JPS5838434B2 - Method for producing 2,3,6-trimethylhydroquinone-1-nicotinic acid ester - Google Patents

Method for producing 2,3,6-trimethylhydroquinone-1-nicotinic acid ester

Info

Publication number
JPS5838434B2
JPS5838434B2 JP12133476A JP12133476A JPS5838434B2 JP S5838434 B2 JPS5838434 B2 JP S5838434B2 JP 12133476 A JP12133476 A JP 12133476A JP 12133476 A JP12133476 A JP 12133476A JP S5838434 B2 JPS5838434 B2 JP S5838434B2
Authority
JP
Japan
Prior art keywords
nicotinic acid
acid ester
trimethylhydroquinone
reaction
chloroform
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
Application number
JP12133476A
Other languages
Japanese (ja)
Other versions
JPS5242884A (en
Inventor
憲義 末田
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.)
Nisshin Seifun Group Inc
Original Assignee
Nisshin Seifun Group Inc
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 Nisshin Seifun Group Inc filed Critical Nisshin Seifun Group Inc
Priority to JP12133476A priority Critical patent/JPS5838434B2/en
Publication of JPS5242884A publication Critical patent/JPS5242884A/en
Publication of JPS5838434B2 publication Critical patent/JPS5838434B2/en
Expired legal-status Critical Current

Links

Landscapes

  • Pyridine Compounds (AREA)
  • Plural Heterocyclic Compounds (AREA)

Description

【発明の詳細な説明】 本発明は、2・3・6−トリメチルハイドロキノン−1
−ニコチン酸エステルの製造法に関スるものである。DETAILED DESCRIPTION OF THE INVENTION The present invention provides 2,3,6-trimethylhydroquinone-1
- This relates to a method for producing nicotinic acid ester.

2・3・6−トリメチルハイドロキノンー1−ニコチン
酸エステルはビタミンEニコチン酸エステルの中間体と
して有用な物質である。2,3,6-trimethylhydroquinone-1-nicotinic acid ester is a substance useful as an intermediate for vitamin E nicotinic acid ester.

ビタミンEニコチン酸エステルはすぐれた末梢血管拡張
作用を有する持続性薬剤で、医薬上有用な物質である。Vitamin E nicotinic acid ester is a long-acting drug that has an excellent peripheral vasodilatory effect and is a pharmaceutically useful substance.

オ* 従来、ビタ
ミンEニコチン酸エステルの製法としては (1)ビタミンEにニコチン酸の反応性誘導体を反応さ
せる方法(特公昭39−24968号公報参照)、 (2)ジケテンの存在下、ビタミンEと遊離のニコチン
酸を反応させる方法(特公昭47−62号公報参照) が知られている。* Conventionally, methods for producing vitamin E nicotinic acid ester include (1) a method in which vitamin E is reacted with a reactive derivative of nicotinic acid (see Japanese Patent Publication No. 39-24968), (2) a method in which vitamin E is reacted with a reactive derivative of nicotinic acid in the presence of diketene. A method of reacting nicotinic acid with free nicotinic acid (see Japanese Patent Publication No. 47-62) is known.

しかしながら、上記(1)の方法では、生成物の収率、
純度ともに低く、精製すれば大幅に収率が低下する。However, in the method (1) above, the yield of the product,
Both purity is low, and the yield will drop significantly if purified.

また上記(2)の方法では、生成物の純度が低いのみな
らず、反応に特殊な溶媒を必要とし、工業的な製法とは
い\難い。In addition, in the method (2) above, not only the purity of the product is low, but also a special solvent is required for the reaction, and it is hardly an industrial production method.

本発明者らは、これらの欠屯を除くべく種々検討の結果
、操作が容易でかつ高収率でビタミンEニコチン酸エス
テルに誘導する一連の工業的製造法を見出すに至ったも
のである。As a result of various studies aimed at eliminating these deficiencies, the present inventors have discovered a series of industrial production methods that are easy to operate and lead to vitamin E nicotinic acid ester in high yield.

本発明方法は、2・3・6−トリメチルハイドロキノン
とニコチン酸またはその反応性誘導体とを反応させた後
加水分解することによって2・3・6−トリメチルハイ
ドロキノン−1−ニコチン酸エステルを得、次いで下式
に示すように得られた2・3・6−トリメチルハイドロ
キノン−1−ニコチン酸エステル(I)とフイトール、
インフイトールまたはそれらのハライド(9)のうちの
1つ以上とを反応させて、ビタミンEニコチン酸エステ
ル叫を得るものである。In the method of the present invention, 2,3,6-trimethylhydroquinone-1-nicotinic acid ester is obtained by reacting 2,3,6-trimethylhydroquinone with nicotinic acid or a reactive derivative thereof, followed by hydrolysis. 2,3,6-trimethylhydroquinone-1-nicotinic acid ester (I) and phytol obtained as shown in the following formula,
Vitamin E nicotinic acid esters are obtained by reacting with infitol or one or more of their halides (9).

ンまたはOH,Yはニコチン酸基を示す)前記2・3・
6−トリメチルハイドロキノン1−ニコチン酸エステル
とフイトール、イソフイトールまたはそれらのハライド
とを反応させる場合、原料の比率は当モルでもよいが、
前者の化合物に対して、後者の化合物をやや過剰に用い
て反応を行うのが好ましい。or OH, Y represents a nicotinic acid group) 2.3.
When reacting 6-trimethylhydroquinone 1-nicotinic acid ester with phytol, isophytol or their halides, the ratio of the raw materials may be equimolar, but
It is preferable to carry out the reaction using a slightly excess amount of the latter compound relative to the former compound.

触媒としては、硫酸等のブレンステツド酸、または塩化
アルミニウム、塩化第二鉄、三弗化ホウ素エーテル錯体
、塩化亜鉛等のルイス酸、またはそれらの混合物を用い
ればよい。As the catalyst, a Brønsted acid such as sulfuric acid, a Lewis acid such as aluminum chloride, ferric chloride, boron trifluoride ether complex, zinc chloride, or a mixture thereof may be used.

この触媒は2・3・6−トリメチルハイドロキノン−1
−ニコチン酸エステルに対して当モル量以上使用するこ
とが必要である。This catalyst is 2,3,6-trimethylhydroquinone-1
- It is necessary to use an equivalent molar amount or more based on the nicotinic acid ester.

溶媒は使用しなくてもよいが、原料を溶解しかつ不活性
の有機溶媒、たとえば、蟻酸、酢酸等の低級カルボン酸
、またはアセトン、メチルエチルケトン等のケトン類、
またはジオキサン、テトラヒド口フラン等のエーテル類
を使用すればさらによい結果が得られる。It is not necessary to use a solvent, but an inert organic solvent that dissolves the raw materials, such as lower carboxylic acids such as formic acid and acetic acid, or ketones such as acetone and methyl ethyl ketone,
Alternatively, better results can be obtained by using ethers such as dioxane and tetrahydrofuran.

反応温度および時間は、触媒、溶媒によって異なるが、
70〜80℃で2時間反応させれば反応は完結する。The reaction temperature and time vary depending on the catalyst and solvent, but
The reaction is completed by reacting at 70 to 80°C for 2 hours.

以上の如くして得られる反応混合物を常法にしたがって
処理すれば、ビタミンEニコチン酸エステルが収率93
%で得られる。When the reaction mixture obtained as described above is treated according to a conventional method, vitamin E nicotinic acid ester is obtained in a yield of 93.
Obtained in %.

このものは必要に応じて、たとえば、シリカゲルのカラ
ムクロマトグラフイー等を行うことにより精製すること
ができる。This product can be purified, if necessary, by, for example, silica gel column chromatography.

なお、本発明の目的生成物である2・3・6ートリメチ
ルハイトロキノンー1−ニコチン酸エステルは文献未載
の新規化合物であり、本発明方法によってほビ定量的に
製造することができる。Note that 2,3,6-trimethylhytroquinone-1-nicotinic acid ester, which is the target product of the present invention, is a new compound that has not been described in any literature, and can be produced quantitatively by the method of the present invention.

次にその具体的製造法を示せば下記のとおりである。Next, the specific manufacturing method is as follows.

第1の方法としては、トリメチルハイドロキノンとニコ
チン酸の反応性誘導体を塩基性物質の存在下にエステル
縮合させて、2・3・6−トリメチルハイドロキノン−
1・4−ジニコチン酸エステルを得る。The first method involves ester condensation of trimethylhydroquinone and a reactive derivative of nicotinic acid in the presence of a basic substance, resulting in 2,3,6-trimethylhydroquinone-
1,4-dinicotinic acid ester is obtained.

ニコチン酸の反応性誘導体としては、たとえば、酸クロ
ライド、酸無水物などがあり、塩基性物質としては、た
とえば、トリエチルアミン、ピリジン、ジメチルアニリ
ン等の第三級アミンを用いればよい。Examples of reactive derivatives of nicotinic acid include acid chlorides and acid anhydrides, and examples of basic substances include tertiary amines such as triethylamine, pyridine, and dimethylaniline.

溶媒としては、ジメチルホルムアミド、ジメチルスルホ
キシド等も用いられるが、後処理の点からクロロホルム
を用いるのが好ましい。Although dimethylformamide, dimethyl sulfoxide, etc. may be used as the solvent, it is preferable to use chloroform from the viewpoint of post-treatment.

反応温度は30〜80℃位がよく、2時間から10時間
反応させればよい。The reaction temperature is preferably about 30 to 80°C, and the reaction may be carried out for 2 to 10 hours.

こうして得た2・3・6−トリメチルハイドロキノン−
1・4ジニコチン酸エステルヲクロロホルムーメタノー
ル(1:1)中に溶解し、触媒量の水酸化ナトリウムで
加水分解して、2・3・6−トリメチルハイドロキノン
−1−ニコチン酸エステルを得る。2,3,6-trimethylhydroquinone thus obtained
The 1,4-dinicotinic acid ester is dissolved in chloroform-methanol (1:1) and hydrolyzed with a catalytic amount of sodium hydroxide to yield the 2,3,6-trimethylhydroquinone-1-nicotinic acid ester.

第2の方法としては、トリメチルハイドロキノンとニコ
チン酸を塩基性物質の存在下に、ジケテンを作用させて
エステル縮合を行イ、2・3・6トリメチルハイドロキ
ノンー1・4−ジニコチン酸エステルを得る。In the second method, trimethylhydroquinone and nicotinic acid are subjected to ester condensation in the presence of a basic substance by the action of diketene to obtain 2,3,6 trimethylhydroquinone-1,4-dinicotinic acid ester.

塩基性物質としては、トリエチルアミン、ピリジン、ジ
メチルアニリン等の第三級アミンを用いればよい。As the basic substance, tertiary amines such as triethylamine, pyridine, and dimethylaniline may be used.

溶媒としては、ジメチルホルムアミド、ジメチルスルホ
キシドまたは上記のアミンを溶媒として大過剰用いるの
もよいが、クロロホルムを用いるのが好ましい。As the solvent, dimethylformamide, dimethylsulfoxide, or the above-mentioned amines may be used in large excess, but chloroform is preferably used.

反応温度60〜80℃で1時間反応させれば反応は完結
する。The reaction is completed by reacting for 1 hour at a reaction temperature of 60 to 80°C.

こうして得た2・3・6−トリメチルハイトロキノン−
1・4−ジニコチン酸エステルを前記方法で加水分解し
て、新規な2・3・6−トリメチルハイドロキノンー1
−ニコチン酸エステルを得る。2,3,6-trimethylhytroquinone thus obtained
1,4-dinicotinic acid ester is hydrolyzed by the above method to produce novel 2,3,6-trimethylhydroquinone-1.
- obtain nicotinic acid ester.

なお、2・3・6−トリメチルハイドロキノン1−ニコ
チン酸エステルは次の性質を有する。In addition, 2,3,6-trimethylhydroquinone 1-nicotinic acid ester has the following properties.

融点 193.0℃ 元素分析 C15H15NO3として 計算値 C:70.02% H:5.88%N:5.4
4% 分析値 C:69.81% H:5.86%N:5.3
3% 赤外吸収スペクトル(nujol ) 30 80、1
730、1600、1280CrrL−l、核磁気共鳴
吸収スペクトル(アセトン−D6中、δ値)2.07(
s、6H)、2.17(s、3H)、6.66(s、I
H)、7. 6 5 ( dd、IH)8.15(bs
、IH)、s.5o(at、IH)、8.8 7 (
dd, IH)、9.3 5 ( d、IH)実施例
1 トリメチルハイドロキノン10.(1(0.066モル
)とニコチン酸クロライド塩酸塩29.3P(0.16
5モル)を乾燥クロロホルム15OrrLl中に懸濁さ
せ、室温で攪拌下、乾燥ピリジン35、0P(0.45
fモル)を滴下した後、一夜放置した。Melting point 193.0℃ Elemental analysis Calculated value as C15H15NO3 C: 70.02% H: 5.88% N: 5.4
4% Analysis value C: 69.81% H: 5.86% N: 5.3
3% Infrared absorption spectrum (nujol) 30 80, 1
730, 1600, 1280CrrL-l, nuclear magnetic resonance absorption spectrum (in acetone-D6, δ value) 2.07 (
s, 6H), 2.17 (s, 3H), 6.66 (s, I
H), 7. 6 5 (dd, IH) 8.15 (bs
, IH), s. 5o (at, IH), 8.8 7 (
dd, IH), 9.3 5 (d, IH) Example 1 Trimethylhydroquinone 10. (1 (0.066 mol) and nicotinic acid chloride hydrochloride 29.3P (0.16 mol)
5 mol) of dry chloroform was suspended in 15 OrrLl of dry chloroform and mixed with dry pyridine 35,0P (0.45 mol) under stirring at room temperature.
f mol) was added dropwise, and the mixture was left overnight.

反応液を約200rrLlの水に注ぎ、クロロホルム層
を分取した後、IN塩酸5oml、IN重炭酸ナトリウ
ム水溶液50rILl、水5Qmlで順次洗滌した後、
無水芒硝で乾燥沢過し、溶媒を減圧留去して白色結晶2
2.6S’を得た(収率95%)。The reaction solution was poured into about 200rrLl of water, the chloroform layer was separated, and then washed sequentially with 50ml of IN hydrochloric acid, 50ml of IN sodium bicarbonate aqueous solution, and 5Qml of water.
Filter it dry with anhydrous sodium sulfate and remove the solvent under reduced pressure to obtain white crystals 2.
2.6S' was obtained (yield 95%).

この結晶をクロロホルムとメタノールの1:1混合溶媒
200TLl中に溶解し、水冷攪拌下、水酸化ナトリウ
ムのメタノール溶液(5%)8TLlを滴下し、室温で
2時間放置した。The crystals were dissolved in 200 TL of a 1:1 mixed solvent of chloroform and methanol, and 8 TL of a methanol solution (5%) of sodium hydroxide was added dropwise to the solution under stirring while cooling with water, and the mixture was allowed to stand at room temperature for 2 hours.

反応液を300mlの水に注ぎ、クロロホルム層を分取
し、水層をさらにクロロホルム100mlで抽出して両
者を合わせた。The reaction solution was poured into 300 ml of water, the chloroform layer was separated, the aqueous layer was further extracted with 100 ml of chloroform, and both layers were combined.

クロロホルム溶液をIN塩酸、IN重炭酸ナトリウム水
溶液、水、各50mlで順次洗滌した後、無水芒硝で乾
燥沢過し、溶媒を減圧留去して、2・3・6−トリメチ
ルハイドロキノン−1−ニコチン酸エステルを淡黄白色
結晶として15.5f得た 収率97%)。The chloroform solution was sequentially washed with 50 ml each of IN hydrochloric acid, IN sodium bicarbonate aqueous solution, and water, then dried and filtered with anhydrous sodium sulfate, and the solvent was distilled off under reduced pressure to obtain 2,3,6-trimethylhydroquinone-1-nicotine. 15.5f of the acid ester was obtained as pale yellowish white crystals (yield 97%).

こうして得た2・3・6−トリメチルハイドロキノン−
1−ニコチン酸エステル5.14P(0.02モル)を
イソフイトール7. 4 f (0.025モル)とと
もに酢酸20rul中に溶解し、室温で攪拌下、濃硫酸
2. 0 mlを滴下し、1時間攪拌した。2,3,6-trimethylhydroquinone thus obtained
1-Nicotinic acid ester 5.14P (0.02 mol) was added to isophytol 7. 4 f (0.025 mol) in 20 rul of acetic acid and 2.0 ml of concentrated sulfuric acid was added under stirring at room temperature. 0 ml was added dropwise and stirred for 1 hour.

温度を80℃に上げ、さらに2時間反応させた後、室温
まで冷却し、イソプロビルエーテル約50rrLlで抽
出した。The temperature was raised to 80° C. and the reaction was continued for an additional 2 hours, then cooled to room temperature and extracted with about 50 rrLl of isopropyl ether.

IN重炭酸ナトリウム水、水各30縦で洗滌した後、無
水芒硝で乾燥沢過し、溶媒を減圧留去して褐色油状物を
11.6P得た。After washing with 30 increments of IN sodium bicarbonate and water, the residue was dried and filtered with anhydrous sodium sulfate, and the solvent was distilled off under reduced pressure to obtain 11.6 P of a brown oil.

シリカゲルクロマトグラフイーにて精製すると、ビタミ
ンEニコチン酸エステルを淡黄色油状物として8.77
1?得た(収率82%)。When purified by silica gel chromatography, vitamin E nicotinic acid ester was obtained as a pale yellow oil with a concentration of 8.77%.
1? (yield 82%).

冷所に放置して針状結晶850グを得た。The mixture was left in a cold place to obtain 850 g of needle-like crystals.

融点 37〜40℃ λ 2 64nm(MeOH) maX E1々82.5 元素分析 C35H5:303Nとして 計算値 C:78.46% H:9.97%N:2.6
1% 分析値 C:78.43% H:10.02%N:2.
50% 参考例 1 実施例1の方法で得た2・3・6−トリメチルハイトロ
キノン−1−ニコチン酸エステル5.142を塩化亜鉛
3.01、濃塩酸2mlとともに酢酸20ml中に溶解
した。Melting point 37-40℃ λ 2 64nm (MeOH) maX E1 each 82.5 Elemental analysis Calculated value as C35H5:303N C: 78.46% H: 9.97% N: 2.6
1% Analysis value C: 78.43% H: 10.02% N: 2.
50% Reference Example 1 5.142 of 2,3,6-trimethylhytroquinone-1-nicotinic acid ester obtained by the method of Example 1 was dissolved in 20 ml of acetic acid together with 3.01 of zinc chloride and 2 ml of concentrated hydrochloric acid.

室温で攪拌下、フィトール7.41を滴下し、1時間攪
拌した後、温度を80℃に上げ、さらに1時間反応させ
た。Phytol 7.41 was added dropwise while stirring at room temperature, and after stirring for 1 hour, the temperature was raised to 80° C. and the reaction was further continued for 1 hour.

溶媒を減圧留去した後、ヘキサン約50m−lで抽出し
、以後実施例1と同様に操作を行って、ビタミンEニコ
チン酸エステル8.67fを得た(収率81%)。After distilling off the solvent under reduced pressure, extraction was performed with about 50 ml of hexane, and the same procedure as in Example 1 was performed to obtain 8.67 f of vitamin E nicotinic acid ester (yield: 81%).

融点 37〜40℃ λmax 2 6 4 nm ( MeOH )E{
々83.0 実施例 2 トリメチルハイドロキノン10.OS’とニコチン酸無
水物3 7. 5 fをクロロホルム100$:lに加
え、さらにピリジン150mlを加えて65℃で5時間
反応させた。Melting point 37-40℃ λmax 264 nm (MeOH)E{
83.0 Example 2 Trimethylhydroquinone 10. OS' and nicotinic anhydride 3 7. 5f was added to 100 $:l of chloroform, 150 ml of pyridine was added, and the mixture was reacted at 65° C. for 5 hours.

反応後沢過して、沢液を減圧濃縮し、クロロホルムl5
0TLlを加えて可溶部分をとり水50rrtlで洗滌
した後、メタノール100mA’を加えた溶液に、室温
攪拌下に水酸化ナトリウムのメタノール溶液(5%)1
0mAを滴下して加水分解した。After the reaction, filter the filtrate, concentrate the filtrate under reduced pressure, and add 15 chloroform.
After adding 0TLl and removing the soluble portion and washing with 50rrtl of water, 100mA' of methanol was added to the solution, and a methanol solution (5%) of sodium hydroxide (5%) was added to the solution with stirring at room temperature.
Hydrolysis was carried out by dropping 0 mA.

反応液を水500771l中に注ぎ、クロロホルム層を
分取し、水層をさらにクロロホルム100縦で抽出して
両者を合わせた。The reaction solution was poured into 500,771 liters of water, the chloroform layer was separated, the aqueous layer was further extracted with 100 liters of chloroform, and both were combined.

以後常法にしたがって処理し、溶媒を減圧留去して、2
・3・6−トリメチルハイドロキノン−1−ニコチン酸
エステルを白色結晶として15.8?得た(収率93%
)。Thereafter, the treatment was carried out according to a conventional method, the solvent was distilled off under reduced pressure, and 2
・3,6-trimethylhydroquinone-1-nicotinic acid ester as white crystal 15.8? (yield 93%)
).

こうして得た2・3・6−トリメチルハイドロキノンー
1−ニコチン酸エステル5.14Pを塩化亜鉛1.Oz
塩化アルミニウム1.01とともにアセトン30TLl
に溶解し、室温攪拌下にイソフィチルクロライド7.5
1を滴下し、1時間攪拌を続げた。The thus obtained 2,3,6-trimethylhydroquinone-1-nicotinic acid ester 5.14P was mixed with 1.4P of zinc chloride. Oz
30 TLl of acetone with 1.01 aluminum chloride
of isophyl chloride under stirring at room temperature.
1 was added dropwise, and stirring was continued for 1 hour.

溶媒を留去した後、温度を80℃に上げ、2時間反応さ
せた。After distilling off the solvent, the temperature was raised to 80°C and the reaction was continued for 2 hours.

ヘキサン約701rLlで抽出した後、実施例1と同様
の操作を行って、ビタミンEニコチン酸エステル8.6
0S’を得た(収率80%)。After extraction with about 701 rL of hexane, the same operation as in Example 1 was carried out to extract 8.6 rL of vitamin E nicotinic acid ester.
0S' was obtained (yield 80%).

融点 37〜40℃ λm2,X2 6 4 nm ( MeOH )E圭々
82,5 参考例 2 実施例2の方法で得た2・3・6−トリメチルハイドロ
キノンー1−ニコチン酸エステル5.142を無水ジオ
キサン60rrLlに溶解し、インフイトール7.4z
を加え窒素気流中で室温攪拌下、三フツ化ホウ素エーテ
ル錯体4.Ozを滴下し、1時間攪拌した。Melting point 37-40°C λm2, Inphytol 7.4z dissolved in dioxane 60rrLl
Boron trifluoride ether complex 4. was added and stirred at room temperature in a nitrogen stream. Oz was added dropwise and stirred for 1 hour.

温度を80℃に上げた後、濃塩酸2S’を加えてさらに
1時間反応させた後、溶媒を減圧留去した。After raising the temperature to 80°C, concentrated hydrochloric acid 2S' was added and the reaction was continued for an additional hour, and then the solvent was distilled off under reduced pressure.

残渣をイソプロビルエーテルで抽出し、以後実施例1と
同様の操作を行って、ビタミンEニコチン酸エステル8
.6Elを得た(収率81%)C融点 37〜40℃ λmax 264nrrL(MeOH) E{層83、0 実施例 3 トリメチルハイドロキノン10.0Pとニコチン酸20
.0Fをジメチルホルムアミド50mlとピリジン3o
mlの混液に溶解し、これにジケテン12.OS’をジ
メチルホルムアミド20mlに溶解したものを徐々に加
えた。The residue was extracted with isoprobyl ether, and the same procedure as in Example 1 was performed to obtain vitamin E nicotinic acid ester 8.
.. 6El was obtained (yield 81%) C Melting point 37-40°C λmax 264nrrL (MeOH) E {layer 83,0 Example 3 Trimethylhydroquinone 10.0P and nicotinic acid 20
.. 0F with 50 ml of dimethylformamide and 30 ml of pyridine
ml of the mixed solution, and add 12.ml of diketene to it. A solution of OS' in 20 ml of dimethylformamide was gradually added.

反応温度を70℃に保って2時間攪拌を続けたあと、室
温まで冷却し、約300mlの水に注いだ。After stirring was continued for 2 hours while keeping the reaction temperature at 70° C., the mixture was cooled to room temperature and poured into about 300 ml of water.

クロロホルム100mlを使用して3回抽出し、合わせ
たクロロホルム層をIN塩酸、1N重炭酸ナ} IJウ
ム、水各50TrLlで順次洗滌したのち、無水芒硝で
乾燥戸過し、溶媒を減圧留去して得た残渣をメタノール
とアセトン混合溶媒より再結晶して、白色結晶19.1
’を得た(収率80%)。Extraction was carried out three times using 100 ml of chloroform, and the combined chloroform layers were sequentially washed with 50 TrL each of IN hydrochloric acid, 1 N sodium bicarbonate, and water, then dried over anhydrous sodium sulfate, and the solvent was distilled off under reduced pressure. The residue obtained was recrystallized from a mixed solvent of methanol and acetone to obtain white crystals 19.1
' was obtained (yield 80%).

この結晶をクロロホルムとメタノールの1:1混合溶媒
200mA’に溶解し、以後実施例1と同様の操作を行
って、2・3・6−トリメチルハイドロキノンー1−ニ
コチン酸エステルを淡黄色結晶として12.9fを得た
(収率96%)。The crystals were dissolved in 200 mA' of a 1:1 mixed solvent of chloroform and methanol, and the same procedure as in Example 1 was carried out to obtain 2,3,6-trimethylhydroquinone-1-nicotinic acid ester as pale yellow crystals. .9f was obtained (yield 96%).

こうして得た2・3・6−トリメチルハイドロキノンー
1−ニコチン酸エステル1 0.3 f?ヲ、塩化第二
鉄5.OS’とともに酢酸50rul中に溶解し、室温
攪拌下にインフイチルクロライド15.Ofを滴下し、
1時間攪拌したあと、温度を80℃に上げ、さらに1時
間反応させた。The thus obtained 2,3,6-trimethylhydroquinone-1-nicotinic acid ester 1 0.3 f? 5. Ferric chloride. Dissolve in 50 ru of acetic acid with OS' and add 15. Drop the Of,
After stirring for 1 hour, the temperature was raised to 80°C and the reaction was continued for an additional 1 hour.

酢酸を減圧留去したのち、n−へキサ7100mlで抽
出し、以後実施例1と同様の操作を行って、ビタミンE
ニコチン酸エステル17.6Fを得た(収率82%)。After acetic acid was distilled off under reduced pressure, it was extracted with 7100 ml of n-hexane, and the same procedure as in Example 1 was carried out to extract vitamin E.
Nicotinic acid ester 17.6F was obtained (yield 82%).

融点 37〜40℃ λmax 2 6 4 nm ( MeOH )E{
准83.0Melting point 37-40℃ λmax 264 nm (MeOH)E{
Standard 83.0

Claims (1)

【特許請求の範囲】[Claims] 1 2・3・6−トリメチルハイドロキノンとニコチン
酸またはその反応性誘導体とを反応させた後、次いで加
水分解することを特徴とする2・3・6−トリメチルハ
イドロキノンー1−ニコチン酸エステルの製造法。1. A method for producing 2,3,6-trimethylhydroquinone-1-nicotinic acid ester, which comprises reacting 2,3,6-trimethylhydroquinone with nicotinic acid or a reactive derivative thereof, followed by hydrolysis. .
JP12133476A 1976-10-12 1976-10-12 Method for producing 2,3,6-trimethylhydroquinone-1-nicotinic acid ester Expired JPS5838434B2 (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
JP12133476A JPS5838434B2 (en) 1976-10-12 1976-10-12 Method for producing 2,3,6-trimethylhydroquinone-1-nicotinic acid ester

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
JP12133476A JPS5838434B2 (en) 1976-10-12 1976-10-12 Method for producing 2,3,6-trimethylhydroquinone-1-nicotinic acid ester

Related Parent Applications (1)

Application Number Title Priority Date Filing Date
JP11705174A Division JPS5143763A (en) 1974-10-14 1974-10-14 Bitamin e nikochinsanesuteruno seizoho

Publications (2)

Publication Number Publication Date
JPS5242884A JPS5242884A (en) 1977-04-04
JPS5838434B2 true JPS5838434B2 (en) 1983-08-23

Family

ID=14808680

Family Applications (1)

Application Number Title Priority Date Filing Date
JP12133476A Expired JPS5838434B2 (en) 1976-10-12 1976-10-12 Method for producing 2,3,6-trimethylhydroquinone-1-nicotinic acid ester

Country Status (1)

Country Link
JP (1) JPS5838434B2 (en)

Families Citing this family (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2004046126A1 (en) * 2002-11-21 2004-06-03 Dsm Ip Assets B.V. Manufacture of tocopheryl acetate

Also Published As

Publication number Publication date
JPS5242884A (en) 1977-04-04

Similar Documents

Publication Publication Date Title
US4130566A (en) Process for producing 5-carboxy-2-acetylthiophene
JP2001233870A (en) 3-(1-hydroxypentylidene)-5-nitro-3h-benzofuran-2-one, method for producing the same and use thereof
JPS6024781B2 (en) Method for producing cis-2-hydroxy-2-phenyl-r-1-cyclohexanecarboxylic acid
EP0271275B1 (en) Trifluorohydroxyaromatic acid and preparation thereof
JPH0378395B2 (en)
JPS5838434B2 (en) Method for producing 2,3,6-trimethylhydroquinone-1-nicotinic acid ester
US3928334A (en) Process for the production of cefamandole
JP3030509B2 (en) Useful intermediates for the synthesis of delphinidin chloride
KR910009236B1 (en) Process for the preparation of n-2'-carboxyl phenyl-4-chloro anthranilic acid
US4153610A (en) Process for producing 5-carboxy-2-acetylthiophene
JP2716243B2 (en) N-benzyl-3-hydroxysuccinamic acid and method for producing the same
JP2718715B2 (en) 9,10-seco-cycloartane derivatives
JPH01238548A (en) 1,4,5,8-tetrakis(hydroxymethyl)naphthalene, its derivative and production thereof
KR910001236B1 (en) Process for the preparation of 2-(4-amino phenyl0-2-methyl propyl alcohol
JPS60197644A (en) Preparation of 2-methylamino-1-propanol derivative and its intermediate
KR900007370B1 (en) Process for the preparation of 2,4-dibromo-5-fluorobenroicacid
JPH01258668A (en) Production of dl-griseofulvin and intermediate thereof
JPH0753436A (en) Phenanthrenedicarbaldehyde, its intermdiate and its preparation
JPS59163370A (en) Preparation of 0-(aminomethyl)phenylacetic lactam
JPS6270336A (en) Production of cyclopentane-1,3-dione
JPH02204469A (en) 1,8-bis(2-hydroxyethyl)naphthalene, derivative thereof and preparation thereof
JPH07145162A (en) Production of 4h-pyran-4-one
JPS603382B2 (en) Novel production method for isoindoline derivatives
JPH0128013B2 (en)
JPS604835B2 (en) Manufacturing method of neothramycin