JPH054944A - Optically active compound and liquid crystal composition containing the same compound - Google Patents
Optically active compound and liquid crystal composition containing the same compoundInfo
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- JPH054944A JPH054944A JP27052991A JP27052991A JPH054944A JP H054944 A JPH054944 A JP H054944A JP 27052991 A JP27052991 A JP 27052991A JP 27052991 A JP27052991 A JP 27052991A JP H054944 A JPH054944 A JP H054944A
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- optically active
- formula
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Abstract
Description
【0001】[0001]
【産業上の利用分野】本発明は新規な光学活性化合物及
びこの光学活性化合物を用いたカイラル液晶組成物に関
する。FIELD OF THE INVENTION The present invention relates to a novel optically active compound and a chiral liquid crystal composition using the optically active compound.
【0002】[0002]
【従来の技術】液晶表示素子は低駆動電圧、低消費電
力、薄形・軽量等の特徴があり、電卓、時計、テレビ等
に適用されている。これらの表示材料には現在ネマチッ
ク液晶が広く用いられているが、応答速度が数十msec.
と遅いという欠点があった。この点の改善の試みの一つ
として、強誘電性液晶を利用する表示方式が提案されて
いる〔N.A.クラーク(N.A.Clark )ら、アプラ
イド フィジクス レターズ( Applied Phys.Lett. )
第36巻、第899頁(1980)〕。この方式は強誘
電性液晶のカイラルスメクチックC相(以下Sc* 相と
略記する) を利用するものであり、強誘電性液晶材料に
は室温を含む広い温度範囲でSc* 相を示すこと、自発
分極が大きいこと、適当なチルト角を持つこと、回転粘
度が小さいこと、長いら旋ピッチを持つこと、化学的に
安定であること等が要求される。しかし、これらの条件
をすべて満たす強誘電性液晶化合物は知られていない。
このため、強誘電性液晶を電気光学素子として実用に用
いる場合には、数種の強誘電性液晶あるいは強誘電性を
誘起する化合物並びに非強誘電性液晶を混合して組成物
として用いる必要がある。Sc* 液晶組成物を得るに
は、Sc* 相を示す化合物を複数混合する方法、Sc*
相を示す化合物に非強誘電性液晶を混合する方法、Sc
相を示す光学活性でない化合物あるいは液晶組成物に光
学活性化合物を添加する方法があり、最後の方法が低粘
度で高速応答をうることが容易であると考えられるた
め、現在では主流になりつつある。2. Description of the Related Art Liquid crystal display devices are characterized by low driving voltage, low power consumption, thinness and light weight, and are applied to calculators, watches, televisions and the like. Currently, nematic liquid crystals are widely used for these display materials, but the response speed is several tens of msec.
There was a drawback that it was slow. As one of attempts to improve this point, a display system using a ferroelectric liquid crystal has been proposed [N. A. Clark et al., Applied Phys. Lett.
36, 899 (1980)]. This method utilizes a chiral smectic C phase (hereinafter abbreviated as Sc * phase) of a ferroelectric liquid crystal, and the ferroelectric liquid crystal material exhibits the Sc * phase in a wide temperature range including room temperature. It is required that the polarization be large, have an appropriate tilt angle, have a small rotational viscosity, have a long helical pitch, be chemically stable, and the like. However, a ferroelectric liquid crystal compound satisfying all of these conditions is not known.
Therefore, when the ferroelectric liquid crystal is practically used as an electro-optical element, it is necessary to mix several kinds of ferroelectric liquid crystals or compounds that induce ferroelectricity and non-ferroelectric liquid crystals and use them as a composition. is there. To obtain a Sc * liquid crystal composition, a method of mixing a plurality of compounds having a Sc * phase is used .
Method for mixing non-ferroelectric liquid crystal with a compound exhibiting a phase, Sc
There is a method of adding an optically active compound to a non-optically active compound exhibiting a phase or a liquid crystal composition, and the final method is considered to be easy to obtain a low-viscosity and high-speed response. Therefore, it is becoming the mainstream at present. .
【0003】[0003]
【発明が解決しようとする課題】添加する光学活性化合
物としては、それ自身大きな自発分極を示すか組成物中
で大きな自発分極を誘起する性質を持つほか、長いら旋
ピッチを与えるものであることが望ましい。本発明の目
的は、化学的に安定で、それ自身大きな自発分極を示す
かSc液晶組成物に添加することにより大きな自発分極
を誘起するという性質をもつ新規な光学活性化合物を提
供すると共に、この光学活性化合物を用いてSc* 相の
温度範囲が広く、かつ高速で応答する新規な強誘電性液
晶材料を提供することにある。The optically active compound to be added has such a property that it exhibits a large spontaneous polarization or induces a large spontaneous polarization in the composition, and that it gives a long helical pitch. Is desirable. The object of the present invention is to provide a novel optically active compound which is chemically stable and exhibits a large spontaneous polarization by itself or induces a large spontaneous polarization by being added to a Sc liquid crystal composition. An object of the present invention is to provide a novel ferroelectric liquid crystal material having a wide temperature range of Sc * phase using an optically active compound and responding at high speed.
【0004】[0004]
【課題を解決するための手段】本発明を概説すれば、本
発明の第1の発明は一般式(化1):The present invention will be summarized as follows. The first invention of the present invention is represented by the general formula (Formula 1):
【0005】[0005]
【化1】 [Chemical 1]
【0006】〔式中、Rは炭素数16以下の直鎖状又は
分岐状アルキル基(Xと一致するものは除く)又はアル
コキシ基、R* は炭素数16以下の光学活性アルキル
基、Xはメチル基、エチル基、フッ素:塩素、ニトリル
基のいずれか、Yは−COO−、−OCO−、−O−の
いずれか、式(化2):[Wherein R is a linear or branched alkyl group having 16 or less carbon atoms (excluding those corresponding to X) or an alkoxy group, R * is an optically active alkyl group having 16 or less carbon atoms, and X is A methyl group, an ethyl group, fluorine: chlorine, or a nitrile group, Y represents any one of —COO—, —OCO—, and —O—;
【0007】[0007]
【化2】 で示される基は、下記式(化3):[Chemical 2] The group represented by is represented by the following formula (Formula 3):
【0009】[0009]
【化3】 [Chemical 3]
【0010】(Zは水素、ハロゲン、ニトリル基のいず
れか)で示される基のいずれか、C* は光学活性炭素を
示し、mは0又は1、nは1又は2であるが、m+n≦
2である〕で表される光学活性化合物で表されることを
特徴とする。(Z is any one of hydrogen, halogen, and nitrile group), C * is optically active carbon, m is 0 or 1, n is 1 or 2, and m + n≤
It is represented by the optically active compound represented by 2].
【0011】そして、本発明の第2の発明はカイラル液
晶組成物に関する発明であって、第1の発明の光学活性
化合物を少なくとも1成分含有することを特徴とする。A second invention of the present invention relates to a chiral liquid crystal composition, which is characterized by containing at least one component of the optically active compound of the first invention.
【0012】本発明の第1の特徴は、コア部にカルボニ
ル基を直結させた部分構造の採用により、大きな自発分
極を誘起する光学活性化合物を実現したことにある。液
晶性化合物の自発分極は液晶の分子軸に垂直なダイポー
ルに起因している。従来報告されている強誘電性液晶で
は、エステル基又はエーテル基のダイポールを利用する
ものがほとんどであった。コアと光学活性炭素に挟まれ
たダイポールをエーテル基、エステル基からカルボニル
基に替えることにより、これらの基の持つグループモー
メントにほぼ比例して自発分極は増大する。カルボニル
基と光学活性炭素の間にはメチレン基が介在してもよい
が、カルボニル基と光学活性炭素を直結させることが自
発分極を増大させる上で顕著な効果がある。1−位に光
学活性炭素を持つR* 基の例として1−メチルプロピル
基、1−メチルブチル基、1−メチルペンチル基、1−
メチルヘキシル基、1−メチルヘプチル基、1−メチル
オクチル基、1−メチルノニル基、1−メチルデシル
基、1−メチルウンデシル基、1−メチルドデシル基、
1,3−ジメチルブチル基、1,6−ジメチルヘプチル
基などが挙げられる。液晶性を高めるためには、カルボ
ニル基と光学活性炭素の間にメチレン基を導入すること
が望ましい。その例として、2−メチルブチル基、2−
メチルペンチル基、2−メチルヘキシル基、3−メチル
ペンチル基、4−メチルヘキシル基などが挙げられる。The first feature of the present invention is to realize an optically active compound which induces a large spontaneous polarization by employing a partial structure in which a carbonyl group is directly bonded to the core portion. The spontaneous polarization of a liquid crystal compound is caused by a dipole perpendicular to the molecular axis of liquid crystal. Most of the ferroelectric liquid crystals reported so far use an ester group or ether group dipole. When the dipole sandwiched between the core and optically active carbon is changed from an ether group or an ester group to a carbonyl group, the spontaneous polarization increases almost in proportion to the group moment of these groups. A methylene group may be interposed between the carbonyl group and the optically active carbon, but the direct connection of the carbonyl group and the optically active carbon has a remarkable effect in increasing spontaneous polarization. Examples of the R * group having optically active carbon at the 1-position are 1-methylpropyl group, 1-methylbutyl group, 1-methylpentyl group, 1-
Methylhexyl group, 1-methylheptyl group, 1-methyloctyl group, 1-methylnonyl group, 1-methyldecyl group, 1-methylundecyl group, 1-methyldodecyl group,
Examples thereof include a 1,3-dimethylbutyl group and a 1,6-dimethylheptyl group. In order to improve liquid crystallinity, it is desirable to introduce a methylene group between the carbonyl group and the optically active carbon. Examples thereof include 2-methylbutyl group, 2-
Examples thereof include a methylpentyl group, a 2-methylhexyl group, a 3-methylpentyl group and a 4-methylhexyl group.
【0013】本発明の第2の特徴は、1分子内に、上記
のカルボニル基を含む光学活性基(光学活性アルカノイ
ル基)と、他の光学活性基とを、コア部を挟んで導入し
たことである。2個の光学活性基が引起こす自発分極の
符号が同じである場合には、それぞれの光学活性基を単
独に有する化合物よりも大きな自発分極を示すか誘起す
る化合物を得ることができる。また2個の光学活性基が
引起こすら旋の向きが逆向きである場合には、ら旋が打
消し合って分子全体としてのら旋ピッチが長くなること
が期待される。The second feature of the present invention is that the above-mentioned optically active group containing a carbonyl group (optically active alkanoyl group) and another optically active group are introduced into one molecule with the core portion sandwiched therebetween. Is. When the signs of spontaneous polarization caused by two optically active groups are the same, it is possible to obtain a compound exhibiting or inducing a larger spontaneous polarization than a compound having each optically active group alone. Further, when the directions of the helices caused by the two optically active groups are opposite to each other, it is expected that the helices cancel each other out to increase the helix pitch of the molecule as a whole.
【0014】2個の光学活性基が引起こす自発分極の符
号を同じにするためには、以下のような組合せをとる必
要がある。In order to make the signs of the spontaneous polarization caused by the two optically active groups the same, the following combinations must be taken.
【0015】 奇数位に分岐を有するR* 基を持つア
ルカノイル基の絶対配置が(S)である場合、
O−の絶対配置は、Rがアルキル基であれば(R)、
キシ基でかつXがメチル基であれば(R)である。When the absolute configuration of the alkanoyl group having an R * group having an odd number of branches is (S), The absolute configuration of O- is (R) when R is an alkyl group, If it is an oxy group and X is a methyl group, it is (R).
【0016】 奇数位に分岐を有するR* 基を持つア
ルカノイル基の絶対配置が(R)である場合、
O−の絶対配置は、Rがアルキル基であれば(S)、
キシ基でかつXがメチル基であれば(S)である。When the absolute configuration of the alkanoyl group having an R * group having a branch at an odd number position is (R), The absolute configuration of O- is (S) when R is an alkyl group, If it is a xy group and X is a methyl group, it is (S).
【0017】 偶数位に分岐を有するR* 基を持つア
ルカノイル基の絶対配置が(S)である場合、
O−の絶対配置は、Rがアルキル基であれば(S)、
キシ基でかつXがメチル基であれば(S)である。When the absolute configuration of the alkanoyl group having an R * group having a branch at an even position is (S), The absolute configuration of O- is (S) when R is an alkyl group, If it is a xy group and X is a methyl group, it is (S).
【0018】 偶数位に分岐を有するR* 基を持つア
ルカノイル基の絶対配置が(R)である場合、
O−の絶対配置は、Rがアルキル基であれば(R)、
キシ基でかつXがメチル基であれば(R)である。When the absolute configuration of the alkanoyl group having an R * group having a branch at an even position is (R), The absolute configuration of O- is (R) when R is an alkyl group, If it is an oxy group and X is a methyl group, it is (R).
【0019】2個の光学活性基が引起こす自発分極の符
号が同じである組合せのうち、1−位に分岐を有するR
* 基を持つ化合物は、特に大きな自発分極を与える。Among the combinations in which the signs of spontaneous polarization caused by two optically active groups are the same, R having a branch at the 1-position
A compound having a * group gives a particularly large spontaneous polarization.
【0020】ら旋ピッチの長い化合物を得るためには、
2個の光学活性基が引起こすら旋の向きが逆向きになる
ようにする必要がある。1−位に分岐を有するR* 基を
持ち、絶対配置が(S)であるアルカノイル基と、Rが
アルコキシ基で、かつXがメチル基である、絶対配置
(R)の光学活性基を組合せた化合物は、その例であ
る。この化合物は、自発分極の符号も一致するため、大
きな自発分極をも示すという点で極めて有用な化合物で
ある。To obtain a compound having a long helical pitch,
It is necessary to make the directions of the helix caused by the two optically active groups opposite to each other. A combination of an alkanoyl group having an R * group having a branch at the 1-position and having an absolute configuration (S) and an optically active group having an absolute configuration (R) in which R is an alkoxy group and X is a methyl group. The compounds are examples. Since this compound also has the same sign of spontaneous polarization, it is a very useful compound in that it also exhibits large spontaneous polarization.
【0021】一般式(化1)中、Rとしてはメチル基、
エチル基、プロピル基、ブチル基、ペンチル基、ヘキシ
ル基、ヘプチル基、オクチル基等の直鎖状アルキル基、
メトキシ基、エトキシ基、プロピルオキシ基、ブトキシ
基、ペンチルオキシ基、ヘキシルオキシ基、ヘプチルオ
キシ基、オクチルオキシ基等の直鎖状のアルコキシ基、
イソプロピル基、1−メチルプロピル基、1−メチルブ
チル基、1−メチルペンチル基、1−メチルヘキシル
基、1−メチルヘプチル基、1−メチルオクチル基、
1,3−ジメチルペンチル基、2−メチルブチル基、3
−メチルヘキシル基、2,6−ジメチルヘプチル基等の
分岐状アルキル基及び対応するアルコキシ基が例として
挙げられるが、大きな自発分極を得るためには、分岐し
たアルキル基又はアルコキシ基の方が望ましい。In the general formula (Formula 1), R is a methyl group,
Linear alkyl groups such as ethyl group, propyl group, butyl group, pentyl group, hexyl group, heptyl group, octyl group,
Linear alkoxy groups such as methoxy group, ethoxy group, propyloxy group, butoxy group, pentyloxy group, hexyloxy group, heptyloxy group, octyloxy group,
Isopropyl group, 1-methylpropyl group, 1-methylbutyl group, 1-methylpentyl group, 1-methylhexyl group, 1-methylheptyl group, 1-methyloctyl group,
1,3-dimethylpentyl group, 2-methylbutyl group, 3
Examples include branched alkyl groups such as -methylhexyl group and 2,6-dimethylheptyl group, and corresponding alkoxy groups, but branched alkyl groups or alkoxy groups are preferable in order to obtain large spontaneous polarization. .
【0022】コアにハロゲン又はシアノ基を導入するこ
とは、液晶性を高めるための手段として、また自発分極
を増大させるための手段としてしばしば用いられるが、
本発明においてもこの方法は有効である。すなわち、フ
ッ素、塩素、臭素やシアノ基の導入は、液晶性を高め、
自発分極の増大に効果を発揮する。Introduction of a halogen or cyano group into the core is often used as a means for increasing liquid crystallinity and a means for increasing spontaneous polarization.
This method is also effective in the present invention. That is, the introduction of fluorine, chlorine, bromine or a cyano group enhances liquid crystallinity,
It is effective in increasing spontaneous polarization.
【0023】本発明において、一般式(化1)で示され
る光学活性化合物を含有するカイラル液晶組成物の他の
成分は、強誘電性の液晶性化合物であってもよく、また
カイラルでない液晶性化合物でもよい。In the present invention, the other component of the chiral liquid crystal composition containing the optically active compound represented by the general formula (Formula 1) may be a ferroelectric liquid crystal compound, or a non-chiral liquid crystallinity. It may be a compound.
【0024】〔化合物の製造方法〕一般式(化1)で表
される光学活性化合物は、例えば下記一般式(化4):[Production Method of Compound] The optically active compound represented by the general formula (Formula 1) is, for example, the following general formula (Formula 4):
【0025】[0025]
【化4】 [Chemical 4]
【0026】で表される化合物のような光学活性なフェ
ノール誘導体と、下記一般式(化5):An optically active phenol derivative such as a compound represented by the following general formula (Formula 5):
【0027】[0027]
【化5】 [Chemical 5]
【0028】で表される化合物のような光学活性なカル
ボン酸をジシクロヘキシルカルボジイミドのような脱水
剤存在下に反応させて得られる〔式中、R、C* 、X、
Y、R* 、(化2)、m及びnは前記に同じ〕。It is obtained by reacting an optically active carboxylic acid such as a compound represented by the formula (I) with R, C * , X, and X in the presence of a dehydrating agent such as dicyclohexylcarbodiimide.
Y, R * , (Chemical Formula 2), m and n are the same as above].
【0029】[0029]
【化6】 [Chemical 6]
【0030】一般式(化4)で示される光学活性なフェ
ノール誘導体は例えば次のような経路で合成し得る。The optically active phenol derivative represented by the general formula (Formula 4) can be synthesized, for example, by the following route.
【0031】[0031]
【化7】 [Chemical 7]
【0032】[0032]
【化8】 [Chemical 8]
【0033】[0033]
【化9】 [Chemical 9]
【0034】〔式中、R、C* 、X、Y、(化2)、及
びmは前記に同じ。また、R′はメチル基又はエチル基
を、Tsはp−トルエンスルホニル基を表す〕[In the formula, R, C * , X, Y, (Chemical Formula 2), and m are the same as above. R'represents a methyl group or an ethyl group, and Ts represents a p-toluenesulfonyl group.]
【0035】また、一般式(化5)で示される光学活性
なカルボン酸は例えば次のような経路で合成できる(式
中、R* 及びnは前記に同じ)。The optically active carboxylic acid represented by the general formula (Formula 5) can be synthesized, for example, by the following route (in the formula, R * and n are the same as above).
【0036】[0036]
【化10】 [Chemical 10]
【0037】[0037]
【化11】 [Chemical 11]
【0038】[0038]
【実施例】以下、本発明を実施例により詳細に説明する
が本発明はこれらの実施例に限定されない。EXAMPLES The present invention will now be described in detail with reference to examples, but the present invention is not limited to these examples.
【0039】実施例1
(R)−2−n−ヘキシルオキシプロピオン酸(S)−
4−{4′−〔4−(2−メチル)ブチロイル〕ベンゾ
イルオキシ−1,1′−ビフェニル}
〔一般式(化1)において、Rがn−ヘキシルオキシ
基、Xがメチル基、Yが
が1である化合物〕Example 1 (R) -2-n-hexyloxypropionic acid (S)-
4- {4 '-[4- (2-methyl) butyroyl] benzoyloxy-1,1'-biphenyl} [In the general formula (1), R is n-hexyloxy group, X is methyl group, and Y is Wherein 1 is 1]
【0040】(1)(S)−2−メチル酪酸塩化物の合
成
(S)−2−メチル酪酸40g(0.39モル)と塩化
チオニル70gを混合し、徐々に加温し、50〜60℃
で2時間反応させた。反応後濃縮し、残渣を常圧蒸留し
てb.p.116〜118℃留分の(S)−2−メチル酪酸
塩化物42gを無色油状物として得た。(1) Synthesis of (S) -2-methylbutyric acid chloride 40 g (0.39 mol) of (S) -2-methylbutyric acid and 70 g of thionyl chloride are mixed and gradually heated to 50-60. ℃
And reacted for 2 hours. After the reaction, the mixture was concentrated, and the residue was distilled under atmospheric pressure to obtain 42 g of (S) -2-methylbutyric acid chloride fraction having a bp of 116 to 118 ° C. as a colorless oil.
【0041】(2)(S)−4−アミノ(2−メチル)
ブチロフェノンの合成
(1)で得た(S)−2−メチル酪酸塩化物36.2g
(0.3モル)をアセトアニリド27.0g(0.2モ
ル)、無水塩化アルミニウム107g及び1,2−ジク
ロロエタン500ml中に注入し、かくはん還流を3時間
行った。反応液を冷却後、希塩酸水溶液中に注入し、有
機層を分取し、水洗した後、溶剤留去して得た残渣を6
N塩酸200ml中でかくはん還流を4時間行った。冷
後、反応液を20%カセイソーダ水溶液で中和し、塩化
メチレン抽出(100ml×2)し、有機層を水洗、濃縮
した後、残渣をカラム分離(充てん剤:ワコーゲルC−
200;溶離液:n−ヘキサン/酢酸エチル=3/1)
し、(S)−4−アミノ−(2−メチル)ブチロフェノ
ン10.3gを微黄色油状物として得た。〔α〕D 25:
+21.5°(c=0.98,CHCl3 )。(2) (S) -4-amino (2-methyl)
36.2 g of (S) -2-methylbutyric acid chloride obtained in the synthesis (1) of butyrophenone
(0.3 mol) was poured into 27.0 g (0.2 mol) of acetanilide, 107 g of anhydrous aluminum chloride and 500 ml of 1,2-dichloroethane, and the mixture was stirred and refluxed for 3 hours. After cooling the reaction solution, it was poured into a dilute hydrochloric acid aqueous solution, the organic layer was separated, washed with water, and the solvent was distilled off to obtain a residue of 6
The mixture was stirred and refluxed in 200 ml of N hydrochloric acid for 4 hours. After cooling, the reaction solution was neutralized with a 20% caustic soda aqueous solution, extracted with methylene chloride (100 ml x 2), the organic layer was washed with water and concentrated, and the residue was separated by column (filler: Wakogel C-
200; Eluent: n-hexane / ethyl acetate = 3/1)
Then, 10.3 g of (S) -4-amino- (2-methyl) butyrophenone was obtained as a pale yellow oil. [Α] D 25 :
+ 21.5 ° (c = 0.98, CHCl 3 ).
【0042】[0042]
【化12】 [Chemical 12]
【0043】IR(neat) :3370,3280,29
40,2850,1660,1605cm-1。IR (neat): 3370, 3280, 29
40, 2850, 1660, 1605 cm -1 .
【0044】(3)(S)−4−(2−メチルブチロイ
ル)安息香酸の合成
(2)で得た(S)−4−アミノ−(2−メチル)ブチ
ロフェノン8.9g(0.05モル)を濃塩酸20ml及
び水20ml中に溶解し、0〜5℃で亜硝酸ナトリウム
4.3g(0.06モル)を水10mlに溶解した液を滴
下し、同温度で1時間かくはんした。反応液を中和後、
CuCN 14.1g(0.157モル)を冷水200
mlに溶解した液に注入し、次いで30分間、かくはん還
流した。反応液を冷却後、エチルエーテル100mlで2
回抽出し、有機層を分取し、水洗し、次いで溶剤留去
し、残渣を40%硫酸水溶液100ml中で3時間還流反
応させた。冷後、析出晶をろ取、水洗し、水−エタノー
ルより再結晶して(S)−4−(2−メチルブチロイ
ル)安息香酸4.6gを白色結晶として得た。mp. 1
01〜103.5℃。
〔α〕D 25:+21.8°(c=1.0,CHC
l3 )。(3) Synthesis of (S) -4- (2-methylbutyroyl) benzoic acid (S) -4-amino- (2-methyl) butyrophenone obtained in (2) 8.9 g (0.05) Mol) was dissolved in 20 ml of concentrated hydrochloric acid and 20 ml of water, and a solution of 4.3 g (0.06 mol) of sodium nitrite in 10 ml of water was added dropwise at 0 to 5 ° C., and the mixture was stirred at the same temperature for 1 hour. After neutralizing the reaction solution,
CuCN 14.1 g (0.157 mol) in cold water 200
It was poured into a solution dissolved in ml and then stirred and refluxed for 30 minutes. After cooling the reaction mixture, 2 ml with 100 ml of ethyl ether.
It was extracted twice, the organic layer was separated, washed with water, then the solvent was distilled off, and the residue was refluxed in 100 ml of 40% aqueous sulfuric acid for 3 hours. After cooling, the precipitated crystals were collected by filtration, washed with water, and recrystallized from water-ethanol to obtain 4.6 g of (S) -4- (2-methylbutyroyl) benzoic acid as white crystals. mp. 1
01-103.5 ° C. [Α] D 25 : + 21.8 ° (c = 1.0, CHC
l 3 ).
【0045】[0045]
【化13】[Chemical 13]
【0046】IR( KBr ):2950,2870,26
50,2540,1680,1605cm-1。IR (KBr): 2950, 2870, 26
50, 2540, 1680, 1605 cm -1 .
【0047】(4)(R)−4−ヒドロキシ−4′−
(2−n−ヘキシルオキシ)プロパノイルオキシ−1,
1′−ビフェニルの合成
(R)−2−n−ヘキシルプロピオン酸塩化物3.9g
(20ミリモル)を4,4′−ジヒドロキシ−1,1′
−ビフェニル3.9g(20ミリモル)、ピリジン40
ml及び塩化メチレン40mlの溶液中に室温で滴下し、同
温度で2時間かくはん反応させた。反応液を希塩酸15
0ml中に注入し、塩化メチレン100mlで2回抽出し、
有機層を水100mlで3回洗浄後、無水MgSO4 で乾
燥した。溶剤留去後、残渣をカラム精製(充てん剤:ワ
コーゲルC−200;溶離液:n−ヘキサン/酢酸エチ
ル=5/1)して(R)−4−ヒドロキシ−4′−(2
−n−ヘキシルオキシ)プロパノイルオキシ−1,1′
−ビフェニル3.2gを白色結晶として得た。mp.9
1〜94.5℃。
〔α〕D 25:+39.4°(c=0.97,CHC
l3)。(4) (R) -4-hydroxy-4'-
(2-n-hexyloxy) propanoyloxy-1,
Synthesis of 1'-biphenyl (R) -2-n-hexylpropionyl chloride 3.9 g
(20 mmol) was added to 4,4'-dihydroxy-1,1 '
-Biphenyl 3.9 g (20 mmol), pyridine 40
ml and methylene chloride 40 ml at room temperature, and the mixture was stirred at the same temperature for 2 hours. Dilute hydrochloric acid 15
Pour into 0 ml and extract twice with 100 ml methylene chloride,
The organic layer was washed 3 times with 100 ml of water and dried over anhydrous MgSO 4 . After the solvent was distilled off, the residue was subjected to column purification (filler: Wakogel C-200; eluent: n-hexane / ethyl acetate = 5/1) and (R) -4-hydroxy-4 '-(2
-N-hexyloxy) propanoyloxy-1,1 '
3.2 g of biphenyl were obtained as white crystals. mp. 9
1-94.5 ° C. [Α] D 25 : + 39.4 ° (c = 0.97, CHC
l 3 ).
【0048】[0048]
【化14】 [Chemical 14]
【0049】IR( KBr ) :3400,2950,28
60,1740,1605cm-1。IR (KBr): 3400, 2950, 28
60,1740,1605 cm -1 .
【0050】(5)(R)−2−n−ヘキシルオキシプ
ロピオン酸(S)−4−{4′−〔4−(2−メチル)
ブチロイル〕ベンゾイルオキシ−1,1′−ビフェニ
ル}の合成
(3)で得た(S)−4−(2−メチルブチロイル)安
息香酸1.1g(5.3ミリモル)及びジシクロヘキシ
ルカルボジイミド1.3g(6.1ミリモル)を塩化メ
チレン50mlに溶解し、10℃以下で(4)で得た
(R)−4−ヒドロキシ−4′−(2−n−ヘキシルオ
キシ)プロパノイルオキシ−1,1′−ビフェニル1.
7g(5.0ミリモル)を塩化メチレン25mlに溶解し
た液を滴下し、室温で24時間かくはん反応させた。反
応後、析出物をろ別し、ろ液を減圧濃縮し、残渣をカラ
ム分離{充てん剤:ワコーゲルC−200〔和光純薬工
業(株)製〕;溶離液:n−ヘキサン/酢酸エチル=2
0/1}して得た粗結晶1.3gをエタノールより再結
晶して(R)−2−n−ヘキシルオキシプロピオン酸
(S)−4−{4′−〔4−(2−メチル)ブチロイ
ル〕ベンゾイルオキシ−1,1′−ビフェニル}600
mgを白色針状晶として得た。
mp. 74.0〜76.0℃及び100.5〜101.
5℃。
〔α〕D 25:+42.1°(c=0.35,CHC
l3)。(5) (R) -2-n-hexyloxypropionic acid (S) -4- {4 '-[4- (2-methyl)
Synthesis of (butyroyl] benzoyloxy-1,1′-biphenyl} 1.1 g (5.3 mmol) of (S) -4- (2-methylbutyroyl) benzoic acid obtained in (3) and 1.3 g of dicyclohexylcarbodiimide (6.1 mmol) was dissolved in 50 ml of methylene chloride and (R) -4-hydroxy-4 '-(2-n-hexyloxy) propanoyloxy-1,1 obtained in (4) at 10 ° C or lower. ′ -Biphenyl 1.
A solution prepared by dissolving 7 g (5.0 mmol) in 25 ml of methylene chloride was added dropwise, and the mixture was stirred at room temperature for 24 hours. After the reaction, the precipitate was filtered off, the filtrate was concentrated under reduced pressure, and the residue was column-separated (filler: Wakogel C-200 [manufactured by Wako Pure Chemical Industries, Ltd.]; eluent: n-hexane / ethyl acetate = Two
The crude crystal 1.3 g obtained by 0/1} was recrystallized from ethanol to give (R) -2-n-hexyloxypropionic acid (S) -4- {4 ′-[4- (2-methyl)). Butyroyl] benzoyloxy-1,1′-biphenyl} 600
mg was obtained as white needles. mp. 74.0 to 76.0 ° C and 100.5 to 101.
5 ° C. [Α] D 25 : + 42.1 ° (c = 0.35, CHC
l 3 ).
【0051】[0051]
【化15】 [Chemical 15]
【0052】IR( KBr ) :2950,2870,17
70,1740,1680,1605cm-1。
元素分析値(C33H38O6 )
計算値:C% 74.69;H% 7.22
実測値:C% 74.77;H% 7.04IR (KBr): 2950, 2870, 17
70, 1740, 1680, 1605 cm -1 . Elemental analysis (C 33 H 38 O 6) Calculated: C% 74.69; H% 7.22 Found: C% 74.77; H% 7.04
【0053】実施例2
(R)−2−(1−メチルブトキシ)プロピオン酸
(S)−4−{4′−〔4−(2−メチル)ブチロイ
ル〕ベンゾイルオキシ−1,1′−ビフェニル}
〔一般式(化1)においてRが1−メチルブトキシ基、
Xがメチル基、Yが
1である化合物〕Example 2 (R) -2- (1-methylbutoxy) propionic acid (S) -4- {4 '-[4- (2-methyl) butyroyl] benzoyloxy-1,1'-biphenyl} [In the general formula (Formula 1), R is a 1-methylbutoxy group,
X is a methyl group, Y is Compound that is 1]
【0054】(1)4−ブロモベンジル−(1−エトキ
シ)エチルエーテルの合成
p−ブロモベンジルアルコール11.2g(60ミリモ
ル)、エチルビニルエーテル5.4g(75ミリモル)
及びp−トルエンスルホン酸ピリジニウム0.37gを
塩化メチレン100mlに溶解し、室温で20時間かくは
ん反応させた。反応後、水150mlで2回洗浄し、無水
MgSO4 で乾燥した後、溶剤留去して残渣の4−ブロ
モベンジル−(1−エトキシ)エチルエーテル15.4
gを無色油状物として得た。(1) Synthesis of 4-bromobenzyl- (1-ethoxy) ethyl ether 11.2 g (60 mmol) of p-bromobenzyl alcohol, 5.4 g (75 mmol) of ethyl vinyl ether.
And 0.37 g of pyridinium p-toluenesulfonate were dissolved in 100 ml of methylene chloride and stirred at room temperature for 20 hours. After the reaction, it was washed twice with 150 ml of water, dried over anhydrous MgSO 4 , and the solvent was distilled off to give the residue 4-bromobenzyl- (1-ethoxy) ethyl ether 15.4.
g was obtained as a colorless oil.
【0055】[0055]
【化16】 [Chemical 16]
【0056】IR( neat ):2990cm-1。IR (neat): 2990 cm -1 .
【0057】(2)(S)−4−(2−メチル)ブチロ
イルベンジルアルコールの合成
金属マグネシウム0.64gと(1)で得た4−ブロモ
ベンジル−(1−エトキシ)エチルエーテル5.18g
(20ミリモル)をテトラヒドロフラン中で反応させて
得たグリニャール試薬を−65℃に冷却し、これに実施
例1の(1)で得た(S)−2−メチル酪酸塩化物2.
37g(19.8ミリモル)の塩化メチレン溶液(20
ml)を−70〜−65℃で滴下し、同温度で3時間、次
いで室温で1時間かくはん反応させた。反応液を0℃に
冷却し、1N塩酸30mlを滴下し、同温度で1時間かく
はんした後、酢酸エチル70mlで2回抽出し、次いで有
機層を水100mlで3回洗浄後、無水MgSO4 で乾燥
した。乾燥剤をろ別後、溶剤留去し残渣の(S)−4−
(2−メチル)ブチロイルベンジルアルコール2.4g
を微黄色油状物として得た。
〔α〕D 25:+24.1°(c=2.0,CH2 C
l2 )。(2) Synthesis of (S) -4- (2-methyl) butyroylbenzyl alcohol 0.64 g of metallic magnesium and 5.18 g of 4-bromobenzyl- (1-ethoxy) ethyl ether obtained in (1)
The Grignard reagent obtained by reacting (20 mmol) with tetrahydrofuran was cooled to -65 ° C, and (S) -2-methylbutyric acid chloride obtained in (1) of Example 1 was added thereto.
37 g (19.8 mmol) of methylene chloride solution (20
ml) was added dropwise at -70 to -65 ° C, and the mixture was stirred at the same temperature for 3 hours and then at room temperature for 1 hour. The reaction solution was cooled to 0 ° C., 30 ml of 1N hydrochloric acid was added dropwise, the mixture was stirred at the same temperature for 1 hour, extracted twice with 70 ml of ethyl acetate, and the organic layer was washed with 100 ml of water three times, and then dried over anhydrous MgSO 4 . Dried. After the desiccant was filtered off, the solvent was distilled off and the residue (S) -4-
2.4 g of (2-methyl) butyroylbenzyl alcohol
Was obtained as a pale yellow oil. [Α] D 25 : + 24.1 ° (c = 2.0, CH 2 C
l 2 ).
【0058】[0058]
【化17】 [Chemical 17]
【0059】IR( neat ):3450、2970、16
80cm-1。IR (neat): 3450, 2970, 16
80 cm -1 .
【0060】(3)(S)−4−(2−メチル)ブチロ
イル安息香酸の合成
(2)で得た(S)−4−(2−メチル)ブチロイルベ
ンジルアルコール5.6g(29.3ミリモル)と過マ
ンガン酸カリウム6.9g(43.5ミリモル)をアセ
トン400mlに懸濁させ、室温で3時間かくはん反応さ
せた。反応液に亜硫酸ナトリウム4gを加えてかくはん
処理後、1N塩酸200mlを注入、かくはんし、不溶物
をろ別した後、溶剤留去した。残渣を塩化メチレン10
0mlで2回抽出し、有機層を水200mlで3回洗浄し、
無水MgSO4 で乾燥した後、溶剤留去した。残渣5.
7gをn−ヘキサン−塩化メチレンより再結晶して
(S)−4−(2−メチル)ブチロイル安息香酸4.1
gを白色結晶として得た。mp.101〜103.5
℃。
〔α〕D 25:+21.8°(c=1.0,CH2 C
l2 )。(3) Synthesis of (S) -4- (2-methyl) butyroylbenzoic acid 5.6 g (29.3) of (S) -4- (2-methyl) butyroylbenzyl alcohol obtained in (2). Mmol) and 6.9 g (43.5 mmol) of potassium permanganate were suspended in 400 ml of acetone and stirred at room temperature for 3 hours. After adding 4 g of sodium sulfite to the reaction solution and stirring the mixture, 200 ml of 1N hydrochloric acid was injected, the mixture was stirred, the insoluble matter was filtered off, and the solvent was distilled off. The residue is methylene chloride 10
Extracted twice with 0 ml, washed the organic layer three times with 200 ml of water,
After drying over anhydrous MgSO 4 , the solvent was distilled off. Residue 5.
7 g was recrystallized from n-hexane-methylene chloride to give (S) -4- (2-methyl) butyroylbenzoic acid 4.1.
g was obtained as white crystals. mp. 101 to 103.5
° C. [Α] D 25 : + 21.8 ° (c = 1.0, CH 2 C
l 2 ).
【0061】[0061]
【化18】 [Chemical 18]
【0062】IR( KBr ) :2950、1680cm-1。IR (KBr): 2950, 1680 cm -1 .
【0063】(4)(R)−2−(1−メチルブトキ
シ)プロピオン酸メチルの合成
(R)−乳酸メチル56g(0.54モル)と2−ヨー
ドペンタン128g(0.65モル)を70℃に加熱
し、これに酸化銀9.3g(0.40モル)を加えて7
0〜80℃で8時間かくはん反応させた。冷後、析出物
をろ別し、ろ液を減圧蒸留しbp104〜106℃/9
6mmHg留分の(R)−2−(1−メチルブトキシ)プロ
ピオン酸メチル18.5gを無色油状物として得た。
〔α〕D 25:+54.4°( neat )。(4) Synthesis of methyl (R) -2- (1-methylbutoxy) propionate 56 g (0.54 mol) of (R) -methyl lactate and 128 g (0.65 mol) of 2-iodopentane were added to 70%. After heating to ℃, add 9.3g (0.40mol) of silver oxide and add
Stirring reaction was carried out at 0 to 80 ° C. for 8 hours. After cooling, the precipitate was filtered off and the filtrate was distilled under reduced pressure to obtain a bp of 104 to 106 ° C / 9.
18.5 g of methyl (R) -2- (1-methylbutoxy) propionate of a 6 mmHg fraction was obtained as a colorless oil.
[Α] D 25 : + 54.4 ° (neat).
【0064】[0064]
【化19】 [Chemical 19]
【0065】IR( neat ):2940、1730cm-1。IR (neat): 2940, 1730 cm -1 .
【0066】(5)(R)−2−(1−メチルブトキ
シ)プロピオン酸の合成
(4)で得た(R)−2−(1−メチルブトキシ)プロ
ピオン酸メチル17.5g(0.1モル)とギ酸20ml
及び濃塩酸10mlを混合し、60〜70℃で6時間かく
はん反応させた。反応液に水150mlを注入した後、酢
酸エチル100mlで2回抽出し、有機層を水200mlで
3回洗浄し、無水MgSO4 で乾燥した。乾燥剤をろ別
後、溶剤留去し残渣の(R)−2−(1−メチルブトキ
シ)プロピオン酸11.2gを無色油状物として得た。
〔α〕D 25:+45.2°( neat)。(5) Synthesis of (R) -2- (1-methylbutoxy) propionic acid 17.5 g (0.1) of methyl (R) -2- (1-methylbutoxy) propionate obtained in (4) Mol) and formic acid 20 ml
And 10 ml of concentrated hydrochloric acid were mixed and agitated at 60 to 70 ° C. for 6 hours. After injecting 150 ml of water into the reaction solution, the mixture was extracted twice with 100 ml of ethyl acetate, the organic layer was washed with 200 ml of water three times, and dried over anhydrous MgSO 4 . After the desiccant was filtered off, the solvent was distilled off to obtain 11.2 g of residual (R) -2- (1-methylbutoxy) propionic acid as a colorless oily substance.
[Α] D 25 : + 45.2 ° (neat).
【0067】[0067]
【化20】 [Chemical 20]
【0068】IR( neat ):2940、1700cm-1。IR (neat): 2940, 1700 cm -1 .
【0069】(6)(R)−4−ヒドロキシ−4′−
〔2−(1−メチルブトキシ)プロパノイルオキシ〕−
1,1′−ビフェニルの合成
(5)で得た(R)−2−(1−メチルブトキシ)プロ
ピオン酸4.65g(29ミリモル)と塩化チオニル
6.9gを塩化メチレン25mlに溶解させ、かくはん還
流を2時間行った後、濃縮した。次いで残渣4.4gに
塩化メチレン20mlに溶解させ、これを4,4′−ジヒ
ドロキシ−1,1′−ビフェニル4.0g(22ミリモ
ル)、ピリジン3.5g及び塩化メチレン20mlの溶液
中に室温で滴下し、以下実施例1の(4)と同様に処理
し、残渣11gをカラム精製(充てん剤:ワコーゲルC
−200;溶離液:n−ヘキサン/酢酸エチル=10/
1)して(R)−4−ヒドロキシ−4′−〔2−(1−
メチルブトキシ)プロパノイルオキシ〕−1,1′−ビ
フェニル3.0gを白色結晶として得た。
mp.107〜115℃。〔α〕D 25:+40.3°(
c=2.03,CH2 Cl2 )。(6) (R) -4-hydroxy-4'-
[2- (1-methylbutoxy) propanoyloxy]-
Synthesis of 1,1'-biphenyl 4.65 g (29 mmol) of (R) -2- (1-methylbutoxy) propionic acid obtained in (5) and 6.9 g of thionyl chloride were dissolved in 25 ml of methylene chloride and stirred. The mixture was refluxed for 2 hours and then concentrated. Then, 4.4 g of the residue was dissolved in 20 ml of methylene chloride, and this was dissolved in a solution of 4.0 g (22 mmol) of 4,4'-dihydroxy-1,1'-biphenyl, 3.5 g of pyridine and 20 ml of methylene chloride at room temperature. Dropwise, and then treated in the same manner as in (4) of Example 1, 11 g of the residue was subjected to column purification (filler: Wakogel C
-200; Eluent: n-hexane / ethyl acetate = 10 /
1) and then (R) -4-hydroxy-4 '-[2- (1-
3.0 g of methylbutoxy) propanoyloxy] -1,1′-biphenyl was obtained as white crystals. mp. 107-115 ° C. [Α] D 25 : + 40.3 ° (
c = 2.03, CH 2 Cl 2 ).
【0070】[0070]
【化21】 [Chemical 21]
【0071】IR( KBr ) :3480、2990、17
50cm-1。IR (KBr): 3480, 2990, 17
50 cm -1 .
【0072】(7)(R)−2−(1−メチルブトキ
シ)プロピオン酸(S)−4−{4′−〔(2−メチ
ル)ブチロイル〕ベンゾイルオキシ−1,1′−ビフェ
ニル}の合成
(3)で得た(S)−4−(2−メチル)ブチロイル安
息香酸1.2g(5.8ミリモル)と(6)で得た
(R)−4−ヒドロキシ−4′−〔2−(1−メチルブ
トキシ)プロパノイルオキシ〕−1,1′−ビフェニル
1.9g(5.8ミリモル)とを用いて実施例1の
(5)と同様に実施し、カラム分離後得られた粗結晶
1.0gをエタノールより再結晶して(R)−2−(1
−メチルブトキシ)プロピオン酸(S)−4−{4′−
〔(2−メチル)ブチロイル〕ベンゾイルオキシ−1,
1′−ビフェニル}610mgを白色針状晶として得た。
mp.59.0〜61.0℃。
〔α〕D 25:+47.9°( c=1.0,CHC
l3 )。(7) Synthesis of (R) -2- (1-methylbutoxy) propionic acid (S) -4- {4 '-[(2-methyl) butyroyl] benzoyloxy-1,1'-biphenyl} 1.2 g (5.8 mmol) of (S) -4- (2-methyl) butyroylbenzoic acid obtained in (3) and (R) -4-hydroxy-4 ′-[2- (2) obtained in (6). (1-Methylbutoxy) propanoyloxy] -1,1′-biphenyl (1.9 g, 5.8 mmol) was used in the same manner as in (5) of Example 1 to obtain a crude product obtained after column separation. Recrystallize 1.0 g of crystals from ethanol to give (R) -2- (1
-Methylbutoxy) propionic acid (S) -4- {4'-
[(2-methyl) butyroyl] benzoyloxy-1,
610 mg of 1'-biphenyl} was obtained as white needle crystals.
mp. 59.0-61.0 ° C. [Α] D 25 : + 47.9 ° (c = 1.0, CHC
l 3 ).
【0073】[0073]
【化22】 [Chemical formula 22]
【0074】IR( KBr ) :2950、1765、17
30、1680cm-1。
元素分析値(C32H36O6 )
計算値:C% 74.40 ; H% 7.02
実測値:C% 74.55 ; H% 6.99IR (KBr): 2950, 1765, 17
30, 1680 cm -1 . Elemental analysis value (C 32 H 36 O 6 ) calculated value: C% 74.40; H% 7.02 measured value: C% 74.55; H% 6.99
【0075】実施例3
(S)−4−〔4′−(2−メチル)オクタノイル−
1,1′−ビフェニル−4−カルボニルオキシ〕安息香
酸(R)−1−メチルヘプチル
化2)がフェニル基、R* が1−メチルヘプチル基、m
が0、nが2である化合物〕Example 3 (S) -4- [4 '-(2-methyl) octanoyl-
1,1'-Biphenyl-4-carbonyloxy] benzoic acid (R) -1-methylheptyl Formula 2) is a phenyl group, R * is a 1-methylheptyl group, m
Is 0 and n is 2]
【0076】(1)4′−アセチル−4−ブロモ−1,
1′−ビフェニルの合成
4−ブロモ−1,1′−ビフェニル25.0g(0.1
1モル)と無水塩化アルミニウム17.2gをニトロベ
ンゼン130ml中で混合し、塩化アセチル9.4g
(0.12モル)を室温で滴下し、次いで70℃で4時
間かくはん反応させた。反応液を水70ml及び濃塩酸2
5mlの混合液に注入し、酢酸エチル150mlで2回抽出
し、有機層を水100mlで5回洗浄した後、無水MgS
O4 で乾燥した。乾燥剤をろ別し、溶剤留去し、残渣を
カラム精製〔充てん剤:ワコーゲルC−200;溶離
液:n−ヘキサン→n−ヘキサン/酢酸エチル=10/
1〕して4′−アセチル−4−ブロモ−1,1′−ビフ
ェニル24.9gを微褐色結晶として得た。
IR( KBr ) :1684cm-1。(1) 4'-acetyl-4-bromo-1,
Synthesis of 1'-biphenyl 2-bromo-1,1'-biphenyl 25.0 g (0.1
1 mol) and 17.2 g of anhydrous aluminum chloride are mixed in 130 ml of nitrobenzene to give 9.4 g of acetyl chloride.
(0.12 mol) was added dropwise at room temperature, and then the mixture was reacted by stirring at 70 ° C. for 4 hours. 70 ml of water and 2 ml of concentrated hydrochloric acid
Poured into a mixed solution of 5 ml, extracted twice with 150 ml of ethyl acetate, washed the organic layer 5 times with 100 ml of water, and dried over anhydrous MgS.
Dry with O 4 . The desiccant was filtered off, the solvent was distilled off, and the residue was purified by column [filler: Wakogel C-200; eluent: n-hexane → n-hexane / ethyl acetate = 10 /
1] to obtain 24.9 g of 4'-acetyl-4-bromo-1,1'-biphenyl as slightly brown crystals. IR (KBr): 1684 cm -1 .
【0077】(2)4′−ブロモ−1,1′−ビフェニ
ル−4−カルボン酸の合成
(1)で得た4′−アセチル−4−ブロモ−1,1′−
ビフェニル24.0g(87ミリモル)と1,4−ジオ
キサン100mlを混合し、冷却した後、これに次亜臭素
酸ナトリウム水溶液〔水酸化ナトリウム58gと水30
0mlの溶液に臭素57.9g(0.36モル)を10℃
以下で滴下して調製した水溶液〕を10℃以下で滴下
し、更に40〜50℃で4時間かくはん反応させた。冷
後、反応液を亜硫酸ナトリウム12.5gで処理し、6
N塩酸300mlを注入し、氷冷下、かくはん晶析させ
た。析出晶をろ取し、水洗、n−ヘキサン洗浄後、乾燥
して4′−ブロモ−1,1′−ビフェニル−4−カルボ
ン酸24.2gを微褐色結晶として得た。mp.250
℃以上。(2) Synthesis of 4'-bromo-1,1'-biphenyl-4-carboxylic acid 4'-acetyl-4-bromo-1,1'-obtained in (1)
After mixing 24.0 g (87 mmol) of biphenyl and 100 ml of 1,4-dioxane and cooling, an aqueous solution of sodium hypobromite [58 g of sodium hydroxide and 30 g of water was added thereto.
Bromine (57.9 g, 0.36 mol) was added to a 0 ml solution at 10 ° C.
The aqueous solution prepared by dropping below was added dropwise at 10 ° C. or lower, and the mixture was further stirred at 40 to 50 ° C. for 4 hours. After cooling, the reaction solution was treated with 12.5 g of sodium sulfite, and 6
300 ml of N hydrochloric acid was injected, and the mixture was stirred and crystallized under ice cooling. The precipitated crystals were collected by filtration, washed with water, washed with n-hexane, and dried to obtain 24.2 g of 4'-bromo-1,1'-biphenyl-4-carboxylic acid as light brown crystals. mp. 250
℃ or more.
【0078】[0078]
【化23】 [Chemical formula 23]
【0079】IR( KBr ) :1690cm-1。IR (KBr): 1690 cm -1 .
【0080】(3)4′−ブロモ−4−ヒドロキシメチ
ル−1,1′−ビフェニルの合成
(2)で得た4′−ブロモ−1,1′−ビフェニル−4
−カルボン酸12.0g(43.3ミリモル)をテトラ
ヒドロフラン80mlに懸濁させ、窒素気流下、1Mボラ
ン−テトラヒドロフラン錯塩〔テトラヒドロフラン溶
液〕57.6mlを5℃以下で滴下し、0〜5℃で1時
間、次いで室温で2時間かくはん反応させた。反応液を
水60ml中に注入し、酢酸エチル100mlで2回抽出
し、有機層を水150mlで1回洗浄した後、無水MgS
O4で乾燥した。乾燥剤をろ別し、溶剤留去して4′−
ブロモ−4−ヒドロキシメチル−1,1′−ビフェニル
10.5gを微褐色結晶として得た。
mp.163〜166℃。(3) Synthesis of 4'-bromo-4-hydroxymethyl-1,1'-biphenyl 4'-bromo-1,1'-biphenyl-4 obtained in (2)
-12.0 g (43.3 mmol) of carboxylic acid was suspended in 80 ml of tetrahydrofuran, and 57.6 ml of 1M borane-tetrahydrofuran complex salt [tetrahydrofuran solution] was added dropwise at 5 ° C or lower under a nitrogen stream, and the mixture was added at 0-5 ° C at 1 ° C. The reaction was stirred for 2 hours and then at room temperature for 2 hours. The reaction solution was poured into 60 ml of water, extracted twice with 100 ml of ethyl acetate, the organic layer was washed once with 150 ml of water, and then dried with anhydrous MgS.
Dry with O 4 . The desiccant is filtered off and the solvent is distilled off to 4'-
10.5 g of bromo-4-hydroxymethyl-1,1'-biphenyl was obtained as light brown crystals. mp. 163-166 ° C.
【0081】[0081]
【化24】 [Chemical formula 24]
【0082】IR( KBr ) :3350cm-1。IR (KBr): 3350 cm -1 .
【0083】(4)4′−ブロモ−4−(1−エトキ
シ)エトキシメチル−1,1′−ビフェニルの合成
(3)で得た4′−ブロモ−4−ヒドロキシメチル−
1,1′−ビフェニル9.5g(36ミリモル)及びエ
チルビニルエーテル3.3g(45.8ミリモル)とを
用いて実施例2の(1)と同様に実施し、4′−ブロモ
−4−(1−エトキシ)エトキシメチル−1,1′−ビ
フェニル12.0gを淡黄色結晶として得た。
mp.49.0〜50.0℃。(4) Synthesis of 4'-bromo-4- (1-ethoxy) ethoxymethyl-1,1'-biphenyl 4'-bromo-4-hydroxymethyl-obtained in (3)
The same procedure as in Example 2 (1) was carried out using 9.5 g (36 mmol) of 1,1'-biphenyl and 3.3 g (45.8 mmol) of ethyl vinyl ether, and 4'-bromo-4- ( 12.0 g of 1-ethoxy) ethoxymethyl-1,1'-biphenyl was obtained as pale yellow crystals. mp. 49.0-50.0 ° C.
【0084】[0084]
【化25】 [Chemical 25]
【0085】IR( KBr ) :2950cm-1。IR (KBr): 2950 cm -1 .
【0086】(5)(S)−2−メチルオクタン酸塩化
物の合成
(S)−2−メチルオクタン酸5.0g(32ミリモ
ル)と塩化チオニル11.3gを塩化メチレン40mlに
溶解し、3時間かくはん還流させた後、減圧濃縮し、残
渣の(S)−2−メチルオクタン酸塩化物5.6gを淡
黄色油状物として得た。(5) Synthesis of (S) -2-methyloctanoic acid chloride 5.0 g (32 mmol) of (S) -2-methyloctanoic acid and 11.3 g of thionyl chloride were dissolved in 40 ml of methylene chloride to give 3 parts. After stirring and refluxing for a period of time, the mixture was concentrated under reduced pressure to obtain 5.6 g of residual (S) -2-methyloctanoic acid chloride as a pale yellow oil.
【0087】[0087]
【化26】 [Chemical formula 26]
【0088】IR( neat ):2940、1800cm-1。IR (neat): 2940, 1800 cm -1 .
【0089】(6)(S)−4−ヒドロキシメチル−
4′−(2−メチル)オクタノイル−1,1′−ビフェ
ニルの合成
(4)で得た4′−ブロモ−4−(1−エトキシ)エト
キシメチル−1,1′−ビフェニル7.0g(21ミリ
モル)と(5)で得た(S)−2−メチルオクタン酸塩
化物3.5g(20ミリモル)とを用いて実施例2の
(2)と同様に実施し、得られた粗結晶7.3gをカラ
ム精製〔充てん剤:ワコーゲルC−200;溶離液:塩
化メチレン〕して(S)−4−ヒドロキシメチル−4′
−(2−メチル)オクタノイル−1,1′−ビフェニル
3.1gを白色結晶として得た。mp.81.0〜8
4.0℃。
〔α〕D 25:+3.0°(c=2.0,CH2 C
l2 )。(6) (S) -4-hydroxymethyl-
Synthesis of 4 '-(2-methyl) octanoyl-1,1'-biphenyl 4'-Bromo-4- (1-ethoxy) ethoxymethyl-1,1'-biphenyl obtained in (4) 7.0 g (21 (5 mmol) and 3.5 g (20 mmol) of (S) -2-methyloctanoic acid chloride obtained in (5) were carried out in the same manner as in (2) of Example 2 to obtain crude crystal 7. Column purification (filler: Wakogel C-200; eluent: methylene chloride) of 3 g of (S) -4-hydroxymethyl-4 '
3.1 g of-(2-methyl) octanoyl-1,1'-biphenyl was obtained as white crystals. mp. 81.0-8
4.0 ° C. [Α] D 25 : + 3.0 ° (c = 2.0, CH 2 C
l 2 ).
【0090】[0090]
【化27】 [Chemical 27]
【0091】IR( KBr ) :3500、2930、16
82cm-1。IR (KBr): 3500, 2930, 16
82 cm -1 .
【0092】(7)(S)−4′−(2−メチル)オク
タノイル−1,1′−ビフェニル−4−カルボン酸の合
成
(6)で得た(S)−4−ヒドロキシメチル−4′−
(2−メチル)オクタノイル−1,1′−ビフェニル
2.5g(7.7ミリモル)を用いて実施例2の(3)
と同様に実施し、得られた粗結晶2.5gをカラム精製
〔充てん剤:ワコーゲルC−200;溶離液:塩化メチ
レン〕して(S)−4′−(2−メチル)オクタノイル
−1,1′−ビフェニル−4−カルボン酸1.9gを白
色結晶として得た。
mp.190〜198℃。(7) Synthesis of (S) -4 '-(2-methyl) octanoyl-1,1'-biphenyl-4-carboxylic acid (S) -4-hydroxymethyl-4' obtained in (6) −
2.5 g (7.7 mmol) of (2-methyl) octanoyl-1,1'-biphenyl was used to prepare (2) of Example 2.
2.5 g of the crude crystals obtained were subjected to column purification [filler: Wakogel C-200; eluent: methylene chloride] to give (S) -4 ′-(2-methyl) octanoyl-1, 1.9 g of 1'-biphenyl-4-carboxylic acid was obtained as white crystals. mp. 190-198 ° C.
【0093】[0093]
【化28】 [Chemical 28]
【0094】IR( KBr ) :2940、1690cm-1。IR (KBr): 2940, 1690 cm -1 .
【0095】(8)4−ベンジルオキシ安息香酸の合成
4−ヒドロキシ安息香酸エチル200g(1.2モル)
と塩化ベンジル190g(1.5モル)及び炭酸カリウ
ム165gをアセトン1.2リットル中でかくはん還流
を12時間行い、冷後、析出物をろ別し、溶剤留去し
た。次いで残渣400gをエタノール500mlに溶解さ
せ、これに水酸化ナトリウム60g及び水1リットルを
加えて60〜70℃でかくはん反応を4時間行った。冷
後、反応液に濃塩酸200mlを注入し、析出結晶をろ
取、水洗次いでエタノール洗浄した後、乾燥して4−ベ
ンジルオキシ安息香酸195gを白色結晶として得た。
mp.191.2〜192.6℃。
IR( KBr ) :1695cm-1。(8) Synthesis of 4-benzyloxybenzoic acid 200 g (1.2 mol) of ethyl 4-hydroxybenzoate
190 g (1.5 mol) of benzyl chloride and 165 g of potassium carbonate were stirred and refluxed in 1.2 liter of acetone for 12 hours. After cooling, the precipitate was filtered off and the solvent was distilled off. Next, 400 g of the residue was dissolved in 500 ml of ethanol, 60 g of sodium hydroxide and 1 liter of water were added thereto, and a stirring reaction was carried out at 60 to 70 ° C. for 4 hours. After cooling, 200 ml of concentrated hydrochloric acid was poured into the reaction solution, and the precipitated crystals were collected by filtration, washed with water, washed with ethanol, and dried to obtain 195 g of 4-benzyloxybenzoic acid as white crystals. mp. 191.2-192.6 ° C. IR (KBr): 1695 cm -1 .
【0096】(9)(R)−4−ベンジルオキシ安息香
酸1−メチルヘプチルの合成
(8)で得た4−ベンジルオキシ安息香酸16.0g
(70ミリモル)と塩化チオニル16.7gを塩化メチ
レン75mlに溶解させ、かくはん還流を3時間行った
後、濃縮した。次いで濃縮残渣を(R)−2−オクタノ
ール9.1g(70ミリモル)、ピリジン10.1g及
び塩化メチレン60mlの溶液中に室温で滴下し、以下実
施例1の(4)と同様に処理して、(R)−4−ベンジ
ルオキシ安息香酸1−メチルヘプチル13.3gを微黄
色油状物として得た。
〔α〕D 25:−31.6°(c=2.06,CH2 Cl
2 )。(9) Synthesis of 1-methylheptyl (R) -4-benzyloxybenzoate 16.0 g of 4-benzyloxybenzoic acid obtained in (8)
(70 mmol) and thionyl chloride (16.7 g) were dissolved in methylene chloride (75 ml), stirred and refluxed for 3 hours, and then concentrated. Then, the concentrated residue was added dropwise to a solution of 9.1 g (70 mmol) of (R) -2-octanol, 10.1 g of pyridine and 60 ml of methylene chloride at room temperature, and treated in the same manner as in (4) of Example 1 below. Thus, 13.3 g of 1-methylheptyl (R) -4-benzyloxybenzoate was obtained as a pale yellow oil. [Α] D 25 : -31.6 ° (c = 2.06, CH 2 Cl
2 ).
【0097】[0097]
【化29】 [Chemical 29]
【0098】IR( neat ):3020、2920、17
05cm-1。IR (neat): 3020, 2920, 17
05 cm -1 .
【0099】(10)(R)−4−ヒドロキシ安息香酸
1−メチルヘプチルの合成
(9)で得た(R)−4−ベンジルオキシ安息香酸1−
メチルヘプチル5.0g(14.7ミリモル)をメタノ
ールに溶解し、5%パラジウム炭素触媒下常圧接触還元
を行い、触媒をろ別し、溶剤留去して(R)−4−ヒド
ロキシ安息香酸1−メチルヘプチル3.6gを淡黄色油
状物として得た。
〔α〕D 25:−34.4°(c=2.01,CH2 Cl
2 )。
IR( neat ):3350、2940、1705cm-1。(10) Synthesis of 1-methylheptyl (R) -4-hydroxybenzoate (R) -4-benzyloxybenzoic acid 1-obtained in (9)
5.0 g (14.7 mmol) of methylheptyl was dissolved in methanol and subjected to catalytic reduction under atmospheric pressure with a 5% palladium carbon catalyst, the catalyst was filtered off, and the solvent was distilled off to give (R) -4-hydroxybenzoic acid. 3.6 g of 1-methylheptyl was obtained as a pale yellow oil. [Α] D 25 : -34.4 ° (c = 2.01, CH 2 Cl
2 ). IR (neat): 3350, 2940, 1705 cm -1 .
【0100】(11)(S)−4−〔4′−(2−メチ
ル)オクタノイル−1,1′−ビフェニル−4−カルボ
ニルオキシ〕安息香酸(R)−1−メチルヘプチルの合
成
(7)で得た(S)−4′−(2−メチル)オクタノイ
ル−1,1′−ビフェニル−4−カルボン酸1.5g
(4.4ミリモル)と(10)で得た(R)−4−ヒド
ロキシ安息香酸1−メチルヘプチル1.1g(4.4ミ
リモル)とを用いて実施例1の(5)と同様に実施し、
カラム分離後、得られた粗結晶2.5gをエタノールよ
り再結晶して(S)−4−〔4′−(2−メチル)オク
タノイル−1,1′−ビフェニル−4−カルボニルオキ
シ〕安息香酸(R)−1−メチルヘプチル1.65gを
白色短針状晶として得た。
mp.82.0〜83.0℃。(11) Synthesis of (R) -1-methylheptyl (R) -1- (S) -4- [4 ′-(2-methyl) octanoyl-1,1′-biphenyl-4-carbonyloxy] benzoate (7) (S) -4 '-(2-methyl) octanoyl-1,1'-biphenyl-4-carboxylic acid obtained in 1.5 g
(4.4 mmol) and 1.1 g (4.4 mmol) of 1-methylheptyl (R) -4-hydroxybenzoate obtained in (10) were used and the same procedure as (5) of Example 1 was carried out. Then
After column separation, 2.5 g of the crude crystals obtained were recrystallized from ethanol to give (S) -4- [4 '-(2-methyl) octanoyl-1,1'-biphenyl-4-carbonyloxy] benzoic acid. 1.65 g of (R) -1-methylheptyl was obtained as white short needle crystals. mp. 82.0-83.0 ° C.
【0101】[0101]
【化30】 [Chemical 30]
【0102】 IR( KBr ) :2940、1740、1720、1680cm-1。 〔α〕D 25:−22.7°(c=2.02,CH2 Cl2 )。 元素分析値(C37H46O5 ) 計算値:C% 77.86 ; H% 8.12 実測値:C% 77.94 ; H% 8.00IR (KBr): 2940, 1740, 1720, 1680 cm -1 . [Α] D 25 : −22.7 ° (c = 2.02, CH 2 Cl 2 ). Elemental analysis value (C 37 H 46 O 5 ) calculated value: C% 77.86; H% 8.12 measured value: C% 77.94; H% 8.00
【0103】実施例1〜3の化合物の相転移温度を、示
差走査熱量計(DSC)測定と温度制御装置を備えた偏
光顕微鏡による観察によって測定した。また、これらの
化合物のSc* 相上限温度から10℃下での自発分極を
三角波法によって測定した。これらの結果を表1に示
す。The phase transition temperatures of the compounds of Examples 1 to 3 were measured by a differential scanning calorimeter (DSC) measurement and observation with a polarizing microscope equipped with a temperature controller. Further, the spontaneous polarization of these compounds at 10 ° C. below the Sc * phase maximum temperature was measured by the triangular wave method. The results are shown in Table 1.
【0104】[0104]
【表1】 [Table 1]
【0105】注1)Cr:結晶、Sc* :カイラルスメ
クティックC、SA :スメクティックA、I:等方液体
注2)・はその相が存在することを示す。また括弧はモ
ノトロピック転移であることを示す。
注3)Sc* 相上限から5℃下での値Note 1) Cr: crystal, Sc * : chiral smectic C, S A : smectic A, I: isotropic liquid Note 2) · indicates that the phase exists. The parentheses indicate that it is a monotropic transition. Note 3) Value at 5 ° C below the upper limit of Sc * phase
【0106】実施例4〜6
実施例1〜3の化合物をメルク社のスメクティックC液
晶組成物ZLI3234Bに10%添加し、相転移温度
を測定した。更にこれらの液晶組成物を試験用液晶セル
(ITOを蒸着したガラス板上にポリイミド膜を設け一
定方向にラビングし、2μm径のガラスビーズをスペー
サに用いて2枚の基板を張合せた)中に封入して、試験
用素子を作製した。この試験用素子に±10Vの電圧を
印加し、偏光顕微鏡により観察したところ、透過光強度
の変化が認められた。その強度変化から応答時間を求め
た。また、三角波法により自発分極を測定した。これら
の結果を表2に示す(測定温度25℃)。Examples 4 to 6 10% of the compounds of Examples 1 to 3 were added to the smectic C liquid crystal composition ZLI3234B manufactured by Merck & Co., Inc., and the phase transition temperature was measured. Further, these liquid crystal compositions were used in a test liquid crystal cell (a polyimide film was provided on a glass plate on which ITO was vapor-deposited and rubbed in a certain direction, and two substrates were bonded together by using glass beads having a diameter of 2 μm as a spacer). Then, a test element was manufactured. When a voltage of ± 10 V was applied to this test device and observed with a polarization microscope, a change in transmitted light intensity was observed. The response time was calculated from the intensity change. Moreover, the spontaneous polarization was measured by the triangular wave method. The results are shown in Table 2 (measurement temperature: 25 ° C).
【0107】[0107]
【表2】 [Table 2]
【0108】[0108]
【発明の効果】本発明の一般式(化1)で示される化合
物群は、化学的に安定な分子構造を有する光学活性化合
物であり、それ自身極めて大きな自発分極を示すものを
含むだけでなく、他の液晶性化合物と混合することによ
り大きな自発分極を誘起して高速動作する強誘電性液晶
組成物を得ることができる。また、分子内に複数の不斉
炭素を持つため、各々の不斉中心の引起こすら旋の向き
が異なる場合には、該強誘電性液晶組成物においてら旋
ピッチの長いものが得られる。INDUSTRIAL APPLICABILITY The compound group represented by the general formula (Formula 1) of the present invention is an optically active compound having a chemically stable molecular structure, and includes not only those which exhibit extremely large spontaneous polarization, By mixing with another liquid crystal compound, a ferroelectric liquid crystal composition that induces large spontaneous polarization and operates at high speed can be obtained. In addition, since the compound has a plurality of asymmetric carbon atoms in the molecule, when the directions of the spirals that cause the respective asymmetric centers are different, the ferroelectric liquid crystal composition has a long spiral pitch.
フロントページの続き (51)Int.Cl.5 識別記号 庁内整理番号 FI 技術表示箇所 C07C 255/22 8519−4H 255/41 8519−4H C07D 213/30 6701−4C 213/63 6701−4C 239/26 7038−4C 239/32 7038−4C C09K 19/20 6742−4H 19/30 6742−4H 19/34 6742−4H G02F 1/13 500 (72)発明者 石橋 重喜 東京都千代田区内幸町一丁目1番6号 日 本電信電話株式会社内 (72)発明者 浦野 文良 埼玉県川越市大字的場1633番地 和光純薬 工業株式会社東京研究所内 (72)発明者 根岸 孝明 埼玉県川越市大字的場1633番地 和光純薬 工業株式会社東京研究所内Continuation of the front page (51) Int.Cl. 5 Identification number Reference number within the agency FI Technical indication C07C 255/22 8519-4H 255/41 8519-4H C07D 213/30 6701-4C 213/63 6701-4C 239 / 26 7038-4C 239/32 7038-4C C09K 19/20 6742-4H 19/30 6742-4H 19/34 6742-4H G02F 1/13 500 (72) Inventor Shigeki Ishibashi 1-chome, Uchiyuki-cho, Chiyoda-ku, Tokyo No. 6 Nihon Telegraph and Telephone Corporation (72) Inventor Fumiyoshi Urano 1633 Matoba, Kawagoe City, Saitama Prefecture Wako Pure Chemical Industries, Ltd. Tokyo Research Laboratory (72) Inventor Takaaki Negishi 1633 Matoba, Kawagoe City, Saitama Prefecture Wako Pure Chemical Industries, Ltd. Tokyo Research Center
Claims (2)
ル基(Xと一致するものは除く)又はアルコキシ基、R
* は炭素数16以下の光学活性アルキル基、Xはメチル
基、エチル基、フッ素、塩素、ニトリル基のいずれか、
Yは−COO−、−OCO−、−O−のいずれか、式
(化2): 【化2】 で示される基は、下記式(化3): 【化3】 (Zは水素、ハロゲン、ニトリル基のいずれか)で示さ
れる基のいずれか、C* は光学活性炭素を示し、mは0
又は1、nは1又は2であるが、m+n≦2である〕で
表されることを特徴とする光学活性化合物。1. The following general formula (Formula 1): [In the formula, R is a linear or branched alkyl group having 16 or less carbon atoms (excluding those corresponding to X) or an alkoxy group, R
* Is an optically active alkyl group having 16 or less carbon atoms, X is a methyl group, an ethyl group, fluorine, chlorine or a nitrile group,
Y is any of -COO-, -OCO-, and -O-, and is represented by the formula (Formula 2): The group represented by is represented by the following formula (Formula 3): (Z is any of hydrogen, halogen, and nitrile group), C * is optically active carbon, and m is 0.
Or 1, and n is 1 or 2, but m + n ≦ 2].
くとも1成分含有することを特徴とするカイラル液晶組
成物。2. A chiral liquid crystal composition comprising at least one component of the optically active compound according to claim 1.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP27052991A JPH054944A (en) | 1990-09-25 | 1991-09-24 | Optically active compound and liquid crystal composition containing the same compound |
Applications Claiming Priority (3)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP25196990 | 1990-09-25 | ||
| JP2-251969 | 1990-09-25 | ||
| JP27052991A JPH054944A (en) | 1990-09-25 | 1991-09-24 | Optically active compound and liquid crystal composition containing the same compound |
Publications (1)
| Publication Number | Publication Date |
|---|---|
| JPH054944A true JPH054944A (en) | 1993-01-14 |
Family
ID=26540462
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP27052991A Withdrawn JPH054944A (en) | 1990-09-25 | 1991-09-24 | Optically active compound and liquid crystal composition containing the same compound |
Country Status (1)
| Country | Link |
|---|---|
| JP (1) | JPH054944A (en) |
Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| WO1999001419A1 (en) * | 1997-07-03 | 1999-01-14 | Taito Co., Ltd. | Processes for producing 2-aminomalonic acid derivatives and 2-amino-1,3-propanediol derivatives, and intermediates for producing the derivatives |
| US6821581B2 (en) * | 2001-06-26 | 2004-11-23 | Mitsubishi Gas Chemical Co., Inc. | Optically active compound and liquid crystal composition containing the compound |
-
1991
- 1991-09-24 JP JP27052991A patent/JPH054944A/en not_active Withdrawn
Cited By (3)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| WO1999001419A1 (en) * | 1997-07-03 | 1999-01-14 | Taito Co., Ltd. | Processes for producing 2-aminomalonic acid derivatives and 2-amino-1,3-propanediol derivatives, and intermediates for producing the derivatives |
| US6284915B2 (en) | 1997-07-03 | 2001-09-04 | Taito Co., Ltd | Process for preparing 2-amino malonic acid derivatives and 2-amino-1,3-propanediol derivatives, and intermediates for preparing the same |
| US6821581B2 (en) * | 2001-06-26 | 2004-11-23 | Mitsubishi Gas Chemical Co., Inc. | Optically active compound and liquid crystal composition containing the compound |
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