが好まし
い。(A) Synthesis of ketal (2) The tartaric acid ester used as a raw material may be either an ester of L-tartaric acid or an ester of D-tartaric acid, depending on the configuration of the tartaric acid ester used and the configuration of the last dihydropanaxacol. The configuration of the final dihydropanaxacol is determined. When an ester of D-tartaric acid is used, the configuration of the glycol moiety of the obtained dihydropanaxacol is the same as that of natural panaxacol. As the ester, other than an alkyl ester, an ester such as benzyl may be used.
The esters may not be derived from the same alcohol. That is, an asymmetric tartaric acid ester can be used. In particular, L-(+)-tartaric acid diethyl ester or D-
It is preferred to use (-)-tartrate diethyl ester.

ケタール化に用いることができる試薬としては、シク
ロヘキサノン、アセトン、メチルエチルケトン等を挙げ
ることが出来るが、特にアセトンジメチルアセタールを
用いることが好ましい。酸触媒を用いる場合には、カン
ファースルホン酸(CSA)、パラトルエンスルホン酸(T
sOH)、ピリジニウムパラトルエンスルホネート(PPT
S)等を用いることができる。溶媒としては通常のケタ
ール化に使用する溶媒、例えばベンゼン、トルエン等を
使用できるが、溶媒を使用しなくても良く、通常20℃〜
150℃の範囲で反応を行えばよい。Examples of the reagent that can be used for ketalization include cyclohexanone, acetone, and methyl ethyl ketone, and it is particularly preferable to use acetone dimethyl acetal. When an acid catalyst is used, camphorsulfonic acid (CSA), paratoluenesulfonic acid (T
sOH), pyridinium paratoluenesulfonate (PPT)
S) and the like can be used. As the solvent, a solvent used for normal ketalization, for example, benzene, toluene, etc. can be used, but it is not necessary to use a solvent, and usually 20 ° C.
The reaction may be performed in a range of 150 ° C.

上記の条件を用いることにより、通常90%以上の収率
でケタール体(2)を得ることができる。By using the above conditions, the ketal compound (2) can be usually obtained in a yield of 90% or more.

(ロ)ジオール(3)の合成 ジエステル(2)からジオール(2)に変換するに
は、無水エーテル、無水テトラヒドロフラン(THF)等
の無水溶媒中で、リチウムアルミニウムハイドライド
(LiAlH4)、リチウムボロハイドライド(LiBH4)等の
エステル還元剤で通常−20℃〜50℃で反応を行えばよ
く、通常80%以上の収率で目的とする(3)を得ること
ができる。(B) Synthesis of diol (3) In order to convert diester (2) to diol (2), lithium aluminum hydride (LiAlH 4 ), lithium borohydride, and the like are used in an anhydrous solvent such as anhydrous ether or anhydrous tetrahydrofuran (THF). The reaction may be carried out usually with an ester reducing agent such as (LiBH 4 ) at −20 ° C. to 50 ° C., and the desired compound (3) can be obtained usually with a yield of 80% or more.

(ハ)脱離基の導入((3)→(4)) ジオール(3)に脱離基として好適なパラトルエンス
ルホニル基(p−Ts基)、メタンスルホニル基(Ms基)
を導入するには、対応するパラトルエンスルホニルクロ
ライド(p−TsCl)やメタンスルホニルクロライド(Ms
Cl)等の対応するクロライド等を(3)に対し1.0モル
〜1.2モル、好ましくは1モル反応させればよく、
(3)の一方の水酸基に選択的に脱離基を導入すること
ができる。溶媒としてピリジン、コリジン等を用い、0
℃〜25℃で5時間反応させることにより、両方の水酸基
に反応した副生成物をほとんど生成すること無く、目的
とする(4)を得ることができる。(C) Introduction of a leaving group ((3) → (4)) Paratoluenesulfonyl group (p-Ts group), methanesulfonyl group (Ms group) suitable as a leaving group for diol (3)
To introduce the corresponding paratoluenesulfonyl chloride (p-TsCl) or methanesulfonyl chloride (Ms
The corresponding chlorides such as Cl) may be reacted with 1.0 mol to 1.2 mol, preferably 1 mol, with respect to (3),
A leaving group can be selectively introduced into one hydroxyl group of (3). Using pyridine, collidine or the like as a solvent,
By reacting at 5 ° C. to 25 ° C. for 5 hours, the desired (4) can be obtained with almost no by-products reacted with both hydroxyl groups.

(ニ)保護基の導入((4)→(5)) 化合物(4)中の未反応の水酸基は、通常用いられる
水酸基の保護基により保護することが好ましい。用いる
ことのできる保護基としては酸の存在で容易に水酸基を
与える保護基、例えばテトラヒドロピラニル基(THP
基)、トリアルキルシリル基等を挙げることができる。
保護基を導入するには、対応する化合物としてジヒドロ
ピラン(DHP)やトリアルキルシリルクロライドと
(4)を反応させれば良く、該反応においては酸触媒と
してCAS等を用いることもできる。溶媒としてジクロル
メタン、クロロホルム等を用い、0℃〜25℃で反応させ
ることにより目的とする水酸基保護体(5)を得ること
ができる。(D) Introduction of a protecting group ((4) → (5)) The unreacted hydroxyl group in the compound (4) is preferably protected by a commonly used hydroxyl protecting group. Protecting groups that can be used include protecting groups that readily provide a hydroxyl group in the presence of an acid, such as a tetrahydropyranyl group (THP
Group), a trialkylsilyl group and the like.
To introduce a protective group, dihydropyran (DHP) or trialkylsilyl chloride may be reacted with (4) as a corresponding compound, and CAS or the like may be used as an acid catalyst in the reaction. The desired hydroxyl-protected compound (5) can be obtained by reacting the mixture at 0 ° C. to 25 ° C. using dichloromethane, chloroform or the like as a solvent.

保護基としてTHP基を導入した場合には、THP基中の不
斉炭素の存在により、得られる(5)はジアステレオマ
ーの混合物となるが、混合物のまま、以後の反応を進行
させることができる。When a THP group is introduced as a protecting group, the resulting (5) becomes a mixture of diastereomers due to the presence of an asymmetric carbon in the THP group, but the subsequent reaction can proceed as it is. it can.

(ホ)ヘキシル化((5)→(6)) 化合物(5)は求核反応によりn−ヘキシル化され、
ヘキシル体(6)を得ることができる。ヘキシル化に用
いることのできる試薬してはn−ヘキシル銅リチウム、
n−ヘキシルリチウム等の金属ヘキシル化合物を挙げる
ことができる。これらの試薬は−20℃〜0℃に於て、無
水エーテル、無水THF等の無水溶媒中で、好ましくは窒
素等の不活性気体の気流下で反応させることができる。
特に好ましいヘキシル化剤としてn−ヘキシル銅リチウ
ムを挙げることができるが、該試薬は用時に調製するこ
とが好ましい。(E) Hexylation ((5) → (6)) Compound (5) is n-hexylated by a nucleophilic reaction,
Hexyl compound (6) can be obtained. Reagents that can be used for hexylation include n-hexyl copper lithium,
Metal hexyl compounds such as n-hexyllithium can be mentioned. These reagents can be reacted at -20 ° C to 0 ° C in an anhydrous solvent such as anhydrous ether or anhydrous THF, preferably under a stream of an inert gas such as nitrogen.
Particularly preferred hexylating agents include lithium n-hexylcopper, but the reagent is preferably prepared at the time of use.

(ヘ)トリオール(7)の合成 ヘキシル化した化合物(7)よりトリオール体(7)
を得るには、例えば塩酸、硫酸、パラトルエンスルホン
酸等の酸の存在下にメタノール、エタノール、等の溶媒
中で反応を行えばよい。反応を0℃〜20℃で通常0.5〜
1.0時間行うことにより好収量で(7)を得ることがで
きる。(F) Synthesis of triol (7) Triol compound (7) from hexylated compound (7)
The reaction may be carried out in a solvent such as methanol or ethanol in the presence of an acid such as hydrochloric acid, sulfuric acid or paratoluenesulfonic acid. The reaction is usually carried out at
By performing for 1.0 hour, (7) can be obtained in good yield.

(ト)脱離基の導入((7)→(8)) 脱離基として好適な基としては、前述した(ハ)に挙
げた脱離基を用いることができ、それらは前述した試薬
により容易に導入することができる。試薬量をに対して
1.0モル〜1.2モルとし、0〜25℃で5時間反応させるこ
とにより、選択的に末端の水酸基に脱離基を導入するこ
とができ、(8)を得ることができる。(G) Introduction of Leaving Group ((7) → (8)) As the suitable group as the leaving group, the leaving groups described in (c) above can be used, and they are obtained by the above-mentioned reagent. Can be easily introduced. Reagent volume
By leaving the mixture at 1.0 mol to 1.2 mol and reacting at 0 to 25 ° C. for 5 hours, a leaving group can be selectively introduced into the terminal hydroxyl group, whereby (8) can be obtained.

(チ)エポキシ−アルコール(9) 化合物(8)をメタノール、エタノール等の溶媒中で
無水炭酸カリウム、無水炭酸ナトリウム等の塩基で処理
することにより、エポキシアルコール体(9)を得るこ
とができる。反応温度を通常0℃〜30℃として、約1時
間反応させることにより収量約90%以上で(9)が得ら
れる。(H) Epoxy-alcohol (9) The epoxy alcohol derivative (9) can be obtained by treating the compound (8) with a base such as anhydrous potassium carbonate or anhydrous sodium carbonate in a solvent such as methanol or ethanol. The reaction is carried out at a reaction temperature of usually 0 ° C. to 30 ° C. for about 1 hour to obtain (9) in a yield of about 90% or more.

(リ)保護基の導入((9)→(10)) 得られた(9)は水酸基を保護しておくことが好まし
いが、保護基としては(ニ)で挙げた保護基を好適に使
用しうる。保護基の導入も前述した方法で行うことがで
き、水酸基保護体(10)を得ることができる。(Ii) Introduction of a protecting group ((9) → (10)) In the obtained (9), it is preferable to protect a hydroxyl group, but the protecting group described in (d) is preferably used as the protecting group. Can. The protecting group can be introduced by the method described above, and the protected hydroxyl group (10) can be obtained.

(ヌ)ジイン化合物(13)及び保護体(14) ジアセチレン(12)とプロピオンアルデヒド、アクロ
レイン等より塩基の存在下、常法によりジイン化合物を
得ることができる。溶媒としてTHF、ジメトキシエタン
等を用い、塩基としてブチルリチウム(ヘキサン溶
液)、メチルリチウム等を用いれば良く、−20℃〜0℃
で1時間反応させれば良い。得られた(13)は水酸基を
保護することが好ましいが、保護基としては(ニ)で挙
げた保護基を好適に使用することができる。保護基の導
入も前述した方法で行えばよく、収率よく保護体(14)
を得ることができる。(Nu) Diyne compound (13) and protected form (14) A diyne compound can be obtained from diacetylene (12) and propionaldehyde, acrolein or the like by a conventional method in the presence of a base. The solvent may be THF, dimethoxyethane, or the like, and the base may be butyllithium (hexane solution), methyllithium, or the like.
And react for 1 hour. The obtained (13) preferably protects a hydroxyl group, and as the protecting group, the protecting groups described in (d) can be suitably used. The protecting group may be introduced by the method described above, and the protected form (14) is obtained in high yield.
Can be obtained.

(ル)化合物(15) 得られた化合物(10)と化合物(14)より化合物(1
5)を合成することができる。化合物(14)をTHF、ジメ
トキシエタン等の溶媒中で、例えばブチルリチウム(ヘ
キサン溶液)、グリニャール試薬、ナトリウムハイドラ
イド、カリウムアミド等の塩基で処理し金属アセチリド
とした後、(10)を、好ましくはTHF等の溶媒に溶解し
て加えれば良い。反応は−20℃〜0℃で行うのがよく、
約3時間反応させることによりエポキシが開環した付加
体(15)を得ることができる。(R) Compound (15) Compound (1) was obtained from compound (10) and compound (14).
5) can be synthesized. Compound (14) is treated with a base such as butyllithium (hexane solution), Grignard reagent, sodium hydride, or potassium amide in a solvent such as THF or dimethoxyethane to form metal acetylide. It may be dissolved in a solvent such as THF and added. The reaction is preferably carried out at -20 ° C to 0 ° C,
The reaction is carried out for about 3 hours to obtain an adduct (15) in which the epoxy is opened.

(ヲ)保護基((15)→(1)) 保護基を除去するには、(ヘ)で述べた方法を用いる
ことができる。脱保護することにより目的とするジヒド
ロパナキサコールを得ることができる。(Ii) Protecting group ((15) → (1)) To remove the protecting group, the method described in (f) can be used. The desired dihydropanaxacol can be obtained by deprotection.

(発明の効果) 本発明の新規合成法により、従来抽出によって極少量
しか得られなかったジヒドロパナキサコール及びその類
縁化合物を大量に合成することが出来るようになった。(Effect of the Invention) According to the novel synthesis method of the present invention, it has become possible to synthesize a large amount of dihydropanaxacol and its related compounds, which were conventionally obtained only in very small amounts by extraction.

次に実施例により本発明を説明する。 Next, the present invention will be described with reference to examples.

(実施例) 実施例1((1)→(2)) L−(+)−酒石酸ジエチルエステル(1)11.0gを
アセトンジメチルアセタール(2,2−dimethoxypropan
e)50mlに溶解後、カンファースルホン酸(CSA)100mg
を加えて、50〜70℃の油浴中で一夜撹拌した。冷後、酢
酸エチル100mlを加え、5%NaHCO3溶液50ml中に注ぎ有
機層を分離した。水層を酢酸エチルにて抽出後有機層と
合せ、飽和食塩水80mlで2回洗浄し、Na2SO4で乾燥、濃
縮した。ここに得られた混合物をシリカゲルカラムクロ
マト(ヘキサン:酢酸エチル=3:1)にて分離し、
(2)(9.0g、収率68.5%)を得ると共に15%の原料を
回収した。(Example) Example 1 ((1) → (2)) L-(+)-tartaric acid diethyl ester (1) was mixed with 11.0 g of acetone dimethyl acetal (2,2-dimethoxypropan).
e) After dissolving in 50ml, camphorsulfonic acid (CSA) 100mg
And stirred in a 50-70 ° C. oil bath overnight. After cooling, 100 ml of ethyl acetate was added, and the mixture was poured into 50 ml of a 5% NaHCO 3 solution to separate an organic layer. The aqueous layer was extracted with ethyl acetate, combined with the organic layer, washed twice with 80 ml of saturated saline, dried over Na 2 SO 4 and concentrated. The mixture obtained here was separated by silica gel column chromatography (hexane: ethyl acetate = 3: 1),
(2) (9.0 g, yield 68.5%) was obtained and 15% of the raw material was recovered.

実施例2((2)→(3)) 無水エーテル100ml中にLiAl4 6.0gを撹拌しながら加
え懸濁液とした後、化合物(2)(7.7g)のエーテル溶
液(40ml)をゆっくりと滴下し、室温で一夜撹拌した。
次いで、酢酸エチル20mlを滴下し30分間撹拌後、飽和ロ
ッシェル塩溶液30mlを加え、濾過補助剤としてセライト
を用いて濾過し濃縮した。ここに得られた油状物をシリ
カゲルカラムクロマト(ヘキサン:酢酸エチル=3:1及
び1:2)に対し、化合物(3)(3.7g、収率77.%)を得
た。得られた(3)は、K.Mori及びS.Tanada(テトラヘ
ドロン35巻:1279−1284頁、1979年)の報告中にある化
合物とNMRスペクトルが一致した。Example 2 ((2) → (3)) 6.0 g of LiAl 4 was added to 100 ml of anhydrous ether with stirring to form a suspension, and then an ether solution (40 ml) of compound (2) (7.7 g) was slowly added. The mixture was added dropwise and stirred at room temperature overnight.
Next, 20 ml of ethyl acetate was added dropwise, and the mixture was stirred for 30 minutes. Then, 30 ml of a saturated Rochelle salt solution was added, and the mixture was filtered and concentrated using celite as a filter aid. Compound (3) (3.7 g, yield: 77.%) was obtained from the obtained oily substance by silica gel column chromatography (hexane: ethyl acetate = 3: 1 and 1: 2). The obtained (3) was identical in NMR spectrum to the compound reported in K. Mori and S. Tanada (Tetrahedron 35: 1279-1284, 1979).

実施例3((3)→(4)) 化合物(3)(3.2g)のピリジン溶液(30ml)に、パ
ラトルエンスルホニルクロライド(p−TsCl 3.0g)を
加え室温で一夜放置した。次いで、飽和食塩水100mlを
加え酢酸エチルにて抽出し、減圧濃縮して油状物質を得
た。この油状物質をシリカゲルカラムクロマト(ヘキサ
ン:酢酸エチル=2:1)に付し、化合物(4)(3.4g、
収率54.5%)を得ると共に10%の原料を回収した。1 H−NMR 1.35(s) (ppm) 1.38(s) 2.20(br,s) 2.45(s) 3.74(m) 4.15(m) 7.35(d,J=8.3Hz) 7.77(d.J=8.3Hz) 実施例4((4)→(5)) 化合物(4)(1.7g)のジクロルメタン溶液(10ml)
に、3,4−シヒドロ−2H−ピラン(DHP、670mg、1.5当
量)とCSA50mgを加えて室温で30分撹拌した。反応終了
後、酢酸エチル50mlを加えたのち飽和NaHCO3水中に注ぎ
酢酸エチルにて抽出した。次いで、有機層を飽和食塩水
(50ml×2)にて2回洗浄し、Na2SO4で乾燥、濃縮し得
られた油状物質をシリカゲルカラムクロマト(ヘキサ
ン:酢酸エチル=3:1)に付し、化合物(5)(2.0g、
収率93.0%)を得た。1 H−NMR 1.35(s) (ppm) 1.38(s) 1.57(br,s) 2.45(s) 3.52(br,m) 3.57(br,m) 4.14(m) 4.61(br,s) 7.34(d,J=8.3Hz) 7.81(d,J=8.3Hz) 実施例5((5)→(6)) ヨウ化第一銅1)(1.34g、3.0eq)を無水エーテル(25
ml)中に懸濁し−40℃に冷却した。次いで、n−ヘキシ
ルリチウム−エーテル2)(4.5ml、1.56mmol/ml)を滴下
し、15分間撹拌した(この時、反応液の色は、淡黄色で
あったが、徐々に褐色から黒褐色となった)。更に、n
−ヘキシルリチウム/エーテル2)4.5ml(1.56mmol/ml)
を滴下し、15分間撹拌した(反応液の色は、黒褐色から
淡紫色から濃青紫色へと変化した)。次に、化合物
(5)(930mg)のエーテル溶液(8ml)を浴温−30℃、
10分間で滴下した。(滴下していくにつれて反応液の色
は、濃青紫色から黒色へと変化した)。更に、この温度
で1時間撹拌した後、飽和塩化アンモニウム溶液(10m
l)を加え20分撹拌した。次いで、この混合物をエーテ
ルで抽出し、飽和食塩水(30ml)で2回洗浄後Na2SO4
乾燥し、濃縮した。得られた粗生成物をシリカゲルカラ
ムクロマト(ヘキサン:酢酸エテル=7:1)により粗分
画後、更にHPLC(Nucleosil 50−5,8×300mm、ヘキサ
ン:酢酸エチル=20:1、3.0ml/min)にて精製し、化合
物(6)(500mg、収率66.4%、17分に溶出)を得た。Example 3 ((3) → (4)) Paratoluenesulfonyl chloride (p-TsCl 3.0 g) was added to a pyridine solution (30 ml) of compound (3) (3.2 g), and the mixture was allowed to stand at room temperature overnight. Then, 100 ml of saturated saline was added, extracted with ethyl acetate, and concentrated under reduced pressure to obtain an oily substance. This oily substance was subjected to silica gel column chromatography (hexane: ethyl acetate = 2: 1) to give compound (4) (3.4 g,
A yield of 54.5%) was obtained and 10% of the raw material was recovered. 1 H-NMR 1.35 (s) (ppm) 1.38 (s) 2.20 (br, s) 2.45 (s) 3.74 (m) 4.15 (m) 7.35 (d, J = 8.3Hz) 7.77 (dJ = 8.3Hz) carried Example 4 ((4) → (5)) Compound (4) (1.7 g) in dichloromethane solution (10 ml)
To the mixture were added 3,4-cyhydro-2H-pyran (DHP, 670 mg, 1.5 equivalents) and 50 mg of CSA, and the mixture was stirred at room temperature for 30 minutes. After the reaction was completed, 50 ml of ethyl acetate was added, and the mixture was poured into saturated NaHCO 3 water and extracted with ethyl acetate. Next, the organic layer was washed twice with a saturated saline solution (50 ml × 2), dried over Na 2 SO 4 , and concentrated. The obtained oil was subjected to silica gel column chromatography (hexane: ethyl acetate = 3: 1). And compound (5) (2.0 g,
Yield 93.0%). 1 H-NMR 1.35 (s) (ppm) 1.38 (s) 1.57 (br, s) 2.45 (s) 3.52 (br, m) 3.57 (br, m) 4.14 (m) 4.61 (br, s) 7.34 (d , J = 8.3 Hz) 7.81 (d, J = 8.3 Hz) Example 5 ((5) → (6)) Cuprous iodide 1) (1.34 g, 3.0 eq) was converted to anhydrous ether (25
ml) and cooled to -40 ° C. Then, n-hexyllithium-ether 2) (4.5 ml, 1.56 mmol / ml) was added dropwise and stirred for 15 minutes (at this time, the color of the reaction solution was pale yellow, but gradually changed from brown to black brown). became). Furthermore, n
-Hexyllithium / ether 2) 4.5 ml (1.56 mmol / ml)
Was added dropwise and stirred for 15 minutes (the color of the reaction solution changed from black-brown to pale purple to dark blue-violet). Next, an ether solution (8 ml) of the compound (5) (930 mg) was added at a bath temperature of −30 ° C.
It was dropped in 10 minutes. (The color of the reaction solution changed from dark blue-purple to black as the solution was dropped). Further, after stirring at this temperature for 1 hour, a saturated ammonium chloride solution (10 m
l) was added and stirred for 20 minutes. Then, the mixture was extracted with ether, washed twice with a saturated saline solution (30 ml), dried over Na 2 SO 4 and concentrated. The obtained crude product was roughly fractionated by silica gel column chromatography (hexane: ether acetate = 7: 1), and then subjected to HPLC (Nucleosil 50-5,8 × 300 mm, hexane: ethyl acetate = 20: 1, 3.0 ml / ml). min) to give Compound (6) (500 mg, yield 66.4%, eluted at 17 minutes).

1) 市販のヨウ化第一銅をソックスレー抽出器を用い
てTHFで洗浄し、真空ポンプで4−5時間乾燥したもの
を使用した。1) Commercially available cuprous iodide was washed with THF using a Soxhlet extractor and dried with a vacuum pump for 4-5 hours.

2) 金属リチウム(30%)デイスパージョン11.8g、
2.5当量)を無水エーテル(60ml)中に加えて撹拌し
た。n−ブロムヘキサン(3ml、使用する全量の約1/3)
を加えて室温で撹拌し、内温が上昇してきたところで、
−15℃に冷却した。次いで、残りのn−ブロモヘキサン
(25ml)を徐々に加えた後、更に3−4時間、−15℃で
撹拌した。得られたヘキシルリチウム溶液を冷蔵庫に静
置し、上澄みのエーテル層の力価をsec−ブタノール
(指示薬:1,10−フェナンスリロン)で検定した後反応
に使用した。2) 11.8g lithium metal (30%) dispersion,
2.5 eq.) In anhydrous ether (60 ml) and stirred. n-bromohexane (3 ml, about 1/3 of the total amount used)
And stir at room temperature, and when the internal temperature rises,
Cooled to -15 ° C. Then, after the remaining n-bromohexane (25 ml) was gradually added, the mixture was further stirred at -15 ° C for 3-4 hours. The obtained hexyllithium solution was allowed to stand in a refrigerator, and the titer of the supernatant ether layer was assayed with sec-butanol (indicator: 1,10-phenanthrilone), and then used for the reaction.

Rf(ヘキサン:酢酸エチル=7:1、シリカゲル薄層ク
ロマトグラフィー、メルク社製Art.5715、0.25mm、以下
実施例において同じ)=0.33 実施例6((6)→(7)) 化合物(6)(400mg)のメタノール溶液(4ml)に2N
−HCl(1ml)を加え室温で1時間撹拌した。次いで、酢
酸エチル40mlを加え飽和食塩水(10Lm)で2回洗浄後、
Na2SO4にて乾燥、濃縮し、化合物(7)(206mg、収率8
8.0%)を無色結晶として得た。1 H−NMR 0.95(t,J=7.1Hz) (ppm) 1.2〜1.4(br,m) 1.50(m) 3.62(m) 3.75(m)13 C−NMR 14.1,22.7,25.8,29.4 (ppm) 29.8,31.9,33.6,64.5 72.4,74.3, m.p. 48℃ IR(CHCl3)cm-1;3400(m),2925(s),2850(m) 実施例7((1)→(8)) 化合物(7)(190mg)のピリジン溶液(2ml)にパラ
トルエンスルホニルクロライド(p−TsCl)(185mg)
を加え室温で1夜放置した。飽和食塩水(30ml)を加
え、酢酸エチルにて抽出し、有機層をNa2SO4にて乾燥、
濃縮した。得られた混合物をシリカゲルクロマト(ヘキ
サン:酢酸エチル=3:1)に付し、化合物(8)(150m
g、収率43.6%)を無色結晶として得た。1 H−NMR 0.88(t,J=7.3Hz) (ppm) 1.2〜1.4(br,m) 2.46(s) 3.72(br,m) 4.09(d,J=5.4Hz) 7.35(d,J=8.1Hz) 7.80(d,J=8.1Hz) m.p. 63℃ IR(cm-1);3550(m),2925(s),2850(m), 1730(m),1600(m),1460(m) 実施例8((8)→(9)) 化合物(8)(114mg)のメタノール溶液(3.5ml)に
無水炭酸カリウム(457mg、10当量)を加え、室温で1
時間撹拌した。反応混合物に飽和食塩水(40ml)を加
え、酢酸エチルにて抽出した。抽出液を飽和食塩水で洗
浄後、Na2SO4にて乾燥し濃縮した。得られた混合物をシ
リカゲルクロマト(ヘキサン:酢酸エチル=2:1)に付
し、化合物(9)(55mg、収率75.5%)を得た。1 H−NMR 0.88(t,J=7.3Hz) (ppm) 1.2〜1.4(br,m) 1.60(m) 1.78(d,J=5.9Hz−CH) 2.72(dd,J=2.7,4.9Hz) 2.83(t,J=4.9Hz) 2.98(m) 3.44(m) IR(cm-1);3600(w),3500(w),3430(s), 3360(m) 実施例9((9)→(10)) 化合物(9)(50mg)のジクロルメタン溶液(1.5m
l)にDHP(40μ)と微量のCSAを加え、室温で30分撹
拌した。次いで、反応液にNaHCO3溶液(20ml)を加え、
酢酸エチルにて抽出した。有機層を飽和食塩水で洗浄
後、Na2SO4にて乾燥し濃縮した。得られた混合物をシリ
カゲルクロマト(ヘキサン:酢酸エチル=3:1)に対
し、化合物(10)(67mg、収率90.0%)を得た。Rf (hexane: ethyl acetate = 7: 1, silica gel thin layer chromatography, Art.5715, manufactured by Merck Ltd., 0.25 mm, the same in the following examples) = 0.33 Example 6 ((6) → (7)) Compound (6) ) (400mg) in methanol solution (4ml)
-HCl (1 ml) was added and the mixture was stirred at room temperature for 1 hour. Then, after adding 40 ml of ethyl acetate and washing twice with a saturated saline solution (10 Lm),
After drying and concentration over Na 2 SO 4 , compound (7) (206 mg, yield 8)
8.0%) as colorless crystals. 1 H-NMR 0.95 (t, J = 7.1 Hz) (ppm) 1.2 to 1.4 (br, m) 1.50 (m) 3.62 (m) 3.75 (m) 13 C-NMR 14.1, 22.7, 25.8, 29.4 (ppm) 29.8, 31.9, 33.6, 64.5 72.4, 74.3, mp 48 ° C IR (CHCl 3 ) cm -1 ; 3400 (m), 2925 (s), 2850 (m) Example 7 ((1) → (8)) Compound (7) Paratoluenesulfonyl chloride (p-TsCl) (185 mg) was added to a pyridine solution (2 ml) of (190 mg).
And left at room temperature overnight. Saturated saline (30 ml) was added, extracted with ethyl acetate, and the organic layer was dried over Na 2 SO 4 ,
Concentrated. The obtained mixture was subjected to silica gel chromatography (hexane: ethyl acetate = 3: 1) to give compound (8) (150 m
g, yield 43.6%) as colorless crystals. 1 H-NMR 0.88 (t, J = 7.3Hz) (ppm) 1.2~1.4 (br, m) 2.46 (s) 3.72 (br, m) 4.09 (d, J = 5.4Hz) 7.35 (d, J = 8.1 Hz) 7.80 (d, J = 8.1 Hz) mp 63 ° C IR (cm -1 ); 3550 (m), 2925 (s), 2850 (m), 1730 (m), 1600 (m), 1460 (m) Example 8 ((8) → (9)) To a solution of compound (8) (114 mg) in methanol (3.5 ml) was added anhydrous potassium carbonate (457 mg, 10 equivalents).
Stirred for hours. A saturated saline solution (40 ml) was added to the reaction mixture, and the mixture was extracted with ethyl acetate. The extract was washed with brine, dried over Na 2 SO 4 and concentrated. The obtained mixture was subjected to silica gel chromatography (hexane: ethyl acetate = 2: 1) to obtain compound (9) (55 mg, yield: 75.5%). 1 H-NMR 0.88 (t, J = 7.3Hz) (ppm) 1.2~1.4 (br, m) 1.60 (m) 1.78 (d, J = 5.9Hz-CH) 2.72 (dd, J = 2.7,4.9Hz) 2.83 (t, J = 4.9 Hz) 2.98 (m) 3.44 (m) IR (cm -1 ); 3600 (w), 3500 (w), 3430 (s), 3360 (m) Example 9 ((9)) → (10)) Compound (9) (50 mg) in dichloromethane (1.5 m
DHP (40μ) and a trace amount of CSA were added to l), and the mixture was stirred at room temperature for 30 minutes. Next, a NaHCO 3 solution (20 ml) was added to the reaction solution,
Extracted with ethyl acetate. The organic layer was washed with brine, dried over Na 2 SO 4 and concentrated. The obtained mixture was subjected to silica gel chromatography (hexane: ethyl acetate = 3: 1) to obtain a compound (10) (67 mg, yield 90.0%).

Rf(ヘキサン:酢酸エチル=5:1)=0.40、0.47(ジア
ステレオマー混合物)1 H−NMR 0.88(t,J=7.3Hz) (ppm) 1.2〜1.4(br,m) 1.5〜1.7(br,m) 1.76(m) 1.84(m) 2.49(dd,J=2.7,4.9Hz) 2.67(dd,J=2.7,4.9Hz) 2.76(t,J=4.9Hz) 2.80(t,J=4.9Hz) 2.95(m) 3.09(m) 3.38(m) 3.50(m) 3.88(m) 4.00(m) 4.70(t,J=4.4Hz) 4.98(t,J=4.4Hz) 実施例10((11)+(12)→(13)→(14)) ジアセチレン(12)のTHF溶液(15ml)(1mmol/ml)
を−50℃に冷却し撹拌した。これにブチルリチウム−ヘ
キサン(10ml、1.5mmol/ml)とプロピオンアルデヒド
((11)、840mg、14.5mmol)を徐々に滴下後、更に30
分撹拌した。次いで、飽和塩化アンモニウム溶液(50m
l)を加え、酢酸エチルにて抽出した。有機層を飽和食
塩水で洗浄後Na2SO4で乾燥し濃縮した。ここに得られた
混合物をシリカゲルクロマト(ヘキサン:酢酸エチル=
5:1)で分離・精製した後、ジクロルメタン(10ml)に
溶解し、DHP(1ml)とCSA(20mg)を加えて室温で1時
間撹拌した。反応液にNaHCO3溶液(20ml)を加え、酢酸
エチルにて抽出し、有機層を飽和食塩水で洗浄後、Na2S
O4で乾燥して濃縮した。得られた混合物をシリカゲルク
ロマト(ヘキサン:酢酸エチル=7:1)に付し、化合物
(14)(1.4g、収率50.0%)を得た。Rf (hexane: ethyl acetate = 5: 1) = 0.40, 0.47 (mixture of diastereomers) 1 H-NMR 0.88 (t, J = 7.3 Hz) (ppm) 1.2 to 1.4 (br, m) 1.5 to 1.7 (br , m) 1.76 (m) 1.84 (m) 2.49 (dd, J = 2.7, 4.9 Hz) 2.67 (dd, J = 2.7, 4.9 Hz) 2.76 (t, J = 4.9 Hz) 2.80 (t, J = 4.9 Hz) 2.95 (m) 3.09 (m) 3.38 (m) 3.50 (m) 3.88 (m) 4.00 (m) 4.70 (t, J = 4.4 Hz) 4.98 (t, J = 4.4 Hz) Example 10 ((11)) + (12) → (13) → (14)) THF solution of diacetylene (12) (15ml) (1mmol / ml)
Was cooled to −50 ° C. and stirred. To this, butyllithium-hexane (10 ml, 1.5 mmol / ml) and propionaldehyde ((11), 840 mg, 14.5 mmol) were gradually added dropwise, followed by another 30 minutes.
For a minute. Then, saturated ammonium chloride solution (50m
l) was added and extracted with ethyl acetate. The organic layer was washed with saturated saline, dried over Na 2 SO 4 and concentrated. The mixture obtained here is subjected to silica gel chromatography (hexane: ethyl acetate =
After separation and purification in 5: 1), the residue was dissolved in dichloromethane (10 ml), DHP (1 ml) and CSA (20 mg) were added, and the mixture was stirred at room temperature for 1 hour. A NaHCO 3 solution (20 ml) was added to the reaction solution, and the mixture was extracted with ethyl acetate. The organic layer was washed with saturated saline, and then washed with Na 2 S
Dried over O 4 and concentrated. The obtained mixture was subjected to silica gel chromatography (hexane: ethyl acetate = 7: 1) to obtain compound (14) (1.4 g, yield 50.0%).

Rf(ヘキサン:酢酸エチル=5:1)=0.60、0.68(ジア
ステレオマー混合物)1 H−NMR 1.00(t,J=7.3Hz) (ppm) 1.04(t,J=7.3Hz) 1.56(m) 1.78(m) 2.14(d,J=0.9Hz) 2.15(d,J=0.9Hz) 3.54(m) 3.80(m) 4.00(m) 4.25(t,J=6.4Hz) 4.41(t,J=6.4Hz) 4.74(t,J=3.4Hz) 4.93(t,J=3.4Hz) 実施例11((10)+(14)→(15)) 化合物(14)(77mg、0.4mmol)のTHF溶液(130μ
)を−30℃に冷却後、ブチルリチウム−ヘキサン(23
0μ、0.3mmol)及びHMPA(50μ、0.3mmol)を徐々
に滴下した。次いで化合物(10)(25mg、0.1mmol)のT
HF溶液(100μ)を滴下し、−30℃で2時間撹拌し
た。反応終了後、飽和NH4Cl溶液(10ml)を加え、酢酸
エチルにて抽出した。有機層を飽和食塩水で洗浄後Na2S
O4で乾燥し濃縮した。得られた混合物をシリカゲルクロ
マト(ヘキサン:酢酸エチル=5:1)に付し、化合物(1
5)(20mg、収率44.4%)を得た。Rf (hexane: ethyl acetate = 5: 1) = 0.60, 0.68 (mixture of diastereomers) 1 H-NMR 1.00 (t, J = 7.3 Hz) (ppm) 1.04 (t, J = 7.3 Hz) 1.56 (m) 1.78 (m) 2.14 (d, J = 0.9 Hz) 2.15 (d, J = 0.9 Hz) 3.54 (m) 3.80 (m) 4.00 (m) 4.25 (t, J = 6.4 Hz) 4.41 (t, J = 6.4) Hz) 4.74 (t, J = 3.4 Hz) 4.93 (t, J = 3.4 Hz) Example 11 ((10) + (14) → (15)) A THF solution of compound (14) (77 mg, 0.4 mmol) ( 130μ
) Was cooled to -30 ° C, and butyllithium-hexane (23
0μ, 0.3mmol) and HMPA (50μ, 0.3mmol) were slowly added dropwise. Then, T of compound (10) (25 mg, 0.1 mmol)
An HF solution (100 μ) was added dropwise, and the mixture was stirred at −30 ° C. for 2 hours. After the completion of the reaction, a saturated NH 4 Cl solution (10 ml) was added, and the mixture was extracted with ethyl acetate. After washing the organic layer with saturated saline, Na 2 S
Dried over O 4 and concentrated. The resulting mixture was subjected to silica gel chromatography (hexane: ethyl acetate = 5: 1) to give the compound (1
5) (20 mg, 44.4% yield) was obtained.

Rf(ヘキサン:酢酸エチル=5:1)=0.22、0.26(ジア
ステレオマー混合物) 実施例12((15)→(1)) 化合物(15)(10mg)のメタノール溶液(500μ)
に微量のCSAを加えて室温で1時間撹拌した。次いで、
酢酸エチル(10ml)を加えて飽和食塩水で洗浄後、Na2S
O4で乾燥し濃縮した。これをHPLC(Nucleosil 50−5,8
×300mm,hexane:EtOAc=2:1、3.0ml/分)にて分離・精
製し、化合物(1)(4mg、収率64.5%、22分に溶出)
を得た。1 H−NMR 0.89(t,J=7.1Hz) (ppm) 1.01(t,J=7.3Hz) 1.2〜1.4(br,m) 1.50(m) 1.74(m) 2.57(dd,J=6.4,16.9Hz) 2.59(dd,J=5.6,16.9Hz) 3.58(m) 3.63(m) 4.35(t,J=6.4Hz) IR(CHCl3)cm-1;3600(w),2930(s) 2860(m),2260(w) ▲〔α〕20゜ D▼=−17.0 本実施例で得られた化合物(1)を、天然より得られ
たパナキサコールを還元して得たジヒドロパナキサコー
ルと比較した。パナキサコールの還元には以下の方法を
用いた。Rf (hexane: ethyl acetate = 5: 1) = 0.22, 0.26 (mixture of diastereomers) Example 12 ((15) → (1)) Compound (15) (10 mg) in methanol (500 μ)
A small amount of CSA was added to the mixture and stirred at room temperature for 1 hour. Then
After adding ethyl acetate (10 ml) and washing with saturated saline, Na 2 S
Dried over O 4 and concentrated. This was analyzed by HPLC (Nucleosil 50-5,8
× 300mm, hexane: EtOAc = 2: 1, 3.0ml / min) to separate and purify the compound (1) (4mg, 64.5% yield, eluted in 22 minutes)
I got 1 H-NMR 0.89 (t, J = 7.1 Hz) (ppm) 1.01 (t, J = 7.3 Hz) 1.2 to 1.4 (br, m) 1.50 (m) 1.74 (m) 2.57 (dd, J = 6.4, 16.9) Hz) 2.59 (dd, J = 5.6, 16.9 Hz) 3.58 (m) 3.63 (m) 4.35 (t, J = 6.4 Hz) IR (CHCl 3 ) cm -1 ; 3600 (w), 2930 (s) 2860 ( m), 2260 (w) 〔[α] 20 ゜ D ▼ = -17.0 The compound (1) obtained in this example was compared with dihydropanaxacol obtained by reducing panaxacol obtained from nature. . The following method was used for the reduction of panaxacol.

パナキサコール(74mg)をメタノール(1.0ml)に溶
解し、撹拌しながら過剰のNaBH4を加えた。約30分後、
飽和食塩水(10ml)を加えて酢酸エチルにて抽出した。
抽出液をNa2SO4で乾燥し、濃縮後、得られた油状物質を
HPLC(Nucleosil 50−5,8×300mm,ヘキサン:酢酸エチ
ル=1:1)にて精製し、ジヒドロパナキサコール(60m
g、収率80.0%)を得た。Panakisakoru a (74 mg) was dissolved in methanol (1.0 ml), was added an excess of NaBH 4 under stirring. After about 30 minutes,
Saturated saline (10 ml) was added, and the mixture was extracted with ethyl acetate.
The extract was dried over Na 2 SO 4 and after concentration, the resulting oil was removed.
Purified by HPLC (Nucleosil 50-5, 8 × 300 mm, hexane: ethyl acetate = 1: 1), dihydropanaxacol (60 m
g, yield 80.0%).

得られたジヒドロパナキサコールと、本発明の方法で
合成された化合物(1)のNMRスペクトルを測定して比
較した。化合物(1)がジヒドロパナキサコールである
ことが確認できた。The NMR spectra of the obtained dihydropanaxacol and the compound (1) synthesized by the method of the present invention were measured and compared. Compound (1) was confirmed to be dihydropanaxacol.

───────────────────────────────────────────────────── フロントページの続き (72)発明者 牛山 敬一 大阪府茨木市下穂積1丁目1番2号 日 東電工株式会社内 ────────────────────────────────────────────────── ─── Continued on the front page (72) Inventor Keiichi Ushiyama 1-1-2 Shimohozumi, Ibaraki-shi, Osaka Nitto Denko Corporation

Claims (1)

(57)【特許請求の範囲】(57) [Claims] 【請求項1】化合物(A) (式中R1は、テトラヒドロピラニル基、トリアルキルシ
リル基のいずれかを示す。) と化合物(B) (式中R2は、テトラヒドロピラニル基、トリアルキルシ
リル基のいずれかを示し、R3はエチル基を示す。) を塩基の存在下に反応させて、化合物(C) (式中、R1及びR2は、それぞれテトラヒドロピラニル
基、トリアルキルシリル基のいずれかを示し、R3はエチ
ル基を示す。) を製造した後、酸で処理することにより化合物(1) (式中、R3はエチル基を示す。) を製造する方法。1. Compound (A) (Wherein R 1 represents one of a tetrahydropyranyl group and a trialkylsilyl group) and the compound (B) (Wherein R 2 represents any one of a tetrahydropyranyl group and a trialkylsilyl group, and R 3 represents an ethyl group.) In the presence of a base to give a compound (C) (Wherein R 1 and R 2 each represent either a tetrahydropyranyl group or a trialkylsilyl group, and R 3 represents an ethyl group.). ) (Wherein, R 3 represents an ethyl group.)
JP63225048A 1988-09-08 1988-09-08 Method for producing panaxacols Expired - Lifetime JP2720176B2 (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
JP63225048A JP2720176B2 (en) 1988-09-08 1988-09-08 Method for producing panaxacols

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
JP63225048A JP2720176B2 (en) 1988-09-08 1988-09-08 Method for producing panaxacols

Publications (2)

Publication Number Publication Date
JPH0273026A JPH0273026A (en) 1990-03-13
JP2720176B2 true JP2720176B2 (en) 1998-02-25

Family

ID=16823223

Family Applications (1)

Application Number Title Priority Date Filing Date
JP63225048A Expired - Lifetime JP2720176B2 (en) 1988-09-08 1988-09-08 Method for producing panaxacols

Country Status (1)

Country Link
JP (1) JP2720176B2 (en)

Families Citing this family (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
KR101496508B1 (en) * 2008-08-27 2015-03-03 더 트러스티이스 오브 콜롬비아 유니버시티 인 더 시티 오브 뉴욕 Compounds, compositions and methods for reducing toxicity and treating or preventing diseases

Also Published As

Publication number Publication date
JPH0273026A (en) 1990-03-13

Similar Documents

Publication Publication Date Title
EP1658295B1 (en) Regioselective synthesis of cci-779
RU2145326C1 (en) Method of preparing ginkgolide b
IE64687B1 (en) Process for the enantioselective preparation of phenylisoserine derivatives
JP2720176B2 (en) Method for producing panaxacols
Back et al. Synthesis of castasterone and formal synthesis of brassinolide from stigmasterol via a selenosulfonation approach
CN109053496B (en) Synthetic method of 3-Boc-aminomethyl cyclobutanone
JPH0639468B2 (en) Hydroquinone derivative
KR20030009347A (en) Synthesis of watersoluble 9-dihydro-paclitaxel derivatives from 9-dihydro-13-acetylbaccatin ⅲ
EP4353728A1 (en) Hydroxy thienoimidazole derivative, vinyl sulfide derivative, n-butylidene sulfide derivative, and production method for saturated straight-chain hydrocarbon-substituted thienoimidazole derivative
CN111793047B (en) Preparation method of eribulin intermediate
Guillerm et al. Deuterium or tritium labeling by ionic hydrogenation. A convenient route to specifically labeled dethiobiotin
JP3228488B2 (en) 20-Episteroid derivative and method for producing the same
PL92979B1 (en)
US5562831A (en) Method for separation of gibberellin mixtures
Piacenza Nucleophilic substitution with inversion of alcohol configuration with the reagent complex triphenylphosphine-diethyl azodicarboxylate-carboxylic acid. A convenient preparation of epicholesterol
KATAOKA et al. Synthesis and Reactions of 10-Chloro-10, 9-(epoxyalkano) selenoxanthenes and 1-Chloro-1-phenyl-3H-2, 1-benzoxaselenoles
CN115710182A (en) Preparation method of compound BCN
Bange et al. Hydroxyhalogenations of acyloxycyclohex-2-enes. Part 3. 1 Iterative 1, 2-hydroxyiodination of acetoxycyclohex-2-ene: preparation of tetraacetyl conduritol D
JP2736916B2 (en) Manufacturing method of cibeton
CN115716799A (en) Method for preparing cis-chiral-3-fluoro-4-hydroxypiperidine and derivatives thereof by reduction of organic borohydride metal reagent
CN117658967A (en) Preparation method of flavan-3, 4-diol derivative
Coville, Neil J.*, Ramsden, Jennifer A.** & Staskun Ferrocenoylacetanilides
JP3495774B2 (en) Method for producing 1-hydroxyindoles
JPS6033392B2 (en) 1,2-benzodiazepine derivative and method for producing the same
JPS6241672B2 (en)