JPH09151168A - Production of beta-alanine salt - Google Patents

Production of beta-alanine salt

Info

Publication number
JPH09151168A
JPH09151168A JP7310893A JP31089395A JPH09151168A JP H09151168 A JPH09151168 A JP H09151168A JP 7310893 A JP7310893 A JP 7310893A JP 31089395 A JP31089395 A JP 31089395A JP H09151168 A JPH09151168 A JP H09151168A
Authority
JP
Japan
Prior art keywords
reaction
alanine
aminopropanol
catalyst
alanine salt
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.)
Pending
Application number
JP7310893A
Other languages
Japanese (ja)
Inventor
Tamotsu Fujii
保 藤井
Kazuhiro Takayashiki
和弘 高屋敷
Seiji Takasaki
誠司 高崎
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.)
Kawaken Fine Chemicals Co Ltd
Original Assignee
Kawaken Fine Chemicals 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 Kawaken Fine Chemicals Co Ltd filed Critical Kawaken Fine Chemicals Co Ltd
Priority to JP7310893A priority Critical patent/JPH09151168A/en
Publication of JPH09151168A publication Critical patent/JPH09151168A/en
Pending legal-status Critical Current

Links

Classifications

    • YGENERAL TAGGING OF NEW TECHNOLOGICAL DEVELOPMENTS; GENERAL TAGGING OF CROSS-SECTIONAL TECHNOLOGIES SPANNING OVER SEVERAL SECTIONS OF THE IPC; TECHNICAL SUBJECTS COVERED BY FORMER USPC CROSS-REFERENCE ART COLLECTIONS [XRACs] AND DIGESTS
    • Y02TECHNOLOGIES OR APPLICATIONS FOR MITIGATION OR ADAPTATION AGAINST CLIMATE CHANGE
    • Y02PCLIMATE CHANGE MITIGATION TECHNOLOGIES IN THE PRODUCTION OR PROCESSING OF GOODS
    • Y02P20/00Technologies relating to chemical industry
    • Y02P20/50Improvements relating to the production of bulk chemicals
    • Y02P20/52Improvements relating to the production of bulk chemicals using catalysts, e.g. selective catalysts

Landscapes

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

Abstract

PROBLEM TO BE SOLVED: To produce a β-alanine salt useful as a raw material for producing a medicine, an agrochemical and a cosmetic in high yield by suppressing the formation of by-products. SOLUTION: The oxidative dehydrogenation reaction of 3-aminopropanol is carried out in the existence of an alkali metallic hydroxide or alkaline earth metallic hydroxide (e.g. NaOH), water and a catalyst containing copper (e.g. a developed Raney copper) at 100-210 deg.C to afford a β-alanine salt. Based on the amount of the 3-aminopropanol, an alkali(ne earth) metallic hydroxide is used in an equivalent amount or more and >=10wt.% water and 1-70wt.% catalyst are used. The high-purity β-alanine salt can simply be obtained in high yield at a low cost because of no need of purification processes for removing by-products due to remarkably suppress the formation of iminodipropionic acid, nitrilotripropionic acid, etc., as by-products.

Description

【発明の詳細な説明】Detailed Description of the Invention

【0001】[0001]

【発明の属する技術分野】本発明は、β−アラニン塩の
製造方法に関するものである。β−アラニン塩は医薬
品、農薬、および化粧料製造用原料として重要なもので
ある。TECHNICAL FIELD The present invention relates to a method for producing a β-alanine salt. β-alanine salt is important as a raw material for manufacturing pharmaceuticals, agricultural chemicals, and cosmetics.

【0002】[0002]

【従来の技術】β−アラニンの製造方法としては、種々
の方法が知られているが、工業的にはアクリロニトリル
にアンモニアを付加して3−アミノプロピオニトリル
(APN)を調製し、次にそのニトリル基をアルカリに
より加水分解して合成されている。Various methods are known as a method for producing β-alanine. Industrially, ammonia is added to acrylonitrile to prepare 3-aminopropionitrile (APN), and then It is synthesized by hydrolyzing the nitrile group with alkali.

【0003】この合成工程を下記に示す。This synthetic process is shown below.

【化1】 Embedded image

【0004】上記反応の問題点は、APNの製造時に、
APNにさらにもう一分子のアクリロニトリルが付加し
てイミノジプロピオニトリル(IDPN)が副生してし
まうことである。IDPNもニトリル基の加水分解時に
同様に加水分解し、イミノジプロピオン酸(IDPA)
塩になってしまう。The problem with the above reaction is that when APN is produced,
Another molecule of acrylonitrile is added to APN, and iminodipropionitrile (IDPN) is by-produced. IDPN also hydrolyzes when the nitrile group is hydrolyzed, and iminodipropionic acid (IDPA)
It becomes salt.

【0005】この副生反応を下記に示す。This by-product reaction is shown below.

【化2】 Embedded image

【0006】したがって、上記方法で得られたβ−アラ
ニン中にはIDPAが少なからず含まれていた。さら
に、ごく少量ではあるがIDPNにさらにもう一分子の
アクリロニトリルが付加したニトリロトリプロピオニト
リルも副生し、これもIDPAの場合と同様の加水分解
反応を受け、ニトリロトリプロピオン酸が副生する。Therefore, the β-alanine obtained by the above method contained a considerable amount of IDPA. Furthermore, nitrilotripropionitrile, which is a small amount of IDPN, to which one more molecule of acrylonitrile is added, is also by-produced, and this also undergoes the same hydrolysis reaction as in the case of IDPA, and nitrilotripropionic acid is by-produced.

【0007】この副生反応を下記に示す。This by-product reaction is shown below.

【化3】 Embedded image

【0008】β−アラニン中のIDPAやニトリロトリ
プロピオン酸の生成量を少なくするには、APN製造時
にアクリロニトリルに対するアンモニア過剰率を高くす
ればよいが、多量のアンモニアの除去の問題、および生
産性低下の問題からこれを工業的に実施するには不適で
ある。また、β−アラニンからIDPAを除去するため
に、イオン交換樹脂などで処理する方法も知られている
が、工程が煩雑になるため実用的ではない。また、ID
PAをアンモニア中、高温で処理することによって、β
−アラニンに変換する方法も知られている。しかし、こ
の方法では200℃以上という高温で処理反応を行う必
要があり、危険を伴うので工業的な製法としては難があ
る。In order to reduce the production amount of IDPA and nitrilotripropionic acid in β-alanine, it is sufficient to increase the ammonia excess ratio with respect to acrylonitrile during APN production. The problem makes it unsuitable for industrial implementation. Further, a method of treating with an ion exchange resin or the like to remove IDPA from β-alanine is also known, but it is not practical because the process becomes complicated. Also, ID
By treating PA at high temperature in ammonia, β
-Methods of converting to alanine are also known. However, in this method, it is necessary to carry out the treatment reaction at a high temperature of 200 ° C. or more, which is dangerous, and thus it is difficult as an industrial manufacturing method.

【0009】このように、アクリロニトリルを出発原料
とするβ−アラニンの製造法には、問題点が多く、この
ため工業的に簡便に実施できるβ−アラニンの製造方法
の開発が望まれていた。As described above, the method for producing β-alanine using acrylonitrile as a starting material has many problems, and therefore, the development of a method for producing β-alanine that can be easily carried out industrially has been desired.

【0010】一方、アミノエタノールを銅含有触媒の存
在下に酸化脱水素反応させて、アミノ酢酸類を得る方法
はすでに知られている(特開昭60−41644号、特
開昭60−41645号、特開昭60−78948号、
特開昭60−78949号、特開昭60−97945
号、および特開昭60−100545号)。On the other hand, a method for obtaining aminoacetic acids by subjecting aminoethanol to an oxidative dehydrogenation reaction in the presence of a copper-containing catalyst has already been known (JP-A-60-41644 and JP-A-60-41645). JP-A-60-78948,
JP-A-60-78949, JP-A-60-97945
And JP-A-60-100545).

【0011】これらの方法において、出発原料として用
いられるアミノエタノールは、モノエタノールアミン、
ジエタノールアミン、トリエタノールアミンのいずれか
であり、水酸基のβ位に窒素原子を有する化合物に限定
されている。アミノエタノール類の酸化脱水素反応は、
比較的容易に進行する。またこの反応は銅触媒のみなら
ず、貴金属触媒の存在下でも比較的選択的に進行する。
つまり、水酸基に対しβ位の窒素が酸化脱水素反応に何
らかの関与をするものと考えられている。したがって、
水酸基に対しβ位に窒素原子を有しない化合物を酸化脱
水素することは難しいと考えられていた。本発明者らの
知る限り、β−アラニンを得るために、水酸基に対しγ
位に窒素原子を有する3−アミノプロパノールについて
直接、酸化脱水素反応を試みた例はない。In these methods, aminoethanol used as a starting material is monoethanolamine,
It is either diethanolamine or triethanolamine and is limited to compounds having a nitrogen atom at the β-position of the hydroxyl group. Oxidative dehydrogenation of aminoethanols
It progresses relatively easily. Further, this reaction proceeds relatively selectively not only in the copper catalyst but also in the presence of the noble metal catalyst.
That is, it is considered that the nitrogen at the β-position with respect to the hydroxyl group has some role in the oxidative dehydrogenation reaction. Therefore,
It has been considered difficult to oxidatively dehydrogenate a compound having no nitrogen atom at the β-position with respect to the hydroxyl group. To the knowledge of the inventors, in order to obtain β-alanine, γ is required for the hydroxyl group.
There is no example in which an oxidative dehydrogenation reaction was directly attempted for 3-aminopropanol having a nitrogen atom at the position.

【0012】[0012]

【発明が解決しようとする課題】本発明は、IDPAを
含有しないか、あるいは含有率の極めて小さいβ−アラ
ニンを、工業的に、簡便かつ安価に製造する方法を提供
しようとするものである。DISCLOSURE OF THE INVENTION The present invention is to provide a method for industrially, conveniently and inexpensively producing β-alanine containing no IDPA or having a very small content.

【0013】[0013]

【課題を解決するための手段】本発明者らは、β−アラ
ニン塩を工業的に簡便な方法で製造するべく、鋭意研究
を重ねた結果、アンモニアにアクリロニトリルを付加さ
せる従来方法ではなく、アミノプロパノールを直接、酸
化脱水素することにより、IDPAの副生がなく、また
は極めて少ないβ−アラニン塩が得られることを見出し
本発明を完成した。Means for Solving the Problems The inventors of the present invention have conducted extensive studies to produce a β-alanine salt by an industrially simple method, and as a result, have found that the method is not the conventional method of adding acrylonitrile to ammonia, but the amino method. The present invention has been completed by finding that a β-alanine salt free of by-produced IDPA or having an extremely small amount can be obtained by directly oxidatively dehydrogenating propanol.

【0014】すなわち、本発明のβ−アラニン塩の製造
方法は3−アミノプロパノールを、アルカリ金属の水酸
化物およびアルカリ土類金属の水酸化物から選ばれた少
なくとも1種と、水と、銅含有触媒との共存下に酸化脱
水素することを特徴とするものである。本発明の方法に
より、アミノプロパノールの−CH2 OH基から2個の
水素原子が脱水素し、酸化されてCO2 −基が生成す
る。That is, the method for producing a β-alanine salt of the present invention comprises 3-aminopropanol, at least one selected from alkali metal hydroxides and alkaline earth metal hydroxides, water, and copper. It is characterized in that oxidative dehydrogenation is carried out in the coexistence with a contained catalyst. According to the method of the present invention, two hydrogen atoms are dehydrogenated from the —CH 2 OH group of aminopropanol and oxidized to form a CO 2 — group.

【0015】[0015]

【発明の実施の形態】本発明方法で使用するアルカリ金
属の水酸化物あるいはアルカリ土類金属の水酸化物とし
ては、水酸化ナトリウム、水酸化カリウム、水酸化カル
シウムなどが用いられるが特に水酸化ナトリウム、水酸
化カリウムなどが好適である。これらはフレーク、粉
末、ペレット、水溶液等どのような形状でも使用できる
が、水溶液で使用することが取り扱いやすさの点で好ま
しい。BEST MODE FOR CARRYING OUT THE INVENTION As the alkali metal hydroxides or alkaline earth metal hydroxides used in the method of the present invention, sodium hydroxide, potassium hydroxide, calcium hydroxide and the like are used, but especially hydroxides are used. Sodium, potassium hydroxide and the like are preferable. These may be used in any shape such as flakes, powders, pellets and aqueous solutions, but it is preferable to use them in an aqueous solution from the viewpoint of easy handling.

【0016】アルカリ金属の水酸化物あるいはアルカリ
土類金属水酸化物の使用量は、当該反応に使用されるア
ミノプロパノールに対して等当量以上であることが好ま
しく、より好ましくは1.0〜2.0当量の範囲内であ
る。The amount of the alkali metal hydroxide or alkaline earth metal hydroxide used is preferably equivalent or more, more preferably 1.0 to 2 with respect to the aminopropanol used in the reaction. Within the range of 0.0 equivalent.

【0017】本発明方法の酸化脱水素反応は、水の存在
下で行われる。すなわち水を使用することにより、アミ
ノプロパノールとアルカリ金属水酸化物あるいはアルカ
リ土類金属水酸化物とを均一に反応させることができ、
その結果、β−アラニンが高収率で得られる。反応に用
いられる水の量はアミノプロパノールに対して10重量
%以上であることが好ましく、より好ましくは50〜5
00重量%の範囲内である。The oxidative dehydrogenation reaction of the method of the present invention is carried out in the presence of water. That is, by using water, it is possible to uniformly react aminopropanol with an alkali metal hydroxide or an alkaline earth metal hydroxide,
As a result, β-alanine is obtained in high yield. The amount of water used in the reaction is preferably 10% by weight or more, more preferably 50 to 5 with respect to aminopropanol.
It is within the range of 00% by weight.

【0018】本発明に用いられる銅含有触媒は、銅を必
須成分として含有する触媒である。触媒における銅の供
給源としては、銅を含有する物質ならどのようなもので
もよく、例えば金属銅、または銅の硝酸塩、硫酸塩、炭
酸塩、酸化物、ハロゲン化物、水酸化物などの無機化合
物、ギ酸塩、酢酸塩、プロピオン酸塩、乳酸塩などの有
機酸塩等を使用することができる。触媒の形状には特に
限定はなく、例えば金属銅表面を酸化脱水素により還元
して得られた触媒、ラネー銅合金をアルカリ水溶液で展
開し得られた触媒、ギ酸銅、炭酸銅などを熱分解および
/または還元して得られた活性化銅等をそのまま、また
は耐アルカリ性担体に担持して使用することができる。
好ましい担体の例としては、酸化チタニウム、酸化ジル
コニウム、シリコンカーバイトなどが挙げられる。The copper-containing catalyst used in the present invention is a catalyst containing copper as an essential component. The source of copper in the catalyst may be any substance containing copper, for example, metallic copper or an inorganic compound such as copper nitrate, sulfate, carbonate, oxide, halide or hydroxide. , Organic acid salts such as formate, acetate, propionate, lactate and the like can be used. The shape of the catalyst is not particularly limited, for example, a catalyst obtained by reducing the surface of metallic copper by oxidative dehydrogenation, a catalyst obtained by developing a Raney copper alloy with an alkaline aqueous solution, thermal decomposition of copper formate, copper carbonate, etc. And / or the activated copper or the like obtained by the reduction can be used as it is or after being supported on an alkali-resistant carrier.
Examples of preferred carriers include titanium oxide, zirconium oxide, silicon carbide and the like.

【0019】本発明に使用される触媒としては、上記に
例示したものの中でも、特に、反応への活性、触媒の寿
命の点から、展開ラネー銅および、共沈法または含浸法
により酸化ジルコニウム担体に担持させた銅触媒を用い
ることが好適である。As the catalyst used in the present invention, among the above-exemplified catalysts, in particular, from the viewpoint of activity for reaction and life of the catalyst, expanded Raney copper and zirconium oxide carrier by coprecipitation method or impregnation method are used. It is preferable to use a supported copper catalyst.

【0020】本発明方法におけるβ−アラニン塩生成の
反応の一例を下記に示す。An example of the reaction for producing β-alanine salt in the method of the present invention is shown below.

【化4】 Embedded image

【0021】本発明方法における触媒の使用量は、アミ
ノプロパノールに対して1〜70重量%であることが好
ましく、より好ましくは10〜40%である。反応温度
はアミノプロパノールおよび生成したβ−アラニンの炭
素−窒素結合の熱分解および水素化分解を防ぐため22
0℃以下の温度で行われることが好ましく、通常100
〜210℃、より好ましくは120〜180℃の温度範
囲内で行われる。The amount of the catalyst used in the method of the present invention is preferably 1 to 70% by weight, more preferably 10 to 40% by weight, based on aminopropanol. The reaction temperature is 22 to prevent thermal decomposition and hydrogenolysis of the carbon-nitrogen bond of aminopropanol and the formed β-alanine.
It is preferably carried out at a temperature of 0 ° C. or lower, usually 100
To 210 ° C, more preferably 120 to 180 ° C.

【0022】本発明方法におけるβ−アラニン塩生成反
応は、酸化脱水素反応であって、水素の発生を伴うた
め、出来るだけ反応圧力を下げることが反応速度の面か
ら好ましい。通常、この反応は、反応を液相で進めるた
めの最低圧力以上で行われ、好ましくは5〜50kg/cm
2Gの範囲内で行われる。反応操作法は回分式、半回分
式、連続式のいずれの方法も用いることができる。The β-alanine salt-forming reaction in the method of the present invention is an oxidative dehydrogenation reaction and is accompanied by the generation of hydrogen. Therefore, it is preferable to lower the reaction pressure as much as possible from the viewpoint of the reaction rate. Usually, this reaction is carried out at a pressure equal to or higher than the minimum pressure for proceeding the reaction in a liquid phase, preferably 5 to 50 kg / cm.
It is done within the range of 2 G. As the reaction operation method, any of batch method, semi-batch method and continuous method can be used.

【0023】本発明の方法による目的生成物を捕集する
には、反応混合物を濾過して触媒を分離すれば濾液とし
て目的とするβ−アラニン塩の水溶液が得られる。ある
いは反応混合物を静置して触媒を沈降させ、目的とする
β−アラニンの水溶液を上澄み液として分離捕集し、こ
れを必要に応じて適宜精製して高品質のβ−アラニン塩
を製品として得ることができる。一方、濾過あるいは沈
降などによって分離した触媒を回収し、それをそのまま
次の反応に再使用することができる。もちろん、回収し
た触媒を必要に応じて適宜再生処理を行って使用しても
よい。In order to collect the desired product by the method of the present invention, the reaction mixture is filtered to separate the catalyst, and an aqueous solution of the desired β-alanine salt is obtained as a filtrate. Alternatively, the reaction mixture is allowed to stand and the catalyst is allowed to settle, and the desired aqueous solution of β-alanine is separated and collected as a supernatant, which is appropriately purified as necessary to obtain a high-quality β-alanine salt as a product. Obtainable. On the other hand, the catalyst separated by filtration or sedimentation can be recovered and reused as it is in the next reaction. Of course, the recovered catalyst may be subjected to a regeneration treatment as needed and used.

【0024】本発明方法により得られるβ−アラニン塩
は高純度であるので、そのまま次の反応又は用途に供す
ことができる。少量の未反応アミノプロパノールの存在
が許されない場合は、これを減圧で容易に留去すること
ができる。微量の副生IDPNを除去する場合は、公知
の方法で行えばよいが、アクリロニトリルから合成した
ものに比べ含有量が少ないことから、精製に要する負荷
は少ない。Since the β-alanine salt obtained by the method of the present invention has high purity, it can be directly used for the next reaction or use. If the presence of small amounts of unreacted aminopropanol is not allowed, it can be easily distilled off under reduced pressure. The removal of a small amount of by-product IDPN may be carried out by a known method, but its content is smaller than that synthesized from acrylonitrile, so that the load required for purification is small.

【0025】[0025]

【実施例】下記実施例により本発明を具体的に説明する
が、本発明はこれら実施例により制限されるものではな
い。The present invention will be described in detail with reference to the following examples, but the present invention is not limited to these examples.

【0026】下記実施例における、アミノプロパノール
の転化率およびβ−アラニンの選択率は下記式から算出
した。 アミノプロパノールの転化率(%)=(反応したアミノ
プロパノールのモル数)÷(反応に供したアミノプロパ
ノールの全モル数)×100 β−アラニンの選択率(%)=(生成したβ−アラニン
のモル数)÷(反応したアミノプロパノールのモル数)
×100The conversion of aminopropanol and the selectivity of β-alanine in the following examples were calculated from the following formulas. Aminopropanol conversion rate (%) = (number of moles of reacted aminopropanol) / (total number of moles of aminopropanol subjected to reaction) × 100 β-alanine selectivity (%) = (of produced β-alanine Number of moles) ÷ (Number of moles of reacted aminopropanol)
× 100

【0027】実施例1 アミノプロパノール210g、水酸化ナトリウム123
g、水262g、および展開ラネー銅21gを、内容積
1リットルのオートクレーブに仕込み、オートクレーブ
内部を窒素ガスで3回置換したのち、反応温度160
℃、反応圧力10kg/cm2Gの条件下で、水素の発生が無
くなるまで反応を行った。反応に要した時間は、160
℃に昇温後3時間であった。反応終了後、反応液を冷却
して触媒を濾別した。濾液を分析したところ、アミノプ
ロパノールの転化率は99%、β−アラニンの選択率は
90%であった。副生物はIDPANaのみで、ニトリ
ロトリプロピオン酸Naの生成がないことが確認され
た。 Example 1 210 g of aminopropanol, 123 of sodium hydroxide
g, 262 g of water, and 21 g of expanded Raney copper were charged into an autoclave having an internal volume of 1 liter, the inside of the autoclave was replaced with nitrogen gas three times, and then the reaction temperature was set to 160.
The reaction was carried out under conditions of ℃ and reaction pressure of 10 kg / cm 2 G until the generation of hydrogen disappeared. The time required for the reaction is 160
It was 3 hours after the temperature was raised to ℃. After completion of the reaction, the reaction solution was cooled and the catalyst was filtered off. When the filtrate was analyzed, the conversion of aminopropanol was 99% and the selectivity of β-alanine was 90%. It was confirmed that the by-product was only IDPANa, and that there was no production of Na nitrilotripropionate.

【0028】実施例2 アミノプロパノール210g、水酸化カリウム168
g、水289g、およびラネー銅42gを、1リットル
のオートクレーブに仕込み、オートクレーブの内部を窒
素ガスで3回置換したのち、反応温度120℃、反応圧
力10kg/cm2Gの条件下で、もはや水素の発生がなくな
るまで反応を行った。反応に要した時間は、120℃に
昇温後7時間であった。反応終了後、反応液を取り出
し、分析を行ったところ、アミノプロパノールの転化率
は90%、β−アラニンの選択率は87%であった。 Example 2 210 g of aminopropanol and 168 of potassium hydroxide
g, 289 g of water, and 42 g of Raney copper were charged into a 1-liter autoclave, and the inside of the autoclave was replaced with nitrogen gas three times, and then hydrogen was no longer added under the conditions of a reaction temperature of 120 ° C. and a reaction pressure of 10 kg / cm 2 G. The reaction was carried out until the generation of The time required for the reaction was 7 hours after the temperature was raised to 120 ° C. After completion of the reaction, the reaction solution was taken out and analyzed, and it was found that the conversion of aminopropanol was 90% and the selectivity of β-alanine was 87%.

【0029】比較例1 濃アンモニア水(濃度:29重量%)176gを500
mlのオートクレーブに仕込み、これを100℃に加熱し
たのち、アクリロニトリル53gを30分かけてオート
クレーブに圧入した。100℃で30分間加熱し、アク
リロニトリルにアンモニアの付加反応を施した。反応終
了後、オートクレーブを冷却し、反応液を取り出し、反
応液から減圧でアンモニアを除去した。この時の、AP
Nの収率はアクリロニトリルに対し48%であった。反
応液のAPN/IDPN比(重量比)を分析した所、6
2/38であった。この反応液にNaOHを40g加
え、70℃で1時間加熱攪拌してニトリル基の加水分解
を行った。得られたβ−アラニンNa水溶液を分析した
所、β−アラニンの収率はアクリロニトリルに対して4
5%であった。また、β−アラニン/IDPA/ニトリ
ロトリプロピオン酸比(重量比)は64/35/1であ
った。 Comparative Example 1 500 g of 176 g of concentrated aqueous ammonia (concentration: 29% by weight)
After being charged into a ml autoclave and heated to 100 ° C., 53 g of acrylonitrile was introduced under pressure into the autoclave over 30 minutes. The mixture was heated at 100 ° C. for 30 minutes to subject the acrylonitrile to the addition reaction of ammonia. After completion of the reaction, the autoclave was cooled, the reaction solution was taken out, and ammonia was removed from the reaction solution under reduced pressure. AP at this time
The yield of N was 48% based on acrylonitrile. When the APN / IDPN ratio (weight ratio) of the reaction solution was analyzed, 6
It was 2/38. 40 g of NaOH was added to this reaction solution, and the nitrile group was hydrolyzed by heating and stirring at 70 ° C. for 1 hour. When the obtained β-alanine Na aqueous solution was analyzed, the yield of β-alanine was 4 with respect to acrylonitrile.
5%. The β-alanine / IDPA / nitrilotripropionic acid ratio (weight ratio) was 64/35/1.

【0030】[0030]

【発明の効果】本発明方法により、アミノプロパノール
から目的化合物としてβ−アラニン塩を、イミノジプロ
ピオン酸やニトリロトリプロピオン酸などの副生を、従
来技術より著しく抑制しながら、簡便かつ、高収率で製
造することができる。また本発明方法により、アクリロ
ニトリルから合成していた従来法に比べ、高収率かつ高
純度でβ−アラニンを製造することが可能となった。よ
って、本発明方法により、副生物を除去するための精製
工程の必要がなくなり、操作も反応後触媒を濾別するだ
けでよくなり、巨大なアンモニアの除害設備が不要とな
った。これらの結果、β−アラニンの製造コストの大幅
な削減が可能となり、工業的実施が容易となった。Industrial Applicability According to the method of the present invention, β-alanine salt as an objective compound from aminopropanol, by-products such as iminodipropionic acid and nitrilotripropionic acid are significantly suppressed from the prior art, while being simple and high in yield. Can be manufactured in. Further, the method of the present invention makes it possible to produce β-alanine in a high yield and a high purity as compared with the conventional method synthesized from acrylonitrile. Therefore, according to the method of the present invention, the purification step for removing the by-product is not required, and the operation only needs to filter the catalyst after the reaction, and a huge equipment for removing ammonia is not required. As a result, the production cost of β-alanine can be significantly reduced, and industrial implementation becomes easy.

Claims (1)

【特許請求の範囲】[Claims] 【請求項1】 3−アミノプロパノールを、アルカリ金
属の水酸化物およびアルカリ土類金属の水酸化物から選
ばれた少なくとも1種と、水と、銅含有触媒との共存下
において、酸化脱水素することを特徴とするβ−アラニ
ン塩の製造方法。1. Oxidative dehydrogenation of 3-aminopropanol in the presence of at least one selected from alkali metal hydroxides and alkaline earth metal hydroxides, water, and a copper-containing catalyst. A method for producing a β-alanine salt, comprising:
JP7310893A 1995-11-29 1995-11-29 Production of beta-alanine salt Pending JPH09151168A (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
JP7310893A JPH09151168A (en) 1995-11-29 1995-11-29 Production of beta-alanine salt

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
JP7310893A JPH09151168A (en) 1995-11-29 1995-11-29 Production of beta-alanine salt

Publications (1)

Publication Number Publication Date
JPH09151168A true JPH09151168A (en) 1997-06-10

Family

ID=18010658

Family Applications (1)

Application Number Title Priority Date Filing Date
JP7310893A Pending JPH09151168A (en) 1995-11-29 1995-11-29 Production of beta-alanine salt

Country Status (1)

Country Link
JP (1) JPH09151168A (en)

Cited By (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2000066539A1 (en) * 1999-05-03 2000-11-09 Monsanto Technology Llc Process for the preparation of carboxylic acid salts from primary alcohols
JP2011132060A (en) * 2009-12-24 2011-07-07 Fukuei Hiryo Kk Liquid fertilizer
CN115888701A (en) * 2022-11-28 2023-04-04 江西宇能制药股份有限公司 Catalyst for preparing L-aminopropanol by catalytic hydrogenation and preparation method and application thereof

Cited By (5)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2000066539A1 (en) * 1999-05-03 2000-11-09 Monsanto Technology Llc Process for the preparation of carboxylic acid salts from primary alcohols
US6646160B2 (en) * 1999-05-03 2003-11-11 Monsanto Technology, Llc Process for the preparation of carboxylic acid salts from primary alcohols
JP2011132060A (en) * 2009-12-24 2011-07-07 Fukuei Hiryo Kk Liquid fertilizer
CN115888701A (en) * 2022-11-28 2023-04-04 江西宇能制药股份有限公司 Catalyst for preparing L-aminopropanol by catalytic hydrogenation and preparation method and application thereof
CN115888701B (en) * 2022-11-28 2023-10-10 江西宇能制药股份有限公司 Catalyst for preparing L-aminopropanol by catalytic hydrogenation and preparation method and application thereof

Similar Documents

Publication Publication Date Title
JP2916256B2 (en) Method for producing aminocarboxylate
JP2939335B2 (en) Method for producing aminocarboxylate
JP3001685B2 (en) Diamine production method
JPH0747125B2 (en) Method for producing acetic acid derivative
JPH09151168A (en) Production of beta-alanine salt
US4539403A (en) Process for the preparation of a 2-alkyl-4-amino-5-aminomethylpyrimidine
JP3422331B2 (en) Method for producing N, N-disubstituted ethylenediamine
JP2002518364A (en) Symmetric and asymmetric disubstitution of carboxamides using organic titanates and Grignard reagents
JP2804877B2 (en) Production method of aminocarboxylate
JP3761231B2 (en) Nickel and molybdenum-containing Raney copper catalyst for aminocarboxylate production and method for producing aminocarboxylate using the same
JP4001937B2 (en) Aminopropionitrile production process
JPH05286889A (en) Production of arylacetic acid and its alkali metal salt
JP3129547B2 (en) Method for producing glycolate
JPH02180854A (en) Production of n,n-diisopropylethylamine
JPH0153863B2 (en)
JPH10316639A (en) Production of 5-amino-2,4,6-triidoisophthalic acid
JP2968104B2 (en) Method for producing aminocarboxylate
JPH072743A (en) Production of aminocarboxylic acid salt
JP4817572B2 (en) Preparation method of organic compound and recovery method of promoter
JPS59157039A (en) Production of xylylene glycol
GB2118172A (en) Preparation of a 2-alkyl-4- amino-5-aminomethylpyrimidine
JPS6017780B2 (en) Method for producing 4-aminomethylbenzoic acid
JPH048423B2 (en)
CN117820217A (en) Synthesis method of regorafenib key intermediate
JP2907523B2 (en) Method for producing cinnamic acids

Legal Events

Date Code Title Description
A977 Report on retrieval

Free format text: JAPANESE INTERMEDIATE CODE: A971007

Effective date: 20051215

A131 Notification of reasons for refusal

Free format text: JAPANESE INTERMEDIATE CODE: A131

Effective date: 20060207

A02 Decision of refusal

Free format text: JAPANESE INTERMEDIATE CODE: A02

Effective date: 20060606