TECHNICAL FIELD

The present disclosure broadly relates to antimicrobial wound dressing materials, to processes suitable for the preparation of such materials, and to the use of such materials as wound dressings.

BACKGROUND

Antiseptic compositions in the form of pastes are often placed in surgical wounds to prevent infections. However, such antiseptic compositions can be sticky and difficult to handle with precision, particularly in a moist environment such as a wound.

There is a continuing need for materials and articles to facilitate wound healing.

SUMMARY

Advantageously, the present disclosure provides antiseptic wound dressing materials that provide antimicrobial protection, even in the presence of cationic antiseptics, and may be fully bioabsorbed by the body during healing.

In one aspect, the present disclosure provides a wound dressing material comprising: a first wound-contact scrim comprising first water-sensitive fibers, wherein the first water- sensitive fibers comprise a first copolymer comprising divalent hydroxyethylene monomer units and divalent dihydroxybutylene monomer units; a second wound-contact scrim comprising second water-sensitive fibers, wherein the second water-sensitive fibers comprise a second copolymer comprising divalent hydroxyethylene monomer units and divalent dihydroxybutylene monomer units; and an antimicrobial layer contacting and disposed between the first wound-contact scrim and the second wound-contact scrim.

In another aspect, the present disclosure provides a method of using a wound dressing material according to the present disclosure , the method comprising contacting the wound dressing material with a wound.

In yet another aspect, the present disclosure provides a method of making a wound dressing material, the method comprising bonding: a first wound-contact scrim comprising first water-sensitive fibers, wherein the first water- sensitive fibers comprise a first copolymer comprising divalent hydroxyethylene monomer units and divalent dihydroxybutylene monomer units; a second wound-contact scrim comprising second water-sensitive fibers, wherein the second water-sensitive fibers comprise a second copolymer comprising divalent hydroxyethylene monomer units and divalent dihydroxybutylene monomer units; and an antimicrobial layer contacting and disposed between the first wound-contact scrim and the second wound-contact scrim.

As used herein: the term "scrim" refers to a lightweight highly porous fabric that may be woven or nonwoven; the term "water-sensitive" means water swellable and/or water-soluble; and the term "wound" refers to an injury to a subject (e g., a mammal) which involves a break in the normal skin barrier exposing tissue below, which is caused by, for example, lacerations, surgery, bums, damage to underlying tissue such as pressure sores, or poor circulation. Wounds are understood to include both acute and chronic wounds.

Features and advantages of the present disclosure will be further understood upon consideration of the detailed description as well as the appended claims.

BRIEF DESCRIPTION OF THE DRAWINGS

FIG. 1 is a schematic side view of an exemplary wound dressing material 100 according to the present disclosure.

It should be understood that numerous other modifications and embodiments can be devised by those skilled in the art, which fall within the scope and spirit of the principles of the disclosure. The figures may not be drawn to scale.

DETAILED DESCRIPTION

Referring now to FIG. 1, wound dressing material 100 comprises first wound-contact scrim 110, second wound-contact scrim 130, and antimicrobial layer 120 contacting and disposed between first wound-contact scrim 110 and second wound-contact scrim 130.

The first wound-contact scrim comprises first water-sensitive fibers 115. First water-sensitive fibers 115 comprise a first copolymer comprising divalent hydroxyethylene monomer units and divalent dihydroxybutylene monomer units. The second wound-contact scrim comprises second water-sensitive fibers 135. Second water-sensitive fibers 135 comprise a second copolymer comprising divalent hydroxyethylene monomer units and divalent dihydroxybutylene monomer units. an antimicrobial layer contacting and disposed between the first wound-contact scrim and the second wound-contact scrim.

The first and second wound-contact scrims may be the same or different. They comprise water- sensitive fibers that comprise first and optionally second copolymers (which may be the same or different), each respective copolymer comprising divalent hydroxyethylene monomeric units (i.e., and divalent dihydroxybutylene monomer units. In preferred embodiments, the divalent dihydroxybutylene monomer units comprise 3,4-dihydroxybutan-l,2-diyl monomer units (i.e., monomer units). Optionally, but typically, the copolymer furthers comprise acetoxyethylene divalent monomeric units ( The copolymer may be obtained by copolymerization of vinyl acetate and 3,4-dihydroxy-l -butene followed by partial or complete saponification of the acetoxy groups to form hydroxyl groups.

Alternatively, in place of 3,4-dihydroxy-l -butene, a carbonate such as can also be used. After copolymerization, this carbonate may be hydrolyzed simultaneously with saponification of the acetate groups. In another embodiment, in place of 3,4-dihydroxy- 1 -butene, an acetal or ketal having the formula: where each R is independently hydrogen or alkyl (e.g., methyl or ethyl). After copolymerization, this carbonate may be hydrolyzed simultaneously with saponification of the acetate groups, or separately. The copolymer can be made according to known methods or obtained from a commercial supplier, for example.

Commercially available copolymers may include those available under the trade designation Nichigo G-Polymer (Nippon Gohsei Synthetic Chemical Industry, Osaka, Japan), a highly amorphous polyvinyl alcohol, that is believed to have divalent monomer units of hydroxyethylene, 3,4- dihydroxybutan-l,2-diyl, and optionally acetoxyethylene. Nippon Gohsei also refers to Nichigo G- Polymerby the chemical name butenediol vinyl alcohol (BVOH). Exemplary materials include Nichigo G-Polymer grades AZF8035W, OKS-1024, OKS-8041, OKS-8089, OKS-8118, OKS-6026, OKS-1011, OKS-8049, OKS-1028, OKS-1027, OKS-1109, OKS-1081, and OKS-1083. These copolymers are believed to have a saponification degree of 80 to 97.9 mole percent, and further contain an alkylene oxide adduct of a polyvalent alcohol containing 5 to 9 moles of an alkylene oxide per mole of the polyvalent alcohol. These materials have melt-processing properties that are suitable for forming melt-blown and spunbond webs.

The first and optional second wound-contact scrims may optionally contain bioabsorbable secondary fibers in addition to the copolymer fibers. Useful bioabsorbable secondary fibers may include, for example, fibers comprising: polycaprolactone; polylactide (PLA); polyglycolide (PGA); polydioxane;poly(glycolide-co-lactide) (PGA-co-PLA); poly(lactic acid-co-caprolactone); and copolyesters of e-caprolactone, trimethylene carbonate, and /i-dioxanonc: and combinations thereof.

Preferably, bioabsorbable polymers used in wound dressings according to the present disclosure have a molecular weight (M _n ) in the range of about 1,000 to about 8,000,000 g/mole, more preferably about 4,000 to about 250,000 g/mole, although this is not a requirement.

Methods of forming the wound-contact scrims will depend on the type of fiber web formed, but will be well-known to those of skill in the textile arts. Suitable methods may include airlaying and/or carding of staple fibers followed by needletacking to density and strengthen the fiber web; melt-blown; spunbond; and wet-laid processes. The wound-contact scrim(s) may be heat-calendered to densify and/or improve the web handling properties.

In some embodiments, the wound-contact scrims may be made by air-laying of staple fibers. Air- laid nonwoven fiber webs may be prepared using equipment such as, for example, that available as a RANDO WEBBER from Rando Machine Company of Macedon, New York. In some embodiments, a type of air-laying may be used that is termed gravity-laying, as described e.g., in U. S. Pat. Application Publication 2011/0247839 (Lalouch). Nonwoven staple fiber webs may be densified and strengthened, for example, by techniques such as crosslapping, stitchbonding, needletacking, chemical bonding, and/or thermal bonding.

Melt-blowing methods are well-known in the art. As used herein, the term "melt-blowing" refers to a process in which fibers are formed by extruding a molten thermoplastic material through a plurality of fine, usually circular, die capillaries into a high velocity gas (e.g., air) stream which attenuates the molten thermoplastic material and forms fibers, which can be any microfiber diameter, typically less than 10 microns in diameter. Thereafter, the melt-blown fibers are carried by the gas stream and are deposited on a collecting surface to form a web of random melt-blown fibers. Such a process is disclosed, for example, in U. S. Pat. Nos. 3,849,241 (Butin et ah); 4,307,143 (Meitner et ah); and 4,707,398 (Wisneski et ah).

Fibers in the wound-contact scrims may be staple and/or continuous, preferably at least substantially continuous. For example, the first and/or optional second wound-contact scrims may comprise a meltblown fiber web or a spunbond fiber web. Fibers in the wound-contact scrims may have any average diameter, preferably from 2 to 200 microns and more preferably 2 to 100 microns. The wound-contact scrims may have any basis weight, but in many embodiments, it is preferably in the range of 5 to 300 grams per square meter (gsm), more preferably 20 to 200 gsm, and more preferably 30 to 100 gsm.

Optionally, the wound-contact scrims may further comprise at least one of addition of a plurality of staple fibers or addition of optional particulates; for example, by one or more methods described in U. S. Pat. Nos. 4,118,531 (Hauser), 6,872,3115 (Koslow), and 6,494,974 (Riddell); and in U. S. Pat. Appl. Publ. Nos. 2005/0266760 (Chhabra et al), 2005/0287891 (Park), and 2006/0096911 (Brey et al.). In other exemplary embodiments, the optional particulates may be added to a nonwoven fiber stream by air laying a fiber web, adding particulates to the fiber web (e.g., by passing the web through a fluidized bed of particulates), optionally with post heating of the particulate-loaded web to bond the particulates to the fibers.

The antimicrobial layer provides effective topical antimicrobial activity and thereby treat and/or prevent a wide variety of afflictions. For example, it can be used in the treatment and/or prevention of afflictions that are caused, or aggravated by, microorganisms (e.g., Gram positive bactena, Gram negative bacteria, fungi, protozoa, mycoplasma, yeast, viruses, and even lipid-enveloped viruses) on skin. Particularly relevant organisms that cause or aggravate such afflictions include Staphylococcus spp., Streptococcus spp., Pseudomonas spp., Enterococcus spp.,Acinetobacter spp., Klebsiella spp., Enterobacter spp., and Eshenchia spp., bacteria, as well as herpes virus, Aspergillus spp., Fusarium spp., Candida spp., as well as combinations thereof. Particularly virulent organisms include Staphylococcus aureus (including resistant strains such as Methicillin Resistant Staphylococcus aureus (MRSA), Staphylococcus epidermidis, Group A and B Streptococcus, Streptococcus pneumoniae, Enterococcus faecalis, Vancomycin Resistant Enterococcus (VRE), Pseudomonas aeruginosa, Acinetobacter baumannii, Klebsiella pneumoniae, Escherichia coli, (including multidrug resistant (MDR) species thereof) Aspergillus niger, Aspergillus fumigatus, Aspergillus clavatus, Fusarium solani, Fusarium oxysporum, Fusarium chlamydosporum, Candida albicans, Candida glabrata, Candida krusei, Candida auris and combinations thereof.

In some embodiments, the antimicrobial layer may be a surface coating (e.g., a paste or gel) on either or both of the first and second wound-contact scrims, or it may be a freestanding layer (e.g., a film).

In some embodiments, antimicrobial layers, when provided as a free thin film (i.e., not as a coating on a substrate) have a basis weight in the range of 20 to 700 gsm, more preferably in the range of 75 to 600 gsm, and more preferably in the range of 100 to 500 gsm, are typically flexible and can be deformed without breaking, shattering, or flaking of the antimicrobial layer.

Each antimicrobial layer comprises at least one antimicrobial compound. Exemplary antimicrobial compounds include antibiotics (e.g., amoxicillin, bacitracin zinc, doxycycline, cephalexin, ciprofloxacin, clindamycin, metronidazole, azithromycin, sulfamethoxazole, trimethoprim, or levofloxacin), and antiseptics such as chlorhexidine and its salts (e.g., chlorhexidine digluconate and chlorhexidine diacetate), antimicrobial lipids, phenolic antiseptics, cationic antiseptics, iodine and/or an iodophor, peroxide antiseptics, antimicrobial natural oils, alkane- 1,2-diols having 6 to 12 carbon atoms, silver, silver salts and complexes, silver oxide, copper, copper salts, and combinations thereof. Preferred antimicrobial compounds include antimicrobial quaternary amine compounds (e.g., benzalkonium chloride) and salts thereof cationic surfactants (e.g., cetylpyridinium chloride or cetyltrimethylammonium bromide), polycationic compounds such as octenidine or a salt thereof biguanide compounds (e.g., chlorhexidine, polyhexamethylenebiguanide (PHMB) or a salt thereof, 1,2- organic diols having 6 to 12 carbon atoms (e.g., 1,2-octanediol), antimicrobial fatty acid monoester compounds, and combinations thereof.

Wound dressing materials according to the present disclosure may have broad-spectrum antimicrobial activity. However, the wound dressing materials are typically sterilized; for example, by sterilized by a variety of industry standard techniques. For example, it may be preferred to sterilize the wound dressing materials in their final packaged form using electron beam. It may also be possible to sterilize the sample by gamma radiation, nitrogen dioxide sterilization and/or heat. Other forms of sterilization may also be used. It may also be suitable to include preservatives in the formulation to prevent growth of certain organisms. Suitable preservatives include industry standard compounds such as parabens (e.g., methylparaben, ethylparaben, propylparaben, isopropylparaben, or isobutylparaben); 2 bromo-2 nitro-l,3-diol; 5 bromo-5-nitro-l,3-dioxane, chlorbutanol, diazolidinyl urea; iodopropyl butyl carbamate, phenoxyethanol, halogenated cresols, methylchloroisothiazolinone; and combinations thereof.

Many preferred antimicrobial layers comprise an effective amount of a polycarboxylic acid chelator compound, alone or in combination with any of the foregoing antimicrobial compounds. The amount is effective to prevent growth of a microorganism and/or to kill microorganisms on a surface to which the composition is contacted.

In certain embodiments, the polycarboxylic acid chelator compound, whether aliphatic, aromatic, or a combination thereof, comprises at least two carboxylic acid groups. In certain embodiments, the polycarboxylic acid chelator compound, whether aliphatic, aromatic or a combination thereof, comprises at least three carboxylic acid groups In certain embodiments, the polycarboxylic acid chelator compound, whether aliphatic or aromatic, comprises at least four carboxylic acid groups.

Polycarboxylic acid-containing chelator compounds suitable for use in antimicrobial layer include aliphatic polycarboxylic acids, aromatic polycarboxylic acids, compounds with both one or more aliphatic carboxylic acids and one or more aromatic carboxylic acids, salts thereof, and combinations of the foregoing. Nonlimiting examples of suitable polycarboxylic acid-containing chelator compounds include citric acid, glutaric acid, glutamic acid, maleic acid, succinic acid, tartaric acid, malic acid, ethylenediaminetetraacetic acid, phthalic acid, trimesic acid, and pyromellitic acid.

Preferred salts include those formed from monovalent inorganic bases and include cations such as

K ⁺ , Na ⁺ , Li ⁺ , and Ag ⁺ , and combinations thereof. In some compositions polyvalent bases may be appropriate and include cations such as Ca , , . Alternatively, the salt of the polycarboxylic acid may be formed using an organic base such as a primary, secondary, tertiary, or quaternary amine.

In many embodiments, the polycarboxylic acid-comprising chelator compound may be present in the antimicrobial layer at relatively high concentrations (on a weight basis) while the composition remains surprisingly nonfrangible. The minimum effective amount of chelator compound in the antimicrobial layer is related to the number of carboxyl groups in the chelator compound. For example, succinic acid (with two carboxyl groups) is generally more efficacious than glutamic acid having the same number of carboxylic acid groups since in glutamic acid carboxyl group forms a zwitterion with an amino group.

Mucic acid is another example with 2 carboxyl groups. Mucic acid is not as efficacious as succinic acid since the carboxyl groups are further apart and sterically hindered. In certain embodiments, efficacy of the composition can be improved by using thicker (greater basis weight) antimicrobial layers. Efficacy may depend on the amount of acid in the antimicrobial layer as well as the total amount (mass) of the antimicrobial layer. Thus, in some embodiments, the chelator compound comprises at least about 5, 10, 15, 20, 25, 30, 35, 40, 45, 50, 55, or even at least 60 percent by weight of an essentially solvent-free antimicrobial layer. The term “essentially solvent-free” is understood to mean that the antimicrobial layer has been processed to remove most of the solvent (e.g., water and/or organic solvent) or has been processed in such a way that no solvent (e.g., water and/or organic solvent) was required. Generally, solvents are relatively volatile compounds having a boiling point at one atmosphere pressure of less than 150 °C. Solvent may be used to process (e.g., coat or film-form) the antimicrobial layer, but is preferably substantially removed to produce the final article for sale. For example, certain precursor compositions used to form the antimicrobial layer are first combined with water as a vehicle to form a solution, emulsion, or dispersion. These precursor compositions are coated and dried on a substrate (e.g., a release liner, , or the wound-contact scrim (s)) such that the water content of the antimicrobial layer is less than 10 percent by weight, preferably less than 5 percent by weight, and more preferably less than 2 percent by weight.

In some embodiments, the chelator compound comprises up to about 15, 20, 25, 30, 35, 40, 45,

50, 55, or even up to about 60 percent by weight of the essentially dry antimicrobial layer on a weight basis.

In certain embodiments, wherein the polycarboxylic acid-comprising chelator compound comprises two aliphatic carboxylic acid groups (e.g., succinic acid), the chelator compound comprises at least about 10 percent by weight of the essentially dry antimicrobial layer on a weight basis. In certain embodiments, wherein the polycarboxylic acid-comprising chelator compound comprises three aliphatic carboxylic acid groups (e.g., citric acid), the chelator compound comprises at least about 10 percent by weight of the essentially dry antimicrobial layer on a weight basis. In certain embodiments, wherein the polycarboxylic acid-comprising chelator compound comprises four aliphatic carboxylic acid groups (e.g., ethylenediaminetetraacetic acid), the chelator compound comprises at least about 5 percent by weight of the essentially dry antimicrobial layer on a weight basis.

When preparing antimicrobial layers of the present disclosure, the polycarboxylic acid-containing chelator compound may be dissolved and/or dispersed in a water-soluble plasticizer component and optionally a solvent such as water. The plasticizer component has a boiling point greater than 105 °C and has a molecular weight of less than 5000 daltons. Preferably, the plasticizer component is a liquid at 23 °C. Typically, but not necessarily, the plasticizer component is the most abundant solvent in the antimicrobial layer in which the polycarboxylic acid-containing chelator compound is dissolved and/or dispersed. In certain embodiments wherein water is used to prepare the antimicrobial layer, substantially all of the water is subsequently removed (e.g., after the antimicrobial layer has been coated onto a substrate and heated to remove water).

In certain embodiments, the chelator compound comprises an aliphatic and/or aromatic polycarboxylic acid, in which two or more of the carboxylic groups are available for chelation without any zwitterionic interaction. Although potential zwitteriomc interactions (e.g., such as in /.-glutamic acid) may decrease antimicrobial efficacy relative to similar compounds (e.g., glutaric acid, succinic acid) that do not comprise a-amino groups, such zwitterionic compounds also exhibit antimicrobial activity. In addition, two or more carboxylic acid groups in the polycarboxylic acid-containing chelator compounds should be disposed in the chelator compound in sufficient proximity to each other or the compound should be capable of folding/conforming to bring the carboxylic acids sufficiently close to facilitate chelation of metal ions.

In certain embodiments, the chelator compound comprises an aliphatic polycarboxylic acid or a salt thereof, an aromatic polycarboxylic acid or a salt thereof, or a combination thereof. In certain embodiments, the chelator compound comprises an aliphatic portion. In certain embodiments, the chelator compound comprises an aliphatic portion. The carboxylic acids may be disposed on the aliphatic portion and/or on the aromatic portion. Nonlimiting examples of chelator compounds that comprise an aliphatic portion with a carboxylic acid group disposed thereon and an aromatic portion with a carboxylic acid group disposed therein include 3-(2-carboxyphenyl)propionic acid, 3-(4-carboxyphenyl)propionic acid, and 4-[(2-carboxyphenyl)amino]benzoic acid.

In certain embodiments, efficacy of the antimicrobial layer can be improved by depositing a higher amount of dried antimicrobial layer. Efficacy is dependent on concentration of chelator compound in the antimicrobial layer as well as total amount of the antimicrobial layer.

The antimicrobial layer may contain plasticizer, preferably bioabsorbable. Suitable plasticizers may include, for example, glycerol, a polyglycerol having 2-20 glycerin units, polyglycerols partially esterified with C _j -C _j c alkylcarboxylic acids having at least two free hydroxyl groups (e.g., hexaglycerol monolaurate, decaglycerol monolaurate, polyglyceryl-6 caprate, polyglyceryl-4 oleate, polyglyceryl- 10 trilaurate and the like), polyethylene oxide, polyethylene glycol, polyethylene glycols initiated by any of the glycols discussed herein such as polyethylene glycol glyceryl ether, propylene glycol, dipropylene glycol, tripropylene glycol, 2-methyl- 1,3-propanediol, sorbitol, dimethylisosorbide, pentaerythritol, trimethylolpropane, ditrimethylolpropane, a random ethylene oxide/propylene oxide (EO/PO) copolymer or oligomer, a block EO/PO copolymer or oligomer, and combinations thereof.

Plasticizer may be present in the antimicrobial layer at relatively high concentrations (on a weight basis). In some embodiments, plasticizer comprises at least about 10 percent by weight of the antimicrobial layer. In some embodiments, plasticizer comprises at least about 10, 15, 20, 25, 30, 35, 40, 45, 50, 55, 60, 65, 70, or even at least 75 percent by weight of the antimicrobial layer. In certain embodiments, the plasticizer component can act as a humectant. Advantageously, this can maintain a moist environment in a wound to help promote healing of wound tissue.

Advantageously, the relatively high concentration of plasticizer and/or water-soluble or water- dispersible polymer in the antimicrobial layer can function as a controlled-release modulator that facilitates delivery of the antimicrobial(s) over an extended period of time. In some embodiments, the plasticizer component can also function as an antimicrobial component.

Antimicrobial layers according to the present disclosure are preferably solid at 25 °C. In certain embodiments, the antimicrobial layer may comprise a solvent having a normal boiling point of less than or equal to 100 °C. Nonlimiting examples of such solvents include water and lower (C2-C5) alcohols. Preferably, before use, the antimicrobial layer comprises very little solvent (e g., less than or equal to about 10 percent by weight) having a normal boiling point of less than or equal to 100 °C. In some embodiments, the antimicrobial layer comprises less than 5 percent by weight, less than 4 percent by weight, less than 3 percent by weight, less than 2 percent by weight, or even less than 1 percent by weight (by weight) of a solvent having a normal boiling point of less than or equal to 100 °C. In certain embodiments, the antimicrobial layer may be substantially free (before use) of such solvents or any compounds having a normal boiling point of less than 100 °C.

In many preferred embodiments, the antimicrobial layer(s) comprise a water-soluble or water- dispersible polymer as a binder. The water-soluble or water-dispersible polymer has a Tg greater than or equal to 20 °C. In use, the polymer can function to form the antimicrobial layer into a cohesive shape such as a fdm while also absorbing wound exudate and to maintain a moist environment that can facilitate healing of the tissue at a wound site.

Exemplary water-soluble and/or water-dispersible polymers that are suitable for use in a antimicrobial layer according to the present disclosure include polyvinylpyrrolidone; polyvinyl alcohol; copolymers of vinyl alcohol; polybutylenediol; polysaccharides (e.g., starch); guar gum; locust bean gum; carrageenan; hyaluronic acid; agar; alginate; tragacanth; gum arabic; gum karraya; gellan; xanthan gum; hydroxyethylated, hydroxypropylated, and/or cationic derivatives of the foregoing; modified cellulose polymers (e.g., hydroxyethylcellulose, hydroxypropyl methylcellulose, carboxymethylcellulose, or cationic cellulose such as polyquaterium 4); copolymers of polyvinylpyrrolidone and vinyl acetate; water- soluble and water-swellable polyacrylates (e.g., based on hydroxyethyl (meth)acrylate, hydroxypropyl (meth)acrylate, (meth)acrylic acid, (meth)aciylamide, PEG (meth)acrylates, methyl (meth)acrylate), and combinations thereof. As used herein the term "(meth)acryl" refers to acryl and/or methacryl. In certain embodiments, the water-soluble or water-dispersible polymers can comprise a polyquatemium polymer.

In some embodiments, the water-soluble or water-dispersible polymer comprises at least about 5 percent by weight of the antimicrobial layer. In some embodiments, the water-soluble or water- dispersible polymer comprises up to about 65 percent by weight of the antimicrobial layer.

When contacting a wound site, the antimicrobial layer and/or articles of the present disclosure are hydrated by the tissue fluids and wound exudate. Antimicrobial layers according to the present disclosure comprise polycarboxylic acid chelator compounds that, in an aqueous environment, have antimicrobial properties at an acidic pH. Thus, antimicrobial layers of the present disclosure comprise appropriate quantities of acidic components (e.g., the free acid of the polycarboxylic acid chelator compound) and basic components (e.g., NaOH or a salt of a polycarboxylic acid chelator compound) such that the antimicrobial layer, when mixed well with deionized water at a 1:9 mass ratio, forms an aqueous mixture having a pH of about 2.5 to 5.5. In certain embodiments, the pH of the resulting aqueous mixture is at least 2.5, 3.0, 3.5, 4.0, 4.5, 5.0, or even at least 5.5.

A variety of other ingredients may be added to the antimicrobial layers according to the present disclosure for desired effect. These include, but are not limited to, surfactants, skin emollients and humectants such as, for example, those described in U. S. Pat. No. 5,951,993 (Scholz et af), fragrances, colorants, and/or tackifiers.

Wound dressing materials according to the present disclosure may have any basis weight, thickness, porosity, and/or density unless otherwise specified.

Wound dressing materials according to the present disclosure may have any desired thickness. . In many embodiments, the basis weight is in the range of 20 to 800 gsm, more preferably 60 to 600 gsm and more preferably 100 to 500 gsm.

The wound dressing material may be provided in roll form, or it may be converted into sheets or bandages (optionally further comprising a peripheral supporting frame).

Preferably, to maintain a low relative humidity, the wound dressing material should be packaged in a package with a low moisture vapor transmission rate (MVTR) such as, for example, a Techni-Pouch package (Technipaq, Inc., Crystal Lake, Illinois) with a PET/Aluminum Foil/LLDPE material construction.

Wound dressing materials according to the present disclosure are useful, for example, for placement in a wound. Typically, the exposed surface of the wound is cleaned and/or treated with antiseptic (if necessary) and then contacted with the wound dressing material, which may be placed within the wound to facilitate healing. In some embodiments, the wound is closed over the wound dressing material which then provides antiseptic agents to facilitate healing, and ultimately being absorbed by the body.

SELECT EMBODIMENTS OF THE PRESENT DISCLOSURE

In a first embodiment, the present disclosure provides a wound dressing material comprising: a first wound-contact scrim comprising first water-sensitive fibers, wherein the first water- sensitive fibers comprise a first copolymer comprising divalent hydroxyethylene monomer units and divalent dihydroxybutylene monomer units; a second wound-contact scrim comprising second water-sensitive fibers, wherein the second water-sensitive fibers comprise a second copolymer comprising divalent hydroxyethylene monomer units and divalent dihydroxybutylene monomer units; and an antimicrobial layer contacting and disposed between the first wound-contact scrim and the second wound-contact scrim.

In a second embodiment, the present disclosure provides a wound dressing material according to the first embodiment, wherein at least one of the first or second water-sensitive fibers have an average fiber diameter of 2 to 100 microns.

In a third embodiment, the present disclosure provides a wound dressing material according to the first or second embodiment, wherein at least one of the first or second copolymers further comprises divalent acetoxy ethylene monomer units.

In a fourth embodiment, the present disclosure provides a wound dressing material according to any of the first to third embodiments, wherein the divalent dihydroxybutylene monomer units comprise divalent 3,4-dihydroxybutan-l,2-diyl monomer units.

In a fifth embodiment, the present disclosure provides a wound dressing material according to any of the first to fourth embodiments, wherein at least one of the first or second wound-contact scrims is melt-blown or spunbonded.

In a sixth embodiment, the present disclosure provides a wound dressing material according to any of the first to fifth embodiments, wherein the antimicrobial layer comprises a film.

In a seventh embodiment, the present disclosure provides a method of using a wound dressing material according to any of the first to six embodiments, the method comprising contacting the wound dressing material with a wound.

In an eighth embodiment, the present disclosure provides a method according to the seventh embodiment, further comprising closing the wound with the wound dressing material remaining inside it.

In a ninth embodiment, the present disclosure provides a method of making a wound dressing material, the method comprising bonding: a first wound-contact scrim comprising first water-sensitive fibers, wherein the first water- sensitive fibers comprise a first copolymer comprising divalent hydroxyethylene monomer units and divalent dihydroxybutylene monomer units; a second wound-contact scrim comprising second water-sensitive fibers, wherein the second water-sensitive fibers comprise a second copolymer comprising divalent hydroxyethylene monomer units and divalent dihydroxybutylene monomer units; and an antimicrobial layer contacting and disposed between the first wound-contact scrim and the second wound-contact scrim.

In a tenth embodiment, the present disclosure provides a method according to the ninth embodiment, wherein said bonding comprises laminating.

In an eleventh embodiment, the present disclosure provides a method according to the ninth or tenth embodiment, wherein at least one of the first or second water-sensitive fibers have an average fiber diameter of 2 to 100 microns.

In a twelfth embodiment, the present disclosure provides a method according to any of the ninth to eleventh embodiments, wherein at least one of the first or second copolymers further comprises divalent acetoxy ethylene monomer units.

In a thirteenth embodiment, the present disclosure provides a method according to any of the ninth to twelfth embodiments, wherein the divalent dihydroxybutylene monomer units comprise divalent 3,4-dihydroxybutan-l,2-diyl monomer units.

In a fourteenth embodiment, the present disclosure provides a method according to any of the ninth to thirteenth embodiments, wherein the first wound-contact scrim is melt-blown or spunbonded.

In a fifteenth embodiment, the present disclosure provides a method according to any of the ninth to fourteenth embodiments, wherein the antimicrobial layer comprises a film.

Objects and advantages of this disclosure are further illustrated by the following non-limiting examples, but the particular materials and amounts thereof recited in these examples, as well as other conditions and details, should not be construed to unduly limit this disclosure.

EXAMPLES

Unless otherwise noted, all parts, percentages, ratios, etc. in the Examples and the rest of the specification are by weight.

Preparation of Fiber Web 1 (9 gsm):

A melt-blown (i.e., blown microfiber, BMF) nonwoven fiber web was made using Nichigo G- Polymer butanediol vinyl alcohol copolymer (BVOH) pellets (obtained as Nichigo G-Polymer OKS 8112 from the Mitsubishi Chemical Corporation, Tokyo, Japan). A conventional melt-blowing process was employed similar to that described in V. A. Wente, "Superfine Thermoplastic Fibers" in Industrial Engineering Chemistry, Yol. 48, pages 1342 et seq. (1956).

More particularly, the melt-blowing die had circular smooth surfaced orifices, spaced 10 to the centimeter, with a 5: 1 length to diameter ratio. Molten (co)polymer was delivered to the die by a 20 mm twin screw extruder (commercially available from the SteerAmerica Corporation, Uniontown, Ohio). The extruder was equipped with two weight loss feeders to control the feeding of the (co)polymer resins to the extruder barrel, and a gear pump to control the (co)polymer melt flow to a die. The extruder temperature was at about 210 °C and it delivered the melt stream to the BMF die, which itself was maintained at 210 °C. The gear pump was adjusted so that a 1.0 lb/hour/inch die width (0.18 kg/hour/cm die width) (co)polymer throughput rate was maintained at the die. The primary air temperature of the air knives adjacent to the die orifices was maintained at approximately 325 °C. This produced a web on a rotating collector spaced 8.2 cm from the die. The speed of the collector was 26.5 meters/minute. The web had a basis weight of approximately 9 gsm and a fiber diameter range of 5-25 micrometers.

Preparation of Fiber Web 2 (20 gsm):

Fiber Web 2 was made in the same manner as Fiber Web 1, except that the collector speed was 13.9 meters/minute. The web had a basis weight of approximately 20 gsm and a fiber diameter range of 5- 25 micrometers.

Preparation of Fiber Web 3 (80 gsm):

Fiber Web 3 was made in the same manner as Fiber Web 1 except that the collector speed was 3.5 meters/minute. The web had a basis weight of approximately 80 gsm and a fiber diameter range of 5-25 micrometers.

Preparation of antimicrobial composition for the antimicrobial layer:

An antimicrobial composition was prepared in a 100 g batch using the components reported in Table 1, below.

TABLE 1

All of the components, except the L-PYPK60 were added to a MAX 100 mixing cup (Flacktec Incorporated, Landrum, SC) and mixed at 3500 rpm (revolutions per minute) for 1 minute using a DAC 400 FVZ SPEEDMIXER instrument (Flacktec). The L-PVPK60 aqueous mixture was added to the cup and the contents were mixed for 1 minute at 3500 rpm.

The viscous composition was knife-coated onto a release liner using a gap of 254 micrometers. The coating was then dried at 80 °C for 10-15 minutes in a convection oven to produce a coating with a basis weight of 100 gsm. EXAMPLE 1

Sections of Fiber Web 1 were laminated to the outside of the antimicrobial layer using hand pressure. One section of the fiber web was laminated to one side of the antimicrobial layer first. Then the release liner was peeled off the antimicrobial layer and another section of fiber web 1 was laminated to the other side of the antimicrobial layer using hand pressure. The resulting construction was cut into 4 inch by 4 inch (10 cm by 10 cm) articles. A schematic of the final article is shown below in FIG. 1.

EXAMPLE 2

Example 2 was the same as Example 1, except that the outer non-woven layer was Fiber Web 2. EXAMPLE 3

Example 3 was the same as Example 1, except that the outer non-woven layer was Fiber Web 3.

Wound dressing materials prepared in Examples 1-3 were non-tacky, flexible, conformable, and dissolved quickly in room temperature water.