ANTIMICROBIAL TITANIUM DIOXIDE NANOPARTICLES FUNCTIONALIZED WITH CATIONIC SILVER IONS

Abstract

The present invention generally relates to Titanium dioxide derivatives of formula TiO2-[L]-Ag+, functionalized with silver cations by a bifunctional mercapto alkylsilane ligand. The present derivatives are useful e.g. as antimicrobic, antiseptic and/or antiviral agent, in particular in the form of pharmaceutical compositions for topical use.

Description

The present invention relates in general term to Titanium dioxide derivatives, functionalized with silver cations by a bifunctional mercapto alkylsilane ligand. The present derivatives are particularly useful e.g. as antimicrobic, antiseptic and/or antiviral agent.

BACKGROUND OF THE ART

The antibacterial activity of the silver Ag⁺ ions is well known in the art since a long time. To this extent, are also known pharmaceutical compositions or medicaments based on silver ions, e.g. silver sulfadiazine, used, for instance, to prevent infections in cases of severe burns, or, in general, as antibacterial agents. Prior studies (see, e.g., Carr, H. S., Wlodkowski, T. J., and Rosenkranz, H. S., 1973, “Antimicrobial agents and chemotherapy”, vol. 4, p. 585) have demonstrated that the antibacterial activity of Ag⁺ ions is directly proportional to their concentration.

On the other hand, it is also known that elemental silver and silver salts usually demonstrate substantially less effectiveness against microbes. In the past, silver salt solutions, such as silver nitrate, were used to bathe the wound. This kind of administration, often requires large amounts of substance, in order to achieve a remarkable antibacterial effect. Ag⁺ based formulations are applied in pharmaceutical preparations, specially for topical use. However, most of the formulations based on silver salts, e.g. silver sulphadiazine or silver nitrate, suffer of photochemical instability.

Colloidal silver nanoparticles have also been a focus of increasing interest, and are being heralded as an excellent candidate for therapeutic purposes. Also such colloidal preparations are, however, photochemically unstable, to such an extent that even a brief exposure to visible light can cause the photoreduction of Ag⁺ to Ag° with a consequent breakdown of the antimicrobial action. Association of silver cations to titanium or silicon dioxide nanoparticles, has previously been described as reported for instance in WO2007/122651. In this publication there is described the stabilization of silver cations on a metal oxide surface, by the use of a bifunctional ligand. The described ligands provided indeed a binding to the metal oxide preventing at the same time the photoreduction of the silver cations to atomic silver, with a percentage of bound silver ions of about 0.2% w/w. Such derivatives were prepared with synthetic routes that can take prolonged reaction times, and final products based on TiO₂ particles can be sometimes associated to a a peculiar smell.

It appears, therefore, that there is still the need to find antimicrobial TiO₂ derivatives, functionalized with a high content of silver ions and that can be rapidly and cheaply obtained, in a reliable and efficient way.

The Applicant has surprisingly found that when a specific mercapto alkyl silane ligand is used, it is possible to obtain a series of TiO₂ derivatives of formula (I), endowed with high antimicrobic, antiseptic and/or antiviral activity, thus overcoming the drawbacks of the state of art.

SUMMARY OF THE INVENTION

In a first aspect, the invention relates to a TiO₂ functionalized derivative of formula (I):

TiO₂-[L]-Ag⁺  (I)

wherein:

• -[L]- is a bivalent mercapto alkyl silane ligand of general formula: -[Si—R—S]-, wherein R is a bivalent C₁-C₄ linear or branched alkyl group, optionally substituted;
• TiO₂ represents a titanium dioxide particle linked to the silica atom of the ligand -[L]-;
• Ag⁺ represents silver ions linked to the sulphur atom of the bivalent ligand -[L]-.

In a further aspect, the invention also refers to a process for the preparation of the above identified derivatives of formula (I), by reaction of titanium dioxide with a trialklyoxy mercapto alkyl silane derivative of formula (II), in the presence of a silver salt (III):

wherein:

• R is as above defined;
• R′ is independently selected from C₁-C₄ monovalent linear or branched alkyl group, optionally substituted;
• Y— is an anionic counterion, preferably selected from: perchlorate (ClO₄⁻), acetate (CH₃COO⁻), and nitrate (NO₃⁻).

In another aspect, the invention refers to a derivative of general formula (I), for use as a medicament, in particular as antibacterial, antimycotic, antiviral and/or sporicidal agent.

In another aspect, the present invention also relates to a pharmaceutical composition comprising the above indicated derivatives of formula (I), in admixture with at least one physiologically acceptable excipient or carrier, and optionally, with another active ingredient. In particular, said composition can be in the form of a cream, a gel or a powder. This composition is suitable for the topical administration route, mainly intended for the use as antibacterial, antimycotic and antiviral agent.

In a final aspect, the invention also relates to a method for treatment of a mammal, including man, comprising the topical administration of an effective amount of a derivative of formula (I), or of a pharmaceutical composition thereof.

DESCRIPTION OF THE DRAWINGS

FIG. 1 is a Petri capsule showing the inhibition of microbial colonies surrounding of the preferred derivative of the invention of formula TiO₂-MPS-Ag⁺, wherein:

A) TiO₂-MPS-Ag⁺ powder with a 0.58% Ag⁺ content.B) TiO₂-MPS-Ag⁺ powder with 2.30% Ag⁺ content.

FIG. 1C is a Petri capsule showing the control TiO₂ powder.

DETAILED DESCRIPTION

The term “bivalent C₁-C₄ linear or branched alkyl group” means a linear or branched alkyl moiety having 1 to 4 carbon atoms, optionally substituted, which is linked to both the end sides to the rest of the molecule. Example of said bivalent group are: methylene (—CH₂—), ethylene (—CH₂CH₂—), propylene (—CH₂CH₂CH₂—) and the like. Likewise, “monovalent C₁-C₄ linear or branched alkyl group”, means a linear or branched alkyl moiety having 1 to 4 carbon atoms, optionally substituted, bonded to the rest of the molecule by one side, such as for examples: methyl (—CH₃), ethyl (—CH₂CH₃), propyl (—CH₂CH₂CH₃) and the like.

As above indicated, the invention deals with titanium dioxide particles, functionalized by silver ion, through a divalent mercapto alkyl silane ligand. The present derivatives are, in fact, characterized by having such a divalent ligand -[L]- of general formula: -[Si—R—S]-, which is able to connect the titanium dioxide particles (TiO₂) to silver ions (Ag⁺), thus forming the derivatives (I) of the invention. The chemical structure of the ligand, in fact, allows the binding to the titanium oxide on one side (via the Si atom), as well as the coordination with the silver ions on the other side, via the sulfur atom of the mercapto (—SH) group. In particular, the silica atom is linked to the titanium atom of the TiO₂ particle via bridging oxygen atoms; whereas the sulphur atom of the —SH moiety is connected to Ag⁺ ions, typically by means of coordination bonds.

By that, the TiO₂ particles can be functionalized with a high amount of silver ions, as below described in detail, in a stable and reliable way, thus forming the present derivatives of formula (I), endowed with the desired pharmaceutical action.

Preferably, in the derivatives (I), the R group is a methylene or, more preferably, a propylene residue, whereby the ligand -[L]- thus has the preferred formulae: —Si—CH₂—S— or —Si—CH₂CH₂CH₃—S—, being this latter even more preferred.

It follows that a preferred derivative of the invention is the compound (I) of formula: Ti—Si—CH₂CH₂CH₃—S—Ag⁺, herein also indicated as TiO₂-MPS-Ag⁺.

As far as the anionic titanium dioxide particles are concerned, it is to be noted that TiO₂ may exist in different allotropic forms: anastase, rutile and brookite, all of them commercially available, and suitable for the present invention. The oxide surface is nevertheless characterised by the presence of Ti—OH groups which may suitably react with the selected trialklyoxy mercapto alkyl silane derivative, thus linking the Si atom via bridging oxygen, and giving the derivatives of the invention.

In a preferred form, the derivatives (I) have a TiO₂ particle size comprised from 100 nm to 600 nm, more preferably comprised from 300 to 500 nm.

Advantageously, the derivatives of the invention are also characterized by having a high percentage of Ag⁺ ions, even up to 3% w/w, more preferably comprised from 0.5 to 3% w/w, wherein the % w/w represents the amount of Ag⁺ over the total weight. In fact, Applicant has found that by varying the amount of silver salt and mercapto trimethoxyalkilsilane derivatives of choice, it is possible to obtain the derivative (I) with the desired amount of silver ions. This means that the present derivatives can be readily used as antimicrobic, antiseptic and/or antiviral agent, even at a low dosage, nevertheless exhibiting a remarkable pharmaceutical action.

In fact, the derivatives (I) present a high surface coverage of the ligand -[L]- on the metal oxide surface, which allows to increase the amount of bounded silver ions, up to 1% w/w and even more. Even further, due to the fast binding reaction of the mercapto alkyl silane ligand -[L]- to the titanium oxide surface, it is possible to prepare the derivatives of the invention in low reaction times, such as in a 20-30 minutes range, as herein below described in detail. It follows that the present invention also addresses the problem of how to find an effective antibacterial agent having a high content of silver ions, which can be prepared in a reliable, cheap and quick way. In this direction, it is worth noting that the Applicant has conducted similar experiments also considering SiO₂ particles, in place of the TiO₂ of the invention. The results showed that, under the same experimental conditions, the use of the silica dioxide did not allow the preparation of the corresponding silver functionalized silica derivatives, of hypothetical formula SiO₂-[L]-Ag⁺. In fact, whilst the functionalized TiO₂ the derivatives (I) of the invention can be obtained in a very short frame of time, also endowed with a high antimicrobial activity (as shown in the experimental part), the use of SiO₂ in lieu of the TiO₂, on the contrary, did not result in any substantial formation of the corresponding silica derivatives. Even further, Applicant has found that the use of SiO₂ led to the formation of an undefined precipitate, only after more than 30 hours. Most importantly, said undefined precipitate did not show any remarkable antimicrobial activity.

Conveniently, the derivatives (I) can be prepared e.g. by purchasing the components (titanium dioxide, the selected ligand and the silver salt), and by following the synthetic process as below reported and described in detail.

In this sense, and according to a further aspect, the invention deals with a process for the preparation of the present derivatives of formula (I), by reaction of titanium dioxide with a trialklyoxy mercapto alkyl silane derivative of formula (II), in the presence of a silver salt (III), as generally illustrated in the following reaction scheme:

wherein:

• R is as above defined;
• R′ is independently selected from C₁-C₄ monovalent linear or branched alkyl group, optionally substituted;
• Y⁻ is an anionic counterion, preferably selected from: perchlorate (ClO₄⁻), Acetate (CH₃COO⁻), and nitrate (NO₃⁻).

The process can be expediently carried out at room temperature (e.g. comprised from about 15° C. to about 40° C.), preferably in a polar organic solvent, even more preferably, in acetone. The reaction can be monitored using technique and procedures known in synthetic chemistry such as atomic spectroscopy and the like.

The silver salt is generally selected among those salts that are soluble in polar organic solvents. According to an embodiment of the invention, the silver salt (III) is preferably selected from: silver perchloride (AgClO₄, CAS No. 7783-93-9) and silver nitrate (AgNO₃, CAS No. 7761-88-8).

As far as the trialklyoxy mercapto alkyl silane derivative of formula (II) is concerned, this is preferably a derivative of formula (II) wherein R is selected from: methylene (—CH₂—) and propylene (—CH₂CH₂CH₂—).

Especially preferred is the compound of formula (II) wherein R is a propylene (—CH₂CH₂CH₂—) residue and R′ is methyl (—CH₃), i.e. the 3-mercaptopropyltrimethoxysilane compound of formula:

Equally preferred are compounds of formula (II) selected from: mercaptomethylmethyldietoxysilane, 3-mercaptopropylmethyldimethoxysilane and 3-mercaptopropyltriethoxysilane.

Practically, the present process for the preparation of the antimicrobial derivatives of formula (I), can be carried out by suspending the TiO₂ in the selected polar solvent, preferably acetone, and then adding thereto the selected trialklyoxy mercapto alkyl silane derivative (II), followed by the addition of the proper silver salt (III). Alternatively, the process of the invention can be carried out by adding to a TiO₂ suspension the ligand-silver [L-Ag⁺] adduct, being preformed by reacting the ligand precursor (II) and the silver salt (III) dissolved in a lower alcohol (intended as an alcohol having from 1 to 4 carbon atoms), preferably methanol.

As denoted in the herein below experimental part (see e.g. Examples 1 and 2), both the above indicated synthetic routes allow the preparation of the present derivatives (I) in high yields, and with a quick and cheap methodology, thus enabling the realization of the present process even on industrial scale.

As heretofore reported, the present derivatives (I) can be used as medicament, preferably as antiviral, antimycotic or, even more preferably, as antibacterial agent. The present derivatives are preferably for the use in the treatment of: cutaneous irritations, inflammations, abrasions, excoriations and/or burns. In a still preferred embodiment, the derivatives of the invention are used in the treatment of diseases selected from: acne, herpes, bed sores, and skin ulcers, preferably decubitus ulcers. In this respect, in fact, when the derivative are used as medical device, they can be applied to the interested site to form an efficacious film or a barrier, against external microbes, substantially avoiding any infection on the affected skin.

The derivatives are also suitable for the use as a skin cicatrizating agent.

When the derivatives (I) are employed as antibacterial agent, it can be preferably used for the treatment of diseases due to at least one of the microbes selected from: HSV-1 (Herpes Simplex Virus-1), Adenovirus, Poliovirus, Pseudomonas aeruginosa, Enterococcus faecalis, Escherica coli, Salmonella enteridis D1, Listeria monocytogenes, Staphylococcus aureus MR, Staphylococcus aureus MS, Streptococcus pyogenes, Streptococcus salivarius, Streptococcus mitis, Candida albicans, Aspergillus niger.

In the Example 4 of the present experimental part, some preliminary tests have been carried out by the Applicant against a series of microbic species, by using the preferred TiO₂-MPS-Ag⁺ derivative. The results clearly confirm the antibacterial activity of the derivatives of the invention, as also illustrated in FIG. 1a and FIG. 1b. From the considered Figures it is apparent not only the potential antimicrobic activity of the derivatives of the invention, but also the increasing of the activity depending to the amount of silver cations. The grey shadow zone around the deposed material, in fact, is broader in FIG. 1b, where derivative (I) with a higher content of Ag+ has been tested. By comparison, FIG. 1C shows that when the TiO₂ powder is used, no activity has been detected.

In another aspect, the present invention also relates to a pharmaceutical composition comprising the above indicated derivatives of formula (I), in admixture with at least one physiologically acceptable excipient or carrier, and optionally, with at least one active ingredient.

Preferably said at least one active ingredient is one or more antibacterial agent, even more preferably selected from:

Chemical formula Chemical name
                 Chlorexidine cation
                 Chlorexidine digluconate
                 Chlorexidine acetate
                 Polyexamethylene Biguanide hydrochloride Cation (CAS No. 32289-58-0)
Where n = 1 to 40 and average molecular weight corresponds to n = 10-13
                 Didecyl Dimethyl- ammonium Cation

The physiologically acceptable carriers and/or excipient of the present pharmaceutical compositions, can be selected among those commonly used in the art. As general examples, when the composition is in the form of a cream, said excipients can be suitably selected from: vaseline, liquid paraffin, stearyl alcohol, polyethylene glycol stearate and the like. Similarly, if the composition is in the form of a gel, the derivatives of the invention can be admixed with, e.g., glycerine, amidopropylene glycol, magnesium or aluminium silicate and the like.

It follows that the present derivatives can also be added to known active ingredient, e.g. which have been reported to promote wound healing by increasing collagen content and granulation tissue, such as famotidine or nizadine (for a general reference see e.g. K. S. Rao et al. Indian J. Med. Res. 125, Feb. 2007, 149-154).

Owing also to this peculiarity of the present derivatives of formula (I), it is possible to obtain topical-treatment products having antiviral, antibacterial, and antimycotic properties, together with other curative properties, basically depending on the pharmaceutical profile of the drug or composition they are added to.

Therefore, according to a further aspect, the anionic derivatives (I), are also useful as additives for pharmaceutical compositions, thus allowing for instance the preparation of very efficacious topical-treatment products, having multiple or enhanced pharmaceutical properties. Moreover, in the preparation of a pharmaceutical composition of the invention, it is not required any particular precautions when compared to the commonly used processes for preparing topical-treatment products. Hence, by providing the adding phase for adding the present derivatives of formula (I), known processes for producing topical-treatment products may be used to prepare topical-treatment products having antibacterial, antimycotic, virucidal and/or sporicidal properties, comprising the present derivatives (I).

The present compositions for use as medicament are preferably for the use as topical-treatment product, even more preferably in the form of cream, powder, spray gel, gel or foam. Still more preferably, the compositions of the invention can be used for treating: acne, herpes simplex, wounds, decubitus ulcers, cutaneous irritations, inflammations, abrasions, excoriations and/or burns.

Finally, the present invention also refers to a method for treatment of a mammal, including man, comprising the topical administration of an effective amount of a derivative of the above indicated formula (I), or a pharmaceutical composition thereof.

As above described in details, the present invention provides titanium particles where silver ions are covalently bound to the particles surface, via bridging oxygen atoms, through the coupling ligand -[L]- which is also able to coordinate high amount of silver ions Ag⁺. The obtained derivatives can be prepared by means of a simple, quick and cheap synthetic process, also applicable on industrial scale.

Of note, the present derivatives (I) can be used as antimicrobic, antiseptic and/or antiviral agent, in particular in the form of pharmaceutical compositions, such as powders, creams, gels, or foam. Said compositions can also be pharmaceutical formulations where the active specie can act as a barrier being, therefore, very useful for the realization of Medical Devices for topical use, whereby the release of the active silver ions to the tissue should be retained or somehow controlled.

The present invention will now be described by way of examples, which are intended to better illustrate the invention, without limiting its scope.

EXPERIMENTAL PART

Example 1

Preparation of TiO₂-Mps-Ag (Procedure A)

A 100 g amount of TiO₂ (Degussa P25) was suspended under stirring in Acetone (900 ml), followed by addition of 1.06 g of 3-mercaptopropyltrimethoxysilane at room temperature. After 10 minutes AgClO₄ (1.14 g) dissolved in Acetone (100 ml) were added and the stirring continued for about 10 minutes. A precipitate occurs, and the solid product thus obtained was filtered off, and dried at 50° C. Elemental analysis, by atomic spectroscopy, confirmed the quantitative formation of the TiO₂-MPS-Ag⁺ derivative, having an Ag⁺ content of about 0.55%.

Higher concentration of Silver ions can be bound to the metal oxide surface following the same procedure, increasing the amount of 3-mercaptopropyltrimethoxysilane and AgClO₄ which were used in stoichiometric amount.

Example 2

Preparation of TiO₂-Mps-Ag (Procedure B)

AgNO₃ (0.93 g) was dissolved in methanol and 3-mercaptopropyltrimethoxysilane (1.06 g) was added under stirring, to instantaneously form the 3-mercaptopropyltrimethoxysilane-Ag adduct. The solution containing the adduct was added to a suspension of TiO₂ (100 g, Degussa P25) in acetone (900 ml). Stirring was maintained for about 20 minutes, and the solid thus formed was filtered off and dried at 50° C.

Elemental analysis of Silver, by atomic spectroscopy, confirmed the quantitative formation of TiO₂-MPS-Ag+ derivative, with an Ag+ content of about 0.58%.

By varying the amount of silver salt and mercapto trimethoxyalkilsilane derivatives, by both procedures A and B it was possible to obtain TiO₂ powders containing up to a 3% of Silver ions stabilized on the surface by the MPS ligand.

Comparative Example 3

The same procedures of Example 1 and 2 were carried out using the same molar amount of SiO₂ in place of TiO₂. Under the same experimental conditions (e.g. time, temperature, molar ratio of the reagents) of Example 1 and 2 the procedure with SiO₂ did not lead to the formation of the precipitate comprising the corresponding functionalized derivative.

Example 4

Antibacterial Activity of the TiO₂-Mps-Ag Powder

The antibacterial activity of the powder TiO₂-MPS-Ag powder prepared according to Example 1 or 2, was tested against the following microbic species, purchased from Diagnostic International Distribution SpA:

Pseudomonas aeruginosa ATCC 15442
Staphylococcus aureus  ATCC 6538
Escherichia coli       ATCC 10536
Enterococcus hirae     ATCC 10541
Candida albicans       ATCC 10231

A mixture of the different microorganism with concentrations in the range 1.5×107-5.5×107 for each species was prepared.

100 μl of the mixture was seeded in Petri capsule containing Tryptone Soya Agar.

Samples of TiO₂-MPS-Ag powders having respectively 0.58% and 2.30% Ag⁺ content prepared according to example 1 and 2, and control powders without silver cations, were put inside the Petri capsule which were then incubated at 37° C. for 24 h.

After this time the capsule were examined evaluating the colonies proliferation and the inhibition ring surrounding the antibacterial powder.

As shown in FIG. 1, the thickness of the inhibition ring surrounding the TiO₂-MPS-Ag powders was observed to be larger the higher was the Ag⁺ content (see FIG. 1A where 0.58% Ag+ composition were used, FIG. 1B where 2.30% Ag+ composition were used), while no inhibition ring was observed on the control sample of TiO₂ powder (see FIG. 1C).

Claims

1. A derivative of formula (I): TiO2-[L]-Ag+  (I)wherein:-[L]- is a bivalent mercapto alkyl silane ligand of general formula: -[Si—R—S]-, wherein R is a bivalent C1-C4 linear or branched alkyl group, optionally substituted;TiO2 represent a titanium dioxide particle linked to the silica atom of the ligand -[L]-; andAg+ represents silver ions coordinated to the sulphur atom of the bivalent ligand -[L]-.

2. The derivative of formula (I) according to claim 1, wherein the titanium dioxide particle has an average diameter ranging from 100 to 600 nm.

3. The derivative of formula (I) according to claim 1, wherein R is —CH2— or —CH2CH2CH2—.

4. The derivative of formula (I) according to claim 3, wherein R is —CH2CH2CH2—.

5. The derivative of formula (I) according to claim 5, wherein the silver ions are present in an amount ranging from 0.5 to 3% w/w.

6. A method of treatment, comprising applying the derivative of formula (I) according to claim 1 on a patient as a medicament.

7. The method according to claim 6, wherein the medicament is an antibacterial, antimycotic, antiviral or sporicidal agent.

8. A method of treatment, comprising applying the derivative of formula (I) according to claim 1 on a patient as a medicament to treat cutaneous irritations, inflammations, abrasions, excoriations and/or burns.

9. A method of treatment, comprising applying the derivative of formula (I) according to claim 1 on a patient as a medicament to treat acne, herpes, bed sores, and/or skin ulcers.

10. The method according to claim 6, wherein the medicament is a skin cicatrizing agent.

11. A method of treatment, comprising applying the derivative of formula (I) according to claim 1 on a patient as an an antibacterial agent to treat microbes in a disease, wherein at least one of the microbes is selected form the group consisting of: HSV-1 (Herpes Simplex Virus-1), Adenovirus, Poliovirus, Pseudomonas aeruginosa, Enterococcus faecalis, Escherica coli, Salmonella eneridis D1, Listeria monocytogenes, Staphylococcus aureus MR, Staphylococcus aureus MS, Streptococcus pyogenes, Streptococcus salivarius, Streptococcus mitis, Candida albicans, and Aspergillus niger.

12. A pharmaceutical composition comprising the derivative of formula (I) according to claim 1, in admixture with at least one physiologically acceptable excipient and/or carrier, and, optionally, with at least one other pharmaceutical active ingredient.

13. The pharmaceutical composition according to claim 12, wherein the composition contains said other pharmaceutical active ingredient, said pharmaceutical active ingredient selected from the group consisting of: Chlorexidine cation, Chlorexidine digluconate, Chlorexidine acetate, Polyexamethylene Biguanide hydrochloride Cation, Didecyl Dimethylammonium Cation, and combinations thereof.

14. The pharmaceutical composition according to claim 12, in the form of a cream, a gel, a foam or a powder.

15. The pharmaceutical composition according to claim 14, wherein the composition is suitable for topic administration.

16. A method for treatment of a mammal, comprising the topical administration of an effective amount of the pharmaceutical composition according to claim 12.

17. A process for the preparation of formula (I) TiO2-[L]-Ag+  (I)wherein:-[L]- is a bivalent mercapto alkyl silane ligand of general formula: -[Si—R—S]-, wherein R is a bivalent C1-C4 linear or branched alkyl group, optionally substituted;TiO2 represent a titanium dioxide particle linked to the silica atom of the ligand -[L]-; andAg+ represents silver ions coordinated to the sulphur atom of the bivalent ligand -[L]-;said process comprising the reaction of the titanium dioxide with a trialklyoxy mercaptosilane derivative of formula (II), in the presence of a silver salt (III):

18. The derivative according to claim 2, wherein the titanium dioxide particle has an average diameter ranging from 300 to 500 nm.

19. The method according to claim 9, wherein the medicament is used to treat decubitus ulcers.

20. The method according to claim 17, wherein the anionic counterion is perchlorate, acetate, or nitrate.