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JPS5899432A - Unsaturated fatty acid or its salt and fungicide containing the same - Google Patents

Unsaturated fatty acid or its salt and fungicide containing the same

Info

Publication number
JPS5899432A
JPS5899432A JP19907181A JP19907181A JPS5899432A JP S5899432 A JPS5899432 A JP S5899432A JP 19907181 A JP19907181 A JP 19907181A JP 19907181 A JP19907181 A JP 19907181A JP S5899432 A JPS5899432 A JP S5899432A
Authority
JP
Japan
Prior art keywords
dimethyl
methyl
acid
salt
stretching vibration
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.)
Granted
Application number
JP19907181A
Other languages
Japanese (ja)
Other versions
JPS6312457B2 (en
Inventor
Akihiro Kawasaki
川崎 明裕
Masanobu Taniguchi
政信 谷口
Masaaki Matsui
松井 正明
Keizo Kase
加勢 啓三
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.)
Cosmo Oil Co Ltd
Original Assignee
Maruzen Oil 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 Maruzen Oil Co Ltd filed Critical Maruzen Oil Co Ltd
Priority to JP19907181A priority Critical patent/JPS5899432A/en
Publication of JPS5899432A publication Critical patent/JPS5899432A/en
Publication of JPS6312457B2 publication Critical patent/JPS6312457B2/ja
Granted legal-status Critical Current

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  • Food Preservation Except Freezing, Refrigeration, And Drying (AREA)
  • Organic Low-Molecular-Weight Compounds And Preparation Thereof (AREA)
  • Agricultural Chemicals And Associated Chemicals (AREA)

Abstract

NEW MATERIAL:An unsaturated fatty acid of the formula[A is CH3-CH2-CH2-, CH3-C(CH3)H-; M is H, Na, Zn; n is M's valency]or its salt. EXAMPLE:2,7-Dimethyl-4-octenoic acid. USE:Fungicide: it has low toxicity and low irritating properties, shows a wide antibiotic activity against various kinds of microorganisms, especially shows excellent antibactericidal effect against gram-negative bacteria. it is used for food, cosmetics, medicines, paints and other purposes. PREPARATION:For example, 2,7-dimethyl-4-octenoic acid (M is H in the formula) and 2-methyl-4-nonenoic acid are prepared by hydroxylating 2,7-dimethyl-1,4- octadiene and 2-methyl-1,4-nonadiene resulting from altenate copolymerization of propylene with butadiene, followed by oxidation of the product.

Description

【発明の詳細な説明】 MはH、NaまたはZnそしてnはMの原子価である)
で表わされる新規な不飽和ロ旨肪酸またはその塩並びに
それを有効成分とするところの抗菌剤に関するものであ
る。[Detailed description of the invention] M is H, Na or Zn and n is the valence of M)
The present invention relates to a novel unsaturated fatty acid represented by the formula or a salt thereof, and an antibacterial agent containing the same as an active ingredient.

食品、化粧品、医薬品、塗料等は微生物による汚染を受
けやすく、その汚染による被害は多大である。従来、こ
れらの製品の微生物汚染防止剤が種々開発され使用され
ている。例えば、有機水銀や有機スズ等の有機金属類や
芳香族フェノール類等が汚染防止剤として使用されてき
たが、毒性が強いうえ残留蓄積性が高く、社会的に問題
になつている。Foods, cosmetics, pharmaceuticals, paints, etc. are easily contaminated by microorganisms, and the damage caused by such contamination is enormous. Conventionally, various microbial contamination inhibitors for these products have been developed and used. For example, organic metals such as organic mercury and organic tin, aromatic phenols, and the like have been used as anti-pollution agents, but they are highly toxic and have a high tendency to accumulate residue, which has become a social problem.

一方、低毒性でかつ低刺激性の微生物汚染防止剤として
ソルビン酸、ウンデシレン酸、2−エチルヘキシル酸等
の脂肪酸あるいはそれらのナトリウム塩や亜鉛塩等が用
いられているが、これらはダラム陰性細菌、例えばPs
eudomonas aeruginosa(緑膿菌)
、に対する抗菌活性が低い。On the other hand, fatty acids such as sorbic acid, undecylenic acid, and 2-ethylhexylic acid, or their sodium salts and zinc salts are used as low-toxicity and hypoallergenic microbial contamination preventive agents, but these are effective against Durum-negative bacteria. For example, Ps
eudomonas aeruginosa (Pseudomonas aeruginosa)
, has low antibacterial activity against.

本発明は、上記従来品の欠点を克服した低毒性、低刺激
性の新規かつ有用な抗菌剤を提供するものであり、本発
明の抗菌剤は新規化合物である。The present invention provides a new and useful antibacterial agent with low toxicity and low irritation that overcomes the drawbacks of the conventional products, and the antibacterial agent of the present invention is a new compound.

本発明の化合物は、低毒性、低刺激性であり各種微生物
に対して幅広い抗菌活性を有し、特にグラろ陰性菌に対
し、すぐれた抗菌性を有する。The compound of the present invention has low toxicity and low irritation, and has a wide range of antibacterial activity against various microorganisms, and particularly has excellent antibacterial activity against Guraro-negative bacteria.

本発明の〔1〕式の化合物のうち、MがHである2、7
−シメチルー4−オクテン酸および2−メチル−4−ノ
ネン酸はさきに本発明者等が提案した方法、すなわちプ
ロピレンとブタジェンとの交互共重合反応によって得ら
れる2、7−ジメチル−1゜4−オクタジエンおよび2
−メチル−1,4−ノナジェンをヒドロキシル化して2
.7−ジメチル−4−オクテン−1−オールおよび2−
メチル−4−ノネン−1−オールとしたのち(特開昭5
6−108721)、さらにそれを酸化することによっ
て得られる。Among the compounds of formula [1] of the present invention, 2, 7 in which M is H
-Simethyl-4-octenoic acid and 2-methyl-4-nonenoic acid are 2,7-dimethyl-1゜4- obtained by the method previously proposed by the present inventors, that is, by alternating copolymerization reaction of propylene and butadiene. Octadiene and 2
- Hydroxylation of methyl-1,4-nonadiene to 2
.. 7-dimethyl-4-octen-1-ol and 2-
After converting it into methyl-4-nonen-1-ol (Unexamined Japanese Patent Publication No.
6-108721) and further oxidize it.

2.7−シメチルー!、4−オクタジエンおよび2−メ
チル−1,4−ノナジェンのヒドロキシル化は、ジポラ
ンを用いてハイドロボレーション反応させた後、酸化加
水分解する方法、またはトリアルキルアルミニウムを用
いてハイドロアルミネーショ/反応させた後、酸化加水
分解する方法によって行われる。2.7-cymethyl! , 4-octadiene and 2-methyl-1,4-nonadiene can be hydroxylated by hydroboration reaction using diporane followed by oxidative hydrolysis, or by hydroalumination/reaction using trialkylaluminium. This is done by oxidative hydrolysis after drying.

また、2.7−シメチルー4−オクテン−1−オールお
よび2−メチル−4−ノネン−1−オールの酸化は、空
気、酸素、硝酸、過マンガン酸塩、クロム酸塩、有機過
酸化物、過硫酸、過酸化水素等の酸化剤を用いる一般の
酸化法によっても酸化することが出来るが、選択率、収
率の点で充分でなくカセイソーダ、カセイカリを反応せ
しめて脱水素によりカルボン酸のアルカリ金属塩を得る
酸化法が好ましい。アルコールとカセイアルカリとの反
応を水素雰囲気下で行なうことが選択率、収率を高める
上で好ましい。この反応に際しては、Mn、 Co、 
Ni、 Ag、 Pt、 Hg、 Zn等の酸化物が触
媒として用いられる。ここで得られた生成物はカルボン
酸のアルカリ金属塩であるので、遊離のカルボン酸を得
るためには加水分解が必要であり、この加水分解は常法
により行われ得る。この加水分解は生成物の純度を高め
るだめの精製工程としても有用である。In addition, 2,7-dimethyl-4-octen-1-ol and 2-methyl-4-nonen-1-ol can be oxidized using air, oxygen, nitric acid, permanganate, chromate, organic peroxide, Oxidation can also be carried out by a general oxidation method using an oxidizing agent such as persulfuric acid or hydrogen peroxide, but it is not sufficient in terms of selectivity and yield. Oxidation methods that yield metal salts are preferred. It is preferable to carry out the reaction between the alcohol and the caustic alkali in a hydrogen atmosphere in order to increase selectivity and yield. During this reaction, Mn, Co,
Oxides such as Ni, Ag, Pt, Hg, and Zn are used as catalysts. Since the product obtained here is an alkali metal salt of a carboxylic acid, hydrolysis is necessary to obtain the free carboxylic acid, and this hydrolysis can be carried out by a conventional method. This hydrolysis is also useful as a purification step to increase product purity.

本発明のCI’3式の化合物のうち、MがNaである2
、7−シメチルー4−オクテン酸ナトリウムおよび2−
メチル−4−ノネン酸ナトリウムは、2゜7−ジメチル
−4−オクテン酸および2−メチル−4−ノネン酸と水
酸化ナトリウムの水溶液とを常温付近の温度で接触させ
ることにより容易に得られる。Among the compounds of formula CI'3 of the present invention, 2 in which M is Na
, sodium 7-dimethyl-4-octenoate and 2-
Sodium methyl-4-nonenoate can be easily obtained by bringing 27-dimethyl-4-octenoic acid and 2-methyl-4-nonenoic acid into contact with an aqueous solution of sodium hydroxide at a temperature around room temperature.

本発明(13式の化合物のうち、MがZnである2、7
−シメチルー4−オクテン酸亜鉛および2−メチル−4
−ノネン酸亜鉛は、2.7−シメチルー、1−オクテン
酸ナトリウムおよび2−メチル−4−ノネン酸ナトリウ
ムと塩化亜鉛の水溶液とを常温付近の温度で接触させる
ことにより容易に得られる。The present invention (among the compounds of formula 13, 2, 7 in which M is Zn)
-zinc cymethyl-4-octenoate and 2-methyl-4
Zinc nonenoate can be easily obtained by bringing 2,7-dimethyl-, sodium 1-octenoate, and sodium 2-methyl-4-nonenoate into contact with an aqueous solution of zinc chloride at a temperature around room temperature.

本発明の抗菌剤としては〔13式で表示される本発明化
合物を単独であるいは2種以上を混合したものをそのま
ま使用することも、あるいは適当々補助剤と併用して使
用することもできる。As the antibacterial agent of the present invention, the compounds of the present invention represented by formula 13 may be used alone or in combination with two or more thereof, or may be used in combination with appropriate adjuvants.

以下に実施例を示して本発明を更に具体的に説明するが
、これらは単に例示の目的で記載するもので計り、本発
明はこれらによって限定されるものと解されるべきでは
ない。EXAMPLES The present invention will be described in more detail with reference to Examples below, but these are merely for illustrative purposes and the present invention should not be construed as being limited by these.

実施例12.7−シメチルー4−オクテン酸攪拌装置の
ついた容量100m1のステンレス製オートクレーブに
参考例1で合成した2、7−シメチルー4−オクテン−
1−オール15.6i、カセイソーダ484?、活性炭
0.8?、酸化亜鉛0.79−及び水0.09iを入れ
、オートクレーブ内の空気を水素ガスで置換した後、攪
拌しながら300Cに加熱した。反応により発生する水
素ガスをオートクレーブの外に放出し、オートクレーブ
の内圧を常時2Q Ky/m 2に保った。300 t
:’に昇温後、約3時間で反応を終了させ、オートクレ
ーブを冷却後内容物を取り出した。Example 12.7-Dimethyl-4-octenoic acid 2,7-dimethyl-4-octenoic acid synthesized in Reference Example 1 was placed in a stainless steel autoclave with a capacity of 100 ml equipped with a stirring device.
1-all 15.6i, caustic soda 484? , activated carbon 0.8? , 0.79 i of zinc oxide, and 0.09 i of water were added, and after replacing the air in the autoclave with hydrogen gas, the autoclave was heated to 300 C with stirring. Hydrogen gas generated by the reaction was discharged to the outside of the autoclave, and the internal pressure of the autoclave was constantly maintained at 2Q Ky/m 2 . 300t
The reaction was completed in about 3 hours after the autoclave was heated to .

オートクレーブから取り出した内容物に30重量係濃度
の硫酸水溶液を加えて酸性とし、油層を水洗してから、
減圧蒸留により無色透明で若干粘性のある液状の2.7
−シメチルー4−オクテン酸を14y−得た。Add an aqueous sulfuric acid solution with a concentration of 30% by weight to the contents taken out from the autoclave to make it acidic, wash the oil layer with water, and then
2.7 is a colorless, transparent and slightly viscous liquid obtained by distillation under reduced pressure.
-Simethyl-4-octenoic acid 14y- was obtained.

赤外吸収(IR)スペクトル 3100〜360ocrn  カルボキシル基伸縮振動
(強度 中)2950 cm   メチル基伸縮振動 
   (〃 強)1720//   カルボニル基伸縮
振動  (〃〃)956 〃  トランス二重結合面外
変角振動(〃〃)生成物のTRスペクトルを第1図に示
す。Infrared absorption (IR) spectrum 3100-360ocrn Carboxyl group stretching vibration (medium intensity) 2950 cm Methyl group stretching vibration
(〃 Strong) 1720// Carbonyl group stretching vibration (〃〃) 956 〃 Trans double bond out-of-plane bending vibration (〃〃) The TR spectrum of the product is shown in FIG.

実施例22,7−シメチルー4−オクテン酸ナトリウム 500+++Jのビーカーに水酸化ナトリウム4?を入
れ、水200m1を加えて溶かした。つぎにその−一カ
ーに攪拌下実施例1と同じ方法で合成した2、7−シメ
チルー4−オクテン酸19.5%を徐々に添加し、約3
0分間室温で反応させた。Example 2 Sodium 2,7-dimethyl-4-octenoate In a beaker of 500++J, add 4% sodium hydroxide. and 200ml of water was added to dissolve it. Next, 19.5% of 2,7-dimethyl-4-octenoic acid synthesized in the same manner as in Example 1 was gradually added to the car with stirring, and about 3.
The reaction was allowed to proceed for 0 minutes at room temperature.

エーテルで未反応の2.7−シメチルー4−オクテン酸
を抽出して除去した後、水層の水を減圧下で追い出し、
乾燥して白色粉末状の2,7−シメチルー4−オクテン
酸ナトリウム19.454を得た。After extracting and removing unreacted 2,7-dimethyl-4-octenoic acid with ether, the water in the aqueous layer was removed under reduced pressure.
After drying, 19.454 sodium 2,7-dimethyl-4-octenoate was obtained as a white powder.

赤外吸収(IR)スペクトル 2960crn  メチル基伸縮振動    (強度 
強)2930 //  メチレン基伸縮振動   (/
///)1550//   カルボン酸イオン逆対称伸
縮振動(//   //)1460//  メチレン基
変角振動   (//  中)1410  //   
カルボン酸イオン対称伸縮振動(〃 強)1375//
  メチル基変角振動   (〃 中)965//)ラ
ンスC−H変角振動 (〃 強)生成物のTRスペクト
ルを第2図に示す。Infrared absorption (IR) spectrum 2960crn Methyl group stretching vibration (intensity
Strong) 2930 // Methylene group stretching vibration (/
///) 1550 // Carboxylic acid ion antisymmetric stretching vibration (// //) 1460 // Methylene group bending vibration (// middle) 1410 //
Carboxylic acid ion symmetrical stretching vibration (strong) 1375//
Figure 2 shows the TR spectrum of the methyl group bending vibration (medium) 965//) lance C-H bending vibration (strong) product.

実施例32.7−シメチルー4−オクテン酸亜鉛500
m1のビーカーに実施例2で得た2、7−シメチルー4
−オクテン酸ナトリウム10y−を入れ、水20(IJ
を加えて溶かした。そのビーカーに攪拌下、塩化亜鉛3
.5f!−を水50ccに溶かした溶液を徐々に添加し
た後、室温で30分間反応させた。Example 3 2.7-dimethyl-4-octenoic acid zinc 500
2,7-dimethyl-4 obtained in Example 2 in a beaker of m1
- Add 10y of sodium octenoate, and add 20y of water (IJ
was added and dissolved. In the beaker, under stirring, add 3 parts of zinc chloride.
.. 5f! - was dissolved in 50 cc of water was gradually added, and the mixture was allowed to react at room temperature for 30 minutes.

析出した2、7−シメチルー4−オクテン酸亜鉛を濾過
により分離し、水洗後減圧乾燥して無色透明々半固体法
の2.7−シメチルー4−オクテン酸亜鉛を9.IJ得
た。The precipitated zinc 2,7-dimethyl-4-octenoate was separated by filtration, washed with water, and dried under reduced pressure to obtain colorless, transparent, semi-solid zinc 2,7-dimethyl-4-octenoate. I got IJ.

赤外吸収(IR)スペクトル 2960crn  メチル基伸縮振動    (強度節
)2930〃  メチレン基伸縮振動   (〃〃)1
550//   カルボン酸イオン逆対称伸縮振動(〃
〃)1460//  メチレン基変角振動   (〃 
中)1430//   カルボ/酸イオン対称伸縮振動
(//  強)1375//  メチル基変角振動  
  (//  中)965〃トランスC−H変角振動 
(〃 強)生成物のIR,スペクトルを第3図に示す。Infrared absorption (IR) spectrum 2960 crn Methyl group stretching vibration (intensity node) 2930〃 Methylene group stretching vibration (〃〃) 1
550// Carboxylic acid ion antisymmetric stretching vibration (〃
〃)1460// Methylene group bending vibration (〃
Medium) 1430// Carbo/acid ion symmetrical stretching vibration (// Strong) 1375// Methyl group bending vibration
(// Medium) 965〃Trans C-H bending vibration
(Strong) The IR spectrum of the product is shown in Figure 3.

実施例42−メチル−4−ノネン酸 実施例1において、2.7−シメチルー4−オクテン−
1−オールの代りに、参考例2で合成した2−メチル−
4−ノネン−1−オール16.0iを使用した以外は同
一の条件下で反応させて無色透明で若干粘性のある液状
の2−メチル−4−ノネン酸15iを得た。Example 4 2-Methyl-4-nonenoic acid In Example 1, 2,7-dimethyl-4-octene-
2-methyl- synthesized in Reference Example 2 instead of 1-ol
The reaction was carried out under the same conditions except that 4-nonen-1-ol 16.0i was used to obtain 2-methyl-4-nonenoic acid 15i as a colorless, transparent and slightly viscous liquid.

IFtスペクトル 3100−3600Crn−1カルボン酸0−H伸縮振
動(強度 中)2960crn−1メチル基伸縮振動 
  (〃 強)2930〃   メチレン基伸縮振動 
 (〃〃)1720//   カルボニル基伸縮振動 
(////)1460 //   メチレン基変角振動
  (〃 中)1375//   メチル基変角振動 
  (////)12401/   C−0伸縮振動 
   (l) 強)965//   l−ランスC−H
変角振動(////)生成物のTRスペクトルを第4図
に示す。IFt spectrum 3100-3600Crn-1 Carboxylic acid 0-H stretching vibration (medium intensity) 2960crn-1 Methyl group stretching vibration
(Strong) 2930 Methylene group stretching vibration
(〃〃)1720// Carbonyl group stretching vibration
(////) 1460 // Methylene group bending vibration (〃 Medium) 1375 // Methyl group bending vibration
(////)12401/ C-0 stretching vibration
(l) Strong) 965// l-Lance C-H
The TR spectrum of the bending vibration (////) product is shown in FIG.

実施例52−メチル−4−ノネン酸ナトリウムの合成 実施例2において、2,7−シメチルー4−オクテン酸
19.5%の代りに、実施例4と同じ方法で得られた2
−メチル−4−ノネン酸18y−を用いた以外は同一の
条件下で反応させて、白色粉末状の2−メチル−4−ノ
ネン酸ナトリウム17.9iを得た。Example 5 Synthesis of sodium 2-methyl-4-nonenoate In Example 2, 2,7-dimethyl-4-octenoic acid (19.5%) was replaced with 2, which was obtained in the same manner as in Example 4.
The reaction was carried out under the same conditions except that -methyl-4-nonenoic acid 18y- was used to obtain 17.9i of sodium 2-methyl-4-nonenoic acid in the form of a white powder.

TRスペクトル 2960crn−1メチル基伸縮振動   (強度節)
2930Crn−1メチレン基伸縮振動   (強度節
)1560 〃  カルボン酸イオン逆対称伸縮振動(
////)1460//  メチレン基変角振動   
(〃 中)1410  〃 カルボン酸イオン対称伸縮
振動(〃 強)1375〃  メチル基変角振動   
 (//  中)965/’l−ランスC−H変角振動
  (〃 強)生成物のIFLスペクトルを第5図に示
す。TR spectrum 2960crn-1 methyl group stretching vibration (intensity node)
2930Crn-1 Methylene group stretching vibration (intensity node) 1560 〃 Carboxylic acid ion antisymmetric stretching vibration (
////)1460// Methylene radical bending vibration
(Medium) 1410 Carboxylic acid ion symmetrical stretching vibration (Strong) 1375 Methyl group bending vibration
(// Medium) 965/'l-Lance C-H bending vibration (Strong) The IFL spectrum of the product is shown in FIG.

実施例62−メチル−4−ノネン酸亜鉛の合成実施例3
において、2,7−シメチルー4−オクテン酸ナトリウ
ム1Ofの代りに実施例5で得られた2−メチル−4−
ノネン酸ナトリウム107を用いた以外は同一の条件下
で反応させて無色透明な半固体状の2−メチル−4−ノ
ネン酸亜鉛9.2g−を得た。Example 6 Synthesis of zinc 2-methyl-4-nonenoate Example 3
2-methyl-4-obtained in Example 5 in place of 1Of sodium 2,7-dimethyl-4-octenoate.
The reaction was carried out under the same conditions except that sodium nonenoate 107 was used to obtain 9.2 g of colorless and transparent semi-solid zinc 2-methyl-4-nonenoate.

IRスペクトル 2960Crn−1メチル基伸縮振動 2930〃  メチレン基伸縮振動 1570/I  カルボン酸イオン逆対称伸縮振動14
60 〃  メチレン基変角振動 1430//  カルボン酸イオン対称伸縮振動137
5crn−’ メチル基変角振動965//)ランスC
−H変角振動 生成物のIRスペクトルを第6図に示す。IR spectrum 2960Crn-1 Methyl group stretching vibration 2930 Methylene group stretching vibration 1570/I Carboxylic acid ion reverse symmetric stretching vibration 14
60 〃 Methylene group bending vibration 1430 // Carboxylic acid ion symmetric stretching vibration 137
5crn-' Methyl group bending vibration 965//) Lance C
The IR spectrum of the -H bending vibration product is shown in FIG.

実施例7 本発明に係る2、7−シメチルー4−オクテン酸、2.
7−シメチルー4−オクテン酸ナトリウム、2゜7−シ
メチルー4−オクテン酸亜鉛、2−メチル−4−ノネン
酸、2−メチル−4−ノネン酸ナトリウムおよび2−メ
チル−4−ノネン酸亜鉛の各種微生物に対する最小発育
阻止濃度(MIC)を表1に、また比較のためにウンデ
シレン酸、つ/デシレン酸ナトリウム、ウンデシレン酸
亜鉛、カゾリル酸、カプリル酸ナトリウム、カゾリル酸
亜鉛およびパラオキシ安息香酸n−ノロぎルのMICを
表2に示す。Example 7 2,7-dimethyl-4-octenoic acid according to the present invention, 2.
Various types of sodium 7-dimethyl-4-octenoate, zinc 2゜7-dimethyl-4-octenoate, 2-methyl-4-nonenoic acid, sodium 2-methyl-4-nonenoate and zinc 2-methyl-4-nonenoate. The minimum inhibitory concentration (MIC) against microorganisms is shown in Table 1, and for comparison, undecylenic acid, sodium decylenate, zinc undecylenate, casorylic acid, sodium caprylate, zinc casorylate, and n-p-oxybenzoate. Table 2 shows the MICs of the samples.

試験法: 細菌用培地は普通寒天培地を、また真菌用培地はポテト
デキストロース寒天培地を使用した。そして抗菌性を検
討するために使用した接種用菌液は、細菌についてはブ
イヨン培地に35C−夜培養したものを用いた。Test method: An ordinary agar medium was used as a bacterial medium, and a potato dextrose agar medium was used as a fungal medium. In the inoculating bacterial solution used to examine antibacterial properties, bacteria were cultured in a bouillon medium at 35C overnight.

ただし、Bacillus 5ubtilis ATC
C6633については胞子懸濁液を用いた。また糸状菌
についてはポテトデキストロース寒天斜面培地に接種培
養後十分に胞子を形成させ、滅菌した0、005qbジ
オクチルコハク酸ナトリウム溶液に胞子を懸濁したもの
(1ml当り約10個)を用いた。However, Bacillus 5ubtilis ATC
For C6633, a spore suspension was used. For filamentous fungi, spores were sufficiently formed after inoculating and culturing potato dextrose agar slant medium, and the spores were suspended in a sterilized 0,005 qb sodium dioctyl succinate solution (approximately 10 per ml).

さらに酵母についてはポテトデキストロース寒天斜面培
地に接種培養後、十分に菌体を形成させ、菌体を滅菌生
理食塩水に懸濁したもの(1ml当り約10 個)を用
いた。Furthermore, yeast was inoculated and cultured on a potato dextrose agar slant medium, allowed to sufficiently form bacterial cells, and suspended in sterile physiological saline (approximately 10 cells per ml).

試験液は試験試薬を一定量精秤後、滅菌脱イオン水また
は50係エチルアルコール溶液等にて任意に希釈し、添
加後の濃度が12.5.25.50.100.200.
400.800.1600ppmになるように調整した
After accurately weighing a certain amount of the test reagent, the test solution is arbitrarily diluted with sterile deionized water or 50% ethyl alcohol solution, etc., and the concentration after addition is 12.5.25.50.100.200.
It was adjusted to 400.800.1600 ppm.

平板は試験液を加熱滅菌後の培地100m1に対し1 
mlの割合に添加後十分混合し、その15mJを分液固
化させてつくった。For the flat plate, add the test solution to 100ml of the medium after heat sterilization.
After adding the solution to a ratio of 1.0 ml, the mixture was thoroughly mixed, and 15 mJ of the solution was separated and solidified.

抗菌力の測定は各濃度段階の平板に接種菌液を一白金耳
塗布し、細菌の場合は35Cで24時間、真菌(糸状菌
、酵母)については30Cで6日間培養後、それぞれの
菌の発育の有無を肉眼にて判定して最小発育阻止濃度(
MIC)を出した。To measure the antibacterial activity, a loopful of the inoculum solution was applied to a plate at each concentration level, and after culturing at 35C for 24 hours for bacteria and 6 days at 30C for fungi (filamentous fungi, yeast), The presence or absence of growth is determined visually and the minimum inhibitory concentration (
MIC) was issued.

なお、使用された菌株は細菌として 5taphylococcus aureus 653
8−p (黄色ブドウ球菌)、Bacillus 5u
btilis ATCC6633(枯草菌)、Esch
erichia coli 0−55 (大腸菌)およ
びPseudomonas aeruginosa (
緑膿菌)の4種類、糸状菌としてAspergillu
s niger (黒コウジカビ)、Aspergil
lus flavus、  Fusarium mon
iliformeNAL−F−616、Penicil
lium citrinum 。The strain used was 5taphylococcus aureus 653 as a bacterium.
8-p (Staphylococcus aureus), Bacillus 5u
btilis ATCC6633 (Bacillus subtilis), Esch
erichia coli 0-55 (E. coli) and Pseudomonas aeruginosa (
4 types of Pseudomonas aeruginosa), Aspergillus as a filamentous fungus
s niger (black aspergillus), Aspergillus
lus flavus, Fusarium mon
iliformeNAL-F-616, Penicil
lium citrinum.

Cladosporium cladosporioi
des%TrichodermaおよびChaetom
ium globosum ATCC6205の7種類
とSaccharomyces cerevisiae
 QC−2(ブドウ酒酵母)である。Cladosporium cladosporioi
des% Trichoderma and Chaetom
Seven types of Saccharomyces globosum ATCC6205 and Saccharomyces cerevisiae
It is QC-2 (grape yeast).

参考例1 2,7−シメチルー4−オクテン−1−オール窒素置換
した滴下ロート付き2!の20フラスコにトランス−2
,7−シメチルー1.4−オクタジエン19ozおよび
テトラヒドロフラン500m/!を仕込み0〜5Cに冷
却した後、攪拌下、滴下ロートよりジボランのテトラヒ
ドロフラン溶液(濃度1モル/、g ) 200 ml
を30分間要して滴下した。さらに、温度0〜IOCで
5時間攪拌した後、3N水酸化ナトIJウム溶液100
iJと30係過酸化水素水100m1を加え酸化加水分
解した。Reference Example 1 2,7-dimethyl-4-octen-1-ol with nitrogen-substituted dropping funnel 2! trans-2 into 20 flasks of
, 7-dimethyl-1,4-octadiene 19oz and tetrahydrofuran 500m/! After cooling to 0-5C, add 200 ml of diborane in tetrahydrofuran solution (concentration 1 mol/g) from the dropping funnel while stirring.
was added dropwise over a period of 30 minutes. Furthermore, after stirring for 5 hours at a temperature of 0 to IOC, 100% of 3N sodium hydroxide solution was added.
iJ and 100 ml of 30% hydrogen peroxide solution were added to carry out oxidative hydrolysis.

生成物をエーテルで抽出し、常法で処理した後減圧蒸溜
により柑橘系の香りの無色透明な液体である2、7−シ
メチルー4−オクテン−1−オール(b、p=68〜7
3C/2mmHg、 n14=1.4.502)を35
7得た。The product was extracted with ether, treated in a conventional manner, and then distilled under reduced pressure to obtain 2,7-dimethyl-4-octen-1-ol (b, p = 68-7), which is a colorless and transparent liquid with a citrus aroma.
3C/2mmHg, n14=1.4.502) to 35
I got 7.

参考例2 2−メチル−4−ノネン−1−オール 窒素置換した滴下ロート付き2!ρ20ナスフラスコに
、2−メチル−1,4−ノナジェン190g−、テトラ
ヒドロフラン500m/!を仕込み、温度0〜5Cに冷
却した後、攪拌下ジボランのテトラヒドロフラン溶液(
濃度1モル々)2oomgを30分間を要し滴下した。Reference Example 2 2-Methyl-4-nonen-1-ol 2 with nitrogen-substituted dropping funnel! In a ρ20 eggplant flask, 190 g of 2-methyl-1,4-nonadiene and 500 m of tetrahydrofuran! After cooling to a temperature of 0 to 5C, a solution of diborane in tetrahydrofuran (
2 oomg (concentration: 1 molar) was added dropwise over 30 minutes.

さらに温度0〜10Cで5時間攪拌した後、3N水酸化
ナトリウム溶1100mlおよび30循過酸化水素水1
00m1を加えて酸化加水分解した。After further stirring for 5 hours at a temperature of 0 to 10C, 1100ml of 3N sodium hydroxide solution and 1100ml of 30% circulating hydrogen oxide solution were added.
00ml was added for oxidative hydrolysis.

生成物をエーテル抽出し、常法で処理した後、減圧蒸溜
によりフローラル臭を有する無色透明な液体である2−
メチル−4−ノネン−1−オール(b、p = 70〜
75 C/2mm+Hg、 n14= 1.4528 
)を36%得た。The product was extracted with ether, treated in a conventional manner, and then distilled under reduced pressure to obtain 2-, which is a colorless and transparent liquid with a floral odor.
Methyl-4-nonen-1-ol (b, p = 70~
75 C/2mm+Hg, n14=1.4528
) was obtained by 36%.

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

第1図は実施例1の、第2図は実施例2の、第3図は実
施例3の、第4図は実施例4の、第5図は実施例5のそ
して第6図は実施例6のそれぞれの生成物のI[スペク
トルである。FIG. 1 shows Example 1, FIG. 2 shows Example 2, FIG. 3 shows Example 3, FIG. 4 shows Example 4, FIG. 5 shows Example 5, and FIG. 6 shows Example 2. I Spectrum of each product of Example 6.

Claims (1)

【特許請求の範囲】 MはH,NaまたはZnセしてnはMの原子価である) で表わされる不飽和脂肪酸またはその塩。 CH3 (2)AがCH3−CI−(−であり、MがZnである
特許請求の範囲第1項に記載の塩。 MはH,NaまたはZnそしてnはMの原子価である)
で表わされる不飽和脂肪酸またはその塩からなる抗菌剤
。 CH3 (4)AがCH3−CH−であり、MがZnである特許
請求の範囲第3項に記載の抗菌剤。 (5)防除の対象となる菌類がダラム陰性菌である特許
請求の範囲第4項に記載の抗菌剤。[Scope of Claims] An unsaturated fatty acid or a salt thereof represented by: M is H, Na or Zn, and n is the valence of M. CH3 (2) The salt according to claim 1, wherein A is CH3-CI- (- and M is Zn. M is H, Na or Zn and n is the valence of M).
An antibacterial agent consisting of an unsaturated fatty acid or a salt thereof. The antibacterial agent according to claim 3, wherein CH3 (4) A is CH3-CH- and M is Zn. (5) The antibacterial agent according to claim 4, wherein the fungi to be controlled are Durum-negative bacteria.
JP19907181A 1981-12-09 1981-12-09 Unsaturated fatty acid or its salt and fungicide containing the same Granted JPS5899432A (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
JP19907181A JPS5899432A (en) 1981-12-09 1981-12-09 Unsaturated fatty acid or its salt and fungicide containing the same

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
JP19907181A JPS5899432A (en) 1981-12-09 1981-12-09 Unsaturated fatty acid or its salt and fungicide containing the same

Publications (2)

Publication Number Publication Date
JPS5899432A true JPS5899432A (en) 1983-06-13
JPS6312457B2 JPS6312457B2 (en) 1988-03-18

Family

ID=16401618

Family Applications (1)

Application Number Title Priority Date Filing Date
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Country Status (1)

Country Link
JP (1) JPS5899432A (en)

Cited By (5)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
EP0399644A2 (en) * 1989-04-10 1990-11-28 Kyowa Hakko Kogyo Co., Ltd. Preservative for plants
US5171351A (en) * 1989-04-10 1992-12-15 Kyowa Hakko Kogyo Co. Preservative for plants comprising epoxy compounds
WO1997034489A1 (en) * 1996-03-20 1997-09-25 Aquaculture Technology, Inc. Antibacterially active marine algae extracts from the class diatomatae and methods of use
JP2013194010A (en) * 2012-03-21 2013-09-30 Kitakyushu Foundation For The Advancement Of Industry Science & Technology Antifungal agent and antifungal method for rush using the same, and rush product subjected to antifungal treatment
JP2015061856A (en) * 2008-12-09 2015-04-02 ユニバーシタト デ レス イイェスバレアス Alpha derivatives of cis-monounsaturated fatty acids for use as drugs

Citations (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
JPS56108721A (en) * 1980-01-30 1981-08-28 Maruzen Sekiyu Kagaku Kk Liquid branched-chain higher aliphatic 1-ol and its preparation

Patent Citations (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
JPS56108721A (en) * 1980-01-30 1981-08-28 Maruzen Sekiyu Kagaku Kk Liquid branched-chain higher aliphatic 1-ol and its preparation

Cited By (8)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
EP0399644A2 (en) * 1989-04-10 1990-11-28 Kyowa Hakko Kogyo Co., Ltd. Preservative for plants
US5112380A (en) * 1989-04-10 1992-05-12 Kyowa Hakko Kogyo Co., Ltd. Preservative for plants comprising alkenylphosphonic acids and, optionally, dipicolinic acid
US5171351A (en) * 1989-04-10 1992-12-15 Kyowa Hakko Kogyo Co. Preservative for plants comprising epoxy compounds
US5298478A (en) * 1989-04-10 1994-03-29 Kyowa Hakko Kagyo Co. Preservative for plants comprising dipicolinic acid
WO1997034489A1 (en) * 1996-03-20 1997-09-25 Aquaculture Technology, Inc. Antibacterially active marine algae extracts from the class diatomatae and methods of use
US5866150A (en) * 1996-03-20 1999-02-02 Aquaculture Technology Incorporated Antibacterially active extracts from the marine algae chaetoceros and methods of use
JP2015061856A (en) * 2008-12-09 2015-04-02 ユニバーシタト デ レス イイェスバレアス Alpha derivatives of cis-monounsaturated fatty acids for use as drugs
JP2013194010A (en) * 2012-03-21 2013-09-30 Kitakyushu Foundation For The Advancement Of Industry Science & Technology Antifungal agent and antifungal method for rush using the same, and rush product subjected to antifungal treatment

Also Published As

Publication number Publication date
JPS6312457B2 (en) 1988-03-18

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