JPWO2016178385A1 - Antiviral agent, antiviral agent composition and antiviral material - Google Patents

Abstract

（式（１）中、Ｒ¹、Ｒ²及びＲ³は、炭素数１〜１８の直鎖状又は分岐状のアルキル基である。Ｒ¹〜Ｒ³は、同一の基でも、それぞれが異なる基であってもよい。Ｒ⁴は、炭素数１〜１８の直鎖状又は分岐状のアルキル基、又は一般式（２）で表されるアルコキシシリル基である。Ｘ^-はアニオン基である。）
一般式（２）：
−（ＣＨ₂）_n−Ｓｉ−（ＯＲ⁵）₃ （２）
（式（２）中、ｎは１〜８の整数である。Ｒ⁵は、炭素数１〜５の直鎖状又は分岐状のアルキル基である。）To provide an antiviral agent having higher antiviral activity than a conventional ammonium salt.
An antiviral agent comprising at least one selected from a phosphonium salt represented by the general formula (1) and a hydrolysis-condensation product thereof.
General formula (1):
[Chemical 1]

(In the formula (1), R ¹ , R ² and R ³ are linear or branched alkyl groups having 1 to 18 carbon atoms. R ^{1 to} R ³ may be the same group but different from each other. R ⁴ is a linear or branched alkyl group having 1 to 18 carbon atoms or an alkoxysilyl group represented by the general formula (2), and X ⁻ is an anionic group. .)
General formula (2):
_{- (CH 2) n -Si- (} OR 5) 3 (2)
(In formula (2), n is an integer of 1 to 8. R ⁵ is a linear or branched alkyl group having 1 to 5 carbon atoms.)

Description

  The present invention relates to an antiviral agent, an antiviral agent composition and an antiviral material having high antiviral activity against viruses, particularly influenza viruses and noroviruses.

  Viruses are 1/10 to 1/200 times the size of bacteria, have no cell wall unlike bacteria, and cannot grow unless other organisms are used as hosts.

  Currently, problems related to viral diseases caused by influenza viruses, noroviruses, and the like are a major problem worldwide.

  In general, the infection route of influenza is known as droplet infection, air infection, contact infection, and the like. Of these, contact infection is a secondary infection caused by the contact of humans with the droplets produced by influenza-infected persons adhering to various objects.

  In addition, the infection route of norovirus is well known as oral infection by eating shellfish such as raw oysters, but it is also known that secondary infection is caused by human touching objects contaminated with norovirus. It has been.

  Such secondary infection leads to mass infection and spread, and is a major cause of the increase in the number of patients.

  It has been proposed to use ammonium salts as antiviral agents against influenza viruses and noroviruses (see, for example, Patent Documents 1 and 2).

  Phosphonium salts are known as compounds having antibacterial activity against bacteria such as Gram-positive bacteria and Gram-negative bacteria (for example, see Patent Documents 3 to 4). Non-Patent Documents 1 and 2 below introduce that alkyl (aryl) phosphonium salts and the like have high antiviral activity against influenza virus.

JP 2011-98976 A JP 2013-40167 A JP-A-6-92911 JP-A-4-266912

Khimiko-Farmatsveticheskij Zhurnal, Vol.24, No.6, p28-30 (1990) Mikrobiologicheskii Zhurnal, Vol.48, No.3, p80-82 (1986)

  However, since norovirus is infected even in the presence of a small amount, the antiviral properties are insufficient with ammonium salts. Therefore, what has higher antiviral activity than ammonium salts is required.

  As for phosphonium salts, as described above, it has been introduced that alkyl (aryl) phosphonium salts and the like have high antiviral activity against influenza virus, but as far as the present applicants know, otherwise. There are no reports of antiviral agents actually using phosphonium salts.

  Accordingly, an object of the present invention is to provide an antiviral agent having a higher antiviral activity than conventional ammonium salts.

  In the search for compounds having antiviral activity against influenza viruses and noroviruses, the present inventors have found that specific phosphonium salts and hydrolysis condensates thereof have high antiviral activity against viruses such as influenza viruses and noroviruses. In particular, the present inventors have found that it has a higher antiviral activity against norovirus than conventional ammonium salts, and have completed the present invention.

That is, this invention (1) provides the antiviral agent characterized by including 1 or more types chosen from the phosphonium salt represented by following General formula (1), and its hydrolysis-condensation product. .
General formula (1):

(In the formula (1), R ¹ , R ² and R ³ are linear or branched alkyl groups having 1 to 18 carbon atoms. R ^{1 to} R ³ may be the same group but different from each other. R ⁴ is a linear or branched alkyl group having 1 to 18 carbon atoms or an alkoxysilyl group represented by the following general formula (2), wherein X ⁻ is an anionic group. is there.)
General formula (2):
_{- (CH 2) n -Si- (} OR 5) 3 (2)
(In formula (2), n is an integer of 1 to 8. R ⁵ is a linear or branched alkyl group having 1 to 5 carbon atoms.)

Moreover, this invention (2) provides the antiviral agent composition characterized by including 1 or more types chosen from the phosphonium salt represented by following General formula (1), and its hydrolysis-condensation product. It is.
General formula (1):

(In the formula (1), R ¹ , R ² and R ³ are linear or branched alkyl groups having 1 to 18 carbon atoms. R ^{1 to} R ³ may be the same group but different from each other. R ⁴ is a linear or branched alkyl group having 1 to 18 carbon atoms or an alkoxysilyl group represented by the following general formula (2), wherein X ⁻ is an anionic group. is there.)
General formula (2):
_{- (CH 2) n -Si- (} OR 5) 3 (2)
(In formula (2), n is an integer of 1 to 8. R ⁵ is a linear or branched alkyl group having 1 to 5 carbon atoms.)

  Moreover, this invention (3) provides the antiviral material obtained by surface-treating the surface of a base material with the antiviral agent composition of (2).

  In addition, the present invention (4) provides an antiviral material obtained by impregnating a base material with the antiviral agent composition of (2).

In addition, the present invention (5) is a raw material for a base material comprising at least one selected from the antiviral composition of (2) or a phosphonium salt represented by the following general formula (1) and a hydrolysis condensate thereof. The antiviral material obtained by mixing in and then molding the resulting antiviral agent-containing base material is provided.
General formula (1):

(In the formula (1), R ¹ , R ² and R ³ are linear or branched alkyl groups having 1 to 18 carbon atoms. R ^{1 to} R ³ may be the same group but different from each other. R ⁴ is a linear or branched alkyl group having 1 to 18 carbon atoms or an alkoxysilyl group represented by the following general formula (2), wherein X ⁻ is an anionic group. is there.)
General formula (2):
_{- (CH 2) n -Si- (} OR 5) 3 (2)
(In formula (2), n is an integer of 1 to 8. R ⁵ is a linear or branched alkyl group having 1 to 5 carbon atoms.)

  ADVANTAGE OF THE INVENTION According to this invention, the antiviral agent which has high antiviral activity with respect to viruses, especially influenza virus and Norovirus can be provided. Moreover, according to the present invention, various antiviral materials having high antiviral activity against viruses, particularly influenza viruses and noroviruses, can be provided.

  The antiviral agent of the present invention is an antiviral agent characterized by containing at least one selected from a phosphonium salt represented by the following general formula (1) and a hydrolysis condensate thereof.

  The phosphonium salt according to the present invention has the general formula (1):

It is a phosphonium salt represented by

In the general formula (1), R ¹ , R ² and R ³ are linear or branched alkyl groups having 1 to 18 carbon atoms, preferably 2 to 10 carbon atoms, and particularly preferably 2 to 6 carbon atoms. is there. Specific examples of R ¹ , R ² and R ³ include a methyl group, an ethyl group, a propyl group, a butyl group and a pentyl group, and a butyl group, particularly an n-butyl group is preferred. R ^{1 to} R ³ may be the same group or different groups.

R ⁴ is a linear or branched alkyl group having 1 to 18 carbon atoms, preferably 1 to 10 carbon atoms, particularly preferably 1 to 8 carbon atoms, or alkoxysilyl represented by the following general formula (2). It is a group.
General formula (2):
_{- (CH 2) n -Si- (} OR 5) 3 (2)

Specific examples of the alkyl group according to R ⁴ include a methyl group, an ethyl group, a propyl group, a butyl group, and a pentyl group.

In the general formula (2), n is an integer of 1 to 8, preferably an integer of 2 to 6, particularly preferably 3. R ⁵ is linear or branched alkyl having 1 to 5 carbon atoms, preferably 1 to 3 carbon atoms. R ⁵ is particularly preferably a methyl group.

In the general formula (1), X ⁻ represents an anionic group. X ⁻ includes benzotriazole ion, fluorine ion, chlorine ion, bromine ion, iodine ion, BF ₄ ⁻ , PF ₆ ⁻ , N (SO ₂ CF ₃ ) ₂ ⁻ , PO ₂ (OMe) ₃ ⁻ and PS ₂ ( Anionic groups such as OEt) ₂ ⁻ and (CO ₂ Me) ₂ PhSO ₃ ^— can be mentioned, and among these, chlorine ions are preferred.

Examples of the phosphonium salt represented by the general formula (1) include an alkoxysilyl group-containing phosphonium salt represented by the following general formula (1 ′).
General formula (1 ′):

In the general formula ^{(1 '), R 1,} R 2, R 3, R 5, n and X ^- is, R ¹ in the formula ^{(1), R 2, R 3, R} 5, n and X ^- and It is the same.

The alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′) is one in which R ¹ , R ² and R ^{3 in} the general formula (1 ′) are all butyl groups and n is 3. Is preferred.

  Since the alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′) has an alkoxysilyl group, it is chemically bonded to a material having an oxygen-containing functional group such as —OH group or —OH— group. Is possible. Therefore, by using the alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′), various parts such as wood, glass, ceramics, fibers, non-woven fabrics, metals, rubbers, etc. can be used for the portion of the phosphonium salt having antiviral activity. Can be applied to the material.

  The antiviral agent of the present invention includes an phosphonium salt represented by the general formula (1), an alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′) and a general formula (1) as an active ingredient exhibiting antiviral activity. 1 ') 1 or more types of compounds chosen from the hydrolysis-condensation product of the alkoxy silyl group containing phosphonium salt represented.

  The phosphonium salt represented by the general formula (1) and the alkoxysilyl group-containing phosphonium represented by the general formula (1 ′) are known compounds (for example, see JP-A-6-92811).

  The method for obtaining the hydrolysis condensate by hydrolyzing the alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′) is not particularly limited, but for example, water selected from water, alkali, or acid. The method of hydrolyzing with a decomposition agent is mentioned.

  In the antiviral agent of the present invention, a phosphonium salt represented by the general formula (1), an alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′), and an alkoxysilyl group represented by the general formula (1 ′) The content of the hydrolyzed condensate of the phosphonium salt (the total content in the case of two or more) is appropriately selected, but is preferably 0.01% by mass or more, particularly preferably 0.01 to 30% by mass. is there. In addition, when it contains the hydrolysis condensate of the alkoxysilyl group containing phosphonium salt represented by general formula (1 '), the content is the alkoxysilyl group represented by general formula (1') before hydrolysis. It is the content converted into the contained phosphonium salt.

  The antiviral agent of the present invention can contain, as a solvent, an alcohol such as methanol or ethanol, water, or a mixed solvent of these alcohol and water. Further, the antiviral agent of the present invention contains auxiliary agents such as surfactants, binders, colorants, dispersants, lubricants, other inorganic or organic diluents, carriers and the like as necessary.

  The method of using the antiviral agent of the present invention is a method of spraying or applying the antiviral agent of the present invention on the surface of an antiviral target article, or the surface of the antiviral target article of the present invention. Examples thereof include a method of wiping with a paper or cloth soaked with a virus agent, or a method of immersing an antiviral target article in the antiviral agent of the present invention. Further, the antiviral agent of the present invention may be used by directly spraying or applying to the human body such as hands, arms and feet. Moreover, in the said use, you may use, after diluting the antiviral agent of this invention with water or alcohol, such as methanol and ethanol, as needed.

  As the virus that exhibits the antiviral activity of the antiviral agent of the present invention, that is, the virus having an antiviral effect by the antiviral agent of the present invention is influenza A virus (human, bird, swine), influenza B virus , Parainfluenza viruses, A to E hepatitis viruses, measles viruses, herpes viruses, mumps viruses, rabies viruses and other enveloped viruses, noroviruses and other non-enveloped viruses. Among these, influenza viruses, Norovirus is preferred, and norovirus is particularly preferred.

  The antiviral agent composition of the present invention is represented by the general formula (1) as a component for introducing a site exhibiting antiviral activity (a phosphonium salt portion in the general formula (1)) into a substrate. One or more compounds selected from hydrolyzed condensates of alkoxysilyl group-containing phosphonium salts represented by the general formula (1 ′) and alkoxysilyl group-containing phosphonium salts represented by the general formula (1 ′) It is an antiviral agent composition characterized by containing.

  The phosphonium salt represented by the general formula (1), the alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′), and the alkoxy represented by the general formula (1 ′) according to the antiviral agent composition of the present invention Hydrolyzed condensates of silyl group-containing phosphonium salts include phosphonium salts represented by general formula (1), alkoxysilyl group-containing phosphonium salts represented by general formula (1 ′) and general This is the same as the hydrolysis-condensation product of the alkoxysilyl group-containing phosphonium salt represented by the formula (1 ′).

  The antiviral composition of the present invention is used for introducing a phosphonium salt moiety having antiviral activity into a substrate. Since the alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′) has an alkoxysilyl group, the chemical reaction with the base material having an oxygen-containing functional group such as —OH group or —OH— group is possible. It is possible to combine. Therefore, the antiviral agent composition of the present invention containing the alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′) fixes the portion of the phosphonium salt having antiviral activity to the substrate by chemical bonding. be able to.

  The antiviral agent composition of the present invention may contain water, methanol, ethanol, isopropanol and other alcohols as a solvent, and other organic solvents such as toluene, hexane, tetrahydrofuran, diethyl ether, dioxane, acetone, ethyl acetate and the like. it can. Further, the antiviral composition of the present invention contains auxiliary agents such as surfactants, binders, colorants, dispersants, lubricants, other inorganic or organic diluents, carriers and the like as necessary.

  The antiviral composition of the present invention can be used in combination with a fluorine-containing compound, if necessary. As the fluorine-containing compound, a fluoroalkyl group-containing oligomer represented by the following general formula (3) or a hydrolysis-condensation product thereof is particularly preferable. The antiviral agent composition of the present invention contains a fluoroalkyl group-containing oligomer or a hydrolyzed condensate thereof, so that the phosphonium salt represented by the general formula (1) and the alkoxy represented by the general formula (1 ′) Even if the addition amount of the hydrolyzed condensate of the silyl group-containing phosphonium salt and the alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′) is small, excellent antiviral functions can be imparted to various substrates. .

In formula (3), R ⁶ and R ⁷ are — (CF ₂ ) p—Y groups, or —CF (CF ₃ ) — [OCF ₂ CF (CF ₃ )] q—OC ₃ F ₇ groups, R ⁶ and R ⁷ may be the same group or different groups, Y in R ⁶ and R ⁷ is a hydrogen atom, a fluorine atom or a chlorine atom, and p and q are 0-10. It is an integer. R ⁸ , R ⁹ and R ¹⁰ may be the same group or different groups, and R ⁸ , R ⁹ and R ¹⁰ may be a linear alkyl group having 1 to 5 carbon atoms or 1 carbon atom. A branched alkyl group of ˜5. m is an integer of 2-3.

  Moreover, in the antiviral agent composition of this invention, it represents with the phosphonium salt represented by General formula (1), the alkoxysilyl group containing phosphonium salt represented by General formula (1 '), and General formula (1'). One or more compounds selected from the hydrolyzed condensates of alkoxysilyl group-containing phosphonium salts are composite particles containing a fluoroalkyl group-containing oligomer represented by the general formula (3) or a hydrolyzed condensate thereof. Also good. Examples of such composite particles include composite particles disclosed in JP2009-209349A and JP2010-77383A.

  The antiviral composition of the present invention is used for imparting an antiviral function to an object to be imparted with an antiviral function. In other words, the antiviral composition of the present invention is used to introduce a site having antiviral activity (a phosphonium salt site in the general formula (1)) into various materials.

  The method of using the antiviral agent composition of the present invention includes, for example, (i) applying or spraying the antiviral agent composition of the present invention to the surface of the substrate, and then applying the general formula (1) to the surface of the substrate. And a method of performing surface treatment by adsorbing or binding a phosphonium salt represented by the formula (1) or a site derived therefrom. In the method (i), examples of the substrate include paper, rubber, resin, fiber, film, sheet, wood, glass, ceramics, and metal. Examples of the rubber include those described later as the rubber for the substrate. Moreover, what is mentioned later as resin for base materials as resin is mentioned. In the method (i), after the surface treatment, the solvent in the antiviral composition of the present invention is appropriately removed by drying.

  Examples of forms of the method (i) and the antiviral composition of the present invention used therein include a phosphonium salt represented by the general formula (1) and an alkoxysilyl group represented by the general formula (1 ′). One or more compounds selected from a hydrolysis condensate of a phosphonium salt and an alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′) are mixed with a solvent for coating, and if necessary, a pigment, coloring Mixtures of known coating film components such as oils, varnish oils, coating film forming resins, drying agents, plasticizers, fillers, anti-aging agents, UV absorbers, light stabilizers, preservatives, diluents, etc. Then, a method of preparing a paint and applying the obtained paint to the object to be coated to coat the object to be coated and anti-virus-treating the surface of the object to be coated can be mentioned. In this embodiment, the paint used for painting the painting object corresponds to the antiviral composition of the present invention, the painting object corresponds to the base material, and the painting object is obtained by painting with a coating material. The above corresponds to the antiviral material of the present invention.

  In addition, (ii) the antiviral agent composition of the present invention is applied to or sprayed on a substrate, or the substrate is immersed in the antiviral agent composition of the present invention, whereby the present invention is incorporated in the substrate. And a method of impregnating the antiviral agent composition. In the method (ii), examples of the substrate include paper, rubber, resin, fiber, film, wood, glass, ceramics, and metal. Examples of the rubber include those described later as the rubber for the substrate. Moreover, what is mentioned later as resin for base materials as resin is mentioned. In the method (ii), after the impregnation treatment, the solvent in the antiviral composition of the present invention is appropriately removed by drying.

  In the above methods (i) and (ii), the method of applying, spraying or impregnating the antiviral agent composition of the present invention to the substrate is not particularly limited, and for example, brush coating, spraying method, roll Well-known methods, such as a coating method, a spin coat method, a dip coat method, are mentioned.

  Moreover, (iii) the method of mixing the antiviral agent composition of this invention in the raw material of a base material, and shape | molding the antiviral agent composition containing base material raw material obtained then is mentioned. In the method (iii), examples of the raw material for the substrate include paper, rubber, and resin.

  When the antiviral agent composition of the present invention is applied, sprayed or impregnated on a base material, the material of the base material is not particularly limited. Fiber, natural resin, non-woven fabric, wood, polybutene resin, polyacrylic acid resin, polyvinyl chloride resin, polyester resin, polypropylene resin, polystyrene resin, polycarbonate resin, polyamide resin, polyamine resin, urethane resin, ABS resin, AS resin, heat Plastic acrylic resin, unsaturated polyester resin, epoxy resin, polyimide resin, cellophane resin, alkyd resin, phenol resin, urea resin, melamine resin, xylene resin, UV curable polyfunctional (meth) acrylate resin, silicone resin or diaryl phthalate resin And resins such as these modified resins, Rubber, styrene-butadiene rubber (SBR), acrylonitrile-butadiene rubber (NBR), butyl rubber (IIR), polybutadiene rubber (BR), ethylene-propylene rubber (EPPM), chlorobutylene rubber (CR), polyisobutylene Rubber, allyl rubber, hydrogenated acrylonitrile-butadiene rubber, polysulfide rubber, urethane rubber, chlorisulfonated rubber, silicone rubber, and modified rubbers thereof, which may be blended products of two or more. Good.

  Further, when the antiviral composition of the present invention is applied, sprayed or impregnated on a substrate, the material of the substrate is a metal powder, metal or non-metal oxide (hydrous) if it is inorganic. ), Metal silicates including aluminosilicates, metal carbides, metal nitrides, metal carbonates, metal sulfates, metal phosphates, metal sulfides, metal salts, metal halides, stainless steel, geralumin, Examples thereof include inorganic materials such as glass, aluminum, ceramics, activated carbon, and clay minerals.

  In addition, when the antiviral agent composition of the present invention is applied, sprayed or impregnated on a substrate, the phosphonium salt represented by the general formula (1) in the antiviral agent composition of the present invention, the general formula (1) The content of the hydrolytic condensate of the alkoxysilyl group-containing phosphonium salt represented by ') and the alkoxysilyl group-containing phosphonium salt represented by the general formula (1') (the total content in the case of two or more types) is: Although it is appropriately selected, it is preferably 0.01% by mass or more, particularly preferably 0.01 to 30% by mass. In the case of the hydrolysis condensate of the alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′), the content thereof is the alkoxysilyl group-containing phosphonium represented by the general formula (1 ′) before hydrolysis. Content in terms of salt.

  When the antiviral agent composition of the present invention is mixed into the base material, and then the antiviral agent-containing base material is molded, the base material is not particularly limited and includes rubber raw materials and resins. It is done. When the base material is rubber, examples of the rubber for the base material, that is, the rubber that becomes the matrix of the antiviral material, include natural rubber, styrene-butadiene rubber (SBR), acrylonitrile-butadiene rubber (NBR), Butyl rubber (IIR), polybutadiene rubber (BR), ethylene-propylene rubber (EPPM), chlorobutylene rubber (CR), polyisobutylene rubber, allyl rubber, hydrogenated acrylonitrile-butadiene rubber, polysulfide rubber, urethane rubber, chlorosulfone Rubbers, silicone rubbers, modified products thereof, and the like, and two or more kinds of blend rubbers may be used. Then, the rubber raw material for producing the rubber for the base material is mixed with the antiviral agent composition of the present invention, and the rubber composition containing the antiviral agent composition of the present invention (antiviral agent-containing group) The rubber composition containing the obtained antiviral agent composition of the present invention is molded and rubberized to produce a rubber, thereby producing a site (general formula) having antiviral activity. A rubber material containing (the phosphonium salt moiety in (1)) is obtained.

  When mixing the antiviral agent composition of the present invention into the base material and then molding the antiviral agent-containing base material, the base resin, that is, the antiviral material matrix Is, for example, thermoplastic resins such as polyvinyl chloride resin, polyethylene resin, polypropylene resin, polyamide resin, polycarbonate resin, polyester resin, polystyrene resin, ABS resin, AS resin, thermoplastic acrylic resin, epoxy resin, unsaturated polyester resin , Thermosetting resins such as diaryl phthalate resin, phenol resin, urea resin, UV curable polyfunctional (meth) acrylate resin, alkyd resin, melanin resin, guanazine resin, vinyl resin, epoxy resin, polyamine resin, acrylic resin, Polybutadiene resin, urethane resin, kettle Fluororesin, fluororesin and the like their modified products thereof. When the substrate is a thermosetting resin or an ultraviolet curable resin, the antiviral agent composition of the present invention is mixed with the thermosetting resin raw material or the ultraviolet curable resin, and the antiviral agent composition of the present invention is mixed. Is obtained, and then the resulting resin composition containing the antiviral agent composition of the present invention is molded and cured to obtain antiviral activity. The resin material containing the site | part (The site | part of the phosphonium salt in General formula (1)) which has is obtained. Further, when the substrate is a thermoplastic resin, a resin composition (an antiviral agent-containing group) containing the antiviral agent composition of the present invention by melting and mixing the antiviral agent composition of the present invention with the thermoplastic resin. And then the resin composition containing the obtained antiviral agent composition of the present invention is heat-processed to give a site having antiviral activity (a site of the phosphonium salt in the general formula (1)) ) Is obtained. Examples of the molded product of the resin material include sheets, films, containers, fibers, and the like.

  As a method for producing an antiviral material using the antiviral agent composition of the present invention, for example, if the substrate is a curable resin such as a thermosetting resin or an ultraviolet curable resin, the antiviral composition of the present invention is used. A method of mixing an agent composition simultaneously with a curable resin and other compounds, a method of mixing the antiviral composition of the present invention in advance with one of the curable resin components, and mixing this with the curable resin In the case of a thermoplastic resin, a method of melt-mixing the antiviral composition of the present invention with an extruder, or a method of mechanically mixing particles together and then molding the mixture simultaneously with an injection molding machine Etc.

  The resin composition includes other components such as white carbon, carbon black, zeolite, calcium carbonate, clay, barium sulfate, magnesium carbonate and other inorganic fillers, high styrene resin, lignin, phenol resin, and the like. Organic fillers, antibacterial agents, UV absorbers, antioxidants, extenders, dispersion aids, vulcanizing agents, vulcanization accelerators, vulcanization aids, softeners, anti-aging agents, plasticizers, photopolymerization starts An additive known in the art such as an agent may be contained.

  When the antiviral agent composition of the present invention is mixed into the raw material of the base material and then the antiviral agent-containing base material is molded, it is represented by the general formula (1) in the antiviral agent-containing base material. Content of hydrolysis condensate of phosphonium salt, alkoxysilyl group-containing phosphonium salt represented by general formula (1 ′) and alkoxysilyl group-containing phosphonium salt represented by general formula (1 ′) (contains two or more kinds) The total content in the case is appropriately selected, but the content in the non-volatile content excluding the volatile content such as the solvent is preferably 0.01% by mass or more, particularly preferably 0.01 to 30% by mass. is there. In the case of the hydrolysis condensate of the alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′), the content thereof is the alkoxysilyl group-containing phosphonium represented by the general formula (1 ′) before hydrolysis. Content in terms of salt.

  As the antiviral material of the present invention, the antiviral agent composition of the present invention obtained by surface-treating the surface of a substrate, the substrate is impregnated with the antiviral agent composition of the present invention. Obtained by mixing the antiviral agent composition of the present invention into the raw material of the substrate, and then molding the obtained antiviral agent-containing substrate raw material.

  In addition, as the antiviral material of the present invention, one or more selected from the phosphonium salt represented by the general formula (1) and its hydrolysis condensate are mixed in the raw material of the base material, and then the antiviral material obtained is obtained. Examples include antiviral materials obtained by molding a virus agent-containing base material. Examples of the phosphonium salt represented by the general formula (1) include an alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′).

  Phosphonium salt represented by general formula (1), alkoxysilyl group-containing phosphonium salt represented by general formula (1 ′), and alkoxysilyl group represented by general formula (1 ′) according to the antiviral material of the present invention The hydrolyzed condensate of the phosphonium salt contains a phosphonium salt represented by the general formula (1), an alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′) and the general formula (1) This is the same as the hydrolysis condensate of the alkoxysilyl group-containing phosphonium salt represented by 1 ′).

  Hydrolysis condensate of phosphonium salt represented by general formula (1), alkoxysilyl group-containing phosphonium salt represented by general formula (1 ′), and alkoxysilyl group-containing phosphonium salt represented by general formula (1 ′) In the case where one or more selected from the above are mixed into the raw material of the base material and then the antiviral agent-containing base material is molded, the phosphonium represented by the general formula (1) in the antiviral agent-containing base material Content of hydrolysis condensate of salt, alkoxysilyl group-containing phosphonium salt represented by general formula (1 ′) and alkoxysilyl group-containing phosphonium salt represented by general formula (1 ′) (when two or more kinds are contained) Is the content in the non-volatile component excluding volatile components such as solvents, preferably 0.01% by mass or more, particularly preferably 0.01-30% by mass. . In addition, when the active ingredient is a hydrolysis condensate of an alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′), the content is the alkoxy represented by the general formula (1 ′) before hydrolysis. The content is converted to a silyl group-containing phosphonium salt.

  Hydrolysis condensate of phosphonium salt represented by general formula (1), alkoxysilyl group-containing phosphonium salt represented by general formula (1 ′), and alkoxysilyl group-containing phosphonium salt represented by general formula (1 ′) As a method of incorporating one or more (antiviral component) selected from the above into the resin, various resins can contain the antiviral component by a generally known method. For example, in the case of a curable resin such as a thermosetting resin or an ultraviolet curable resin, a method of mixing these antiviral components simultaneously with the curable resin and other blends, one of the curable resin components in advance. A method of mixing these antiviral components in advance and mixing them with a curable resin. If a thermoplastic resin, a method of melting and mixing these antiviral components with an extruder, or a method of mixing particles. Examples thereof include a method in which uniform mechanical mixing is performed and then molding is performed simultaneously with mixing in an injection molding machine.

  An antiviral material imparted with an antiviral function, that is, a phosphonium salt represented by the general formula (1), an alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′), and a general formula (1 ′) A site having an antiviral activity (phosphonium salt portion in the general formula (1)) is introduced into the substrate using one or more selected from the hydrolyzed condensates of alkoxysilyl group-containing phosphonium salts As a virus that exhibits the antiviral activity of the material obtained by the above, that is, viruses having an antiviral effect due to the antiviral material of the present invention include influenza A virus (human, bird, swine), influenza B virus , Parainfluenza virus, A to E hepatitis virus, measles virus, herpes virus, mumps virus, rabies Virus with envelope such as pulse, which go up non-envelope viruses such as Norovirus, among these, influenza virus, norovirus Preferably, Norovirus is particularly preferred.

  As described above, the antiviral material of the present invention comprises, on a base material, a phosphonium salt represented by the general formula (1), an alkoxysilyl group-containing phosphonium salt represented by the general formula (1 ′), and the general formula (1 ′). 1) One or more selected from hydrolysis-condensation products of alkoxysilyl group-containing phosphonium salts represented by formula (1), or a site having antiviral activity derived therefrom, that is, a site of phosphonium salt in general formula (1) It is a material that has been.

  The antiviral material of the present invention includes, for example, medical materials, medical devices, masks, gloves, towels, handrails, various fabrics, clothing, furniture, cloths, tableware, rugs, paper bags, cardboard containers, trash cans, trunks, Handbag, shoes, jacket, raincoat, tent, carpet, curtain, chair, desk, window, door handle, door knob, wood, brick, concrete, floor, wall tile, glass, stone, blaster, wallpaper, exterior wall material , Wall material for bath, magnetic tape, floppy disk, hard disk, mouse, keyboard, electronic device, air conditioner filter, touch panel, glasses, sink, kitchen area, toilet, toilet area, bathtub, bathtub Excellent resistance to various items such as surroundings, wash bowls, washrooms, refrigerators, washing machines, or parts of vehicles such as airplanes, cars, trains, etc. Grant pulse activity, it is used as an antiviral material.

EXAMPLES Hereinafter, although an Example is given and this invention is demonstrated, this invention is not limited to these.
<Antiviral active ingredient>
As the antiviral active ingredient, four kinds of compounds shown in Table 1 below were used.

(Example 1 and Comparative Example 1)
<Evaluation of anti-influenza virus>
A filter paper was laid in the deep petri dish, and a small amount of sterilized water was added. Place a glass stand of about 5 mm on the filter paper, apply a methanol solution containing 20% by mass of the above antiviral active ingredient on it, vacuum dry for 24 hours to remove the solvent, and antiviral active ingredient A glass plate (50 mm × 50 mm) chemically fixed was placed. On top of this, 0.1 ml of a QB phage (NBRC20012) solution of an influenza virus substitute virus that has been acclimated in advance and whose concentration has been clarified is dropped, and a polypropylene film (KOYUYO, 40 mm × 40 mm) is brought into contact with the material surface. ). The petri dish was covered with a glass plate. The same number of sets for measurement was prepared for the number of times the number of phages was scheduled to be measured, and was left to stand in the dark at 25 ° C. for 4 hours.
Next, based on JIS R 1706, the host bacteriophage infectivity titer was evaluated using host E. coli (NBRC106373), and the antibacterial activity was determined based on the calculation formula of the effect in the dark of the hybrid photocatalytic antiviral processing material of the following formula (1). Viral activity was assessed as V _D. The results are shown in Table 2. Moreover, the untreated glass plate was evaluated similarly, the result was evaluated as the blank 1, and the result was written together in Table 2.
Incidentally, indicating that the antiviral activity, the higher the value of V _D is larger.

V _D : dark effect of antiviral processed material B _D : average value (pfu) of bacteriophage infectivity of 3 test pieces after storing non-antiviral processed test pieces in the dark for 4 hours
C _D : Average value (pfu) of bacteriophage infectivity of 3 test pieces after storing the anti-virus processed test pieces in the dark for 4 hours

(Example 2 and Comparative Example 2)
<Evaluation of anti-norovirus>
Example 1 and Comparative Example 1 and Comparative Example 1 were used except that instead of QB phage (NBRC20012), Norovirus-replaced ф6 phage (NBRC105899) was used, and host Pseudomonas aeruginosa (NBRC105640) was used instead of host E. coli (NBRC106373). Similarly, antiviral activity was evaluated as V _D. The results are shown in Table 3. Moreover, the untreated glass plate was evaluated similarly, the result was evaluated as the blank 2, and the result was written together in Table 3.

  From the results shown in Tables 2 and 3, it was found that the phosphonium salt according to the present invention has superior antiviral activity against influenza viruses and noroviruses than the commonly used ammonium salts. In particular, it has been found that it has an excellent antiviral activity against norovirus compared to conventional ammonium salts.

(Example 3)
The anti-influenza virus and anti-norovirus were evaluated in the same manner as in Example 1 and Example 2 except that TOSP-Cl was used as the antiviral active ingredient, and the antiviral activity was evaluated as V _D. The results are shown in Table 4.

(Comparative Example 3)
The antiviral activity and antiviral activity were evaluated as V _{D in the same} manner as in Example 1 and Example 2 except that DPSP-Cl was used as the antiviral active ingredient, and the antiviral activity was evaluated as V _D. The results are shown in Table 5.

Claims (12)

1. An antiviral agent comprising at least one selected from a phosphonium salt represented by the following general formula (1) and a hydrolysis-condensation product thereof.
General formula (1):

(In the formula (1), R ¹ , R ² and R ³ are linear or branched alkyl groups having 1 to 18 carbon atoms. R ^{1 to} R ³ may be the same group but different from each other. R ⁴ is a linear or branched alkyl group having 1 to 18 carbon atoms or an alkoxysilyl group represented by the following general formula (2), wherein X ⁻ is an anionic group. is there.)
General formula (2):
_{- (CH 2) n -Si- (} OR 5) 3 (2)
(In formula (2), n is an integer of 1 to 8. R ⁵ is a linear or branched alkyl group having 1 to 5 carbon atoms.) The antiviral agent according to claim 1, wherein the phosphonium salt represented by the general formula (1) is an alkoxysilyl group-containing phosphonium salt represented by the following general formula (1 ').

(In the formula (1 ′), R ¹ , R ² and R ³ are linear or branched alkyl groups having 1 to 18 carbon atoms. R ^{1 to} R ³ may be the same groups, (X ⁻ is an anionic group, n is an integer of 1 to 8. R ⁵ is a linear or branched alkyl group having 1 to 5 carbon atoms.) The antiviral agent according to claim 2, wherein R ^{1 to} R ³ in the general formula (1 ') are all butyl groups and n is 3.   The antiviral agent according to any one of claims 1 to 3, wherein the virus is at least one selected from influenza viruses and noroviruses. The antiviral agent composition characterized by including 1 or more types chosen from the phosphonium salt represented by following General formula (1), and its hydrolysis-condensation product.
General formula (1):

(In the formula (1), R ¹ , R ² and R ³ are linear or branched alkyl groups having 1 to 18 carbon atoms. R ^{1 to} R ³ may be the same group but different from each other. R ⁴ is a linear or branched alkyl group having 1 to 18 carbon atoms or an alkoxysilyl group represented by the following general formula (2), wherein X ⁻ is an anionic group. is there.)
General formula (2):
_{- (CH 2) n -Si- (} OR 5) 3 (2)
(In formula (2), n is an integer of 1 to 8. R ⁵ is a linear or branched alkyl group having 1 to 5 carbon atoms.) 6. The antiviral agent composition according to claim 5, wherein the phosphonium salt represented by the general formula (1) is an alkoxysilyl group-containing phosphonium salt represented by the following general formula (1 ′).

(In the formula (1 ′), R ¹ , R ² and R ³ are linear or branched alkyl groups having 1 to 18 carbon atoms. R ^{1 to} R ³ may be the same groups, (X ⁻ is an anionic group, n is an integer of 1 to 8. R ⁵ is a linear or branched alkyl group having 1 to 5 carbon atoms.) 7. The antiviral composition according to claim 6, wherein R ^{1 to} R ³ in the general formula (1 ′) are all butyl groups and n is 3.   The antiviral composition according to any one of claims 5 to 7, wherein the virus is at least one selected from influenza viruses and noroviruses.   The antiviral material obtained by surface-treating the surface of a base material with the antiviral agent composition of any one of Claims 5-8.   The antiviral material obtained by making a base material impregnate the antiviral agent composition of any one of Claims 5-8. The antiviral agent composition according to any one of claims 5 to 8, or one or more selected from a phosphonium salt represented by the following general formula (1) and a hydrolysis-condensation product thereof in the raw material of the base material An antiviral material obtained by mixing and then molding the resulting antiviral agent-containing base material.
General formula (1):

(In the formula (1), R ¹ , R ² and R ³ are linear or branched alkyl groups having 1 to 18 carbon atoms. R ^{1 to} R ³ may be the same group but different from each other. R ⁴ is a linear or branched alkyl group having 1 to 18 carbon atoms or an alkoxysilyl group represented by the following general formula (2), wherein X ⁻ is an anionic group. is there.)
General formula (2):
_{- (CH 2) n -Si- (} OR 5) 3 (2)
(In formula (2), n is an integer of 1 to 8. R ⁵ is a linear or branched alkyl group having 1 to 5 carbon atoms.) The antiviral material according to any one of claims 9 to 11, wherein the virus is at least one selected from influenza viruses and noroviruses.