TREA

Antimicrobial compositions containing synergistic combinations of quaternary ammonium compounds and essential oils and/or constituents thereof

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Information

  • Patent Grant
  • 9421263
  • Patent Number
    9,421,263
  • Date Filed
    Monday, November 29, 2010
    13 years ago
  • Date Issued
    Tuesday, August 23, 2016
    7 years ago
Information
Abstract
The present invention relates to compositions comprising quaternary ammonium compounds and essential oils or individual constituents thereof which exhibit enhanced antimicrobial effects. Such combinations may be comprised in lotions, gels, creams, soaps, etc. for application to skin or mucous membranes. The invention is based, at least in part, on the observation that synergistic antimicrobial effects are achieved with combinations of essential oils or individual constituents thereof and low concentrations of quaternary ammonium compounds.
Description
2. INTRODUCTION

The present invention relates to compositions comprising combinations of quaternary ammonium compounds and essential oils and/or individual constituents thereof, and methods of using such compositions. It is based, at least in part, on the discovery that such combinations exhibit synergistically enhanced antimicrobial effects.


3. BACKGROUND OF THE INVENTION

Essential oils are volatile oils obtained from plant or animal sources and are composed of complex mixtures of several constituents, such as monoterpenes and sesquiterpene hydrocarbons, monoterpene and sesquiterpene alcohols, esters, ethers, aldehydes, ketones, oxides and the like. These essential oils and their isolated constituents are frequently utilized as fragrance and flavor agents, and have been widely used in folk medicine for wound healing properties.


Scientific research has corroborated the beneficial effects of essential oils. Essential oils of eucalyptus have been found to “possess central and peripheral analgesic effects as well as neutrophil-dependent and independent anti-inflammatory activities” (Silva et al., 2003, J. Ethnopharmacol. 89(2-3); 277-283), and similar activity has been observed in essential oils from Lavendula angustifolia Mill. (Hajhashemi et al., 2003, J. Ethnopharmacol. 89(1):67-71). Essential oils have been demonstrated to exhibit antibacterial (Bezic et al., 2003, Phytother. Res. 17(9):1037-1040; Goren et al., 2003, Z. Naturforsch. 58(9-10):687-690; de Abreu Gonzaga et al., 2003, Planta Med. 69(8):773-775; Valero and Salmera, 2003, Int. J. Food Microbiol. 85(1-2): 73-81) and antifungal (Paranagama et al., 2003, Lett. Appl. Microbiol. 37(1):86-90; Shin, 2003, Arch. Pharm. Res. 26(5):389-393; Velluti et al., 2003, Int. J. Food Microbiol. 89:145-154) activities. Virucidal activity of essential oils has also been observed, including direct virucidal effects against Herpes simplex viruses types 1 and 2 (Garcia et al., Phytother. Res. 17(9):1073-1075; Minami et al., 2003, Microbial Immunol. 47(a):681-684; Schuhmacher et al., 2003, Phytomedicine 10:504-510).


Quaternary ammonium compounds (“QAC”) are a group of ammonium salts in which organic radicals have been substituted for all four hydrogens of the original ammonium cation. They have a central nitrogen atom which is joined to four organic radicals and one acid radical. QACs have a tendency to distribute to the interface of two phases (liquid-liquid or solid-liquid) to introduce continuity between the two different phases. QACs are known to have potent antimicrobial activity, capable of disrupting bacterial cell processes. QACs have been used as antiseptics, disinfectants, preservatives, biocides, etc.


Johnson et al. (U.S. Pat. No. 6,319,958 and US20020165130) relates to the use of sesquiterpenoids to promote uptake of exogenous antimicrobial compounds. Similarly, a related article discloses the use of sesquiterpenoids, such as nerolidol, farnesol, bisabolol and apritone, in enhancing bacterial permeability and susceptibility to exogenous antimicrobial compounds, suggesting that sesquiterpenoids have a non-specific and general effect (Brehm-Stecher et al. 2003, Antimicrobial Agents and Chemotherapy, 47(10):3357-3360). In particular, Brehm-Stecher et al. report that nerolidol, farnesol, bisabolol and apritone enhanced the susceptibility of S. aureus to the antibiotics erythromycin, gentamicin, vancomycin, ciproflaxin, clindamycin, and tetracycline. In addition, Brehm-Stecher et al. does not disclose the use of QACs as antimicrobial agents.


There is a continuing desire for an antimicrobial composition that is non-irritating, safe, and effective for repeated use in various professional and non-professional settings.


4. SUMMARY OF THE INVENTION

The present invention relates to antimicrobial compositions comprising combinations of quaternary ammonium compounds and essential oils and/or individual constituents thereof. Such combinations may be comprised in lotions, gels, creams, soaps, etc. for application to skin or mucous membranes. The invention is based, at least in part, on the observation that synergistic antimicrobial effects are achieved with combinations of essential oils and/or individual constituents thereof and low concentrations of quaternary ammonium compounds.







5. DETAILED DESCRIPTION OF THE INVENTION

The present invention relates to compositions and methods for their use, wherein the antimicrobial activities of gels, creams, ointments, lotions or soaps is enhanced by the inclusion of synergistic amounts of quaternary ammonium compounds and essential oils and/or one or more individual constituent(s) thereof. The formulations of the instant invention comprise a synergistically effective amount of at least one quaternary ammonium compound and at least one essential oil and/or individual constituent(s) thereof.


The use of the terms, “synergistic” and “synergistically effective,” are used in the present invention to mean a biological effect created from the application of two or more agents to produce a biological effect that is greater than the sum of the biological effects produced by the application of the individual agents.


Examples of quaternary ammonium compounds suitable for use in the instant invention include, but are not limited to, benzalkonium chloride (“BZK”), benzethonium chloride (“BZT”), other benzalkonium or benzethonium halides, including, but not limited to, benzalkonium or benzethonium bromide or fluoride, cetyl pyridinium chloride, alkylamidopropalkonium chloride, behenalkonium chloride, behentrimonium methosulphate, behenamidopropylethyldimonium ethosulphate, stearalkonium chloride, olealkonium chloride, cetrimonium chloride, dequalinium chloride, N-myristyl-N-methyl-morpholinium methyl sulfate, poly[N-[3-(dimethylammonio)propyl]-N′-[3-(ethyleneoxyethelenedimethylammoinio)propyl]urea dichloride], alpha-4-[1-tris(2-hydroxyethyl)ammonium chloride-2-butenyl]-omega-tris(2-hydroxyethyl)ammonium chloride, poly[oxyethylene(dimethyliminio)ethylene(dimethyliminio)-ethylene dichloride].


The concentrations of quaternary ammonium compound may be between about 0.01 and 0.5 percent; preferably the quaternary ammonium compound is benzethonium chloride or benzalkonium chloride at a concentration between 0.05 and 0.3 percent, more preferably between 0.1 and 0.2 percent. These percentages, and other percentages herein, unless specified otherwise, are weight/weight.


Essential oils (“EOs”), as defined herein, are volatile oils obtained from plant or animal sources, or their synthetic equivalents, and are composed of complex mixtures of several constituents as monoterpenes and sesquiterpene hydrocarbons, monoterpene and sesquiterpene alcohols, esters, ethers, aldehydes, ketones, oxides and the like. Examples of EOs include, but are not limited to, bergamot oil, clary sage oil, ylang-ylang oil, neroli oil, sandalwood oil, frankincense oil, ginger oil, peppermint oil, lavender oil, jasmine absolute, geranium oil bourbon, spearmint oil, clove oil, patchouli oil, rosemary oil, rosewood oil, sandalwood oil, tea tree oil, vanilla oil, lemongrass oil, cedarwood oil, balsam oils, tangerine oil, Hinoki oil, Hiba oil, ginko oil, eucalyptus oil, lemon oil, orange oil, and sweet orange oil.


Individual constituents (“ICs”) of essential oils may be isolated from the oil (natural) or entirely or partially synthetic, and include, but are not limited to, 1-citronellol, α-amylcinnamaldehyde, lyral, geraniol, farnesol, hydroxycitronellal, isoeugenol, eugenol, eucalyptol, linalool, citral, thymol, limonene and menthol.


Further examples of ICs include sesquiterpenoid compounds, which may be the active compounds in the essential oils. Sesquiterpenoid compounds, containing 15 carbons, are formed biosynthetically from three 5-carbon isoprene units. Sesquiterpenoid compounds include, but are not limited to, farnesol, nerolidol, bisabolol, apritone, chamazulene, santalol, zingiberol, carotol, and caryophyllen.


Mixtures of one or more EO, one or more IC, and one or more EO as well as one or more IC, are encompassed by the present invention.


The concentrations of EOs and ICs may be between about 0.01 and 10 percent; preferably between 0.05 and 1.0 percent or between 0.05 and 0.5 percent, and more preferably between 0.2 and 0.5 percent. In preferred embodiments, the EO is lemon oil and/or the IC is farnesol.


In certain specific, non-limiting embodiments, the present invention provides for formulations, including but not limited to gels, creams, lotions or ointments further comprising an amount of zinc that inhibits irritation of the skin or mucosa to which the formulation is applied. Zinc may be added counteract the irritating effects of essential oils. The use of zinc in topical compositions is known in the art and disclosed in the following patents: U.S. Pat. Nos. 5,708,023, 5,965,610, 5,985,918 and 6,037,386.


In a preferred embodiment of the invention, low concentrations of two or more water-soluble salts of zinc are used. The term “low concentration” means percentages of free zinc ions (Zn2+) in the gel or cream at less than 0.5% on a weight to weight (w/w) basis. Suitable zinc salts for use in these compositions include zinc acetate (molar solubility in water of 1.64 moles/l), zinc butyrate (molar solubility in water of 0.4 moles/l), zinc citrate (molar solubility in water of <0.1 moles/l), zinc gluconate (molar solubility in water of 0.28 moles/l), zinc glycerate (moderately water soluble), zinc glycolate (moderately water soluble), zinc formate (molar solubility in water of 0.33 moles/l), zinc lactate (molar solubility in water of 0.17 moles/l), zinc picolinate (moderately water soluble), zinc proprionate (molar solubility in water of 1.51 moles/l), zinc salicylate (low water solubility), zinc tartrate (moderately water soluble) and zinc undecylenate (moderately water soluble). In particularly preferred embodiments, the zinc salts comprise a combination of effective amounts of two or more of the following: zinc acetate (0.05-2.0%), zinc citrate (0.05-2.0%), zinc gluconate (0.05-2.0%) and zinc lactate (0.05-2.0%). In preferred embodiments, the zinc salts are 0.2-0.6% zinc gluconate, 0.1-0.3% zinc acetate and 0.1-0.3% zinc lactate. In particularly preferred embodiments, the zinc salts are 0.3% zinc gluconate, 0.1% zinc acetate, and 0.1% zinc lactate, or 0.2% zinc zinc lactate and 0.2% zinc gluconate. Additional compositions that may comprise the synergistic combinations of the invention are described in International Patent Application No. PCT/US03/03896, published on Aug. 14, 2003, as WO03/066001, incorporated by reference herein in its entirety.


The gels, ointments, lotions or creams of the invention may be applied topically to the skin or to the various mucous membranes of the body, including but not limited to those of the oral, nasal, vaginal or rectal cavities.


In preferred embodiments, the gel, lotion, ointment or cream may comprise a mixture of water, a gelling agent, a thickening agent, a hydrophilic or hydrophobic polymer, an emulsifying agent, an emollient, and/or alcohol, such as ethanol. In preferred embodiments, the presently claimed compositions comprise alcohol present at 10-90% w/w, water present at 15-70% w/w, thickeners and/or gelling agents present at 0.05-3.0% w/w, and emollients present at 0.1-3.0% w/w.


In preferred embodiments, if a thickener is present, it is not a polyacrylic acid-based thickener, such as but not limited to, carbomer, carbopol, or ultrez, as polyacrylic acid-based thickeners have been found to be incompatible with quaternary ammonium compounds. Without being bound by any particular theory, it is believed that anionic groups of such thickeners may interact with cationic groups of the quaternary ammonium compound. Preferably, if a gelling agent is used, it is not an anionic agent, but rather a non-ionic or cationic agent.


The compositions of the invention may optionally further include one or more additional antimicrobial agent such as, but not limited to, antiviral, antibacterial, or antifungal substances. Antimicrobial agents also include substances possessing any combination of virucidal or virustatic, bacteriocidal or bacteriostatic, or fungicidal or fungistatic properties. Antimicrobial agents are well known to those of ordinary skill in the art. Examples of antimicrobial agents include, but are not limited to, iodophors, iodine, benzoic acid, dehydro acetic acid, propionic acid, sorbic acid, methyl paraben, ethyl paraben, propyl paraben, butyl paraben, cetrimide, chlorhexidine (free base and/or salts), other biguanides, such as polyhexamethyl biguanide (PHMB) and chlorohexidine gluconate (CHG), chloroeresol, chlorxylenol, benzyl alcohol, bronopol, chlorbutanol, ethanol, phenoxyethanol, phenylethyl alcohol, 2,4-dichlorobenzyl alcohol, thiomersal, clindamycin, erythromycin, benzoyl peroxide, mupirocin, bacitracin, polymyxin B, neomycin, triclosan, parachlorometaxylene, foscarnet, miconazole, fluconazole, itriconazole, ketoconazole, and pharmaceutically acceptable salts thereof. These and further examples of antimicrobial agents useful in this invention can be found in such references as Goodman and Gilman's The Pharmacological Basis of Therapeutics (Goodman Gilman A, Rall T W, Nies A S, Taylor P, ed. (Pergamon Press; Elmsford, N.Y.: 1990)), the contents of which are hereby incorporated by reference.


In an embodiment, the compositions of the invention comprises a biguanide compound selected from the group consisting of chlorohexidine gluconate (CHG) and polyhexamethyl biguanide (PHMB). Preferably, the biguande compound is present at a concentration of between 0.1 to 2.0% w/w.


Pharmaceutically acceptable chlorhexidine salts are well known to those of ordinary skill in the art and include, but are not limited to, chlorhexidine palmitate, chlorhexidine diphosphanilate, chlorhexidine digluconate (“CHG”), chlorhexidine diacetate, chlorhexidine dihydrochloride, chlorhexidine dichloride, chlorhexidine dihydroiodide, chlorhexidine diperchlorate, chlorhexidine dinitrate, chlorhexidine sulphate, chlorhexidine sulphite, chlorhexidine thiosulphate, chlorhexidine di-acid phosphate, chlorhexidine difluorophosphate, chlorhexidine diformate, chlorhexidine dipropionate, chlorhexidine di-iodobutyrate, chlorhexidine di-n-valerate, chlorhexidine dicaproate, chlorhexidine malonate, chlorhexidine succinate, chlorhexidine malate, chlorhexidine tartrate, chlorhexidine dimonoglycolate, chlorhexidine monodiglycolate, chlorhexidine dilactate, chlorhexidine di-α-hydroxyisobutyrate, chlorhexidine diglucoheptonate, chlorhexidine di-isothionate, chlorhexidine dibenzoate, chlorhexidine dicinnamate, chlorhexidine dimandelate, chlorhexidine di-isophthalate, chlorhexidine di-2-hydroxynapthoate, and chlorhexidine embonate.


In formulating compositions of this invention, it is contemplated that the formulations may further comprise ingredients which, while not having the activity of the above-named ingredients, will aid in the formulation and use of the composition as a whole. Examples of such ingredients are well-known to those of ordinary skill in the art of producing formulations for biological purposes. Examples of these ingredients include such substances as binders, emollients, preservatives (such as methyl paraben), lubricants, colorants, perfumes, and the like. Accordingly, when the surface contemplated is skin, the composition of this invention may contain ingredients which are added to known lotions or medicaments, which are physiologically acceptable to skin and which do not contain ingredients which will reverse or retard the action of the irritant-inactivating agent.


In certain non-limiting embodiments of the invention, the composition may be added to pre-existing formulations provided that the ingredients in those formulations do not prevent or retard the activity of the claimed composition. In a preferred embodiment, the claimed composition can be added to creams, ointments, gels or lotions which are commercially available. Examples of commercially available lubricants include, but are not limited to, those lubricants sold under the tradenames “KY JELLY,” “ASTROGLIDE,” and “PREVACARE.” Examples of commercially available lotions include, but are not limited to, those lotions sold under the tradenames “SOFT-SENSE,” “LOTION SOFT,” “CUREL,” and “KERI”. SOFT-SENSE (Johnson & Son, Inc., Racine, Wis.) is known to contain purified water, glycerin USP, distearyldimonium chloride, petrolatum USP, isopropyl palmitate, 1-hexadecanol, tocopheryl acetate (vitamin E USP), dimethicone, titanium dioxide USP, methyl paraben, propyl paraben, sodium chloride, and fragrance. LOTION SOFT (Calgon Vestal, St. Louise, Mo.) is a nonionic moisturizing lotion which is known to contain mucopolysaccharide. CUREL (Bausch & Lomb Incorporated, Rochester, N.Y.) is known to contain deionized water, glycerin, quatemium-5, petrolatum, isopropyl palmitate, 1-hexadecanol, dimethicone, sodium chloride, fragrance, methyl paraben, and propyl paraben.


The claimed compositions may be used in anti-perspirants, aftershave lotions, hydroalcoholic skin disinfectants, and therapeutic creams, etc.


Certain preferred embodiments of the invention comprise, for example but not by way of limitation, one or more of the following: alcohol (10-90% w/w), which could include one or more of ethanol, n-propanol and iso-propanol; one or more zinc compound in an anti-irritant amount; one or more polymeric quaternary ammonium salts of hydroxyethyl cellulose reacted with trimethyl ammonium substituted epoxide (Polyquaternium), such as U-care polymer such as Ucare JR125, JR 400, JR 30M, LR 400, LR30M, or Ucare polymer LK; hydroxypropyl methyl cellulose such as the Methocel A,E,K, and 40 series products as Methocell K4MS, Methocel K100, Methocell 40-202, Methocel K15MS and others; one or more quaternary ammonium compound such as BZK or BZT; cetyltrimethyl ammonium chloride (“CTAC”); cetyl trimethyl ammonium bromide (“CTAB”); olealkonium chloride; stearalkonium chloride; Incroquat BA 85 (babassuamidopropalkonium chloride); dibehenyldimonium methosulfate; Incroquat BES-35 S (Behenamidopropylethyldimonium Ethosulfate and stearyl alcohol); Incroquat B-65C (Behenalkonium chloride and cetyl alcohol); Incroquat Behenyl TMS (Behentrimonium methosulfate and cetearyl alcohol); and one or more emollient, such as Procetyl 10 PPG-10 cetyl ether, Procetyl 50 PPG-50 cetyl ether, Promyristyl PM-3 PPG-3Myristyl ether, PPG-3 benzyl ether myristate (Crodamol STS of Croda), PEG 20 Almond Glycerides, Probutyl DB-10, Glucam P20, Glucam E-10, Glucam P-10, Glucam E-20, Glucam P-20 distearate, glycerin, propylene glycol, cetyl acetate and acetylated lanolin alcohol (Acetulan), hydroxylated milk glycerides (Cremerol HMG); a silicone fluid such as Dow Corning Silicone Fluid 245, 244, 246, 344, 345, 556; an essential oil such as lemon oil, citronella oil, sandalwood oil, lemongrass oil, patchouli oil, clove oil, thyme oil, geranium oil, basil oil; an individual constituent of an essential oil, such as farnesol, citronellol, linalool, eugenol, citral, thymol, eucalyptol, menthol; and a biguanide such as chlorhexidine gluconate or polyhexamethyl biguanide.


The invention provides for methods of using the foregoing compositions to achieve an antimicrobial effect comprising applying an effective amount of the composition to the surface. An antimicrobial effect significantly diminishes the risk of infection or progression of existing infection by one or more pathogenic infectious agent. The risk of infection need not be reduced to zero, but preferably is reduced by at least 10, 20, 30, 40, 50, 60, 70, 80, or 90 percent. Examples of infectious agents against which protection may be afforded include, but are not limited to, Staphylococcus species such as Staphylococcus aureus and Staphylococcus epidermidis, Streptococcus species such as Streptococcus pneumoniae, Enterococcus species, Salmonella species such as Salmonella typh, Escherichia species such as Escherichia coli, Vibrio species, Neisseria species, such as Neisseria meningitidis and Neisseria gonnorhoea, Human Immunodeficiency Virus (HIV), Human Papilloma Virus (HPV), Herpes Simplex Virus (HSV), Chlamydia trachomatis, Trichomonas vaginalis, and Candida albicans.


In an embodiment of the invention, the compositions of the present invention do not contain antibiotics, including, but are not limited to, tetracycline, ampicillin, rifampin, vancomycin, amphotericin B, nystatin, and bacitracin.


The following are specific, non-limiting examples of formulations of the present invention with and without zinc salts.


Formulations without Zinc Salts


General Formula
















Ingredients
Percent Range (w/w %)









Ethanol
50-90



Water
15-35



U-care polymers
01.-0.5



Germall+
0.15-0.3 



Quaternary ammonium compounds
0.05-0.2 



Quaternary conditioners
0.2-1.0



Emollients
0.3-1.0



Phenoxyethanol (if present)
0.5-1.0



Silicone fluids
0.2-1.0



Essential oils/individual constituents
0.3-1.0



Biguanides (if present)
0.05-2.0 











Specific Formulas


(A) Alcohol Surgical Hand Prep-1
















Ingredients
Percent (w/w)



















Ethanol
68



Babassuamidopropalkonium Chloride
0.5



Water
28.12



U-care JR 30
0.2



Panthenol
1.0



BZT
0.18



Silicone fluid (DC245)
0.5



Procetyl 10 (PPG-10, cetyl ether)
0.5



Farnesol
0.5



Phenoxyethanol
0.5











(B) Alcohol Surgical Hand Prep-2
















Ingredients
Percent (w/w)



















Ethanol
68



Babassuamidopropalkonium Chloride
0.5



Water
27.97



U-care JR 30
0.2



Panthenol
1.0



BZT
0.18



Silicone fluid (DC245)
0.5



Procetyl 10 (PPG-10, cetyl ether)
0.5



Farnesol
0.5



Phenoxyethanol
0.5



PHMB
0.15











(C) Alcohol Surgical Hand Prep-3
















Ingredients
Percent (w/w)



















Ethanol
68



Babassuamidopropalkonium Chloride
0.5



Water
28.12



U-care JR 30
0.2



Panthenol
1.0



BZT
0.18



Silicone fluid (DC245)
0.5



Procetyl 10 (PPG-10, cetyl ether)
0.5



Farnesol
0.25



Geranium oil
0.25



Phenoxyethanol
0.5











(D) Pre-Op Skin Disinfectant-1
















Ingredients
Percent (w/w)



















Ethanol
60



Povidone iodine
7.5



Water
31.07



U-care JR 30
0.2



BZT
0.18



CHG
0.05



Farnesol
0.5



Phenoxyethanol
0.5











Formulations with Zinc Salts


General Formula
















Ingredients
Percent range (w/w)









Ethanol
50-90



Water
15-35



U-care polymers
01.-0.5



Germall+
0.15-0.3 



Quaternary ammonium compounds
0.05-0.2 



Quaternary conditioners
0.2-1.0



Emollients
0.3-2.0



Phenoxyethanol (if present)
0.5-1.0



Silicone fluids
0.0-1.0



Essential oils/individual ingredients
0.3-1.0



Biguanides (if present)
0.05-2.0 



Zinc gluconate
0.3-0.6



Zinc acetate
0.1-0.3



Zinc lactate
0.1-0.3











Specific Formulas


(E) Alcohol Hand Disinfectant-1
















Ingredients
Percent (w/w)



















Ethanol
60



Babassuamidopropalkonium Chloride
0.3



Water
36.23



U-care JR 30
0.2



Zinc acetate
0.2



Zinc gluconate
0.3



Zinc lactate
0.1



Panthenol
1.0



Chlorhexidine gluconate (CHG)
0.05



BZK
0.12



Silicone fluid (DC245)
0.5



Procety-10 (PPG-10 cetyl ether)
0.5



Farnesol
0.5











(F) Alcohol Hand Disinfectant-2
















Ingredients
Percent (w/w)



















Ethanol
60



Babassuamidopropalkonium Chloride
0.3



Water
36.08



U-care JR 30
0.2



Zinc acetate
0.2



Zinc gluconate
0.3



Zinc lactate
0.1



Panthenol
1.0



Chlorhexidine gluconate (CHG)
0.05



BZK
0.12



Silicone fluid (DC245)
0.5



Procety-10 (PPG-10 cetyl ether)
0.5



Farnesol
0.5



PHMB
0.15











(G) Alcohol Surgical Hand Prep-1
















Ingredients
Percent (w/w)



















Water
26.87



Zinc lactate
0.2



Zinc gluconate
0.2



Methocell K4MS
0.1



UcareJR 30
0.2



Panthenol 50W
1.0



Ethanol
68.0



CrodamolSTS
1.0



Babassuamidopropalkonium Chloride
0.3



Procetyl 10
0.5



PHMB
0.15



Farnesol
0.3



BZT
0.18



Propylene Glycol
1.0











(H) Alcohol Surgical Hand Prep-2
















Ingredients
Percent (w/w)



















Ethanol
68



Babassuamidopropalkonium Chloride
0.5



Water
27.32



U-care JR 30
0.2



Zinc acetate
0.2



Zinc gluconate
0.4



Zinc lactate
0.2



Panthenol
1.0



BZT
0.18



Silicone fluid (DC245)
0.5



Procety-10 (PPG-10 cetyl ether)
0.5



Farnesol
0.5



Phenoxyethanol
0.5











(I) Alcohol Surgical Hand Prep-3
















Ingredients
Percent (w/w)



















Ethanol
68



Babassuamidopropalkonium Chloride
0.5



Water
27.02



U-care JR 30
0.2



Zinc acetate
0.2



Zinc gluconate
0.4



Zinc lactate
0.2



Panthenol
1.0



BZT
0.18



Germall+
0.15



Silicone fluid (DC245)
0.5



Procety-10 (PPG-10 cetyl ether)
0.5



Farnesol
0.5



Phenoxyethanol
0.5



PHMB
0.15











(J) Alcohol Surgical Hand Prep-3
















Ingredients
Percent (w/w)



















Ethanol
68



Babassuamidopropalkonium Chloride
0.5



Water
27.27



U-care JR 30
0.2



Zinc acetate
0.2



Zinc gluconate
0.4



Zinc lactate
0.2



Panthenol
1.0



BZT
0.18



Silicone fluid (DC245)
0.5



Procety-10 (PPG-10 cetyl ether)
0.5



Farnesol
0.5



Phenoxyethanol
0.5



CHG
0.05











(K) Anti-Irritant Surgical Hand Prep-4
















Ingredients
Percentage (w/w)



















Water
27.15



Zinc lactate
0.2



Zinc gluconate
0.2



Methocell K4MS
0.1



U Care-JR 30M
0.2



D,L-Panthenol
0.5



Benzethonium chloride
0.18



Ethanol
68.0



Crodamol STS
1.0



Procetyl
0.5



Babassuamidopropalkonium Chloride
0.3



Propylene Glycol
1.0



Farnesol
0.5



Polyhexamethylene biguanide
0.15



Fragrance
0.02











(L) Anti-Irritant Surgical Hand Prep-5
















Ingredients
Percentage (w/w)



















Water
26.45



Zinc lactate
0.2



Zinc gluconate
0.2



Klucell MCS
0.8



U Care-JR 30M
0.2



D,L-Panthenol
0.5



Benzethonium chloride
0.18



Ethanol
68.0



Crodamol STS
1.0



Procetyl
0.5



Babassuamidopropalkonium Chloride
0.3



Propylene Glycol
1.0



Farnesol
0.5



Polyhexamethylene biguanide
0.15



Fragrance
0.02











(M) Alcohol Surgical Hand Prep Containing Zinc Gel


The following formulation is advantageously used by persons who wear latex gloves, but who have a latex allergy.
















Ingredients
Percent (w/w)



















Ethanol
68



Babassuamidopropalkonium Chloride
0.5



Water
22.93



U-care JR 30
0.6



Zinc acetate
0.2



Zinc gluconate
0.7



Zinc lactate
0.2



Zinc oxide
2.0



Panthenol
1.0



CHG
0.05



Incroquat TMS Behenyl
0.5



Silicone fluid (DC245)
0.5



Procety-10 (PPG-10 cetyl ether)
0.5



Glycerol
1.0



Farnesol
0.5



Germal Plus
0.2



Phenoxyethanol
0.5



Benzalkonium chloride
0.12











(N) Alcohol Based Anti-Irritant Surgical Prep
















Ingredients
Percent (w/w)



















Water
26.87



Zinc lactate
0.2



Zinc gluconate
0.2



Methocell K4MS
0.1



UcareJR 30
0.2



Panthenol 50W
1.0



Alcohol.SDA-40B
68.0



CrodamolSTS
1.0



Babassuamidopropalkonium Chloride
0.3



Procetyl 10
0.5



PHMB
0.15



Farnesol
0.3



BZT
0.18



Propylene Glycol
1.0











(O) Topical Cream-1
















Ingredients
Percent (w/w)



















Incroquat TMS Behenyl
0.8



Polawax NF
0.8



Petroleum Jelly
3.0



Crothix
1.0



Crodomol MM
1.0



Cremerol HMG
1.0



Propylene glycol
2.0



Glycerin
8.0



Water
78.22



UCare JR30-M
0.2



Germall Plus
0.2



BZT
0.18



Geranium oil
0.5



Zinc acetate
0.2



Zinc gluconate
0.7



Zinc lactate
0.2



Zinc oxide
2.0











(P) Topical Cream-2
















Ingredients
Percent (w/w)



















Incroquat TMS Behenyl
0.8



Polawax NF
0.8



Petroleum Jelly
3.0



Crothix
1.0



Crodomol MM
1.0



Cremerol HMG
1.0



Propylene glycol
2.0



Glycerin
8.0



Water
78.22



UCare JR30-M
0.2



Germall Plus
0.2



BZT
0.18



Basil Oil
0.5



Zinc acetate
0.2



Zinc gluconate
0.7



Zinc lactate
0.2



Zinc oxide
2.0











(Q) Topical Cream-3
















Ingredients
Percent (w/w)



















Incroquat TMS Behenyl
0.8



Polawax NF
0.8



Petroleum Jelly
3.0



Crothix
1.0



Crodomol MM
1.0



Cremerol HMG
1.0



Propylene glycol
2.0



Glycerin
8.0



Water
78.22



UCare JR30-M
0.2



Germall Plus
0.2



BZT
0.18



Sandalwood oil
0.25



Farnesol
0.25



Zinc acetate
0.2



Zinc gluconate
0.7



Zinc lactate
0.2



Zinc oxide
2.0











(R) Topical Cream-4
















Ingredients
Percent (w/w)



















Incroquat TMS Behenyl
0.8



Polawax NF
0.8



Petroleum Jelly
3.0



Crothix
1.0



Crodomol MM
1.0



Cremerol HMG
1.0



Propylene glycol
2.0



Glycerin
8.0



Water
78.22



UCare JR30-M
0.2



Germall Plus
0.2



BZT
0.18



Thyme oil
0.5



Zinc acetate
0.2



Zinc gluconate
0.7



Zinc lactate
0.2



Zinc oxide
2.0











(S) Pre-Op Skin Disinfectant-1
















Ingredients
Percent (w/w)



















Ethanol
60



Povidone iodine
7.5



Water
30.47



U-care JR 30
0.2



Zinc acetate
0.2



Zinc gluconate
0.3



Zinc lactate
0.1



BZT
0.18



CHG
0.05



Farnesol
0.5



Phenoxyethanol
0.5











(T) Pre-Op Skin Disinfectant-2
















Ingredients
Percent (w/w)



















Ethanol
60



Povidone iodine
2.0



Water
35.97



U-care JR 30
0.2



Zinc acetate
0.2



Zinc gluconate
0.3



Zinc lactate
0.1



BZT
0.18



CHG
0.05



Farnesol
0.5



Phenoxyethanol
0.5











(U) Pre-Op Skin Disinfectant-3
















Ingredients
Percent (w/w)



















Ethanol
60



Povidone iodine
2.0



Water
35.52



U-care JR 30
0.2



Zinc acetate
0.2



Zinc gluconate
0.3



Zinc lactate
0.1



BZT
0.18



CHG
0.5



Farnesol
0.5



Phenoxyethanol
0.5











(V) Pre-Op Skin Disinfectant-4
















Ingredients
Percent (w/w)



















Ethanol
60



Povidone iodine
2.0



Water
34.02



U-care JR 30
0.2



Zinc acetate
0.2



Zinc gluconate
0.3



Zinc lactate
0.1



BZT
0.18



CHG
2.0



Farnesol
0.5



Phenoxyethanol
0.5











(W) Zinc Gel Hand Wash #1
















Ingredient
Percent (w/w)



















UCare JR30-M
0.05



Methocel K100
0.1



Water
36.08



Zinc gluconate
0.3



Zinc acetate
0.1



Zinc lactate
0.1



Germall Plus
0.2



Ethanol
58



Ispropanol
2.0



Silicone (Dimethicone)
0.2



Incroquat Behentyl TMS
0.7



Polawax A31
0.3



Glycerin
1.0



Cetyl ether (PPG10)
0.5



CHG
0.05



BZK
0.02



Farnesol
0.3











(X) Zinc Gel Hand Wash #2
















Ingredient
Percent (w/w)



















Water
33.45



Ethanol
62.0



Farnesol
0.3



Propylene glycol
1.0



Polyhexamethylene biguanide
0.15



Babassuamidopropalkonium Chloride
0.3



Procetyl-10 (PPG-10 Cetyl ether
0.5



Crodamol STS
1.0



BZT
0.1



Zinc lactate
0.2



Zinc gluconate
0.2



D,L-Panthenol
0.5



UCare JR 30M
0.2



Methocel K4MS
0.1











(Y) Zinc Gel Cream/Lotion for Under Latex Gloves
















Ingredients
Percent (w/w)



















Ucare JR30-M
0.8



Methocel K100
0.3



Water
26.63



Zinc gluconate
0.6



Zinc acetate
0.2



Zinc lactate
0.2



Germall Plus
0.2



Zinc stearate
1.5



Zinc oxide
1.0



Glucate DO
5.0



Ethanol
55.0



Isopropanol
3.0



Silicone (Dimethicone)
0.5



Incroquat Behenyl TMS
1.0



Polawax A31
0.5



Glycerin
2.0



Cetyl ether (PPG10)
1.0



CHG
0.05



BZK
0.02



Farnesol
0.3



Vitamin E
0.2











(Z) Anti-Irritant Disinfectant Soap
















Ingredients
Percent (w/w)



















Polyox WSR 205
0.1



UCare Jr30-M
0.2



Germall Plus
0.2



Water
86.93



Pluronic F87
2.0



Cocoamidopropylbetaine
1.0



Mirapol A-15
1.0



Propylene glycol
2.0



Polyquaternium-47(Merquat 3330)
3.0



Glycerin
2.0



CHG
0.05



BZK
0.12



Triclosan
0.3



Farnesol
0.3



Lemon oil
0.3



Zinc acetate
0.1



Zinc lactate
0.1



Zinc gluconate
0.3










6. WORKING EXAMPLES
6.1. Example 1

Topical formulations containing zinc salts as anti-irritants were prepared in the presence and absence of EO and IC and in the presence and absence of antimicrobial compounds, such as benzalkonium chloride (BZK), chlorhexidine gluconate (CHG), zinc pyrithione (ZP) and triclosan (TC). The following EO and IC were evaluated: lemon oil as a representative essential oil, farnesol and linalool as representative terpene alcohols, and citral as a representative aldehyde. The resulting formulations then were evaluated for their antimicrobial activity.


6.1.1. Method


Preparation of Alcohol Based Zinc Gel


An alcohol based gel was prepared as follows, and the antimicrobials, EOs and/or ICs were added to this base:


Base #1
















Ingredient
% by weight



















UCare JR30-M
0.1



Methocel K100
0.1



Water
36.4



Zinc gluconate
0.3



Zinc acetate
0.1



Zinc lactate
0.1



Germall Plus
0.2



Ethanol
58



Isopropanol
2.0



Silicone (Dimethicone)
0.2



Incroquat Behenyl TMS
0.7



Polawax A31
0.3



Glycerin
1.0



Cetyl ether (PPG10)
0.5











Evaluation of Rapid Antimicrobial Activity in Presence of Serum.


To determine the efficacy of the antimicrobial composition on the skin, which may be contaminated with blood or other proteinaceous fluids containing bacteria, the antimicrobial activity was evaluated in the presence of serum as follows. Briefly, 0.5 ml of 108 CFU of S. aureus/ml was added to 0.5 ml of bovine adult serum in a sterile culture tube and mixed. 0.5 ml of the test formulation was added to each tube and vortexed. After 15 seconds, it was further diluted 1:100 with drug inactivating media (LTSB) and 0.5 ml was plated on a TSA plate. The plates were incubated at 37° C. for 24 hours and the colony count per ml of culture was determined.


6.1.2. Results


It was observed that farnesol, linanool, citral and lemon oil showed synergistic antimicrobial effects when combined with BZK. No such synergism was observed when farnesol was combined with other antimicrobial compounds, CHG, ZP or TC. See Table 1 below.









TABLE 1







Synergistic effect of EO and IC ingredients


with antimicrobial agents


Test organism: S. aureus











Group
CFU/mL
Log10 reduction







Control (Base)
3.4 × 107




BZK
5.4 × 105
1.8



CHG
6.6 × 105
1.7



TC
1.5 × 106
1.3



ZP
1.4 × 106
1.4



F
8.4 × 106
0.6



LI
1.5 × 106
1.3



CI
1.5 × 106
1.3



LO
1.6 × 106
1.3



BZK + F
3.0 × 102
5.0



BZK + CI
2.0 × 102
5.2



BZK + LI
6.0 × 102
4.7



BZK + LO
1.4 × 103
4.4



CHG + BZK + F
2.3 × 102
5.2



CHG + BZK + LO
1.4 × 103
4.4



CHG + BZK + LI
2.0 × 102
5.2



CHG + BZK + CI
1.0 × 102
5.5



CHG + BZK + LO + TC
1.4 × 103
4.4



CHG + BZK + F + TC
1.5 × 102
5.3



CHG + BZK + F + ZP + LO
2.0 × 102
5.2



CHG + LO
1.6 × 106
2.3



TC + LO
1.4 × 106
1.4



ZP + LO
1.4 × 106
1.4



CHG + F
6.8 × 104
2.7



TC + F
1.2 × 106
1.4



ZP + F
1.3 × 106
1.4







Key:



BZK: Benzalkonium chloride (0.12%);



PHMB: Polyhexamethylenebiguanide hydrochloride (0.15%);



CHG: Chlorhexidene gluconate (0.05%);



TC: Triclosan (0.3%);



ZP: Zinc pyrithione (0.5%);



F: Farnesol (0.3%);



LO: Lemon oil (0.3%);



LI: Linalool; (0.3%);



CI: Citral (0.3%)






It can be seen from Table 1 that, among the antimicrobial compounds used, only the quaternary ammonium compound, benzalkonium chloride, exhibited significant synergistic activity in combination with EOs and ICs.


6.2. Example 2

The present example shows the antimicrobial activity of compositions comprising a quaternary ammonium compound, benzethonium chloride (BZT) and farnesol in the presence and absence of zinc salts. The antimicrobial activity was evaluated as described in Example 1.


Farnesol and BZT were incorporated into Base #1 (containing zinc salts) and Base #2 (not containing zinc salts) shown below in proportions shown in Table 2.


Base #2 (Without Zinc Salts)
















Ingredient
% by weight



















UCare JR30-M
0.1



Methocel K100
0.1



Water
36.9



Germall Plus
0.2



Ethanol
58



Ispropanol
2.0



Silicone (Dimethicone)
0.2



Incroquat Behenyl TMS
0.7



Polawax A31
0.3



Glycerin
1.0



PPG-10 Cetyl ether (Procetyl-10)
0.5

















TABLE 2







Test organism: S. aureus










Without zinc salts
With zinc salts











Quantity in Gel

log10

log10


(% w/w)
cfu/ml
reduction
cfu/ml
reduction





Control Gel
4.1 × 107
0.0
1.4 × 107
0.0


BZT (0.18%)
7.5 × 105
1.7
3.3 × 105
1.6


Farnesol (0.5%)
8.9 × 105
1.7
4.5 × 105
1.5


BZT (0.18%) + Farnesol
2.0 × 102
5.4
6.7 × 101
5.3


(0.5%)









These results demonstrate the synergistic antimicrobial effects of BZT and farnesol, which occur both in the presence or absence of zinc salts.


6.3. Example 3

The antimicrobial effects of varying proportions of farnesol and quaternary ammonium compounds, incorporated into Base #2, were evaluated using the same method described in Example 1. The results are shown in Table 3.









TABLE 3







Test organism: S. aureus













log10



Groups in Gel Base (% w/w)
cfu/ml
reduction







Control Gel
1.4 × 107
0.0



BZT (0.18%) (preservative level)
3.3 × 105
1.6



BZT (0.12%)
4.7 × 105
1.5



BZT (0.06%)
5.7 × 105
1.4



BZK (0.12%) (preservative level)
5.4 × 105
1.4



BZK (0.06%)
1.8 × 106
0.9



Farnesol (0.5%)
4.5 × 105
1.5



Farnesol (0.3%)
4.6 × 105
1.5



BZT (0.18%) + Farnesol (0.5%)
6.7 × 101
5.3



BZT (0.18%) + Farnesol (0.3%)
6.7 × 101
5.3



BZT (0.12%) + Farnesol (0.3%)
1.0 × 102
5.1



BZT (0.06%) + Farnesol (0.3%)
1.0 × 102
5.1



BZK (0.12%) + Farnesol (0.5%)
2.0 × 102
4.8



BZK (0.12%) + Farnesol (0.3%)
3.7 × 103
3.6



BZK (0.06%) + Farnesol (0.3%)
7.9 × 103
3.2










These results demonstrate that both quaternary ammonium compounds, BZK and BZT, exhibit synergistic antimicrobial activity when used in combination with farnesol on S. aureus in a rapid serum-based assay.


6.4. Example 4

The antimicrobial effects of various EO and IC, in the presence or absence of quaternary ammonium compounds, BZK and BZT, incorporated into Base #2, were evaluated using the same assay described in Example 1. The amounts of various agents used are presented in Table 4. In addition to S. aureus, the rapid assay was also performed with E. coli. The results are shown in Table 4.












TABLE 4










S. aureus


E. coli














log10

log10


Group
cfu/ml
reduction
cfu/ml
reduction





Control (Base)
1.4 × 107
0.0
2.6 × 107
0.0


BZK
3.3 × 105
1.6
5.8 × 105
1.6


BZT
5.3 × 105
1.4
4.3 × 105
1.8


Farnesol
4.5 × 105
1.5
4.3 × 105
1.8


Patchouli oil
2.0 × 106
0.8
2.0 × 106
1.1


Basil oil
1.4 × 106
1.0
6.2 × 104
2.6



Eucalyptus oil
1.6 × 106
0.9
1.9 × 106
1.1


Thyme oil
1.3 × 106
1.0
4.9 × 105
1.7


Clove oil
1.6 × 106
0.9
1.4 × 105
2.3



Geranium oil
3.8 × 106
0.6
8.0 × 104
2.5


Orange oil
6.9 × 106
0.3
4.9 × 105
1.7


Mullein oil
6.1 × 105
1.4
6.2 × 105
1.6


Citronella oil
4.7 × 105
1.5
2.2 × 105
2.1


Sandalwood oil
7.4 × 105
1.3
4.9 × 105
1.7


Farnesol + BZK
2.0 × 102
4.8
3.4 × 104
2.9


Farnesol + BZT
5.3 × 102
4.4
6.8 × 104
2.6


Patchouli oil + BZT
6.7 × 101
5.3
1.1 × 104
3.4


Basil oil + BZT
3.3 × 101
5.6
6.7 × 101
5.6



Eucalyptus oil + BZT
3.3 × 101
5.6
4.2 × 103
3.8


Thyme oil + BZT
3.3 × 101
5.6
3.3 × 101
5.9


Clove oil + BZT
3.3 × 101
5.6
2.0 × 102
5.1



Geranium oil + BZT
3.3 × 101
5.6
3.3 × 101
5.9


Orange oil + BZT
3.3 × 103
3.6
3.5 × 104
2.9


Mullein oil + BZT
2.4 × 105
1.8
9.8 × 104
2.4


Citronella oil + BZT
6.7 × 102
5.3
2.8 × 103
4.0


Sandalwood oil + BZT
2.0 × 102
4.8
4.7 × 103
3.7





Key:


BZK: Benzalkonium chloride (0.12% w/w: preservative level);


BZT: Benzethonium chloride (0.18% w/w: preservative level); all other EO/IC (0.5% w/w).






These results demonstrate that various essential oils, when used in combination with quaternary ammonium compounds, exhibit rapid synergistic antimicrobial activity on S. aureus in a rapid serum-based assay. In particular, patchouli oil, basil oil, eucalyptus oil, thyme oil, clove oil, geranium oil, and citronella oil show pronounced antimicrobial effects.


6.5. Example 5

The effect of the addition of various biguanide antimicrobial compounds to combinations of farnesol and quaternary ammonium compound, incorporated into Base #2 was tested using the assay described in Example 1. The results are shown in Table 5.












TABLE 5










S. aureus


E. coli














log10

log10


Group
cfu/ml
reduction
cfu/ml
reduction





Gel base
1.4 × 107
0.0
2.6 × 107
0.0


CHG (0.05%)
6.6 × 105
1.3
4.8 × 105
1.7


BZT (0.18%)
5.3 × 105
1.4
4.3 × 105
1.8


PHMB (0.15%)
4.3 × 104
2.9
6.0 × 105
1.6


Farnesol (0.5%)
4.5 × 105
1.5
4.3 × 105
1.8


Farnesol (0.5%) + CHG
6.8 × 104
2.3
7.2 × 104
2.5


(0.05%)


Farnesol (0.5%) +
2.7 × 103
4.1
6.5 × 102
4.6


PHMB (0.15%)


Farnesol (0.5%) + BZT
5.3 × 102
4.4
6.8 × 104
2.6


(0.18%)


Farnesol (0.5%) + BZT
5.0 × 102
4.5
2.0 × 102
5.1


(0.18%) + CHG (0.05%)


Farnesol (0.5%) + BZT
3.0 × 102
5.0
1.0 × 102
5.4


(0.18%) + PHMB


(0.15%)









PHMB appears to enhance the activity of the combination of BZT and farnesol.


6.6. Example 6

This example demonstrates the antimicrobial activity of gels comprising farnesol in combination with various antimicrobial agents. The concentrations of the antimicrobial agents were selected in keeping with the permissible levels of these ingredients in leave-on skin care formulations. The antimicrobial activity was assayed using the method described in Example 1 using Gel Base #1. The data has been presented in Table 6.









TABLE 6







Test organism: S. aureus










Recommended




range as
log10 reduction in


Ingredients in the Gel
preservatives
colony count from


(% w/w)
(% w/w)
the controla,b





Farnesol (0.3%)

0.6


CHG (0.05%)
 0.0-0.05
1.7


PHMB (0.15%)
0.1-0.3
2.9


TC (0.3%)
0.3-0.5
1.3


BZT (0.18%)
0.1-0.2
1.6


BZK (0.12%)
 0.1-0.12
1.8


Farnesol (0.3%) + CHG (0.05%)

2.7


Farnesol (0.3%) + PHMB (0.15%)

3.4


Farnesol (0.3%) + TC (0.3%)

1.4


Farnesol (0.3%) + BZT (0.18%)

5.3


Farnesol (0.3%) + BZK (0.12%)

5.0






aThe colony count of the Control Base experiment was 3.4 × 107 cfu/ml.



bFor Control, the same Gel Base as used for the Gels shown in Table 6, but without any antimicrobial agents.






The results show that farnesol's ability to enhance the activity of the antimicrobial agents ranges from compound to compound. Farnesol shows synergy with the quaternary ammonium compounds, benzalkonium chloride (BZT) and benzethonium chloride (BZK). Among biguanide antimicrobial compounds, it enhances the activity of polyhexamethylene biguanide hydrochloride (PHMB), but not that of chlorhexidine gluconate (CHG). Farnesol also does not show any synergy with triclosan, nor does it enhance triclosan's action. Therefore, the ability of farnesol to show synergy or enhance the action of biocides/preservatives is specific to the antimicrobial agents in question.


A similar study was performed using the same concentration of farnesol above in Table 6 (0.3% w/w, i.e. 1.35 mM per 100 g gel) and the various antimicrobial agents were added to the gel in the same molar concentration (0.06 mM per 100 g of gel). The data has been presented in Table 7 below.









TABLE 7







Test organism: S. aureus











log10 reduction in



Ingredients in the Gel
colony count from



(gram millimoles per 100 g Gel)
the controla,b







Farnesol (1.35 mM)
1.8



CHG (0.06 mM)
1.9



PHMB (0.06 mM)
2.1



TC (1.04 mM)c
1.3



BZT (0.06 mM)
1.9



Farnesol (1.35 mM) + CHG (0.06 mM)
2.0



Farnesol (1.35 mM) + PHMB (0.06 mM)
3.2



Farnesol (1.35 mM) + TC (1.04 mM)c
1.4



Farnesol (1.35 mM) + BZT (0.06 mM)
5.5








aThe colony count of the Control Base experiment was 6.4 × 107 cfu/ml.




bFor Control, the same Gel Base as used for the Gels shown in Table 7 but without any preservatives/biocides was used.




cSince Triclosan is not effective even at 1.04 mM concentration, experiment was not performed with 0.06 mM concentration.






Similar to the results shown in Table 6, farnesol has a varying effect on enhancement of the antimicrobial activity of the various antimicrobial agents. Farnesol appears to exhibit synergistic antimicrobial activity in combination with BZT, but not with triclosan. PHMB appears to enhance the activity of farnesol. The mechanism of farnesol to show synergy or enhance the activity of the antimicrobial agents varies for different compounds, but is the same for the same compound, irrespective of the concentration (whether the compound is taken in % w/w or in molar proportions).


Various references, patents, publications, product descriptions, etc., are cited throughout this specification, the disclosures of which are incorporated herein by reference in their entireties for all purposes.

Claims
  • 1. An antimicrobial composition for topical use consisting essentially of: (a) benzalkonium chloride present at a concentration of between 0.01 and 0.5% w/w,(b) chlorhexidine gluconate present at a concentration of between 0.05 and 2.0% w/w, and(c) an individual constituent of an essential oil selected from the group consisting of lemon oil, orange oil, lemongrass oil, neroli oil, bergamot oil and combinations thereof, present at a concentration of between 0.05 and 1.0% w/w.
  • 2. An antimicrobial composition for topical use consisting essentially of: (a) benzalkonium chloride present at a concentration of between 0.01 and 0.5% w/w,(b) chlorhexidine gluconate present at a concentration of between 0.05 and 2.0% w/w,(c) an individual constituent of an essential oil selected from the group consisting of lemon oil, orange oil, lemongrass oil, neroli oil, bergamot oil and combinations thereof, present at a concentration of between 0.05 and 1.0% w/w, and(d) one or more zinc salts each present at a concentration of between 0.1% and 0.5% w/w.
  • 3. The composition of claim 2, wherein the one or more zinc salts are selected from the group consisting of zinc acetate, zinc citrate, zinc gluconate, zinc glycerate, zinc glycolate, zinc formate, zinc lactate, zinc picolinate, zinc proprionate, zinc salicylate, zinc tartrate, zinc undecylenate, zinc oxide, and zinc stearate.
  • 4. An antimicrobial composition for topical use consisting essentially of: (a) benzalkonium chloride present at a concentration of between 0.01 and 0.5% w/w,(b) chlorhexidine gluconate present at a concentration of between 0.05 and 2.0% w/w,(c) an individual constituent of an essential oil selected from the group consisting of lemon oil, orange oil, lemongrass oil, neroli oil, bergamot oil and combinations thereof, present at a concentration of between 0.05 and 1.0% w/w,(d) one or more zinc salts each present at a concentration of between 0.1% and 0.5% w/w, and(e) panthenol present at a concentration of between 0.5% and 2% w/w.
1. CROSS REFERENCE TO RELATED APPLICATIONS

This present application is a divisional application of U.S. patent application Ser. No. 10/891,624, filed Jul. 15, 2004, U.S. Pat. No. 7,871,649 which claims the benefit of U.S. Provisional Application Ser. Nos. 60/488,349 and 60/530,864, filed Jul. 17, 2003, and Dec. 18, 2003, respectively, each of which are incorporated herein by reference.

US Referenced Citations (138)
Number Name Date Kind
3257276 Broh-Khan et al. Jun 1966 A
3485915 Gerstien et al. Dec 1969 A
3960745 Billany et al. Jun 1976 A
4243657 Okumura et al. Jan 1981 A
4318907 Kligman et al. Mar 1982 A
4393076 Noda et al. Jul 1983 A
4478853 Chaussee et al. Oct 1984 A
4587266 Verdicchio May 1986 A
4604384 Smith et al. Aug 1986 A
4664909 Marschner May 1987 A
4670185 Fujiwara et al. Jun 1987 A
4814334 Salkin Mar 1989 A
4853978 Stockum Aug 1989 A
4868169 O'Laughlin et al. Sep 1989 A
4870108 Page Sep 1989 A
4889844 Silvetti, Sr. et al. Dec 1989 A
4910205 Kogan et al. Mar 1990 A
4919837 Gluck Apr 1990 A
4956170 Lee et al. Sep 1990 A
4963591 Fourman et al. Oct 1990 A
4966754 Purohit et al. Oct 1990 A
5031245 Milner Jul 1991 A
5059416 Cherukuri et al. Oct 1991 A
5073372 Turner et al. Dec 1991 A
5089205 Huang et al. Feb 1992 A
5110809 Wang et al. May 1992 A
5116602 Robinson et al. May 1992 A
5133090 Modak et al. Jul 1992 A
5147648 Bannert Sep 1992 A
5164107 Khan et al. Nov 1992 A
5208031 Kelly May 1993 A
5357636 Dresdner, Jr. et al. Oct 1994 A
5403864 Bruch et al. Apr 1995 A
5447930 Nayak Sep 1995 A
5516510 Beilfuss et al. May 1996 A
5591442 Diehl et al. Jan 1997 A
5599549 Wivell et al. Feb 1997 A
5612324 Lin et al. Mar 1997 A
5624675 Kelly Apr 1997 A
5624962 Takeuchi et al. Apr 1997 A
5648389 Gans et al. Jul 1997 A
5658575 Ribier et al. Aug 1997 A
5705532 Modak et al. Jan 1998 A
5708023 Modak et al. Jan 1998 A
5736574 Burnier et al. Apr 1998 A
5747021 McKenzie et al. May 1998 A
5750122 Evans et al. May 1998 A
5753270 Beauchamp et al. May 1998 A
5763412 Khan et al. Jun 1998 A
5776430 Osborne et al. Jul 1998 A
5804203 Hahn et al. Sep 1998 A
5827529 Ono et al. Oct 1998 A
5830488 Suzuki et al. Nov 1998 A
5866168 De Lacharriere et al. Feb 1999 A
5869071 Wieselman et al. Feb 1999 A
5885562 Lowry et al. Mar 1999 A
5888562 Hansen et al. Mar 1999 A
5902572 Luebbe et al. May 1999 A
5906808 Osborne et al. May 1999 A
5951993 Scholz et al. Sep 1999 A
5965137 Petrus Oct 1999 A
5965610 Modak et al. Oct 1999 A
5980477 Kelly Nov 1999 A
5980925 Jampani et al. Nov 1999 A
5985918 Modak et al. Nov 1999 A
5985931 Modak et al. Nov 1999 A
5989531 Schamper et al. Nov 1999 A
6022551 Jampani et al. Feb 2000 A
6037386 Modak et al. Mar 2000 A
6040347 Cupferman et al. Mar 2000 A
6045817 Ananthapadmanabhan et al. Apr 2000 A
6107261 Taylor et al. Aug 2000 A
6110908 Guthery Aug 2000 A
6136771 Taylor et al. Oct 2000 A
6183766 Sine et al. Feb 2001 B1
6187327 Stack Feb 2001 B1
6204230 Taylor et al. Mar 2001 B1
6211243 Johnson Apr 2001 B1
6248343 Jampani et al. Jun 2001 B1
6287577 Beerse Sep 2001 B1
6287583 Warren et al. Sep 2001 B1
6294186 Beerse et al. Sep 2001 B1
6319958 Johnson et al. Nov 2001 B1
6321750 Kelly Nov 2001 B1
6323171 Fonsny et al. Nov 2001 B1
6344218 Dodd Feb 2002 B1
6352701 Scholz et al. Mar 2002 B1
6376522 Holzl et al. Apr 2002 B1
6387357 Chopra et al. May 2002 B1
6403067 Schamper et al. Jun 2002 B1
6403071 Scavone et al. Jun 2002 B1
6414032 Johnson Jul 2002 B1
6420431 Johnson Jul 2002 B1
6426062 Chopra et al. Jul 2002 B1
6485716 Fei et al. Nov 2002 B1
6511657 Avendano et al. Jan 2003 B2
6582711 Asmus et al. Jun 2003 B1
6613312 Rizvi et al. Sep 2003 B2
6682749 Potechin et al. Jan 2004 B1
6723689 Hoang et al. Apr 2004 B1
6846846 Modak et al. Jan 2005 B2
7122211 Jensen et al. Oct 2006 B2
7435429 Modak et al. Oct 2008 B2
7563461 Modak et al. Jul 2009 B2
7745425 Modak et al. Jun 2010 B2
7759327 Modak et al. Jul 2010 B2
7871649 Modak et al. Jan 2011 B2
7879365 Modak et al. Feb 2011 B2
7951840 Modak et al. May 2011 B2
8207148 Modak et al. Jun 2012 B2
20020022009 De La Poterie et al. Feb 2002 A1
20020022660 Jampani et al. Feb 2002 A1
20020098159 Wei et al. Jul 2002 A1
20020165130 Johnson et al. Nov 2002 A1
20020187168 Jensen et al. Dec 2002 A1
20020187268 Owens et al. Dec 2002 A1
20030134780 Patt Jul 2003 A1
20030152644 Modak et al. Aug 2003 A1
20030157138 Eini et al. Aug 2003 A1
20030211066 Scholz Nov 2003 A1
20040102429 Modak et al. May 2004 A1
20040126604 Wang Jul 2004 A1
20040208908 Modak et al. Oct 2004 A1
20040219227 Modak et al. Nov 2004 A1
20040247685 Modak et al. Dec 2004 A1
20040253275 Eini et al. Dec 2004 A1
20050019431 Modak et al. Jan 2005 A1
20050048139 Modak et al. Mar 2005 A1
20050238602 Modak et al. Oct 2005 A1
20050281762 Modak et al. Dec 2005 A1
20060141017 King et al. Jun 2006 A1
20100249227 Modak et al. Sep 2010 A1
20100305211 Modak et al. Dec 2010 A1
20100317743 Macinga et al. Dec 2010 A1
20110070316 Modak et al. Mar 2011 A1
20110117140 Modak et al. May 2011 A1
20120101155 Modak et al. Apr 2012 A1
20120129950 Macinga et al. May 2012 A1
Foreign Referenced Citations (60)
Number Date Country
2006344431 Dec 2007 AU
4140474 Jun 1993 DE
4240674 Mar 1994 DE
19523320 Jan 1997 DE
0041448 Dec 1981 EP
0231080 Aug 1987 EP
304802 Mar 1989 EP
0308210 Mar 1989 EP
402078 Dec 1990 EP
0521455 Jan 1993 EP
0604848 Jul 1994 EP
0674896 Oct 1995 EP
0694310 Jan 1996 EP
0313302 Apr 1998 EP
1001012 May 2000 EP
2729050 Jul 1996 FR
1-151522 Jun 1989 JP
2003-120210 May 1991 JP
H09-510976 Nov 1997 JP
10328284 Dec 1998 JP
2002-521416 Jul 2002 JP
2002-527351 Aug 2002 JP
2003-515615 May 2003 JP
2003-246726 Sep 2003 JP
2166309 May 2001 RU
833240 May 1981 SU
WO8400111 Jan 1984 WO
WO8704350 Jul 1987 WO
WO8800795 Feb 1988 WO
WO8803799 Jun 1988 WO
WO8905645 Jun 1989 WO
WO9307903 Apr 1993 WO
WO9318745 Sep 1993 WO
WO9318852 Sep 1993 WO
WO9415461 Jul 1994 WO
WO9418939 Sep 1994 WO
WO9526134 Oct 1995 WO
WO9822081 May 1998 WO
WO9824426 Jun 1998 WO
WO9851275 Nov 1998 WO
WO9903463 Jan 1999 WO
WO9938505 Aug 1999 WO
WO9951192 Oct 1999 WO
WO9960852 Dec 1999 WO
WO9963816 Dec 1999 WO
WO0037042 Jun 2000 WO
WO 0047183 Aug 2000 WO
WO0141573 Jun 2001 WO
WO03003896 Jan 2003 WO
WO03034994 May 2003 WO
WO03057713 Jul 2003 WO
WO03066001 Aug 2003 WO
WO03070231 Aug 2003 WO
WO03083028 Oct 2003 WO
WO2004014416 Feb 2004 WO
WO2005009352 Feb 2005 WO
WO2006074359 Jul 2006 WO
WO2006099359 Sep 2006 WO
WO2007069214 Jun 2007 WO
WO2007142629 Dec 2007 WO
Non-Patent Literature Citations (225)
Entry
U.S. Appl. No. 10/785,207, Jan. 10, 2013 Notice of Allowance.
U.S. Appl. No. 13/343,452, Mar. 28, 2013 Non-Final Office Action.
U.S. Appl. No. 13/343,452, Feb. 28, 2013 Response to Restriction Requirement.
U.S. Appl. No. 12/972,036, Apr. 2, 2013 Non-Final Office Action.
U.S. Appl. No. 08/218,666, filed Mar 28, 1994 (Abandoned).
U.S. Appl. No. 10/786,681, filed Feb. 25, 2004 (Abandoned).
U.S. Appl. No. 08/871,071, Jun. 2, 1999 Issue Fee payment.
U.S. Appl. No. 08/871,071, Apr. 16, 1999 Notice of Allowance.
U.S. Appl. No. 08/871,071, Mar. 19, 1999 Response to Non-Final Office Action.
U.S. Appl. No. 08/871,071, Dec. 16, 1998 Non-Final Office Action.
U.S. Appl. No. 08/871,071, Nov. 9, 1998 Response to Non-Final Office Action.
U.S. Appl. No. 08/871,071, May 8, 1998 Non-Final Office Action.
U.S. Appl. No. 09/387,550, Jan. 18, 2000 Issue Fee payment.
U.S. Appl. No. 09/387,550, Nov. 9, 1999 Notice of Allowance.
U.S. Appl. No. 10/047,631, Sep. 13, 2004 Issue Fee Payment.
U.S. Appl. No. 10/047,631, Jul. 12, 2004 Notice of Allowance.
U.S. Appl. No. 10/047,631, Apr. 16, 2004 Response to Non-Final Office Action.
U.S. Appl. No. 10/047,631, Nov. 14, 2003 Non-Final Office Action.
U.S. Appl. No. 10/047,631, Aug. 27, 2003 Response to Restriction Requirement.
U.S. Appl. No. 10/047,631, Jul. 2, 2003 Restriction Requirement.
U.S. Appl. No. 08/218,666, Jun. 24, 1996 Notice of Abandonment.
U.S. Appl. No. 08/218,666, Dec. 18, 1995 Final Office Action.
U.S. Appl. No. 08/821,666, Sep. 7, 1995 Response to Non-Final Office Action.
U.S. Appl. No. 08/821,666, Mar. 3, 1995 Non-Final Office Action.
U.S. Appl. No. 08/821,666, Nov. 18, 1994 Response to Restriction Requirement.
U.S. Appl. No. 08/821,666, Oct. 17, 1994 Restriction Requirement.
U.S. Appl. No. 08/760,054, Sep. 7, 1999 Issue Fee payment.
U.S. Appl. No. 08/760,054, Jun. 21, 1999 Notice of Allowance.
U.S. Appl. No. 08/760,054, Mar. 17, 1999 Response to Non-Final Office Action.
U.S. Appl. No. 08/760,054, Nov. 24, 1998 Non-Final Office Action.
U.S. Appl. No. 08/760,054, Aug. 17, 1998 Continuing Prosecution Application (CPA).
U.S. Appl. No. 08/760,054, May 15, 1998 Advisory Action.
U.S. Appl. No. 08/760,054, Apr. 17, 1998 Notice of Appeal.
U.S. Appl. No. 08/760,054, Nov. 19, 1997 Final Office Action.
U.S. Appl. No. 08/760,054, Jul. 28, 1997 Response to Non-Final Office Action.
U.S. Appl. No. 08/760,054, Mar. 28, 1997 Non-Final Office Action.
U.S. Appl. No. 08/492,080, Sep. 29, 1997 Issue Fee payment.
U.S. Appl. No. 08/492,080, Aug. 6, 1997 Notice of Allowance.
U.S. Appl. No. 08/492,080, Aug. 5, 1997 Examiner Interview Summary.
U.S. Appl. No. 08/492,080, Jul. 9, 1997 Response to Final Office Action.
U.S. Appl. No. 08/492,080, Apr. 9, 1997 Final Office Action.
U.S. Appl. No. 08/492,080, Jan. 13, 1997 Response to Non-Final Office Action.
U.S. Appl. No. 08/492,080, Sep. 13, 1996 Non-Final Office Action.
U.S. Appl. No. 08/492,080, Jun. 28, 1995 Preliminary Amendment.
U.S. Appl. No. 10/622,272, Apr. 19, 2011 Issue Fee payment.
U.S. Appl. No. 10/622,272, Jan. 19, 2011 Notice of Allowance.
U.S. Appl. No. 10/622,272, Oct. 21, 2010 Response to Non-Final Office Action and Terminal Disclaimer Filed.
U.S. Appl. No. 10/622,272, Jul. 22, 2010 Non-Final Office Action.
U.S. Appl. No. 10/622,272, Apr. 21, 2010 Response to Non-Final Office Action.
U.S. Appl. No. 10/622,272, Dec. 21, 2009 Non-Final Office Action.
U.S. Appl. No. 10/622,272, Sep. 29, 2009 Amendment and Request for Continued Examination (RCE).
U.S. Appl. No. 10/622,272, Jul. 2, 2009 Final Office Action.
U.S. Appl. No. 10/622,272, Apr. 22, 2009 Response to Non-Final Office Action.
U.S. Appl. No. 10/622,272, Jan. 22, 2009 Non-Final Office Action.
U.S. Appl. No. 10/622,272, Nov. 21, 2008 Amendment and Request for Continued Examination (RCE).
U.S. Appl. No. 10/622,272, Jul. 24, 2008 Final Office Action.
U.S. Appl. No. 10/622,272, Apr. 28, 2008 Response to Non-Final Office Action.
U.S. Appl. No. 10/622,272, Jan. 30, 2008 Non-Final Office Action.
U.S. Appl. No. 10/622,272, Oct. 15, 2007 Response to Non-Final Office Action.
U.S. Appl. No. 10/622,272, Apr. 13, 2007 Non-Final Office Action.
U.S. Appl. No. 10/622,272, Feb. 2, 2007 Response to Restriction Requirement.
U.S. Appl. No. 10/622,272, Jan. 5, 2007 Restriction Requirement.
U.S. Appl. No. 10/892,034, Dec. 17, 2010 Issue Fee payment.
U.S. Appl. No. 10/892,034, Sep. 24, 2010 Notice of Allowance.
U.S. Appl. No. 10/892,034, Aug. 17, 2010 Response to Non-Final Office Action.
U.S. Appl. No. 10/892,034, May 17, 2010 Non-Final Office Action.
U.S. Appl. No. 10/892,034, Feb. 8, 2010 Amendment & Request for Continued Examination (RCE).
U.S. Appl. No. 10/892,034, Oct. 9, 2009 Final Office Action.
U.S. Appl. No. 10/892,034, Jul. 2, 2009 Response to Non-Final Office Action.
U.S. Appl. No. 10/892,034, Apr. 8, 2009 Non-Final Office Action.
U.S. Appl. No. 10/892,034, Jan. 27, 2009 Amendment and Request for Continued Examination (RCE).
U.S. Appl. No. 10/892,034, Aug. 27, 2008 Final Office Action.
U.S. Appl. No. 10/892,034, Jun. 17, 2008 Response to Non-Final Office Action.
U.S. Appl. No. 10/892,034, Jan. 29, 2008 Non-Final Office Action.
U.S. Appl. No. 10/892,034, Nov. 5, 2007 Response to Restriction Requirement.
U.S. Appl. No. 10/892,034, May 4, 2007 Restriction Requirement.
U.S. Appl. No. 11/446,347, Jun. 14, 2010 Issue Fee payment.
U.S. Appl. No. 11/466,347, May 18, 2010 Amendment after Notice of Allowance.
U.S. Appl. No. 11/466,347, Mar. 15, 2010 Notice of Allowance.
U.S. Appl. No. 11/466,347, Feb. 26, 2010 Response to Non-Final Office Action.
U.S. Appl. No. 11/466,347, Sep. 1, 2009 Non-Final Office Action.
U.S. Appl. No. 11/466,347, May 11, 2009 Preliminary Amendment.
U.S. Appl. No. 12/715,026, Oct. 27, 2011 Amendment and Request for Continued Examination (RCE).
U.S. Appl. No. 12/715,026, Jul. 27, 2011 Notice of Allowance.
U.S. Appl. No. 12/715,026, May 16, 2011 Response to Non-Final Office Action and Terminal Disclaimer Filed.
U.S. Appl. No. 12/715,026, Nov. 16, 2010 Non-Final Office Action.
U.S. Appl. No. 10/785,207, Aug. 6, 2010 Amendment and Request for Continued Examination (RCE).
U.S. Appl. No. 10/785,207, Aug. 5, 2010 Examiner Interview Summary.
U.S. Appl. No. 10/785,207, May 13, 2010 Final Office Action.
U.S. Appl. No. 10/785,207, Jan. 29, 2010 Supplemental response.
U.S. Appl. No. 10/785,207, Nov. 2, 2009 Response to Non-Final Office Action.
U.S. Appl. No. 10/785,207, Aug. 11, 2009 Non-Final Office Action.
U.S. Appl. No. 10/785,207, May 28, 2009 Amendment and Request for Continued Examination (RCE).
U.S. Appl. No. 10/785,207, Mar. 5, 2009 Final Office Action.
U.S. Appl. No. 10/785,207, Dec. 18, 2008 Response to Non-Final Office Action.
U.S. Appl. No. 10/785,207, Sep. 22, 2008 Non-Final Office Action.
U.S. Appl. No. 10/785,207, Aug. 13, 2008 Amendment and Request for Continued Examination (RCE).
U.S. Appl. No. 10/785,207, May 14, 2008 Final Office Action.
U.S. Appl. No. 10/785,207, Feb. 19, 2008 Response to Non-Final Office Action.
U.S. Appl. No. 10/785,207, Nov. 19, 2007 Non-Final Office Action.
U.S. Appl. No. 10/785,207, Nov. 2, 2007 Response to Restriction Requirement.
U.S. Appl. No. 10/785,207, Oct. 2, 2007 Restriction Requirement.
U.S. Appl. No. 10/786,681, Dec. 9, 2010 Notice of Abandonment.
U.S. Appl. No. 10/786,681, Mar. 30, 2010 Non-Final Office Action.
U.S. Appl. No. 10/786,681, Feb. 24, 2010 Amendment and Request for Continued Examination (RC E).
U.S. Appl. No. 10/786,681, Nov. 24, 2009 Final Office Action.
U.S. Appl. No. 10/786,681, Aug. 27, 2009 Response to Non-Final Office Action.
U.S. Appl. No. 10/786,681, May 27, 2009 Non-Final Office Action.
U.S. Appl. No. 10/786,681, Mar. 23, 2009 Amendment and Request for Continued Examination (RC E).
U.S. Appl. No. 10/786,681, Dec. 23, 2008 Final Office Action.
U.S. Appl. No. 10/786,681, Oct. 2, 2008 Response to Non-Final Office Action.
U.S. Appl. No. 10/786,681, Jul. 7, 2008 Non-Final Office Action.
U.S. Appl. No. 10/786,681, Apr. 18, 2008 Amendment and Request for Continued Examination (RC E).
U.S. Appl. No. 10/786,681, Apr. 16, 2008 Advisory Action.
U.S. Appl. No. 10/786,681, Feb. 21, 2008 Amendment and Continuing Prosecution Application (CPA).
U.S. Appl. No. 10/786,681, Nov. 21, 2007 Final Office Action.
U.S. Appl. No. 10/786,681, Sep. 6, 2007 Response to Non-Final Office Action.
U.S. Appl. No. 10/786,681, May 21, 2007 Non-Final Office Action.
U.S. Appl. No. 11/327,677, May 14, 2010 Issue Fee payment.
U.S. Appl. No. 11/327,677, Apr. 16, 2010 Amendment after Notice of Allowance and Terminal Disclaimer Filed.
U.S. Appl. No. 11/327,677, Feb. 23, 2010 Notice of Allowance.
U.S. Appl. No. 11/327,677, Jan. 27, 2010 Request for Continued Examination (RCE).
U.S. Appl. No. 11/327,677, Nov. 2, 2009 Notice of Allowance.
U.S. Appl. No. 11/327,677, Aug. 27, 2009 Response to Non-Final Office Action.
U.S. Appl. No. 11/327,677, Jun. 1, 2009 Non-Final Office Action.
U.S. Appl. No. 11/327,677, May 11, 2009 Preliminary Amendment.
U.S. Appl. No. 11/031,258, Mar. 5, 2008 Issue Fee payment.
U.S. Appl. No. 11/031,258, Dec. 6, 2007 Notice of Allowance.
U.S. Appl. No. 11/031,258, Aug. 22, 2007 Response to Non-Final Office Action and Terminal Disclaimer Filed.
U.S. Appl. No. 11/031,258, Jun. 6, 2007 Non-Final Office Action.
U.S. Appl. No. 11/143,012, Jun. 22, 2009 Issue Fee payment.
U.S. Appl. No. 11/143,012, Mar. 24, 2009 Notice of Allowance.
U.S. Appl. No. 11/143,012, Jan. 16, 2009 Response to Non-Final Office Action and Terminal Disclaimer Filed.
U.S. Appl. No. 11/143,012, Oct. 31, 2008 Non-Final Office Action.
U.S. Appl. No. 11/143,012, Oct. 31, 2007 Preliminary Amendment.
U.S. Appl. No. 10/891,624, Nov. 30, 2010 Issue Fee payment.
U.S. Appl. No. 10/891,624, Aug. 30, 2010 Notice of Allowance.
U.S. Appl. No. 10/891,624, Jul. 22, 2010 Supplemental Response to Non-Final Office Action.
U.S. Appl. No. 10/891,624, Jun. 4, 2010 Response to Non-Final Office Action.
U.S. Appl. No. 10/891,624, Mar. 5, 2010 Non-Final Office Action.
U.S. Appl. No. 10/891,624, Nov. 4, 2009 Response to Non-Final Office Action.
U.S. Appl. No. 10/891,624, Aug. 6, 2009 Non-Final Office Action.
U.S. Appl. No. 10/891,624, Apr. 23, 2009 Amendment and Request for Continued Examination (RCE).
U.S. Appl. No. 10/891,624, Jan. 26, 2009 Final Office Action.
U.S. Appl. No. 10/891,624, Oct. 22, 2008 Response to Non-Final Office Action.
U.S. Appl. No. 10/891,624, Jul. 24, 2008 Non-Final Office Action.
U.S. Appl. No. 10/891,624, Apr. 7, 2008 Amendment and Request for Continued Examination (RCE).
U.S. Appl. No. 10/891,624, Dec. 18, 2007 Final Office Action.
U.S. Appl. No. 10/891,624, Oct. 3, 2007 Response to Non-Final Office Action.
U.S. Appl. No. 10/891,624, Apr. 10, 2007 Non-Final Office Action.
U.S. Appl. No. 10/891,624, Jan. 29, 2007 Response to Restriction Requirement.
U.S. Appl. No. 10/891,624, Dec. 27, 2006 Restriction Requirement.
Modak et al., 2005, A topical cream containing a zinc gel (allergy guard) as a prophylactic against latex glove related contact dermatitis. Dermatitis. 16(1) 22-7.
de Abreu Gonzaga et al., Composition and antibacterial activity of the essential oils from Zanthoxylum rhoifolium. 2003, Planta Med. 69(8):773-775.
Bezic et al., 2003, Composition and antimicrobial activity of Achillea clavennae L. essential oil. Phytother. Res. 17(9):1037-1040.
Brehm-Stecher et al. 2003, Sensitization of Staphylococcus aureus and Escherichia coli to antibiotics by the sesquiterpenoids nerolidol, farnesol, bisabolol, and apritone. Antimicrobial Agents and Chemotherapy, 47(10):3357-3360.
Cimiotti et al., 2003, “Adverse reactions associated with an alcohol-based hand antiseptic among nurses in a neonatal intensive care unit.” Am. J. Infect. Control 31:43-48.
Garcia et al., 2003, Virucidal activity of essential oils from aromatic plants of San Luis, Argentina. Phytother. Res. 17(9):1073-1075.
Goren et al., 2003, Analysis of essential oil of Coridothymus capitatus (L.) and its antibacterial and antifungal activity. Z. Naturforsch. 58(9-10):687-690.
Hajhashemi et al., 2003, Anti-inflammatory and analgesic properties of the leaf extracts and essential oil of Lavandula angustifolia Mill. J. Ethnopharmacol. 89(1):67-71.
Minami et al., 2003, The inhibitory effect of essential oils on herpes simplex virus type-1 replication in vitro. Microbial Immunol. 47(a):681-684.
Paranagama et al., 2003, Fungicidal and anti-aflatoxigenic effects of the essential oil of Cymbopogon citratus (DC.) Stapf. (lemongrass) against Aspergillus flavus Link. isolated from stored rice. Lett. Appl. Microbiol. 37(1):86-90.
Schuhmacher et al., 2003, Virucidal effect of peppermint oil on the enveloped viruses herpes simplex virus type 1 and type 2 in vitro. Phytomedicine 10:504-510.
Shin, 2003, Anti-Aspergillus activities of plant essential oils and their combination effects with ketoconazole or amphotericin B. Arch. Pharm. Res. 26(5):389-393.
Silva et al., 2003, Analgesic and anti-inflammatory effects of essential oils of Eucalyptus. J. Ethnopharmacol. 89(2-3);277-283.
Valero and Salmera, 2003, Antibacterial activity of 11 essential oils against Bacillus cereus in tyndallized carrot broth. Int. J. Food Microbiol. 85(1-2): 73-81.
Velluti et al., 2003, Inhibitory effect of cinnamon, clove, lemongrass, oregano and palmarose essential oils on growth and fumonisin B1 production by Fusarium proliferation in maize grain. Int. J. Food Microbiol. 89:145-154.
Bleasel et al., 2002, “Allergic contact dermatitis following exposure to essential oils” Australian Journal of Dermatology 43:211-213.
Vilaplana et al., 2002, “Contact dermatitis from the essential oil of tangerine in fragrances” Contact Dermatitis 46:108.
Larsen et al., 2001 “Fragrance contact dermatitis: a worldwide multicenter investigation (Part II)” Contact Dermatitis 44:344-346.
Nair, 2001, “Final report on the safety assessment of Mentha piperita (Peppermint) oil, Mentha piperita (Peppermint) Leaf extract, Mentha piperita (Peppermint) leaf and Mentha piperita (Peppermint) water” International Journal of Toxicology 20 (Suppl 3):61-73.
Wohrl, 2001 “The significance of fragrance mix, balsam of Peru, colophony and propolis as screening tools in the detection of fragrance allergy” British Journal of Dermatology 145(2):268-273.
Sugiura., 2000, “Results of patch testing with lavender oils in Japan” Contact Dermatitis 43:157-160.
De Groot et al., 1997, “Adverse reactions to fragrances: a clinical review.” Contact Dermatitis 36:57-86.
Modak et al., A Topical Zinc Gluconate Gel Composition for the Prevention of latex/Starch Glove Related Allergic Reactions: Pilot Study in Volunteers. In: Programs and Abstracts of the 37th Interscience Conference on Antimicrobial Agents and Chemotherapy, Toronto: 1997; American Society for Microbiology Washington DC. Abstract J-52.
Goodman and Gilman's The Pharmacological Basis of Therapeutics (Goodman Gilman A, Rall TW, Nies AS, Taylor P, ed. (Pergamon Press; Elmsford, N.Y.: 1990).
Bush et al., 1986, “Pig skin as test substrate for evaluating topical antimicrobial activity” J Clin Microbiol 24:343-348.
Meyer et al., 1978, “The skin of domestic mammals as a model for the human skin, with special reference to domestic pig.” Curr. Problem Dematol 7:39-52.
Ebner et al. Am. J. Clin. Dermatol., vol. 3, No. 6, pp. 427-433.
Aiko Tanaka et al. “Effect of Various Types of Disinfectants on Skin Physiological Function.” J. Nursing Science. Toyama Medical and Pharmaceutical University, 1999, vol. 2 pp. 49-58 (Abstract).
3M Avagard Surgical and Healthcare Personnel Hand Antiseptic with Moisturizers news release, 3M Company, Jun. 11, 2001.
3M Avagard Surgical and Healthcare Personnel Hand Antiseptic with Moisturizers product description, 3M Company, 2001.
A-Z of exhibitors; at Central European Coatings show, PPC1. Polymers Paint colour Journal, Oct. 1, 2000; 4433(190): 42.
Beilfuss, “A multifunctional ingredient for deodorants”, SOFW journal, 1998, vol. 124, pp. 360, 362-364 and 366.
“Drug information for the Health Care Professional”, vol. 1A, USP-D1, 1989, ninth Edition, pp. 792-793, Banta Company, VIR.
Fitzgerald, K.A., et al., “Mechanism of action of chlorhexidine diacitate and phenoxyethanol singly and in combination against gram-negative bacteria”, 1992, 215 Microbio, 70:215-229.
“Fraicheur de Peau Fresh Sin Body Mist”, International Product Alert, May 5, 1997, 9(14).
Happi, Household & personal Products Industry: New ingerdients galore at SCC supplier's day, Chemical Business Newsbase, Aug. 1, 2000.
Heard, et al., “The Colloidal properties of chlorhexidine and its interaction with some macromolecules”, J. Pharm. Pharmac., 1968, 20: 505-512.
Lansdown, “Interspecies variations in response to topical application of selected zinc compounds”, Food Chem Toxicol., Jan. 1991, 29(1): 57-64.
Lawrence, et al., “Evauation of Phenoxeotol-chlorhexidine cream as a prophylactic antibacterial agent in burns”, the Lancet, May 8, 1992, pp. 1037-1040.
Manufacturing Chemist: Japan approve Schulke & Mayr;s Sensiva SC 50, Chemical Business Newsbase, Jul. 14, 2000.
Modak et al., “Rapid Inactivation of infections pathogess by chlorhexidine coated gloves”, Infection Control and Hospital epidemiology, 1992, 13: 463-471.
Molnycke Healthcare, “hibiclens antiseptic/antimicrobial skin cleanser”, Nov. 10, 2006.
“Parfums, Cosmetiques, Aromes: Japan approves sale of new cosmetics ingredient,” Chemical Business Newsbase, Jan. 16, 2001.
Physicians Desk Reference—39th Edition, 1985, p. 1858, Lotrisone.
Physicians Desk Reference—39th Edition, 1985, pp. 2037-2038, chlorhexidine.
Physicians Desk Reference—40th Edition, 1986, pp. 1781-1782, chlorhexidine.
Pfizer “Purell Instant Hand Sanitizer, Product Description” Nov. 10, 2006.
Prevacare: Antimicrobial Hand Gel product description, Johnson & Johnson, Advanced Wound care, 2001.
Prevacare: Total Solution Skin Care Spray product description, Johnson & Johnson, Advanced Wound Care, 2001.
Robinson, K. “Heat beating technology; deodorant market,” Soap Perfumery and Cosmetics, v. 69 No. 7 p. 34, Jul. 1996.
Rubbo et al., A review of sterilization and disinfection, year book medical publishers, Chicago, 1965, pp. 161-162.
“S & M in Japan—Schulke & Mayr's Sensiva SC 50 deodorant active ingredient received approval for use in the Japanese market,” SPC Asia No. 21, p. 35, May 2000.
Schmolka, I.R., “The synergistic effects of nonionic surfactants upon cationic germicidal agents”, J. soc. Cosmet. chem., 1973, 24: 577-592.
“Schwarzkopf cares”, European Cosmetic Makets, No. 5, vol. 13, May 1, 1996.
“Schwarzkopf: Moving into a new area,” European Cosmetic Markets, No. 9, Sep. 1, 1996.
“SPC, Soap Perfumery and Cosmetics: New for deodorants: Sensiva SC 50,” Chemical Business Newsbase, Aug. 12, 1999.
Sensiva® SC 50 now also approved in Japan, Norderstedt, Aug. 2000, product description from manufacturer website,archived news report from manufacturer website (www.schulke-mayr.com), Schülke & Mayr, manufacturer, printed Apr. 4, 2001.
“Vichy launches oil-free moisturiser” Chemist & Druggist p. 792, Jun. 8, 1996.
Woodruff, J. “Mixed feelings,” Soap Perfumery & Cosmetics, No. 9, vol. 73, p. 39, Sep. 1, 2000.
Lawless, Julia, “The illustrated encyclopedia of essential oils: the complete guide to the use of oils in aromatherapy and herbalism”, Element Books, 1995, USA, pp. 132, 162-164, 169, 223, 227 and 228.
Rosenthal, S.L., Effect of Medicaments on the Motility of the Oral Flora with Special Reference to the Treatment of Vincent's Infection. II. Journal of Dental Research. 1943, vol. 22, pp. 491-494.
Supplementary European Search Report for EP Application No. 06717623.
Supplementary European Search Report for EP Application No. 06772072, dated Jun. 6, 2011.
U.S. Appl. No. 13/343,452, filed Jan. 4, 2012.
U.S. Appl. No. 12/715,026, Feb. 23, 2012 Notice of Allowance.
U.S. Appl. No. 12/715,026, Feb. 6, 2012 Request for Continued Examination (RCE).
U.S. Appl. No. 10/785,207, Mar. 15, 2012 Non-Final Office Action.
U.S. Appl. No. 12/853,977, Mar. 12, 2012 Response to Non-Final Office Action.
U.S. Appl. No. 12/715,026, May 23, 2012 Issue Fee payment.
U.S. Appl. No. 13/532,345, filed Jun. 25, 2012.
U.S. Appl. No. 12/853,977, Jun. 22, 2012 Notice of Allowance.
U.S. Appl. No. 12/853,977, Nov. 10, 2011 Non-Final Office Action.
U.S. Appl. No. 12/715,026, Nov. 4, 2011 Notice of Allowance.
Related Publications (1)
Number Date Country
20110070316 A1 Mar 2011 US
Provisional Applications (2)
Number Date Country
60488349 Jul 2003 US
60530864 Dec 2003 US
Divisions (1)
Number Date Country
Parent 10891624 Jul 2004 US
Child 12955432 US