FR2758724A1 - Controlling cellulite and fat deposition - Google Patents

Abstract

A topical cosmetic and/or pharmaceutical composition for controlling cellulite and fat deposition contains protamine (PA) or its salt or ester as active agent (I). The composition is an emulsion, lotion, gel or cream containing 0.001-10 wt.% (I), especially 0.05-1 wt.% PA. The salt or ester of PA is the sulphate, hydrochloride, sorbate, hyaluronate, heparinate, gluconate or lactate. The composition further contains a lipolysis promoter (specifically caffeine) and/or an alpha -2 blocker.

Description

 The present invention relates to a new application of protamine, and more particularly to the application of protamine, its salts or esters, in cosmetics and therapeutics, as well as cosmetic and pharmaceutical compositions containing it.

 Adipose overloads and accumulations of cellulite are considered depending on the case as defects likely to harm the aesthetic appearance or as abnormal physiological states of individuals, in men, but especially in women. These states should not, however, be confused with obesity, which constitutes a pathology requiring systemic treatment. Very often it is not useful to resort to a therapeutic treatment to fight against adipose overloads, but in most cases their presence is considered unsightly, and a cosmetic treatment is then desired to mitigate the effects.

 Skin cells, called adipocytes, synthesize triglycerides by lipogenesis from free fatty acids and glycerol from the breakdown of glucose.

Fatty acids and glucose are brought to the body through food. Conversely, the triglycerides contained in adipocytes undergo lipolysis under the action of enzymes and release glycerol or glycerol esters as well as fatty acids which can in turn circulate in the organism and / or be taken up by adipocytes. where they are again transformed into triglycerides by lipogenesis. If there is an imbalance between lipogenesis and lipolysis, there can be an excessive accumulation of triglycerides which does not result in fat overloads.

 Patent FR-A-2,712,811 proposes an in vivo treatment method using glucose uptake inhibitors such as serine and rutin, which prevent glucose from being used by adipocytes to fix, in the form of triglycerides, free fatty acids from food or released by lipolysis. The interest of these inhibitors is still discussed because of their annoying action on the nerve cells, very dependent on these transport systems in the event of systemic effect.

 Various compositions intended for combating cellulite are commercially available and in particular compositions containing xanthic bases such as theophylline and caffeine, because of its effect of increasing the intracellular level of AMPC by inhibiting a phosphodiesterase and by a supposed phenomenon of interaction on a membrane receptor having the same effect. Its in vitro action on lipolysis is clearly established, as well as its transepidermal penetration. However, no evidence has been provided indicating any action in vivo, particularly in individuals who regularly consume significant amounts of coffee.

 Also known are alpha-2 inhibitors or alpha-2 blockers such as those described in patent FR-A-2,669,537 which block the binding of catecholamines to alpha-2 receptors, strongly inhibiting lipolysis. These receptors are more numerous in female subjects, in particular in overweight subjects.

 To combat cellulite, it has also been proposed to use compositions based on various substances of plant origin, supposed capable of acting effectively on the drainage and elimination of toxins.

 However, none of these substances or compositions has been found capable of providing effects making it possible to use them advantageously and effectively for the treatment of adipose overloads and cellulite.

 Protamine is a protein which releases by hydrolysis several basic amino acids, in particular arginine which is the main component, as well as alanine and serine. Several types of protamine exist and can be extracted from substances of animal origin, especially milt from fish such as salmon.

 Protamine and some of its salts, such as protamine sulfate, are used as food preservatives, as described for example in patent EP 273,606, because of their inhibitory effect on the multiplication of certain bacteria. Protamine sulfate is also used in some pharmaceutical compositions due to its hemostatic effects, and it can be used to neutralize the anticoagulant action of heparin. Finally, patent FR 2,656,311 describes inhibitors of lipolytic enzymes comprising basic proteins or polypeptides such as purothionines, protamine, a histone or a polylysine, formulated in compositions for oral administration for the prevention of obesity.

 The work carried out by the applicant has shown quite surprisingly that protamine, as well as its salts and esters, can be used effectively at reduced concentrations in topical cosmetic and / or pharmaceutical compositions, intended for combating cellulite and adipose overloads.

 The present invention therefore relates to the use of protamine, its salts and esters, in cosmetic and / or pharmaceutical compositions which can be administered topically and which are intended to combat cellulite and overweight and to attenuate its effects.

 The invention also relates to the use of protamine, its salts and esters, for the preparation of a medicament for the treatment of cellulite and overweight.

 According to conventional terminology, topical administration means any method consisting in applying the substance or composition directly to the skin.

 The protamine which can be used in the present invention may be any of the commercially available forms of protamine, the amino acid composition of which may vary, or one of its cosmetically or pharmaceutically compatible salts or esters, such as sulfate, hydrochloride, sorbate, hyaluronate, heparinate, gluconate and protamine lactate.

 In all that follows, the expression "protamine" will denote both the protamine itself and its salts or esters mentioned above.

 In accordance with the present invention, the composition which can be administered topically may advantageously contain, in addition to protamine, its salts or esters, one or more other substances known to exert complementary effects, and more particularly a compound promoting lipolysis, for example an inhibitor phosphodiesterase such as caffeine, as well as an alpha-2 blocker, for example escin, ivy extracts, yohimbine and ginkgo biloba extracts.

 Cosmetic or pharmaceutical compositions containing protamine, in accordance with the present invention, are intended for topical administration, and contain carriers and excipients commonly used in compositions of this type, such as O / W or W / O emulsions, creams, gels or lotions. In the case of emulsions, the fatty phase can represent between 10 and 60% approximately of the weight of the composition, the aqueous phase between 10 and 80% approximately and the emulsifying agent between 2 and 20%, the rest being constituted by protamine and the other components listed below.

 Thus, the compositions can contain emulsifying agents, moisturizing agents, viscosifying agents, preservatives, perfumes, oils, lipids, a specific solvent as well as water.

The emulsifier can be chosen from high molecular weight carboxyvinyl polymers (for example Carbopol3), polysorbates (for example Tween 60 or
Tween 80), sorbitan esters and in particular a monostearate, a tristearate, a monopalmitate, and a sorbitan laurate (for example Arlacel. It is also possible to use other emulsifying agents such as various derivatives of stearic acid or palmitic, and for example PEG 50 stearate, mono- or diglycerides of stearic or palmitic acid, a self-emulsifying propylene glycol stearate, or also polyglyceryl-2-sesquioleate, polyoxyethylene cetyl ether, a polyglucoside of siloxane, or an emulsifiable silicone. It is also possible to use nonionic emulsifying mixtures such as Protegin X.

 The viscosifiers used in the compositions of the invention may be chosen from various polymers of acrylic acid, a cellulose gum, a silica, carboxyvinyl polymers, an aluminum and magnesium silicate, and it is possible, for example, to use the colloidal silica sold under the brand Aerosil 200 or a crosslinked polyacrylic acid such as Carbopol 940.

 The hydrating agents used in the invention are preferably glycerol or glycerol derivatives.

 The constituents of the fatty phase, that is to say the oils and lipids, can be chosen from jojoba oil, corn oil, petroleum jelly oil, hydrogenated coconut oil, safflower oil, glycerides of saturated fatty acids, stearic acid, palmitic acid, octyl stearate, glyceryl palmitate, 2-octyl-dodecanol, lanolin alcohol, polyethylene glycol, 2-ethylhexyl adipate, or alternatively silicone oils such as methyl phenyl polysiloxane, dimethicone, cyclomethicone / dimethicone copolyol, phenyl trimethicone.

The composition can also contain, in addition to water (preferably demineralized water), a specific solvent, such as an alcohol such as ethyl alcohol, or a diethylene glycol ether such as ethoxydiglycol or monomethyl ether diethylene glycol (Transcutol
All the excipients and additives commonly used can be used in the invention provided that they are compatible with protamine. One of the advantages resulting from the present invention is the possibility of reducing the amount of preservative compared to conventional compositions, due to the anti-bacterial power of protamine. It is even possible to prepare protamine-based compositions containing no usual preservative.

 Protamine is used in an amount of 0.001 to 10% by weight, and preferably 0.05 to 1%, of the total weight of the composition, in the case of formulations for topical administration. This mode of administration is particularly advantageous in the present invention because it allows a very localized application on the parts of the body to be treated. This application can be accompanied by a massage of the area to be treated.

 The absence of well-known toxicity of protamine and of its available salts and esters makes it possible to use it without risk of complication in both cosmetic and pharmaceutical compositions. In particular, the atherogenic risk is zero because protamine is known as an anti-atherogenic agent by normalization of blood lipid indices.

 The tests carried out with the compositions in accordance with the present invention have demonstrated an effect of reduction of adipose overloads and of cellulite, in particular in the case of topical application in the form of emulsion or gel, one or more times. per day for a period ranging from a few days to a few weeks.

 Although the mode of action of protamine is not fully understood, it appears that the uptake of free fatty acids by the adipocyte in the subcutaneous adipose tissue is partially or completely inhibited by the protamine. In fact, the adipocyte produces a lipoprotein lipase which is normally transported to the endothelial cells covering the lumen of the capillaries, and which detaches the circulating fatty acids from the proteins which transport them.

The inhibition of this fixation by protamine has the effect of preventing the entry and accumulation of lipids in the adipocyte and is complementary to the action of conventional lipolytic agents.

 The following examples illustrate the invention without limiting its scope. They describe topical formulations which can be prepared by the usual methods of the cosmetic technique.

EXAMPLE 1
SLIMMING W / O EMULSION
A water-in-oil emulsion is prepared by a usual method using the following ingredients.

Protamine gluconate ....................... 0.5 g
Polyglyceryl-4 isostearate and
cetyl dimethicone ............................ 5.0 g
2-ethylhexyl adipate ..................... 5.0 g
Cyclomethicone ............................... 8.0 g
Vaseline oil ............................ 5.0 g
Aerosil 200 .................................. 0.4 g
Octyl stearate ............................ 14.0 g
Sodium chloride ........................... 0.5 g
Ethoxy diglycol .............................. 3.0 g
Ginkgo biloba extract ..................... 0.7 g
Caffeine ...................................... 1.0 g
Preservative ................................. 0.3 g
Demineralized water ......... qs ............... 100.0 g
This emulsion is applied directly to the skin of a patient, at the level of an adipose overload, at the rate of two applications per day supplemented by a localized massage, for a period of four weeks.

 There is then a significant reduction in adipose overload.

 The same operation is repeated on five other patients, with the same emulsion, for a period of between four and six weeks. Comparable results are observed.

Example 2
SLIMMING W / O EMULSION
Protamine sulfate ......................... 0.5 g
Protegin X ................................... 20.0 g
Vaseline oil ............................ 10.0 g
Aromatic composition ....................... 1.0 g
Corn oil ................................ 15.0 g
Preservative ................................. 0.3 g
Glycerol ..................................... 5.0 g
Ivy extract ............................. 0.5 g
polyethylene glycol (7) glyceryl monococoate. 4.0g
Demineralized water ......... qs ............... 100.0 g
EXAMPLE 3
SLIMMING O / W EMULSION WITHOUT PRESERVATIVE
Protamine sorbate ......................... 2.5 g
Cyclomethicone ............................... 10.0 g
Phytosqualane ................................ 18.0 g
Vaseline oil ............................ 5.0 g
Liquid lanolin ............................. 4.0 g
Glyceryl stearate and PEG 100 stearate. . . 6.0 g
Tween 60 ..................................... 2.0 g
Cetyl alcohol ............................. 1.2 g
Stearic acid .............................. 2.5 g
Triethanolamine 99% .......................... 0.1 g
Antioxidants ................................. 0.3 g
Caffeine ...................................... 1.0 g
Propylene glycol ............................. 5.0 g
Escine ....................................... 0.5 g
Demineralized water ......... qs ............... 100.0 g
EXAMPLE 4
SLIMMING O / W EMULSION
Protamine .................................... 0.01g
Polyethylene glycol .......................... 2.0 g
PEG 8 ........................................ 3.0 g
Ginkgo biloba extract ..................... 0.3 g
Caffeine ...................................... 3.0 g
Sodium benzoate ........................... 3.0 g
Preservative ................................. 0.3 g
Perfume ....................................... 0.5 g
Caboxyvinyl polymer 981 ................. 0.2 g
2-ethylhexyl adipate ..................... 1.0 g
Cetyl alcohol ............................. 3.0 g
Stearic acid .............................. 3.0 g
Glycerol monostearate ..................... 3.0 g
Sunflower oil ........................... 2.0 g
Triethanolamine 99% .......................... 1.0 g
Demineralized water ......... qs ............... 100.0 g
EXAMPLE 5
HYDROALCOHOLIC SLIMMING GEL
Protamine lactate ......................... 5.0 g
Carboxyvinyl polymer 980 ................ 0.9 g
Ethyl alcohol ............................. 20.0 g
Triethanolamine 99% .......................... 0.3 g
Perfume ....................................... 0.3 g
Preservative ................................. 0.3 g
Ethoxydiglycol ............................... 5.0 g
Ivy extract ............................ 1.0 g
Demineralized water ......... qs ............... 100.0 g
EXAMPLE 6
SLIMMING M / W EMULSION GEL
Protamine hyaluronate ..................... 1.0 g
Carboxyvinyl polymer 980 ................ 0.6 g
Cyclomethicone ............................... 3.0 g
Cetaryl octanoate ........................... 7.0 g
PEG-6-32 stearate ............................ 3.0 g
Preservative ................................. 0.3 g
Perfume ....................................... 0.4 g
Ethyl alcohol ............................. 10.0 g
Triethanolamine .............................. 0.2 g
Caffeine ...................................... 1.0 g
Polyethylene glycol (7) glyceryl monococoate. 2.0 g
Demineralized water ......... qs ............... 100.0 g
EXAMPLE 7
SLIMMING GEL
Protamine hydrochloride .................... 5.0 g
Carboxyvinyl polymer 940 ................ 0.6 g
Ethoxy diglycol .............................. 5.0 g
Triethanolamine 99% .......................... 0.3 g
Preservative ................................. 0.3 g
Propylene glycol ............................. 3.0 g
Ivy extract ............................ 1.0 g
Caffeine ...................................... 1.0 g
Demineralized water ......... qs ............... 100.0 g
EXAMPLE 8
IONIZING LIQUID
Protamine sulfate ......................... 1.0 g
Sodium benzoate ........................... 3.0 g
Preservatives ................................ 0.2 g
Water ....................... qs ............... 100.0 g
EXAMPLE 9
LIPOSOME CREAM
Protamine .................................... 0.25 g
Cetyl alcohol polyglycerolated ............... 3.8 g
B-sitosterol ................................. 3.8 g
Diketyl phosphate ............................ 0.4 g
Preservative ................................. 0.3 g
Corn oil ................................ 35.0 g
Perfume ....................................... 0.6 g
Carboxyvinyl polymer 980 ................ 0.2 g
Triethanolamine 99% .......................... 0.2 g
Demineralized water ......... qs ............... 100.0 g

Claims (7)

 1. Cosmetic and / or pharmaceutical composition intended to fight against cellulite and adipose overloads, characterized in that it is in topically applicable form, and that it contains protamine or one of its salts or esters compatible with cosmetic or pharmaceutical.  2. Composition according to claim 1, characterized in that it is in the form of an emulsion, a lotion, a gel or a cream containing between 0.001% and 10% by weight of protamine or one of its salts and esters.  3. Composition according to claim 1, characterized in that it contains between 0.05% and 1% by weight of protamine.  4. Composition according to any one of the preceding claims, characterized in that the protamine salt or ester is chosen from sulphate, hydrochloride, sorbate, hyaluronate, heparinate, gluconate and protamine lactate .  5. Composition according to any one of the preceding claims, characterized in that it also contains an agent promoting lipolysis and / or an alpha-2 blocker.  6. Composition according to claim 5, characterized in that the agent promoting lipolysis is caffeine.  7. Use of protamine or a pharmaceutically acceptable salt or ester thereof, for the preparation of a medicament for the treatment of cellulite and adipose overloads.