JPH0724680B2 - Antibacterial processing method - Google Patents
Antibacterial processing methodInfo
- Publication number
- JPH0724680B2 JPH0724680B2 JP2267296A JP26729690A JPH0724680B2 JP H0724680 B2 JPH0724680 B2 JP H0724680B2 JP 2267296 A JP2267296 A JP 2267296A JP 26729690 A JP26729690 A JP 26729690A JP H0724680 B2 JPH0724680 B2 JP H0724680B2
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- Prior art keywords
- antibacterial
- test
- processing method
- agent
- processing
- 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.)
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- Apparatus For Disinfection Or Sterilisation (AREA)
- Chemical Or Physical Treatment Of Fibers (AREA)
- Treatments For Attaching Organic Compounds To Fibrous Goods (AREA)
- Paper (AREA)
Description
【発明の詳細な説明】 [産業上の利用区分] 本発明は糸、生地、紙、不織布、フィルム等各種の素材
に対し均一に、しかも後加工によって恒久的な抗菌性を
付与することのできるセラミック抗菌剤を用いた加工法
の提供に関する。DETAILED DESCRIPTION OF THE INVENTION [Industrial application category] The present invention can impart a permanent antibacterial property to various materials such as yarn, cloth, paper, nonwoven cloth, and film uniformly and by post-processing. The present invention relates to the provision of a processing method using a ceramic antibacterial agent.
[従来の技術] 我々人間の日常生活においては衣類、履物類等、特に人
体の肌に直接接触する製品は皮膚面から分泌される汗、
皮脂、表面細胞の角質化に伴って生ずる皮膚垢や、空気
中の埃によって生ずる汚れに起因する不快臭を発し、汚
れた部分には細菌・カビ等の微生物が繁殖する。[Prior Art] In our daily lives, clothes, footwear, etc., especially products that come into direct contact with the skin of the human body, produce sweat that is secreted from the skin surface.
Sebum, dirt on skin caused by keratinization of surface cells, and unpleasant odor caused by dirt caused by dust in the air, and microorganisms such as bacteria and mold propagate on the dirty part.
このため腐敗、発酵現象が起こり、アンモニアなどを生
成し、悪臭を発したり、皮膚を刺激して炎症を誘発する
こともある。また、微生物の作用により、繊維材料が被
害を受け、変色・着色、脆化などを起こすこともある。As a result, decay and fermentation phenomena occur, which may produce ammonia and the like, which may give off a bad odor or may irritate the skin and induce inflammation. In addition, the action of microorganisms may damage the fiber material, causing discoloration / coloring, embrittlement, and the like.
かかる点に鑑み、従来より各種薬剤による防菌・防カビ
加工が行なわれ、その代表的なものとして有機ハロゲン
化合物や有機金属化合物が用いられた。In view of this point, antibacterial and antifungal treatments have been conventionally performed with various chemicals, and typical examples thereof include organic halogen compounds and organic metal compounds.
[発明が解決しようとする問題点] かかる抗菌加工は、当初、菌に対する効果が優先され、
次いで人体に対する安全性が問題になるという歴史を辿
り、その中においてこれに適合しないスズや水銀の有機
化合物は姿を消し、また、最近では直接人体に接して害
を生じないまでも焼却によってオキシダントを発生させ
たり、塩素を発生させたりする、即ち、環境汚染の問題
を生じるものも淘汰されてきている。[Problems to be Solved by the Invention] In such an antibacterial treatment, the effect on fungi is given priority at first.
Next, we trace the history that safety to the human body becomes a problem, in which organic compounds such as tin and mercury that are not compatible with it disappear, and recently, even if it does not directly contact the human body and causes no harm, it is incinerated by oxidant. Those that generate chlorine or chlorine, that is, those that cause the problem of environmental pollution have been eliminated.
かかる状況の中において、近年無害の新しい抗菌剤とし
て無機系の金属化合物、即ち、例えば、 ゼオライトの結晶構造内のナトリウムイオンを銀イオ
ン、或いは他の抗菌性金属イオンと置換したもの 特殊ガラス(水溶性ガラス)の中に銀イオン、或いは
他の抗菌性金属イオンを含有させたもの ハイドロキシパタイトのカルシウムイオンを銀イオ
ン、或いは他の抗菌性金属イオンと置換したもの 等のセラミックタイプの抗菌剤が用いられるようになっ
てきている。Under such circumstances, as a new harmless new antibacterial agent, an inorganic metal compound, that is, for example, sodium ion in the crystal structure of zeolite is replaced with silver ion or other antibacterial metal ion Special glass (water soluble Glass) containing silver ions or other antibacterial metal ions. Ceramic type antibacterial agents such as those in which calcium ions of hydroxypatite are replaced with silver ions or other antibacterial metal ions. It is being used.
しかしながら、かかる抗菌剤は後加工において均一な処
理、更には、耐久的な処理が難しいことから、現状にお
いては合成繊維、再生繊維等、紡糸時にこれを練り込ん
だり、プラスチックスの成型時に混入させたりという方
法が用いられているに過ぎない。However, since such an antibacterial agent is difficult to be uniformly processed in post-processing and further difficult to be durable, at present, synthetic fibers, recycled fibers, etc. are kneaded during spinning or mixed during molding of plastics. Only the method called "Tori" is used.
本発明は、かかる点、いかなる素材に対しても均一に、
しかも、恒久的な処理が可能な加工法を提供したもので
ある。The present invention, in this respect, uniform for any material,
Moreover, it provides a processing method capable of permanent treatment.
[問題点を解決するための手段] しかるに、本発明は、その加工法において、無機系の金
属化合物より成るセラミック系抗菌剤とカルボン酸型高
分子界面活性剤及び、脂肪族ウレタンポリマーを重量比
において概ね1:1:0.5の割合で混合して成る処理剤にて
処理することに特徴を有する抗菌加工法に関する。[Means for Solving the Problems] However, in the processing method of the present invention, a ceramic antibacterial agent comprising an inorganic metal compound, a carboxylic acid type polymer surfactant and an aliphatic urethane polymer are used in a weight ratio. The present invention relates to an antibacterial processing method characterized by treating with a treating agent which is mixed at a ratio of approximately 1: 1: 0.5.
[作用] 一般に微粉化されたセラミックは沈殿しやすく、常に均
一な分散状態を維持することは難しい。従って、このよ
うな状態によって処理しても均一な処理は望めない。[Operation] Generally, finely divided ceramics easily precipitate, and it is difficult to always maintain a uniform dispersion state. Therefore, even if the processing is performed in such a state, uniform processing cannot be expected.
一方、一旦付着させたセラミックを抗菌性を阻害するこ
となく長期にわたってその効果を発現させることも極め
て重要なことである。On the other hand, it is also extremely important to develop the effect of the once-adhered ceramic for a long period of time without inhibiting the antibacterial property.
本発明はかかる点、特に、カルボン酸型高分子界面活性
剤及び、脂肪族ウレタンポリマーとの混合処理液を構成
することによって、セラミックの均一分散と、付着した
抗菌性セラミックの耐久性を付与したもので、特に、カ
ルボン酸型高分子界面活性剤による分散効果と、脂肪族
ウレタンポリマーによるバインダー効果によって両機能
を加えたものである。The present invention imparts the uniform dispersion of the ceramic and the durability of the attached antibacterial ceramic by forming a mixed treatment liquid with the carboxylic acid type polymer surfactant and the aliphatic urethane polymer, in particular. In particular, both functions are added by the dispersing effect of the carboxylic acid type polymer surfactant and the binder effect of the aliphatic urethane polymer.
特に、かかる処理剤の構成は、水分の作用によって徐々
に溶解し、混入された抗菌性イオンが長期にわたって溶
出するような水溶性ガラスより成る抗菌剤との組み合わ
せにおいて好適である。In particular, the composition of such a treating agent is suitable in combination with an antibacterial agent composed of water-soluble glass that is gradually dissolved by the action of water and the mixed antibacterial ions are eluted over a long period of time.
以下、銀イオンを抗菌剤として含む水溶性ガラスを例に
挙げて説明する。Hereinafter, a water-soluble glass containing silver ions as an antibacterial agent will be described as an example.
しかるに、先ず、本発明における水溶性ガラスとは、制
御された溶解速度を持つようにガラスの物理的、化学的
特性を考慮して組成を調整したガラスをさし、例えば、
その組成が、B2O3 50モル%,SiO2 40モル%,NaO 10モル
%より成るもの、或は、P2O5 65モル%,CaO 15モル%,N
a2O 14モル%,Al2O3 6モル%より成るもの等が例示でき
る。However, first, the water-soluble glass in the present invention refers to a glass having a composition adjusted in consideration of the physical and chemical characteristics of the glass so as to have a controlled dissolution rate, for example,
The composition is composed of B 2 O 3 50 mol%, SiO 2 40 mol%, NaO 10 mol%, or P 2 O 5 65 mol%, CaO 15 mol%, N
An example is a mixture of a 2 O 14 mol% and Al 2 O 3 6 mol%.
また、粒径は当該用途においては10〜30ミクロンのもの
が用いられ、これにAg2Oが数重量%のオーダーで添加さ
れる。In addition, the particle size used is 10 to 30 μm in this application, and Ag 2 O is added thereto in the order of several wt%.
かかるイオンを放出する金属としては銀のほか銅、或は
その他の抗菌能を有する金属化合物を用いてもよいが、
安全性、その抗菌性から銀イオンを放出するものが最適
である。As the metal that releases such ions, copper, as well as other metal compounds having antibacterial activity, may be used in addition to silver.
The one that releases silver ions is most suitable because of its safety and antibacterial properties.
また、分散剤としては構造的にカルボン酸を有するもの
で、具体的にはアクリル酸系をモノマーとする重合体で
分子量が1000以上のカルボン酸型高分子界面活性剤を例
示することができる。Further, as the dispersant, a dispersant structurally having a carboxylic acid, and specifically, a carboxylic acid type polymer surfactant having a molecular weight of 1000 or more, which is a polymer having acrylic acid as a monomer, can be exemplified.
また、バインダーとしては構造的に脂肪族を有するもの
が例示でき、具体的にはポリオールとジ・イソシアネー
トを反応させ、中和後粒径0.1ミクロンのコロイド状に
分散させたものが例示できる。Examples of the binder include structurally aliphatic ones, and specifically, a binder obtained by reacting a polyol with diisocyanate, neutralized and dispersed in a colloidal form having a particle size of 0.1 micron can be exemplified.
かかる処理剤の配合比率としては、概ね重量比におい
て、 抗菌剤(銀イオン放出水溶性ガラス) 1 分散剤(カルボン酸型高分子界面活性剤) 1 バインダー(脂肪酸ウレタンポリマー) 0.5 の割合で用いるのが良く、その配合比において分散剤が
抗菌剤に対し多すぎると、銀イオンとのコンプレックス
により沈殿が生じ、また、少なすぎると分散状態が不均
一となって斑付きの原因となるため好ましくない。Regarding the compounding ratio of such a treating agent, the antibacterial agent (silver ion-releasing water-soluble glass) 1 dispersant (carboxylic acid type polymer surfactant) 1 binder (fatty acid urethane polymer) 0.5 is generally used in a weight ratio. If the amount of the dispersant is too much with respect to the antibacterial agent in the blending ratio, precipitation occurs due to the complex with silver ions, and if it is too small, the dispersed state becomes non-uniform and unevenness is caused, which is not preferable. .
また、バインダーもその量が多すぎると抗菌剤の溶解を
妨げ、銀イオンの放出を妨げるため好ましくない。ま
た、逆に、少なすぎると付着した抗菌剤の剥離が起り、
耐久性上問題を生ずる。Also, if the amount of the binder is too large, the dissolution of the antibacterial agent is hindered and the release of silver ions is hindered, which is not preferable. On the contrary, if it is too small, peeling of the attached antibacterial agent occurs,
This causes a problem in durability.
尚、具体的には、以下の処理が例示できる。In addition, specifically, the following processes can be illustrated.
a)浸漬法(バッド・キュア法) 水溶性抗菌ガラス 1〜10% Sol 分散剤 1〜10% 〃 バインダー 0.5〜5% 〃 b)コーティング法 水溶性抗菌ガラス 20〜30重量% 分散剤 8〜24% 〃 バインダー 10〜15% 〃 但し、粘度を7000〜12000cpsとする。a) Immersion method (bad cure method) Water-soluble antibacterial glass 1-10% Sol dispersant 1-10% 〃 Binder 0.5-5% 〃 b) Coating method Water-soluble antibacterial glass 20-30% by weight Dispersant 8-24 % 〃 Binder 10 to 15% 〃 However, the viscosity should be 7000 to 12000 cps.
以下、実施例を挙げて説明する。Examples will be described below.
[実施例] 被加工素材としてナイロン不織布を使用し、以下の条件
による加工を行った。[Example] A nylon non-woven fabric was used as a material to be processed, and processing was performed under the following conditions.
(処理浴組成) 水溶性ガラス(セラミックス) 5g/l 消臭剤(セラミックス) 5 〃 分散剤 10 〃 バインダー 5 〃 (加工法) パッド、ドライ(120℃×3分)による処理を行った。(Treatment bath composition) Water-soluble glass (ceramics) 5 g / l Deodorant (ceramics) 5 〃 Dispersant 10 〃 Binder 5 〃 (Processing method) A pad and dry (120 ° C x 3 minutes) treatment were performed.
[実施例2] 被加工素材としてウレタン系吸湿性樹脂を使用し、以下
の条件による加工を行った。[Example 2] A urethane-based hygroscopic resin was used as a material to be processed, and processing was performed under the following conditions.
(処理浴組成) 水溶性ガラス(セラミックス) 10g/l 消臭剤(セラミックス) 10 〃 分散剤 20 〃 バインダー 10 〃 (加工法) パッド、ドライ(40℃×3分,乾燥室に放置)による処
理。(Treatment bath composition) Water-soluble glass (ceramics) 10 g / l Deodorant (ceramics) 10 〃 Dispersant 20 〃 Binder 10 〃 (Processing method) Pad, dry (40 ℃ x 3 minutes, leave in drying room) Treatment .
[実施例3] ソックスとして編成された半製品の足底部の裏側のみ下
記の加工剤をプリントした。[Example 3] The following processing agent was printed only on the back side of the sole of a semi-finished product knitted as socks.
(処理浴組成) 水溶性ガラス(セラミックス) 14パーツ 消臭剤(セラミックス) 14 〃 バインダー 22 〃 増粘剤 14 〃 水 36 〃 (加工法) プリント後自然乾燥し、110℃×3分のセットを行っ
た。(Treatment bath composition) Water-soluble glass (ceramics) 14 parts Deodorant (ceramics) 14 〃 Binder 22 〃 Thickener 14 〃 Water 36 〃 (Processing method) After printing, air-dry and set at 110 ℃ x 3 minutes went.
[実施例4] 綿100%のメリヤス生地を使用し、下記の加工液による
処理を行った。[Example 4] A 100% cotton knit fabric was used and treated with the following processing liquid.
(処理浴組成) 水溶性ガラス(セラミックス) 50g/l 消臭剤(セラミックス) 50g/l 分散剤 100 〃 バインダー 50 〃 (加工法) パッド、、ドライ(120℃×3分)、キュア(150℃×3
分)による処理。(Treatment bath composition) Water-soluble glass (ceramics) 50g / l Deodorant (ceramics) 50g / l Dispersant 100〃 Binder 50〃 (Processing method) Pad, Dry (120 ℃ × 3min), Cure (150 ℃) × 3
Min) processing.
[実施例5] 壁紙用ナイロン不織布に以下の加工を行った。[Example 5] The following processing was performed on the nylon nonwoven fabric for wallpaper.
(処理浴組成) 水溶性ガラス(セラミックス) 50g/l 消臭剤(セラミックス) 50 〃 分散剤 100 〃 バインダー 50 〃 (加工法) パッド、ドライ(120℃×3分)処理。(Treatment bath composition) Water-soluble glass (ceramics) 50g / l Deodorant (ceramics) 50〃 Dispersant 100〃 Binder 50〃 (Processing method) Pad, dry (120 ℃ x 3 minutes) treatment.
尚、各実施例とも処理剤は以下のものを使用した。The following treatment agents were used in each example.
水溶性ガラス−−イオンピュア WPA-13(石塚硝子
(株)製、商品名) 分散剤−−ポイズ(花王(株)製、商品名) バインダー−−−2104(サンキュア(株)製、商品名) 消臭剤(セラミッスク)−−アサヒクリーン(旭硝子
(株)製商品名) また、パディングにおける絞り率は全て100%とした。Water-soluble glass-Ionpure WPA-13 (manufactured by Ishizuka Glass Co., Ltd., trade name) Dispersant-Poise (manufactured by Kao Corporation, trade name) Binder--2104 (manufactured by Suncure Co., Ltd., trade name) ) Deodorant (ceramics)-Asahi Clean (trade name, manufactured by Asahi Glass Co., Ltd.) Further, the squeezing ratio in the padding was 100%.
[発明の効果] 実施例1により得たナイロン不織布の評価結果を以下に
示す。[Effects of the Invention] The evaluation results of the nylon nonwoven fabric obtained in Example 1 are shown below.
<抗菌性の評価> 1)尿素分解菌に対する抗菌性 ・試験菌株 Protus vnlgaris IFO 3045 ・試験方法 試験菌の混合平板培地上に直径20mmの試料を密着貼付
し、37℃,24時間培養後、生じた試料周辺の透明な生育
阻止帯(ハロー)の幅を測定した。<Evaluation of antibacterial properties> 1) Antibacterial properties against urea-decomposing bacteria • Test strain Protus vnlgaris IFO 3045 • Test method A sample with a diameter of 20 mm was adhered to a mixed plate medium of test bacteria and incubated at 37 ° C for 24 hours. The width of the transparent growth inhibition zone (halo) around the sample was measured.
・試験結果 ハローの幅(mm) 7.0mm 2)黄色葡萄状球菌に対する抗菌性 ・試験菌株 Staphylococcus aureus IFO 12732 ・試験方法 試験菌の混合平板培地上に直径20mmの試料を密着貼付
し、37℃,24時間培養後、生じた試料周辺の透明な生育
阻止帯(ハロー)の幅を測定した。・ Test result Halo width (mm) 7.0mm 2) Antibacterial activity against Staphylococcus aureus ・ Test strain Staphylococcus aureus IFO 12732 ・ Test method A sample with a diameter of 20mm was adhered on a mixed plate medium of the test strains at 37 ℃, After culturing for 24 hours, the width of the transparent growth inhibition zone (halo) around the resulting sample was measured.
・試験結果 ハローの幅(mm) 7.2mm 3)白癬菌に対する抗菌性 ・試験菌株 trichophyton mentagrophytes IFO 5466 ・試験方法 試験菌の胞子を塗抹した混合平板培地上に直径20mmの
試料を密着貼付し、27℃,7日間培養後、生じた試料周辺
の透明な生育阻止帯(ハロー)の幅を測定した。・ Test result Halo width (mm) 7.2mm 3) Antibacterial activity against Trichophyton ・ Test strain trichophyton mentagrophytes IFO 5466 ・ Test method A sample with a diameter of 20mm was adhered on a mixed plate medium smeared with spores of the test strain, and 27 After culturing at ℃ for 7 days, the width of the transparent growth inhibition zone (halo) around the resulting sample was measured.
・試験結果 ハローの幅(mm) 4.3mm <安全性に対する評価> 1)急性毒性試験 試験機関・・・日本食品分析センター 試験結果・・・LD50:5g/kg以上 技術的投与可能最大値の5g/kgで雌雄マウスともに観察
期間中(14日間)に死亡例、その他の異常は観察されな
かった。また、観察期間終了後の剖検では、主要臓器に
異常は認められなかった。・ Test result Harrow width (mm) 4.3mm <Evaluation for safety> 1) Acute toxicity test Testing institute ・ ・ ・ Japan Food Analysis Center Test result ・ ・ ・ LD50: 5g / kg or more Technically administrable maximum value 5g Both male and female mice died during the observation period (14 days), and no other abnormalities were observed. No abnormalities were found in the major organs at autopsy after the observation period.
2)皮膚一次刺激性試験 試験機関・・・日本食品分析センター 試験結果・・・皮膚一次刺激性はない 日本ウサギ3匹とも各観察時点(1,24,48,72時間)にお
いて、皮膚刺激反応は観察されなかった。2) Primary skin irritation test Laboratory: Japan Food Analysis Center Test result: No primary skin irritation Skin irritation reaction at all observation points (1, 24, 48, 72 hours) for all 3 Japanese rabbits Was not observed.
3)変異原性試験 試験機関・・・日本食品分析センター 試験結果・・・いずれの場合も復帰変異コロニー数の
増加は認められなく、突然変異起性は陰性であった。3) Mutagenicity test Laboratory: Japan Food Research Center Test result: No increase in the number of revertant colonies was observed in any case, and mutagenicity was negative.
4)皮膚障害(バッチ)試験 試験機関・・・日本産業皮膚衛生協会 試験結果・・・準陰性 加工した試料を皮膚にバッチした結果、特に異常は認め
られなかった。4) Skin disorder (batch) test Testing institute ... Japan Industrial Skin Hygiene Association test result ... Quasi-negative As a result of batching processed samples on the skin, no particular abnormality was observed.
<菌減少率についての評価> 試験方法・・・シェーク法 試験菌株・・・Klebsiella pneumoniae ATTC 4532肺
炎捍菌 試験方法・・・滅菌試料布に試験菌の懸濁緩衝液を注
加し、密閉容器中で150回/分、1時間振とう後の生産
菌を計測し、注加懸濁液の菌数に対する減少率を求め
た。<Evaluation of bacterial reduction rate> Test method: Shaking method Test strain: Klebsiella pneumoniae ATTC 4532 Streptococcus pneumoniae test method: Suspension buffer solution of test bacteria was added to a sterilized sample cloth, and sealed container The number of bacteria produced after shaking at 150 times / min for 1 hour was measured, and the reduction rate with respect to the number of bacteria in the added suspension was determined.
試験結果 当初菌数−−−−−−−−−20000 未加工布振とう後の菌数−−20400 加工布振とう後の菌数−−−0 (減少率99.9%以上) <耐久性についての評価> 試験項目・・菌数測定法 試験菌株 Staphlococcus aureus IFO 13277 試験方法・・通常の家庭洗濯を30回繰返したた後、加
工布に試験菌のブイヨン懸濁を注加し、密閉容器中で37
℃、18時間培養後の生菌数を計測し、無加工布に対する
増減値差を求めた。Test results Initial number of bacteria -------------- 20000 Number of bacteria after unprocessed cloth shaking --- 20400 Number of bacteria after unprocessed cloth shaking --- 0 (reduction rate 99.9% or more) <Durability Evaluation of test items ・ ・ Measurement method for bacterial count Test strain Staphlococcus aureus IFO 13277 Test method ・ ・ After repeating normal home washing 30 times, add broth suspension of test bacteria to the work cloth and put in a closed container. At 37
The number of viable bacteria after culturing at 18 ° C. for 18 hours was counted, and the difference in increase / decrease value with respect to the untreated cloth was obtained.
試験結果 加工布培養後回収菌数 2000以下 (増減値差 5.08以上) 対照区培養後回収菌数 270万 (増減値差 1.95) 尚、対照区はバインダーとして非ホルムアルデヒド架橋
剤を50g/l(NF500−K(住友化学(株)製、商品名),
触媒として同社の同X−60を用いた他は、実施例と同様
の処理剤を用い、同様の処理を行って得たものである。Test results Collected bacteria after processed cloth culture 2000 or less (increase / decrease difference 5.08 or more) Collected bacteria after control culture 2.7 million (increase / decrease difference 1.95) In the control plot, 50 g / l of non-formaldehyde crosslinking agent (NF500 -K (Sumitomo Chemical Co., Ltd., trade name),
It was obtained by using the same treating agent as in the example except that the same X-60 manufactured by the same company was used as the catalyst and performing the same treatment.
以上の結果より明らかなように一般に存在している細菌
に対して充分な効果が確認され、また、人体に対する高
い安全性も確認された。As is clear from the above results, a sufficient effect was confirmed against commonly existing bacteria, and high safety against humans was also confirmed.
更に、洗濯等に対する効果の持続性についても殆どその
効果が失われることがなかっった。Furthermore, the effect of washing was hardly lost.
以上のように本発明は抗菌加工として、その効果、持続
性、安全性、耐久性とも極めて優れたもの、各種の素材
加工に適用して格別の効果を発現するものである。As described above, the present invention, as an antibacterial treatment, has extremely excellent effects, sustainability, safety and durability, and is applied to various kinds of material processing to exert a remarkable effect.
尚、本発明においては、加工剤付与のための方法とし
て、処理剤への浸漬,パッドドライ、処理剤によるスプ
レー等任意の方法をとることができ、また、その処理浴
には実施例のように他の抗菌剤、消臭剤を添加すること
も任意である。In the present invention, as the method for applying the processing agent, any method such as dipping in the processing agent, pad dry, spraying with the processing agent can be used, and the processing bath is the same as in the example. It is also optional to add other antibacterial agents and deodorants.
───────────────────────────────────────────────────── フロントページの続き (56)参考文献 特開 昭55−165927(JP,A) 特開 昭62−142559(JP,A) 特開 昭64−52705(JP,A) 特開 平2−213350(JP,A) ─────────────────────────────────────────────────── ─── Continuation of the front page (56) Reference JP-A-55-165927 (JP, A) JP-A-62-142559 (JP, A) JP-A 64-52705 (JP, A) JP-A-2- 213350 (JP, A)
Claims (2)
抗菌剤とカルボン酸型高分子界面活性剤及び、脂肪族ウ
レタンポリマーを重量比において概ね1:1:0.5の割合で
混合して成る処理剤にて処理することを特徴とする抗菌
加工法。1. A treatment agent comprising a ceramic antibacterial agent comprising an inorganic metal compound, a carboxylic acid type polymer surfactant and an aliphatic urethane polymer in a weight ratio of about 1: 1: 0.5. An antibacterial processing method characterized by treating with.
抗菌剤が銀イオンを放出する水溶性ガラスであることを
特徴とする請求項1記載の抗菌加工法。2. The antibacterial processing method according to claim 1, wherein the ceramic antibacterial agent comprising an inorganic metal compound is water-soluble glass that releases silver ions.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP2267296A JPH0724680B2 (en) | 1990-10-03 | 1990-10-03 | Antibacterial processing method |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP2267296A JPH0724680B2 (en) | 1990-10-03 | 1990-10-03 | Antibacterial processing method |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| JPH04144564A JPH04144564A (en) | 1992-05-19 |
| JPH0724680B2 true JPH0724680B2 (en) | 1995-03-22 |
Family
ID=17442862
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP2267296A Expired - Fee Related JPH0724680B2 (en) | 1990-10-03 | 1990-10-03 | Antibacterial processing method |
Country Status (1)
| Country | Link |
|---|---|
| JP (1) | JPH0724680B2 (en) |
Families Citing this family (5)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| JP2722300B2 (en) * | 1991-10-28 | 1998-03-04 | 旭光学工業株式会社 | Method for producing functional nonwoven fabric |
| JPH08113898A (en) * | 1994-10-11 | 1996-05-07 | Dainippon Printing Co Ltd | Antimicrobial wall-decorating material |
| US20040106340A1 (en) * | 2002-11-29 | 2004-06-03 | Kreider Jason L. | Fabrics having a topically applied silver-based finish exhibiting improved wash durability |
| US20040106341A1 (en) * | 2002-11-29 | 2004-06-03 | Vogt Kirkland W. | Fabrics having a topically applied silver-based finish exhibiting a reduced propensity for discoloration |
| JP2008038100A (en) * | 2006-08-09 | 2008-02-21 | Vido:Kk | Detergent composition having antimicrobial property |
Family Cites Families (5)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| JPS55165927A (en) * | 1979-06-11 | 1980-12-24 | Teijin Ltd | Production of sheet material having antibacterial property |
| JPH0622540B2 (en) * | 1985-12-18 | 1994-03-30 | 株式会社祥光化学研究所 | Structure with deodorant and antibacterial activity |
| JP2719613B2 (en) * | 1987-05-26 | 1998-02-25 | ダウコーニングアジア株式会社 | Antibacterial agent |
| JP2649388B2 (en) * | 1988-09-16 | 1997-09-03 | テイカ株式会社 | Antimicrobial composition |
| JPH02152913A (en) * | 1988-12-02 | 1990-06-12 | Dow Corning Kk | Antibacterial treatment composition |
-
1990
- 1990-10-03 JP JP2267296A patent/JPH0724680B2/en not_active Expired - Fee Related
Also Published As
| Publication number | Publication date |
|---|---|
| JPH04144564A (en) | 1992-05-19 |
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