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JPH0244313B2 - - Google Patents
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JPH0244313B2 - - Google Patents

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Publication number
JPH0244313B2
JPH0244313B2 JP57046417A JP4641782A JPH0244313B2 JP H0244313 B2 JPH0244313 B2 JP H0244313B2 JP 57046417 A JP57046417 A JP 57046417A JP 4641782 A JP4641782 A JP 4641782A JP H0244313 B2 JPH0244313 B2 JP H0244313B2
Authority
JP
Japan
Prior art keywords
compound
reaction
group
compounds
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
JP57046417A
Other languages
Japanese (ja)
Other versions
JPS58164592A (en
Inventor
Kyokazu Mizutani
Hitoshi Kato
Yoshihisa Ogasawara
Takeshi Endo
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.)
Toagosei Co Ltd
Original Assignee
Toagosei Co Ltd
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 Toagosei Co Ltd filed Critical Toagosei Co Ltd
Priority to JP57046417A priority Critical patent/JPS58164592A/en
Publication of JPS58164592A publication Critical patent/JPS58164592A/en
Publication of JPH0244313B2 publication Critical patent/JPH0244313B2/ja
Granted legal-status Critical Current

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  • Heterocyclic Carbon Compounds Containing A Hetero Ring Having Oxygen Or Sulfur (AREA)
  • Addition Polymer Or Copolymer, Post-Treatments, Or Chemical Modifications (AREA)

Description

【発明の詳现な説明】[Detailed description of the invention]

本発明は新芏化合物であり、䞋蚘䞀般匏〔〕
で瀺される−ヒドロキシメチル−−
トリオキサスピロ〔〕アルカンここでは
は〜の敎数を衚わす。さらに具䜓的には
−ヒドロキシメチル−−トリオキサ
スピロ〔〕ノナン、−ヒドロキシメチル
−−トリオキサスピロ〔〕デカ
ンおよび−ヒドロキシメチル−−ト
リオキサスピロ〔〕りンデカンを提䟛する
ものであ぀お、本発明に係るこれらの化合物以
䞋化合物〔〕ず総称するは、䟋えば重合性単
量䜓およびスピロオル゜゚ステル基含有化合物の
合成原料ずしお有甚である。 ここでは〜の敎数を衚わす。 化合物〔〕はγ−ブチロラクトン、Ύ−バレ
ロラクトンおよびε−カプロラクトンから遞ばれ
るラクトン類ずグリシドヌルずの付加反応によ぀
お補造するこずができ、この反応を瀺すず以䞋の
ごずくになる。 ここでは〜の敎数を衚わす。 化合物〔〕を補造するに際しおは、グリシド
ヌルモルに察しお奜たしくはラクトン類モル
以䞊、さらに奜たしくは1.2〜モルのラクトン
過剰で反応させるのが適圓であり、これらを䟋え
ば塩化メチレンやテトラヒドロフラン等のごずき
溶媒䞭で、觊媒ずしおBF3OEt2、SnCl4、TiCl4、
FeCl3等のごずきルむス酞を䜿甚しお反応させ
る。反応枩床に特に制限はないが、℃〜60℃で
行なうのが望たしい。 望たしい補造方法の䟋ずしおは、ラクトン類
ずラクトン類に察しお〜10重量倍量の溶媒ずを
反応噚に仕蟌み、液枩を所定枩床に維持し぀぀、
通垞ラクトン類ず溶媒からなる溶媒に察しお0.03
〜重量ラクトン類に察しおは0.05〜10重量
の觊媒を添加し、続いおグリシドヌルを単独
でたた重量倍皋床たでの溶媒ずの溶液ずしお滎
䞋する方法がある。 反応の進行皋床は反応液を䟋えばガスクロマト
グラフたたは液䜓クロマトグラフで分析するこず
によ぀お容易に知るこずができ、反応終了時には
反応埌にアルカリを加えお酞觊媒を䞭和する。反
応液からの化合物〔〕の分離取埗は、䟋えば぀
ぎのようにしお行なわれる。反応埌を氷氎により
冷华しながら、これにアルカリ氎溶液䟋えば皀氎
酞化ナトリりム氎溶液を添加し撹拌混合埌、氎局
ず有機局に分別する。有機局䞭の未反応ラクトン
がほが零になるたで䞊蚘操䜜を繰り返した埌有機
局を氎掗し、次に硫酞マグネシりムにより有機局
を脱氎する。぀ぎに溶媒を留去し、残枣を枛圧蒞
留するこずにより、化合物〔〕を取埗する。 スピロオル゜゚ステル化合物のカチオン重合に
関しおは、ゞダヌナル・オブ・マクロモレキナラ
ヌ・サむ゚ンス、ケミストリむJournal of
Macromolecular Science、Chemistry、A9(5)、
849〜8651975などに蚘茉されおいるが、本発
明の化合物〔〕も同様にカチオン重合し、重合
物を䞎える。 本発明の化合物〔〕のカチオン重合は、䞀般
によく知られおいる方法、すなわちカチオン重合
開始剀の存圚䞋䟋えば玫倖線、赀倖線、熱たたは
マむクロ波などによ぀お行なわれる。 玫倖線照射の堎合のカチオン重合觊媒ずしお、
䟋えば φ−≡・PE6 -、φ−≡・BF4 -などの
芳銙族ゞアゟニりム塩φ−−φ・BF4 -等の
芳銙族ハロニりム塩 等の呚期埋衚第Va族元玠の芳銙族オニりム塩 The present invention is a new compound, which has the following general formula [1]
2-hydroxymethyl-1,4,6-
Trioxaspiro[4,m]alkane (here, m represents an integer of 4 to 6) More specifically, 2-hydroxymethyl-1,4,6-trioxaspiro[4,4]nonane, 2 -Hydroxymethyl-1,4,6-trioxaspiro[4,5]decane and 2-hydroxymethyl-1,4,6-trioxaspiro[4,6]undecane, comprising: These compounds (hereinafter collectively referred to as compounds [1]) are useful, for example, as raw materials for the synthesis of polymerizable monomers and spiro-orthoester group-containing compounds. (Here, m represents an integer of 4 to 6.) Compound [1] can be produced by an addition reaction between lactones selected from γ-butyrolactone, Ύ-valerolactone, and ε-caprolactone and glycidol. , this reaction is as follows. (Here, m represents an integer of 4 to 6.) When producing compound [1], the reaction is carried out with an excess of lactone of preferably 1 mol or more, more preferably 1.2 to 5 mol, of lactone per 1 mol of glycidol. It is suitable to use BF 3 OEt 2 , SnCl 4 , TiCl 4 , etc. as a catalyst in a solvent such as methylene chloride or tetrahydrofuran.
The reaction is carried out using a Lewis acid such as FeCl3 . There is no particular restriction on the reaction temperature, but it is preferably carried out at 0°C to 60°C. As an example of a desirable production method, lactones and a solvent in an amount of 1 to 10 times the weight of the lactones are charged into a reactor, and while maintaining the liquid temperature at a predetermined temperature,
0.03 for solvents usually consisting of lactones and solvents
There is a method in which ~3% by weight (0.05~10% by weight for lactones) of catalyst is added, and then glycidol is added dropwise either alone or as a solution with a solvent up to about 5 times the weight. The degree of progress of the reaction can be easily determined by analyzing the reaction solution using, for example, a gas chromatograph or a liquid chromatograph, and when the reaction is completed, an alkali is added after the reaction to neutralize the acid catalyst. Separation and acquisition of compound [1] from the reaction solution is performed, for example, as follows. After the reaction is cooled with ice water, an alkaline aqueous solution such as a dilute aqueous sodium hydroxide solution is added thereto, stirred and mixed, and then separated into an aqueous layer and an organic layer. After repeating the above operation until the amount of unreacted lactone in the organic layer becomes almost zero, the organic layer is washed with water, and then the organic layer is dehydrated with magnesium sulfate. Next, the solvent is distilled off, and the residue is distilled under reduced pressure to obtain compound [1]. Regarding the cationic polymerization of spiro-orthoester compounds, please refer to the Journal of Macromolecular Science and Chemistry.
Macromolecular Science, Chemistry), A9(5),
849-865 (1975), the compound [1] of the present invention is similarly cationically polymerized to give a polymer. The cationic polymerization of the compound [1] of the present invention is carried out by a generally well-known method, that is, by using, for example, ultraviolet rays, infrared rays, heat, or microwaves in the presence of a cationic polymerization initiator. As a cationic polymerization catalyst in the case of ultraviolet irradiation,
For example, aromatic diazonium salts such as φ-N + ≡N·PE 6 - and φ-N + ≡N·BF 4 - ; aromatic halonium salts such as φ-I-φ·BF 4 - ; Aromatic onium salts of Group Va elements of the periodic table, such as;

【匏】等の呚期埋衚第 族元玠の芳銙族オニりム塩Periodic table number of [formula] etc. Aromatic onium salt of group a element;

【匏】等の呚期埋衚第 −族元玠のゞカルボニル錯化合物が䜿甚
されうる。 たた、その他合カチオン重合觊媒ずしおは、䟋
えばBF3、FeCl3、SnCl4、SbF3、TiCl4などのル
むス酞BF3OEt2、BF3−アニリンコンブレツク
ス等のごずきルむス酞ず、、などを有する
化合物ずの配䜍化合物ルむス酞のオキ゜ニりム
塩、ゞアゟニりム塩、カルボニりム塩ハロゲン
化合物、混合ハロゲン化合物たたは過ハロゲン酞
誘導䜓などがあげられる。 觊媒の䜿甚量は䞀般に重合しようずする単量䜓
に察し、0.001〜10重量奜たしくは0.1から重
量の範囲が奜適である。 重合枩床に関する制限は特にないが、通垞垞枩
〜200℃で行なわれる。 重合時に溶媒を䜿甚する堎合は、生長カチオン
ず反応しおその掻性を䜎䞋させない化合物を遞ぶ
こずが望たしい。䜿甚に適した溶媒ずしおは、ヘ
キサン、オクタン等の脂肪族炭化氎玠トル゚
ン、キシレン等の芳銙族炭化氎玠塩化メチレ
ン、−ゞクロル゚タン等のハロゲン化炭化
氎玠その他がある。 たた本発明の化合物〔〕の官胜基OH基
を利甚しお、求栞反応により皮々のスピロオル゜
゚ステル基を含有する化合物を合成する事が出来
る。 その化合物を䟋瀺するず、䟋えば次の䞀般匏
〔〕で瀺されるラゞカル重合䜓基をも぀単量䜓
以䞋化合物〔〕ずいうがある。 ここでは氎原子又はメチル基を衚わし、は
〜の敎数を衚わす。 化合物〔〕は化合物〔〕ずアクリル酞クロ
ラむドたたはメタクリル酞クロラむド以䞋メ
タアクリル酞クロラむドず略蚘するずの脱塩
化氎玠反応により合成され、その反応匏を瀺すず
以䞋のごずくになる。 ここでは、は䞀般匏〔〕ず同矩である。
䞊蚘反応は䟋えば化合物〔〕を適圓な溶媒䞭
で、トリ゚チルアミン等の有機塩基性物質の存圚
䞋、メタアクリル酞クロラむドを滎䞋しお脱
塩化氎玠させる。 䞊蚘化合物〔〕は、メタアクリロむル基
を利甚しお、単独でたたぱチレン性䞍飜和化合
物ずラゞカル重合させるこずにより、重合物にス
ピロオル゜゚ステル基を導入するこずができる有
甚な化合物である。 たた他の䟋ずしおは、化合物〔〕ずむ゜シア
ネヌト化合物ず反応させるこずにより、スピロオ
ル゜゚ステル基を含有すする䞋蚘䞀般匏〔〕で
瀺されるりレタン化合物以䞋化合物〔〕ずい
うがある。 ここではむ゜シアネヌトたたはりレタン化合
物残基を衚わし、は〜の敎数を衚わしは
以䞊の敎数を衚わす。 化合物〔〕の敎造法に関しお説明するず以䞋
のたたはの方法がある。 () む゜シアネヌト化合物ず化合物〔〕のり
レタン化反応。 () 䞋蚘化合物(A)、(B)および(C)のりレタン化反
応。 (A) む゜シアネヌト基を少なくずも個有する
ポリむ゜シアネヌト化合物の少なくずも
皮。 (B) ヒドロキシル基を少なくずも個有するポ
リヒドロキシ化合物の少なくずも皮。 (C) 䞀般匏〔〕で瀺されるスピロオル゜゚ス
テルの少なくずも皮。 䞊蚘、で䜿甚されうるむ゜シアネヌ
ト化合物ずしおは、脂肪族および芳銙族モノむ゜
シアネヌトあるいは分子内に個以䞊のむ゜シア
ネヌト基を有する脂肪族、脂環族および芳銙族ポ
リむ゜シアネヌトがあり、たた他の原料である二
぀以䞊のヒドロキシル基をも぀ポリヒドロキシ化
合物ずしおは、倚䟡アルコヌル、ポリ゚ステルポ
リオヌル、ポリ゚ヌテルポリオヌル、ポリマヌポ
リオヌルがある。 それらの化合物を具䜓的に䟋瀺するずモノむ゜
シアネヌトずしおは特開昭56−167688号公報第
頁巊䞋欄13行目から同頁右䞋欄行目に蚘茉され
おいる、たた分子内に個以䞊のむ゜シアネヌト
基を有するむ゜シアネヌトおよびポリヒドロキシ
化合物ずしおは特開昭57−21417号公報第頁巊
䞊欄䞋から行目から第頁右䞊欄䞋から行目
に蚘茉されおいる化合物等であり、これらのいず
れを甚いおもよい。 䞊蚘の化合物(A)、(B)および(C)をりレタン
化反応させるこずにより、りレタン基をも぀スピ
ロオル゜゚ステルを補造する方法の䟋を䟋瀺す
るず代衚的な方法は二段反応による補法で、たず
第の工皋で、ポリむ゜シアネヌト化合物ずポリ
ヒドロキシ化合物ずのりレタン化反応により末端
およびたたは偎鎖にむ゜シアネヌト基を有する
郚分りレタン化物を補造する。このずきポリヒド
ロキシ化合物に含たれる氎酞基圓量に察お、ポ
リむ゜シアネヌト化合物のむ゜シアネヌト基は玄
1.1圓量以䞊の割合で反応させるのがよく、この
圓量比を倉化させるこずにより、最終の生成組成
物の分子量を調節するこずができる。氎酞基圓
量に察しお、む゜シアネヌト基が玄1.1圓量より
䜎い割合で䜿甚されたずきは、最終生成組成物の
分子量が著しく倧きくなり粘床が増倧したり、硬
化性が充分でない堎合がある。 たた氎酞基に察するむ゜シアネヌト基の圓量比
を倧きくする事により、最終生成組成物におい
お、郚分りレタン化ポリむ゜シアネヌト化合物の
む゜シアネヌト基を化合物〔〕でりレタン化た
䞋蚘化合物〔〕で瀺される化合物以䞋化合物
〔〕ずいう。の割合を倧きくする事が出来る。 −NH−COO− 〔〕 ここではA dicarbonyl complex compound of an element of group a-a of the periodic table, such as [Formula] may be used. In addition, other combined cationic polymerization catalysts include, for example, Lewis acids such as BF 3 , FeCl 3 , SnCl 4 , SbF 3 , TiCl 4 ; Lewis acids such as BF 3 OEt 2 , BF 3 -aniline complexes, and O, S , N, etc.; oxonium salts, diazonium salts, and carbonium salts of Lewis acids; halogen compounds, mixed halogen compounds, and perhalogen acid derivatives. The amount of catalyst used is generally 0.001 to 10% by weight, preferably 0.1 to 5% by weight, based on the monomer to be polymerized. Although there are no particular restrictions regarding the polymerization temperature, it is usually carried out at room temperature to 200°C. When using a solvent during polymerization, it is desirable to choose a compound that does not react with the growing cation and reduce its activity. Suitable solvents for use include aliphatic hydrocarbons such as hexane and octane; aromatic hydrocarbons such as toluene and xylene; halogenated hydrocarbons such as methylene chloride, 1,1-dichloroethane, and others. Further, the functional group (OH group) of the compound [1] of the present invention
Using this, various compounds containing spiro-orthoester groups can be synthesized by nucleophilic reactions. An example of such a compound is a monomer having a radical polymer group represented by the following general formula [2] (hereinafter referred to as compound [2]). (Here, R represents a water atom or a methyl group, and m represents an integer of 4 to 6.) Compound [2] is a compound [1] and acrylic acid chloride or methacrylic acid chloride (hereinafter referred to as (meth)acrylic acid chloride). The reaction formula is as follows. (Here, R and m have the same meaning as in general formula [2].)
In the above reaction, for example, compound [1] is dehydrochlorinated by dropping (meth)acrylic acid chloride in a suitable solvent in the presence of an organic basic substance such as triethylamine. The above compound [2] is a useful compound that can introduce a spiro-orthoester group into a polymer by using a (meth)acryloyl group alone or by radical polymerization with an ethylenically unsaturated compound. . Another example is a urethane compound represented by the following general formula [3] (hereinafter referred to as compound [3]) containing a spiro-orthoester group by reacting compound [1] with an isocyanate compound. (Here, Q represents an isocyanate or urethane compound residue, m represents an integer of 4 to 6, and n represents an integer of 1 or more.) The following () or ( ) There is a method. () Urethane-forming reaction between an isocyanate compound and compound [1]. () Urethanization reaction of the following compounds (A), (B) and (C). (A) at least one polyisocyanate compound having at least two isocyanate groups;
seed. (B) At least one polyhydroxy compound having at least two hydroxyl groups. (C) At least one type of spiroorthoester represented by the general formula [1]. Isocyanate compounds that can be used in () and () above include aliphatic and aromatic monoisocyanates, aliphatic, alicyclic and aromatic polyisocyanates having two or more isocyanate groups in the molecule, and others. Examples of polyhydroxy compounds having two or more hydroxyl groups that are raw materials include polyhydric alcohols, polyester polyols, polyether polyols, and polymer polyols. Specific examples of these compounds include monoisocyanates as described in JP-A-56-167688 No. 2.
Isocyanates and polyhydroxy compounds having two or more isocyanate groups in the molecule, which are described from line 13 in the lower left column of the page to line 6 in the lower right column of the same page, are disclosed in JP-A No. 57-21417 No. 5. These are the compounds described in the third line from the bottom of the upper left column of the page to the fourth line from the bottom of the upper right column of page 6, and any of these may be used. An example of a method for producing a spiro-orthoester having a urethane group by subjecting the compounds (A), (B) and (C) in () above to a urethanization reaction is as follows: A typical method is a two-step reaction. In the production method, in the first step, a partially urethanized product having an isocyanate group at the terminal and/or side chain is produced by a urethanization reaction between a polyisocyanate compound and a polyhydroxy compound. At this time, the isocyanate group of the polyisocyanate compound is approximately 1 equivalent of hydroxyl group contained in the polyhydroxy compound.
It is preferable to carry out the reaction at a ratio of 1.1 equivalents or more, and by changing this equivalent ratio, the molecular weight of the final product composition can be adjusted. If the isocyanate group is used in a ratio lower than about 1.1 equivalents per equivalent of hydroxyl group, the molecular weight of the final product composition may become significantly large, resulting in increased viscosity or insufficient curability. In addition, by increasing the equivalent ratio of isocyanate groups to hydroxyl groups, in the final product composition, a compound represented by the following compound [4] in which the isocyanate group of a partially urethanized polyisocyanate compound is urethanized with compound [1] [4]) can be increased. Y(-NH-COO-X)f [4] (where X is

【匏】 で瀺される基を、は郚分りレタン化ポリむ゜シ
アネヌト残基を、はポリむ゜シアネヌト化合物
の䟡数に盞圓する敎数を、たたは〜の敎数
を衚わす。 この化合物〔〕は個以䞊のスピロオル゜゚
ステル基を有するこずになり、これは倚官胜重合
性化合物であるから最終の生成組成物を硬化させ
るずき、橋かけ結合の生成床を増倧させるのに圹
立぀。 該りレタン化反応は、、発熱による急激な枩床
䞊昇をさけるために、必芁に応じポリむ゜シアネ
ヌト化合物にポリヒドロキシ化合物を分割添加、
たたは滎䞋するこずによ぀お枩床を調節しながら
行なう。 次に第の工皋では、第の工皋でえられた郚
分りレタン化物の末端およびたたは偎鎖のむ゜
シアネヌト基に化合物〔〕を反応させ結合させ
る。なお、この皮の郚分りレタン化物のある物は
垂販されおおり、本発明においおはかかる垂販品
を利甚するこずもできる。 この郚分りレタン化物に化合物〔〕を添加す
る割合は、郚分りレタン化物䞭の残存む゜シアネ
ヌト基の圓量数ず化合物〔〕の氎酞基の圓量数
ずが等しくなるようにするのが䞀般的である。目
的により化合物〔〕の割合を圓量数以䞊にする
こずもできる。 該りレタン化反応は発熱による急激な枩床䞊昇
をさけるため、郚分りレタン化物に化合物〔〕
を分割添加たたは滎䞋するこずによ぀お、枩床を
調節しながら進める。 䞀般に埓来のカチオン重合性モノマヌは重合時
に䟋えば゚チレンオキシド23、プロピレンオキ
シド17、スチレンオキシド、゚ピクロルヒ
ドリン12等ず非垞に倧きな䜓積収瞮を䌎う。重
合時の䜓瞟収瞮が倧きいず、䟋えば成圢材料ずし
お䜿甚した堎合に寞法粟床ができないずか、泚型
材料ずしお利甚した堎合にはうめこみ物に収瞮に
よるひずみがかかるずか、型ずの接着力の䜎䞋や
隙間が生じるなどの問題がある。たた、塗料ずし
お䜿甚した堎合、内郚ひずみによる塗板ずの密着
性の䜎䞋やそりがおこるずか、接着剀ずしお䜿甚
した堎合、内郚ひずみによる接着力の䜎䞋やそ
り、倉圢などの䜿甚䞊の問題を生ずる。 本発明の化合物〔〕、化合物〔〕から誘導
される化合物〔〕の重合䜓、および化合物
〔〕から補造される化合物〔〕等は、いずれ
もスピロオル゜゚ステル基がカチオン開環重合を
し、しかも重合時の䜓積収瞮が非垞に小さいずい
う特長をも぀おいる。埓぀お本発明の化合物
〔〕及び化合物〔〕より誘導される各皮の化
合物は、成圢材料、耇合材料、接着剀、泚型材
料、塗料などに利甚出来る極めお有甚な化合物で
ある。 ぀ぎに本発明の実斜䟋、参考䟋を掲げ本発明を
具䜓的に説明する。 実斜䟋  撹拌機、コンデンサヌ、枩床蚈及び滎䞋ロヌト
を備えた぀口フラスコに、γ−ブチロラク
トン215.22.5モル及び塩化メチレン1000ml
を仕蟌み、滎䞋ロヌトにグリシドヌル74.1
モル及び塩化メチレン150mlを仕蟌んだ。釜液
を氷氎で10℃に冷华埌、BF3、OEt2を1.5ml添加
した。釜液を撹拌しながら玄1.5時間かけお、グ
リシドヌル溶液を滎䞋した。滎䞋埌さらに時間
撹拌した。なお反応の間釜液は氎で冷华し、玄10
℃に保持した。次にトリ゚チルアミンmlを加
え、觊媒を倱掻させた。次に反応液を氷氎で冷华
し、撹拌しながら10NaOH氎溶液1000mlを
埐々に加え、添加完了埌30分間撹拌した埌、アル
カリ氎溶液局ず有機局を分離した。この有機局を
500mlの氎で掗浄した。次に硫酞マグネシりムで
脱氎した埌、、脱溶剀をした。その残枣にトリ
−オクチルアミン0.2を添加した埌、枛圧
蒞留し、沞点83℃0.7mmHgにおいお、−ヒド
ロキシメチル−−トリオキサスピロ
〔〕ノナン11.9収率7.4を埗た。 その物性倀は䞋蚘の通りである。 Γ沞点83℃0.7mmHg Γ比重1.19625℃ ΓIR赀倖吞収スペクトル3450cm-1−、
1334cm-1、1247cm-1、1132cm-1、1042cm-1、
954cm-1 ΓNMR栞磁気共鳎スペクトルCDCl3䞭 Ύppm3.4〜4.67H、3CH2−、CH−
、1.8〜2.34H、−CH2−CH2 実斜䟋  実斜䟋ず同様なフラスコにε−カプロラクト
ン2852.5モル、塩化メチレン1000ml及びト
リ゚チルアミン0.7mlを仕蟌み、滎䞋ロヌトにグ
リシドヌル74.1モル及び塩化メチレン
150mlを仕蟌んだ。釜液を氷氎10℃に冷华埌、
BF3OEt2を1.5ml添加した。釜液を撹拌しながら
玄時間かけおグリシドヌル溶液を滎䞋した。さ
らに時間撹拌した。なお反応の間釜液は氎で冷
华し、玄10℃に保持した。次にトリ゚チルアミン
mlを加え觊媒を倱掻させた。次に反応液を氷氎
で冷华しながら10NaOH氎溶液1000mlを埐々
に加え、30分撹拌した埌、アルカリ氎溶液ず有機
局を分離した。この有機局を500mlの氎で掗浄し
遠心分離により分離する操䜜を回行な぀た埌、
硫酞マグネシりムで脱氎した。 次にトリ−オクチルアミン0.2を添加
埌脱溶剀を行ない、さらに枛圧蒞留し沞点95℃
0.7mmHgにおいお、−ヒドロキシメチル−
−トリオキサスピロ〔〕りンデカン
13.3収率7.1を埗た。 その物性倀は䞋蚘の通りである。 Γ沞点95℃0.7mmHg Γ比重1.16125℃ ΓIR3450cm-1−、1240cm-1、1133cm-1、
1072cm- 1、1037cm-1、960cm-1 ΓNMRCDCl3䞭 Ύppm3.4〜4.57H、3CH2−、CH−
1.9〜2.12H、In the group represented by the formula: Y represents a partially urethanized polyisocyanate residue, f represents an integer corresponding to the valence of the polyisocyanate compound, and m represents an integer of 4 to 6. ) This compound [4] has two or more spiro-orthoester groups, and since it is a polyfunctional polymerizable compound, it increases the degree of cross-linking when curing the final product composition. useful for. In the urethanization reaction, in order to avoid a rapid temperature rise due to heat generation, a polyhydroxy compound is added to the polyisocyanate compound in portions as necessary.
Alternatively, the temperature may be controlled by dripping. Next, in the second step, compound [1] is reacted and bonded to the terminal and/or side chain isocyanate groups of the partially urethanized product obtained in the first step. Note that some partially urethanized products of this type are commercially available, and such commercial products can also be used in the present invention. The ratio of adding compound [1] to this partially urethanized product is generally such that the number of equivalents of residual isocyanate groups in the partially urethanized product is equal to the number of equivalents of hydroxyl groups in compound [1]. Depending on the purpose, the proportion of compound [1] can be increased to an equivalent number or more. In the urethanization reaction, in order to avoid rapid temperature rise due to heat generation, compound [1] is added to the partially urethanized product.
Proceed while controlling the temperature by adding in portions or dropwise. In general, conventional cationic polymerizable monomers undergo very large volume shrinkage during polymerization, such as 23% ethylene oxide, 17% propylene oxide, 9% styrene oxide, 12% epichlorohydrin, etc. If the actual shrinkage during polymerization is large, for example, when used as a molding material, dimensional accuracy may not be achieved, when used as a casting material, the injected material may be subject to distortion due to shrinkage, or the adhesive strength with the mold may be affected. There are problems such as deterioration and gaps. In addition, when used as a paint, internal strain may cause a decrease in adhesion to the painted plate and warping, and when used as an adhesive, internal strain may cause problems such as a decrease in adhesive strength, warpage, and deformation. . In the compound [1] of the present invention, the polymer of compound [2] derived from compound [1], and the compound [3] produced from compound [1], the spiro-orthoester group is cationically ring-opened. It polymerizes, and its volumetric shrinkage during polymerization is extremely small. Therefore, the compound [1] of the present invention and various compounds derived from the compound [1] are extremely useful compounds that can be used in molding materials, composite materials, adhesives, casting materials, paints, etc. Next, the present invention will be specifically explained with reference to Examples and Reference Examples. Example 1 215.2 g (2.5 mol) of γ-butyrolactone and 1000 ml of methylene chloride were placed in a 4-necked 2 flask equipped with a stirrer, condenser, thermometer, and dropping funnel.
and add 74.1 g of glycidol (1 g) to the dropping funnel.
mol) and 150 ml of methylene chloride were charged. After cooling the pot solution to 10° C. with ice water, 1.5 ml of BF 3 and OEt 2 were added. The glycidol solution was added dropwise to the pot solution over about 1.5 hours while stirring. After the addition, the mixture was further stirred for 5 hours. During the reaction, the pot liquid was cooled with water and heated for about 10 minutes.
It was kept at ℃. Next, 3 ml of triethylamine was added to deactivate the catalyst. Next, the reaction solution was cooled with ice water, and while stirring, 1000 ml of a 10% NaOH aqueous solution was gradually added. After the addition was completed, the mixture was stirred for 30 minutes, and then the alkali aqueous solution layer and the organic layer were separated. This organic layer
Washed with 500ml of water. Next, after dehydrating with magnesium sulfate, the solvent was removed. After adding 0.2 g of tri(n-octyl)amine to the residue, it was distilled under reduced pressure, and at a boiling point of 83°C/0.7 mmHg, 2-hydroxymethyl-1,4,6-trioxaspiro[4,4]nonane 11.9 g (yield 7.4%). Its physical property values are as follows. Γ boiling point: 83℃/0.7mmHg Γ specific gravity: 1.196 (25℃) ΓIR (infrared absorption spectrum): 3450cm -1 (O-H),
1334cm -1 , 1247cm -1 , 1132cm -1 , 1042cm -1 ,
954cm -1 ΓNMR (Nuclear Magnetic Resonance Spectrum) (in CDCl 3 ); ή (ppm); 3.4-4.6 (7H, 3CH2 -O, CH-
O), 1.8 to 2.3 (4H, C-CH 2 -CH 2 ) Example 2 285 g (2.5 mol) of ε-caprolactone, 1000 ml of methylene chloride, and 0.7 ml of triethylamine were charged into the same flask as in Example 1, and the mixture was poured into a dropping funnel. Glycidol 74.1g (1 mol) and methylene chloride
I prepared 150ml. After cooling the pot liquid to ice water at 10℃,
1.5 ml of BF 3 OEt 2 was added. The glycidol solution was added dropwise to the pot over about 2 hours while stirring the solution. The mixture was further stirred for 5 hours. During the reaction, the pot liquid was cooled with water and maintained at about 10°C. Next, 3 ml of triethylamine was added to deactivate the catalyst. Next, 1000 ml of a 10% NaOH aqueous solution was gradually added to the reaction solution while cooling it with ice water, and after stirring for 30 minutes, the alkali aqueous solution and the organic layer were separated. After washing this organic layer with 500 ml of water and separating it by centrifugation twice,
Dehydrated with magnesium sulfate. Next, 0.2 g of tri(n-octyl)amine was added, the solvent was removed, and the boiling point was 95℃/
At 0.7 mmHg, 2-hydroxymethyl-1,
4,6-trioxaspiro[4,6]undecane
13.3g (yield 7.1%) was obtained. Its physical property values are as follows. Γ Boiling point: 95℃/0.7mmHg Γ Specific gravity: 1.161/25℃ ΓIR: 3450cm -1 (O-H), 1240cm -1 , 1133cm -1 ,
1072 cm -1 , 1037 cm -1 , 960 cm -1 Γ NMR (in CDCl 3 ); ή (ppm); 3.4-4.5 (7H, 3CH2 -O, CH-O)
1.9~2.1 (2H,

【匏】1.4〜1.9 6H、CH2−CH2−CH2 Γ質量スペクトルGC−MS 芪ピヌク188 参考䟋  実斜䟋で埗た化合物にカチオン重合觊媒ずし
おBF3OEt2をモル添加お80℃においお時
間加熱し透明のやわらかい重合物を埗た。 この重合物はIR分析より1730cm-1の゚ステル
の吞収が認められた。重合による䜓積収瞮率ほ
がゞであ぀た。 参考䟋  実斜䟋で埗られた化合物にカチオン重合觊媒
ずしおBF3OEt2をモル添加しお80℃におい
お時間加熱し透明のやわらかい重合物を埗た。 この重合物はIR分析により1730cm-1の゚ステ
ルの吞収が認められた。たた重合による䜓積収瞮
率はほがであ぀た。[Formula]) 1.4-1.9 (6H, CH 2 -CH 2 -CH 2 ) Γ mass spectrum (GC-MS); Parent peak; m/e = 188 Reference example 1 A cationic polymerization catalyst was added to the compound obtained in Example 1. 3 mol% of BF 3 OEt 2 was added thereto and heated at 80° C. for 3 hours to obtain a transparent soft polymer. IR analysis revealed that this polymer had ester absorption at 1730 cm -1 . The volume shrinkage rate due to polymerization was approximately 0. Reference Example 2 3 mol% of BF 3 OEt 2 was added as a cationic polymerization catalyst to the compound obtained in Example 2, and the mixture was heated at 80° C. for 3 hours to obtain a transparent soft polymer. An IR analysis of this polymer revealed that it had an ester absorption of 1730 cm -1 . Further, the volume shrinkage rate due to polymerization was approximately 0.

【図面の簡単な説明】[Brief explanation of drawings]

第図は実斜䟋で埗た−ヒドロキシメチル
−−トリオキサスピロ〔〕ノナ
ンのIR図であり、第図は同化合物のNMR図で
あり、第図は実斜䟋で埗た−ヒドロキシメ
チル−−トリオキサスピロ〔〕
りンデカンのIR図であり、第図は同化合物の
NMR図である。 Figure 1 is an IR diagram of 2-hydroxymethyl-1,4,6-trioxaspiro[4,4]nonane obtained in Example 1, Figure 2 is an NMR diagram of the same compound, and Figure 3 is an NMR diagram of the same compound. The figure shows 2-hydroxymethyl-1,4,6-trioxaspiro[4,6] obtained in Example 2.
This is an IR diagram of undecane, and Figure 4 shows the IR diagram of the same compound.
It is an NMR diagram.

Claims (1)

【特蚱請求の範囲】  䞋蚘䞀般匏〔〕で瀺される−ヒドロキシ
メチル−−トリオキサスピロ〔
〕アルカン。 ここでは〜の敎数を衚わす。[Scope of Claims] 1 2-hydroxymethyl-1,4,6-trioxaspiro[4,
m] Alkane. (Here, m represents an integer from 4 to 6.)
JP57046417A 1982-03-25 1982-03-25 2-hydroxymethyl-1, 4, 6-trioxaspiro(4, m)alkane Granted JPS58164592A (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
JP57046417A JPS58164592A (en) 1982-03-25 1982-03-25 2-hydroxymethyl-1, 4, 6-trioxaspiro(4, m)alkane

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
JP57046417A JPS58164592A (en) 1982-03-25 1982-03-25 2-hydroxymethyl-1, 4, 6-trioxaspiro(4, m)alkane

Publications (2)

Publication Number Publication Date
JPS58164592A JPS58164592A (en) 1983-09-29
JPH0244313B2 true JPH0244313B2 (en) 1990-10-03

Family

ID=12746568

Family Applications (1)

Application Number Title Priority Date Filing Date
JP57046417A Granted JPS58164592A (en) 1982-03-25 1982-03-25 2-hydroxymethyl-1, 4, 6-trioxaspiro(4, m)alkane

Country Status (1)

Country Link
JP (1) JPS58164592A (en)

Families Citing this family (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
JPS61243823A (en) * 1985-04-23 1986-10-30 Dainippon Ink & Chem Inc Highly branched polyester ether copolymer and curable composition containing same
US5231197A (en) * 1992-06-01 1993-07-27 General Electric Company Method for producing ethylenically unsaturated graftable orthoesters

Also Published As

Publication number Publication date
JPS58164592A (en) 1983-09-29

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