EP2854758A1

EP2854758A1 - Pharmaceutical composition of a papillomavirus inhibitor

Info

Publication number: EP2854758A1
Application number: EP13721713.9A
Authority: EP
Inventors: Marta Blumenfeld; Delphine Compere; Patricia FRANCON; Michel HUTIN
Original assignee: Anaconda Pharma SAS
Current assignee: Anaconda Pharma SAS
Priority date: 2012-05-07
Filing date: 2013-05-07
Publication date: 2015-04-08
Also published as: CA2872832A1; JP2015522529A; AR090965A1; RU2014148528A; RU2661007C2; FR2990134A1; CN104427971A; US20150152051A1; FR2990134B1; WO2013167583A1; HK1206273A1; CN104427971B; US9670159B2

Abstract

The invention relates to a pharmaceutical composition including a compound of general formula (I) combined with a solvent and a viscosity-enhancing agent, as well as to the use thereof as a drug, in particular for treating and preventing infection with the papillomavirus, and to the method for preparing same.

Description

PHARMACEUTICAL COMPOSITION OF A VIRUS INHIBITOR

PAPILLOMA

The present invention relates to a pharmaceutical composition of compounds useful for the treatment and prevention of infections related to the papillomavirus, described in particular in the application WO 2007/135106.

The compounds described in the application WO 2007/135106 have the structure

for which :

A represents an optionally substituted aryl, cycloalkyl, cycloalkenyl or heterocycle group,

B represents an aryl or an optionally substituted heterocycle,

R1 and R2 independently represent a hydrogen atom or various substituents,

R3 represents an acid function or a prodrug radical or a bioisostere of this function,

Gi represents a bond or a hydrocarbon chain, and

W

I

p

- G ₂ represents a group, with R representing a hydrogen atom or various substituents, W representing O, S or NH and G representing a bond or a hydrocarbon chain.

However, no formulation of these compounds is described in WO 2007/135106.

These compounds useful in the treatment and prevention of infections related to the papillomavirus are intended in particular to be applied topically to the skin and mucous membranes, especially in the anogenital area. The inventors have thus discovered that pharmaceutical compositions of very simple preparation allow rapid and high release of the active principle.

The subject of the present invention is therefore a pharmaceutical composition comprising a compound of formula (I):

or a pharmaceutically acceptable salt thereof,

in which :

^■ G is a bond or a hydrocarbon chain, linear or branched, saturated or unsaturated, comprising 1 to 4 carbon atoms, optionally substituted by one or two alkyl groups, preferably identical,

^■ A represents an aryl group such as phenyl, optionally substituted:

- in meta or para position by:

A halogen atom or a cyano, alkoxy, haloalkoxy, acylaminoalkyl or -XR group where X represents -O-, -S-, -SO-, -SO ₂ - or -CO- and R represents an arylalkyl or cycloalkyl group; or aryl, each optionally substituted with one or two substituents, which may be identical or different, such as a halogen atom, an alkoxy or acyl group, or

A cycloalkyl, aryl or arylalkyl group, each optionally substituted by one or two substituents, which may be identical or different, such as an acyl or alkoxy group,

and / or in the ortho or meta position with an alkyl group,

^■ B represents an aryl group, preferably phenyl, substituted in the ortho position with a heterocycle, preferably a N-cycloalkyl, such as a group piperidin-l-yl, and optionally substituted at ortho 'position with an alkyl group, such as methyl,

^■ n is an integer between 1 and 4, preferably between 1 and 2, and more preferably is 1, ^■ RI represents an alkoxy group such as methoxy, preferably in the position ortho to R3,

^■ R2 represents a hydrogen or halogen atom, such as chlorine or bromine, or an alkyl group such as methyl, preferably in meta position with respect to R3, and

^■ R 3 is an acid or ester group, and preferably acidic,

in combination with a viscosifying agent.

In the present invention, the term "pharmaceutically acceptable" means that which is useful in the preparation of a pharmaceutical composition which is generally safe, non-toxic and neither logically nor otherwise undesirable and which is acceptable for veterinary use as well as human pharmaceutical.

By "pharmaceutically acceptable salts" of a compound is meant in the present invention salts which are pharmaceutically acceptable, as defined herein, and which possess the desired pharmacological activity of the parent compound. Such salts include:

(1) hydrates and solvates,

(2) acid addition salts formed with inorganic acids such as hydrochloric acid, hydrobromic acid, sulfuric acid, nitric acid, phosphoric acid and the like; or formed with organic acids such as acetic acid, benzenesulfonic acid, benzoic acid, camphorsulfonic acid, citric acid, ethanesulfonic acid, fumaric acid, glucoheptonic acid, gluconic acid, glutamic acid, glycolic acid, hydroxynaphthoic acid, 2-hydroxyethanesulfonic acid, lactic acid, maleic acid, malic acid, mandelic acid, acid methanesulfonic acid, muconic acid, 2-naphthalenesulfonic acid, propionic acid, salicylic acid, succinic acid, dibenzoyl-L-tartaric acid, tartaric acid, p-toluenesulfonic acid trimethylacetic acid, trifluoroacetic acid and the like; and

(3) the salts formed when an acidic proton present in the parent compound is replaced by a metal ion, for example an alkali metal ion (Na ⁺ , K ⁺ or Li ⁺ for example), an alkaline metal ion; earthy (such as Ca ²⁺ or Mg ²⁺ ) or an ion aluminum; either coordinates with an organic or inorganic base. Acceptable organic bases include diethanolamine, ethanolamine, N-methylglucamine, triethanolamine, tromethamine and the like. Acceptable inorganic bases include aluminum hydroxide, calcium hydroxide, potassium hydroxide, sodium carbonate and sodium hydroxide.

It will be in particular an alkali metal salt, and in particular a potassium salt.

By "unsaturated" is meant, within the meaning of the present invention, that the group comprises one or more unsaturations.

By "unsaturation" is meant in the sense of the present invention a double bond or a triple bond.

For the purposes of the present invention, the term "halogen" means a fluorine, bromine, chlorine or iodine atom. Advantageously, it is a fluorine, bromine or chlorine atom.

By "alkyl" group is meant, in the sense of the present invention, a saturated hydrocarbon chain, linear or branched, comprising from 1 to 6 carbon atoms, in particular the methyl, ethyl, n-propyl, isopropyl, n-propyl groups. butyl, isobutyl, sec-butyl, tert-butyl, n-pentyl or n-hexyl. Advantageously, it is methyl.

For the purposes of the present invention, the term "cycloalkyl" group is intended to mean a monocyclic or polycyclic, preferably mono-, bi- or tri-cyclic, saturated system comprising from 3 to 12 carbon atoms, the cycles being able to be two or more carbon atoms. two fused or bridged, such as cyclopropyl, cyclopentyl, cyclohexyl, cycloheptyl, cyclooctyl, adamantyl, decalinyl or norbornyl.

By "N-cycloalkyl" group is meant, in the sense of the present invention, a cycloalkyl group as defined above for which a carbon atom has been substituted by a nitrogen atom, the bond with the molecule being by this nitrogen atom. It is advantageously a piperidin-1-yl or pyrrolidin-1-yl group.

By "acyl" group is meant, within the meaning of the present invention, a group of formula -C (O) -Z, where Z represents an alkyl group as defined above. or phenyl. It may advantageously be an acetyl, ethylcarbonyl or benzoyl group.

By "alkoxy" group is meant, in the sense of the present invention, an alkyl group as defined above bonded to the molecule through an oxygen atom. It may be in particular a methoxy, ethoxy, n-propoxy, isopropoxy, n-butoxy, iso-butoxy, sec-butoxy or tert-butoxy group.

By "haloalkoxy" group is meant, in the sense of the present invention, an alkoxy group as defined above substituted with one or more halogen atom (s) as defined above. Preferably, it will be fluoroalkoxy, that is to say an alkoxy group substituted by one or more fluorine atom (s), such as a group -OCF ₃ or -OCH ₂ CF ₃ .

By "aryl" group is meant, in the sense of the present invention, an aromatic group, preferably comprising from 5 to 10 carbon atoms and comprising one or more contiguous rings, such as for example a phenyl or naphthyl group. Advantageously, it is phenyl.

For the purposes of the present invention, the term "heterocycle" is intended to mean a monocyclic or polycyclic, and preferably mono- or bi-cyclic, saturated, unsaturated or aromatic system comprising from 3 to 12 ring members, the rings being two fused, spiro-fused or bridged, and comprising 1 to 4 heteroatoms, identical or different, selected from O, S and N, and optionally comprising one or two oxo or thioxo groups, being understood only in the case of a polycyclic system one of the cyles may be aromatic while the other may be aromatic, saturated or unsaturated. Advantageously, these will be piperidyl, piperazyl, furyl, thienyl, pyrrolyl, pyrazolyl, imidazolyl, pyridyl, pyrimidyl, pyrazinyl, pyradizinyl, benzofuryl, benzothienyl, indolyl, quinolyl, isoquinolyl, benzodioxolyl, benzodioxinyl, benzo [l, 2, 5] thiadiazolyl, benzo [1,2,5] oxadiazolyl, [1,2,3] triazolyl and [1,2,4] triazolyl.

By "arylalkyl" group is meant, in the sense of the present invention, an aryl group as defined above linked to the molecule through an alkyl group as defined above. Preferably, it is a benzyl group. For the purposes of the present invention, the term "acylaminoalkyl" means a group of formula -Alk-NHCO-Alk ', in which Alk and Alk' represent, independently of one another, an alkyl group as defined herein. -above.

For the purposes of the present invention, the term "acid" means a COOH group.

By "ester" is meant, within the meaning of the present invention, a -CO-O-Alk group, where Alk represents an alkyl group as defined above.

For the purposes of the present invention, the term "viscosifying agent" is intended to mean a compound which makes it possible to increase the viscosity of a fluid, such as a liquid. This thus makes it possible to modify the rheological properties of the fluid, which then becomes more viscous.

Advantageously, the composition according to the invention will comprise 0.01 to 10%, especially 2 to 8%, preferably about 5% by weight of a compound of formula (I) relative to the total weight of the composition.

The viscosifying agent may be hydroxypropylcellulose, hydroxypropylmethylcellulose or a carbomer. The viscosifying agent could also be in the form of a mixture thereof. Preferably, the viscosifying agent will be hydroxypropylcellulose.

The composition according to the invention may comprise 0.01 to 50%, in particular 0.05 to 10%, especially 0.5 to 5%, preferably 1 to 5% by weight of this viscosifying agent relative to the total weight of the composition.

The composition according to the invention will also advantageously comprise a solvent such as propylene glycol, glycerol or polyethylene glycol. The solvent could also be in the form of a mixture thereof. Preferably, the solvent will be propylene glycol.

The composition according to the invention may comprise 40 to 99.9%, in particular 80 to 99.5%, especially 85 to 99%, preferably 90 to 95% by weight of this solvent relative to the total weight of the composition. Thus, the composition according to the present invention will advantageously comprise, and preferably will consist of, a compound of formula (I), a viscosifying agent and a solvent.

This pharmaceutical composition may in particular comprise or be constituted by (the percentages by weight being expressed relative to the total weight of the pharmaceutical composition):

- 0.01 to 10%, especially 2 to 8% by weight of the compound of formula (I),

- 0.01 to 50%, in particular 0.05 to 10%, especially 0.5 to 5%, preferably 1 to 5% by weight of the viscosifier, and

- 40 to 99.9%, in particular 80 to 99.5%, especially 85 to 99%, preferably 90 to 95% by weight of the solvent.

Advantageously, this pharmaceutical composition will comprise or consist of (the percentages by weight being expressed relative to the total weight of the pharmaceutical composition):

- 0.01 to 10%, especially 2 to 8%, and preferably about 5% by weight of the compound of formula (I),

- 0.05 to 10%, especially 0.5 to 5%, especially 1 to 5%, preferably about 3% by weight of a viscosifier selected from hydroxypropylcellulose, hydroxypropylmethylcellulose, a carbomer and mixtures thereof, and

- 80 to 99.5%, especially 85 to 99%, especially 90 to 95%, preferably about 92% by weight of a solvent selected from propylene glycol, glycerol, polyethylene glycol and mixtures thereof.

Preferably, the composition according to the present invention will comprise, and preferably will consist of, a compound of formula (I), hydroxypropylcellulose and propylene glycol.

This composition according to the invention will thus have in particular the following composition, with respect to the total weight of the composition:

- 0.01 to 10%, especially 2 to 8%, preferably about 5% by weight of a compound of formula (I),

- 0.01 to 50%, in particular 0.05 to 10%, in particular 0.5 to 5%, especially 1 to 5%, preferably approximately 3% by weight of hydroxypropylcellulose, and - 40 to 99.9%, especially 80 to 99.5%, especially 85 to 99%, especially 90 to 95%, preferably about 92% by weight of propylene glycol.

The composition according to the invention will be in particular in gel form.

In this case, the gel will have in particular a viscosity of 5,000 to 50,000 mPa.s, in particular 15,000 to 25,000 mPa.s, measured according to the standards of European Pharmacopoeia 2.2.10. The viscosity is measured more particularly at 25 ° C. using a Brookfield model HDBV + apparatus or equivalent, with a No. 21 needle for a rotation speed of 10 rpm. The values are determined after 1 minute of rotation.

Advantageously, G 1 represents a bond and a linear and saturated hydrocarbon-based chain comprising 1 to 4 carbon atoms, and preferably represents a bond.

Advantageously, the radical A defined above is an aryl, preferably a phenyl, substituted in meta or para, preferably para, with an alkoxy group, such as methoxy, or with an aryl or arylalkyl group, such as phenyl or benzyl, optionally substituted with one or two substituents, identical or different, such as an acyl or alkoxy group.

Advantageously, B represents an aryl group, preferably a phenyl, substituted in the ortho position by a heterocycle, preferably an N-cycloalkyl, such as a piperidin-1-yl group, and optionally substituted in the ortho 'position by an alkyl group. , such as methyl.

Advantageously, R2 represents a halogen atom, such as a bromine atom, preferably in the meta position relative to R3.

Preferably, the compound of formula (I) has the following characteristics:

A represents a phenyl group substituted in the para position by a benzyl group,

B represents a phenyl group substituted in the ortho position by a piperidin-1-yl group and in the ortho-position with a methyl group, Gl represents a bond, and

R1, R2, R3 and n are as defined above.

In particular, the compound of formula (I) is 4- [N '- (4-benzylphenyl) -N' - (2-methyl-6-piperidin-1-yl-phenyl) -hydrazinocarbonylmethyl] - 5-bromo-2-methoxy-benzoic acid or a pharmaceutically acceptable salt thereof, and in particular its potassium salt.

Indeed, the potassium salt makes it possible to increase the solubility of this compound, especially in comparison with its hydrochloride, and to facilitate the formulation of the product.

The subject of the present invention is therefore also the potassium salt of 4- [N '- (4-benzyl-phenyl) -N' - (2-methyl-6-piperidin-1-yl-phenyl) -hydrazino acid. carbonylmethyl] -5-bromo-2-methoxybenzoic acid.

The present invention also relates to this particular salt for use as a medicament, especially for preventing or treating an infection with the papilloma virus, and in particular HPV6 or HP VI 1.

This potassium salt makes it possible in particular to prevent or treat lesions or diseases associated with papillomavirus infections, and in particular ano-genital warts, such as condyloma acuminata and flat condyloma, laryngeal, conjunctival or oral papillomas, recurrent respiratory papillomatosis, low-grade and high-grade intraepithelial neoplasia, bowenoid papulosis, vulvar, plantar, myrmcial, superficial or flat warts, verruciform epidermodysplasias, and carcinomas, especially anogenital.

It will be particularly useful for the treatment of lesions caused in particular by HPV6 and HPV11 virus infections, including warts and warts.

The present invention also relates to any pharmaceutical composition comprising this potassium salt in combination with at least one pharmaceutically acceptable excipient. The present invention also relates to a composition according to the present invention for its use as a medicament, in particular for preventing or treating an infection with the papilloma virus, and in particular HPV6 or HP VI 1.

The present invention also relates to the use of a composition according to the invention for the preparation of a medicament useful for preventing or treating an infection with the papilloma virus, and in particular HPV6 or HP VI 1.

The present invention also relates to a method for preventing or treating an infection with the papilloma virus, and in particular HPV6 or HPV11, comprising administering an effective amount of a composition according to the invention to a person in need.

The composition will be used in particular topically, especially in gel form, oral administration may also be considered.

By "topical" is meant, in the sense of the present invention, a local application. This application can be performed on the skin or the mucous membranes (external or internal) such as the respiratory tract, the oral cavity or the ano-genital area. It could also be performed by local injection in or around a lesion or tumor. Preferably, it is carried out on the skin and / or the mucous membranes, and in particular in the ano-genital zone.

The composition according to the present invention makes it possible in particular to prevent or treat lesions or diseases associated with papillomavirus infections, and in particular ano-genital warts, such as condyloma acuminata and flat condyloma, laryngeal, conjunctival papillomas or oral, recurrent respiratory papillomatosis, low-grade and high-grade intraepithelial neoplasia, bowenoid papulosis, vulvar, plantar, myrmcial, superficial or flat warts, verruciform epidermodysplasias, and carcinomas, especially anogenital.

The composition according to the present invention will in particular be useful for the treatment of lesions caused in particular by HPV6 and HPV11 virus infections, in particular warts and condylomas.

The compositions according to the present invention can be prepared by mixing the different ingredients. The present invention therefore also relates to a method for preparing a composition according to the present invention comprising a compound of formula (I), a viscosifying agent and a solvent, comprising the following steps:

(i) mixing the compound of formula (I) in a portion of the solvent to give a solution A,

(ii) mixing the viscosifier in the remaining portion of the solvent to give a solution B, and

(iii) mixing solutions A and B to give the composition according to the invention. Preferably, step (i) will be carried out at room temperature.

Preferably, step (ii) will be carried out hot to obtain a homogeneous solution of the viscosifying agent. This step will in particular be carried out at a temperature between 60 and 100 ° C, preferably between 70 and 80 ° C. Solution B will then be cooled before being used in step (iii).

Preferably, step (iii) will be carried out at a temperature of between 20 and 40 ° C. In this case, the reactor containing solution A will be transferred to the reactor containing solution B, or vice versa. The reactor thus transferred may also be rinsed with a little solvent according to common practice. The present invention will be better understood in the light of the nonlimiting examples which follow.

FIGURE:

FIG. 1 represents the diagram of the process for manufacturing a composition according to the invention.

EXAMPLES

The active ingredient used in the examples is the potassium salt of 4- [N '- (4-benzyl-phenyl) -N' - (2-methyl-6-piperidin-1-yl-phenyl) -hydrazinocarbonylmethyl) 5-bromo-2-methoxy-benzoic (compound (la)). One of the methods for obtaining the potassium salt of the active ingredient is based on the transformation of the neutral form of the compound of interest solubilized in ethanol with ethanolic potassium hydroxide. The neutral form is itself obtained from the washing with water of the compound in hydrochloride form as claimed in the patent WO 2007/135106.

Compositions according to the invention with 5% by weight of active principle in the form of a gel

The pharmaceutical composition is a gel containing 5% by weight of compound (Ia). Hydroxypropylcellulo is:

The specifications are those of EP Monograph No. 0337 (European Pharmacopoeia). The source of hydroxypropyl cellulose is Klucel ^® sold by the supplier ASHLAND with the following grades: MF-Pharm, MXF-Pharm and Pharm GF.

Propylene glycol :

The specifications are those of EP monograph No. 0430 (European Pharmacopoeia). Manufacture of pharmaceutical compositions (a) to (g)

The active ingredient (Ia) is dissolved in a propylene glycol fraction. Hydroxypropylcellulo was dispersed in "cold" propylene glycol and the mixture was then heated to dissolve the viscosifier. When the gel is cooled to 40 ° C, the active ingredient solution (1a) in propylene glycol is added (the container having contained this solution is rinsed with a little propylene glycol) and the mixture is homogenized. Stirring is maintained until room temperature.

The process for producing the gel is shown in FIG. The following batch of 5000 g (corresponding to the composition (g)) was prepared in particular according to this process:

* KLUCEL GF-Pharm The active ingredient is dissolved in about 750 g of propylene glycol for a batch of 5000 g gel at room temperature. The hydroxypropylcellulose is dispersed in about 3,600 g of propylene glycol. The mixture is heated with stirring at 75 ± 5 ° C until a homogeneous gel is obtained. The preparation is allowed to cool to 40 ° C or lower while maintaining agitation.

With stirring, the active ingredient in solution is poured into the hydroxypropylcellulose solution and the container with the remaining propylene glycol (250 g) is rinsed. The final gel is allowed to cool to 30 ± 5 ° C with stirring before conditioning.

The pharmaceutical composition obtained is a viscous gel, translucent, colorless to pale yellow.

Study of diffusion through a synthetic membrane of the active ingredient from the pharmaceutical composition (d)

Diffusion studies through a synthetic cellulose dialysis membrane mounted on a Franz diffusion cell were conducted with the pharmaceutical composition (d).

The kinetics of the diffusion of the compound (Ia) through the membrane was monitored for 6 h. At the end of kinetics, more than 20% of the active ingredient was released from the pharmaceutical composition.

Biological activity of the pharmaceutical composition The activity against papillomavirus of an active ingredient can be evaluated in various in vitro and cellular assays such as those described by Chiang et al. (1992), Proc. Natl. Acad. Sci. USA, 89: 5799-5803, by White et al. (2003), Journal of Biological Chemistry, 278: 26765-26772, or by Fradet-Turcotte et al. (2010), Virology, 399: 65-76.

In the present invention two types of assays are used to study the biological activity of compounds against papillomavirus. A first test ("E1 / E2 interaction test") evaluates the interaction between HPV (human papillomavirus) proteins El and E2 in human cells. A second test ("replication test") measures the replication of viral genomic DNA in human cells.

• Interaction test

The interaction test between El and E2 is similar to tests often called 'mammalian 2 Hybrid'. It is based on the co-transfection of a reporter vector containing DNA binding sites for HPV E2 protein in the promoter controlling the expression of the reporter gene, and expression vectors encoding the E1 proteins and E2 HPV, the El protein being fused to the transactivator domain VP16. This test makes it possible to follow the interaction between the proteins El and E2, this interaction being a necessary step for the replication of the HPV genome.

For the interaction tests between E1 and E2, a reporter vector containing several DNA binding sites for the E2 protein (palindrome 5 'ACCGNNNNCGGT-3') upstream of the minimal promoter MLP (Adenovirus Major) was constructed. Late Promoter) controlling transcription of the gene encoding firefly luciferase. N-terminal fused HPV E1 expression vectors were also constructed with the HSV-1 virus transactivator domain VP16. Co-transfection into cell lines of this reporter vector containing E2 sites and HPV E2 protein expression vectors leads to a marginal increase in luciferase activity. Co-transfection of this reporter vector containing E2 sites, expression vectors of HPV E2 proteins and expression vectors of E1 proteins fused to the VP16 domain allows the formation in cells of the E2 / E1-VP16 protein complex. strongly transactivating, and leads to a strong increased luciferase activity. This reflects the interaction between E1 and E2 proteins in cells.

• Replication test

The viral genomic DNA replication test is based on the co-transfection of a reporter vector containing an HPV viral origin of replication (ori) and expression vectors encoding the HPV El and E2 proteins. It makes it possible to follow all the biological functions of El and E2 necessary for the replication of the HPV genome.

For replication assays for viral genomic DNA, a 'replicon' reporter vector containing the origin of HPV11 / HPV6 viral replication (also called LCR, which carries HPV E1 and E2 binding sites) was constructed. ) and the gene encoding firefly luciferase under the transcriptional control of the SV40 promoter. It has been verified that the presence of the HPV origin of replication has no transcriptional effect on the expression of the luciferase gene, in the presence or absence of the E1 or E2 viral proteins. Co-transfection of this vector-replicon and expression vectors of HPV E1 and E2 proteins in human cell lines leads to an increase in luciferase activity dependent on the presence of E1 and E2, reflecting the increase number of reporter vectors. This is due to the activity of the viral proteins El and E2 which allow the replication, in mammalian cells, of this vector-replicon containing an origin of viral replication.

In order to demonstrate that the formulation of the active principle in the pharmaceutical composition according to the invention does not change the biological activity of the non-formulated active ingredient, the activity of the compound (Ia) was measured by studying the biological activity against the virus of the papilloma, either pharmaceutical compositions (a), (d), (f) and (g) according to the invention, or of the compound (la) in a Tris-DMSO buffer solution (25 mM Tris, pH 8.0, % DMSO) freshly prepared.

The pharmaceutical compositions (a), (d), (f) and (g) were diluted in the same buffer solution to be tested at the same concentrations as the active ingredient, namely in a range of 0.25 to 40 μΜ. The compound (Ia), either in solution or in the pharmaceutical compositions (a), (d), (f) and (g), was evaluated for its inhibitory activity of the interaction between HPV11 proteins E1 and E2. HPV6 in human cell lines derived from renal epithelial cells or cervical carcinoma. Various doses (0.25-40 μl) were incubated in the cell medium for 2 days after transfection and luciferase activity was measured to determine the ICso of the compound on the interaction between the E1 and E2 proteins of the cells. HPV.

The compound (Ia), either in solution or in the pharmaceutical compositions (a), (d), (f) and (g), was also evaluated for its inhibitory activity of HPV 11 E1 and E2 viral replication. / HPV6 in human cell lines derived from renal epithelial cells or cervical carcinoma. Various doses (0.25-40 μl) were incubated in the cell medium for 2-6 days after transfection, and luciferase activity was measured using a luminometer to determine the ICso of the compound on the replication of the HPV genome.

The pharmaceutical compositions described above have the same biological activity as the compound (Ia) in solution (not formulated). The compound (Ia) in solution and the pharmaceutical compositions (a), (d), (f) and (g) both inhibit the interaction between the HPV 11 / HPV6 E1 and E2 proteins in the cells, as well as the replication. viral, dependent on proteins El and E2 of HPV11 in cells, with an IC ₅₀ of the order of 1 μΜ.

Percutaneous absorption in vitro and in vivo

The percutaneous absorption of the compound (Ia) from the pharmaceutical composition (g) was studied after the application of a dose of 10 mg / cm ² on human skin mounted in Franz's cell. This study was done by comparing percutaneous absorption on healthy skin and delaminated skin, as a model of the weak keratinization of the anogenital area.

After 8 or 24 hours of exposure to the pharmaceutical composition (g), the amount of the compound (Ia) present in each layer of the skin (stratum corneum, epidermis, dermis), as well as what passed through the skin (receiving fluid ) is quantified by HPLC. The results obtained after 8 hours of diffusion are presented in the table below.

The horny layer of non-delaminated skin is removed from the epidermis by adhesive peeling.

The latter is applied to the skin surface under a constant and controlled pressure.

NA: not applicable

The concentrations of the compound (la) measured in the skin after 8 hours of diffusion correspond to a local concentration of 100 (healthy skin) to 1000 times (delaminated skin) activity of the active ingredient (IC ₅₀ ) measured in cellulo. Similar results were obtained after 24 hours of diffusion. Similarly, similar results have been observed in in vitro percutaneous absorption studies on miniporc skin, a highly predictive animal model of the behavior of human skin.

On the other hand, while the local concentration of the active ingredient in the skin is high, only a small amount of the compound (1a) has passed through Franz's mini-pig skin. On the order of 0.1% of the applied dose was thus measured in the receiving liquid after 24 hours of exposure to a dose of 10 mg / cm ² of the pharmaceutical composition (g).

The percutaneous absorption of the compound (Ia) from the pharmaceutical composition (g) was also measured in vivo during a toxicokinetic study, performed by twice-daily application of a dose of 10 mg / cm ² on the flank. minipigs for 42 days. The presence of the compound (Ia) was measured and quantified on the first day and the last day of the study in the blood of animals treated using a highly sensitive LC-MS / MS bioanalytical method (limit of detection = 0.5 ng / ml). In a similar manner to the in vitro percutaneous absorption studies on human skin and miniporc described above, small amounts of compound (Ia) were detected in blood minipigs. Thus, about 0.1% of the applied dose was measured, showing the low in vivo percutaneous absorption of the compound (Ia) from the pharmaceutical composition. All of these results show a high local concentration of the active ingredient (compound (la)) in the skin after application of the pharmaceutical composition and low systemic exposure thereof, as desired for topical medicaments. Tolerance

A very good tolerance to the pharmaceutical composition (g) has been demonstrated both in the miniporc during a preclinical toxicity study and in the healthy volunteer during a Phase I clinical study. In the miniporc, a dose of 10 mg / cm ² was applied twice daily to 25, 125 or 250 cm ² on the flank of the animals for 42 days. Regardless of the surface treated, a high tolerance to the pharmaceutical composition has been observed. In addition, a very good tolerance to the pharmaceutical composition was demonstrated at twice-daily application for 7 days at a dose of 10 mg / cm ² on a 25 cm ^{2 surface} on the lower back of healthy volunteers. No local reactions or adverse effects were observed in the 8 healthy volunteers treated.

Microbiological Properties

The efficacy of the antimicrobial preservation of the pharmaceutical compositions (a) and (g) was tested according to the European Pharmacopoeia method (method 5.1.3 with application of the standards 5.1.3-2).

The results are shown in the table below: Pharmaceutical composition (a):

PA: No Increase

U.F.C .: Colony Forming Unit

Pharmaceutical composition (g):

PA: No Increase

U.F.C .: Colony Forming Unit

The results are in accordance with criterion A of method 5.1.3-2 of European Pharmacopoeia.

Thanks to the presence of propylene glycol known to those skilled in the art for its antimicrobial preservative properties, the formulation is protected against microbial contamination and, therefore, does not require additional preservatives. Stability study

The stability of the pharmaceutical composition (g) was studied on a 5 kg laboratory batch.

The following storage conditions have been tested according to the ICH recommendations:

- Long term condition: 5 ° C ± 3 ° C,

- Intermediate condition: 25 ° C ± 2 ° C / 60% ± 5% RH (relative humidity), and

- Accelerated condition: 40 ° C ± 2 ° C / 75% ± 5% RH.

The test methods are those used routinely and include:

checking the appearance,

measuring the viscosity, and

the determination of the active ingredient (Ia) by HPLC.

The results obtained are presented in the following tables:

Stability data at 5 ° C

ND: not determined Stability data at 25 ° C / 60% RH

ND: not determined

Stability data at 40 ° C / 75% RH

ND: not determined

The viscosity remains stable whatever the conditions and duration of storage.

The dosage of the active ingredient (Ia) and the appearance of the gel remain in the expired standards, regardless of the conditions and duration of storage, demonstrating the stability of the gel on storage.

Claims

A pharmaceutical composition comprising a compound of general formula (I)

or a pharmaceutically acceptable salt thereof,

in which :

A represents an aryl group, such as phenyl, which is optionally substituted:

- in meta or para position by:

and / or in the ortho or meta position with an alkyl group,

N is an integer between 1 and 4, preferably between 1 and 2, and more preferably is 1,

^■ RI represents an alkoxy group such as methoxy, preferably in the position ortho to R3, ^■ R2 represents a hydrogen or halogen atom, such as chlorine or bromine, or an alkyl group such as methyl, preferably in meta position with respect to R3, and

^■ R 3 is an acid or ester group, and preferably acidic,

in combination with a solvent and a viscosity agent.

2. Pharmaceutical composition according to claim 1, characterized in that it comprises 0.01 to 10%, especially 2 to 8%, and preferably about 5% by weight of the compound of formula (I) relative to the total weight of the pharmaceutical composition.

3. Pharmaceutical composition according to any one of claims 1 and 2, characterized in that the viscosifier is hydroxypropylcellulose, hydroxypropylmethylcellulose, a carbomer or a mixture thereof, and preferably is hydroxypropylcellulose.

4. Pharmaceutical composition according to any one of claims 1 to 3, characterized in that it comprises 0.01 to 50%, in particular 0.05 to 10%, especially 0.5 to 5%, preferably 1 to 5% by weight of the viscosifying agent relative to the total weight of the pharmaceutical composition.

5. Pharmaceutical composition according to any one of claims 1 to 4, characterized in that the solvent is propylene glycol, glycerol, polyethylene glycol or a mixture thereof, in particular is propylene glycol.

6. Pharmaceutical composition according to any one of claims 1 to 5, characterized in that it comprises 40 to 99.9%, in particular 80 to 99.5%, especially 85 to 99%, preferably 90 to 95%. by weight of the solvent relative to the total weight of the pharmaceutical composition.

7. Pharmaceutical composition according to any one of claims 1 to 6, characterized in that it comprises, relative to the total weight of the pharmaceutical composition: - 0.01 to 10%, especially 2 to 8% by weight of the compound of formula (I),

- 0.01 to 50%, in particular 0.05 to 10%, especially 0.5 to 5%, preferably 1 to 5% by weight of the viscosifying agent, and

8. Pharmaceutical composition according to claim 7, characterized in that it comprises, relative to the total weight of the pharmaceutical composition:

- 0.05 to 10%, especially 0.5 to 5%, especially 1 to 5%, preferably about 3% by weight, of a viscosifier selected from hydroxypropylcellulose, hydroxypropylmethylcellulose, a carbomer and mixtures thereof, and

9. Pharmaceutical composition according to claim 8, characterized in that it has the following composition, relative to the total weight of the pharmaceutical composition: - 0.01 to 10%, especially 2 to 8%, and preferably about 5 % by weight of the compound of formula (I),

- 0.05 to 10%, especially 0.5 to 5%, especially 1 to 5%, preferably about 3% by weight of hydroxypropylcellulose, and

80 to 99.5%, especially 85 to 99%, especially 90 to 95%, preferably about 92% by weight of propylene glycol.

10. Pharmaceutical composition according to any one of claims 1 to 9, characterized in that it is in gel form.

11. Pharmaceutical composition according to claim 10, characterized in that the gel has a viscosity of 5000 to 50000 mPa.s, in particular from 15,000 to 25,000 mPa.s.

12. Pharmaceutical composition according to any one of claims 1 to 11, characterized in that the compound of formula (I) has the following characteristics:

- G1 represents a linear and saturated hydrocarbon linkage or chain, comprising 1 to 4 carbon atoms, and preferably represents a bond,

A represents an aryl, preferably a phenyl, substituted in meta or para, preferably in para, with an alkoxy group, such as methoxy, or with an aryl or arylalkyl group, such as phenyl or benzyl, optionally substituted by a or two substituents, identical or different, such as an acyl or alkoxy group,

B represents an aryl group, preferably a phenyl, substituted in the ortho position by a heterocycle, preferably an N-cycloalkyl, such as a piperidin-1-yl group, and optionally substituted in the ortho 'position by an alkyl group; such as methyl, and

R2 represents a halogen atom, such as a bromine atom, preferably in the meta position relative to R3.

13. Pharmaceutical composition according to any one of claims 1 to 12, characterized in that the compound of formula (I) has the following characteristics:

A represents a phenyl group substituted in the para position by a benzyl group,

B represents a phenyl group substituted in the ortho position by a piperidin-1-yl group and in the ortho-position with a methyl group, and

- Gl represents a bond.

14. Pharmaceutical composition according to any one of claims 1 to 13, characterized in that the compound of formula (I) is 4- [N '- (4-benzyl-phenyl) - N' - (2-) methyl-6-piperidin-1-yl-phenyl) hydrazinocarbonylmethyl] -5-bromo-2-methoxybenzoic acid or a pharmaceutically acceptable salt thereof, and in particular its potassium salt.

15. The pharmaceutical composition according to any one of claims 1 to 14 as a medicament.

16. Pharmaceutical composition according to any one of claims 1 to 14 for its use in the treatment and prevention of infection with papillomavirus, and in particular HPV6 or HP VI 1.

17. Pharmaceutical composition according to claim 16 for its use in the prevention or treatment of lesions or diseases associated with papillomavirus infections, and in particular ano-genital warts, such as condyloma acuminata and flat condyloma, laryngeal papillomas. , conjunctival or oral, recurrent respiratory papillomatosis, low-grade and high-grade intraepithelial neoplasia, bowenoid papulosis, vulvar, plantar, myrmcial, superficial or flat warts, verruciform epidermodysplasias, and carcinomas, in particular ano -génitaux.

18. Process for the preparation of a pharmaceutical composition according to any one of claims 1 to 17, comprising the following steps:

(iii) mixing solutions A and B to give the pharmaceutical composition.

19. 4- [N '- (4-Benzyl-phenyl) -N' - (2-methyl-6-piperidin-1-yl-phenyl) -hydrazinocarbonylmethyl] -5-bromo-2-potassium salt methoxy-benzoic acid.