FR2619008A1 - Use of synergistins in pharmaceutical or cosmetic anti-acne compositions - Google Patents

Abstract

Use of a synergistin as active ingredient in the preparation of topically, orally or rectally administerable pharmaceutical anti-acne compositions, the aforementioned synergistin consisting of at least one streptogramin A and at least one streptogramin B.

Description

 The subject of the present invention is the use of antibiotics of the synergistin class in the treatment of acne.

 We know that acne is a common skin condition in adolescents and also in adults. This condition is characterized by a disorder of the keratinization of the pores of the seborrheic areas of the face, the presternal region and the back. This results in the formation of horny plugs with accumulation of sebum, which constitute an environment conducive to the development of bacteria which cause an inflammatory lesion. Propionibacterium acnes (P.acnes) is the main bacterial agent responsible for these lesions.

 Acne treatments aim to combat either the keratinization disorder, or seborrhea, or microbial proliferation. In particular, it has been proposed to combat microbial proliferation using oral or local antibiotics, often over very long periods ranging from 6 months to 2 years. Antibiotics The most commonly used for this purpose are tetracyclines and erythromycin, orally or topically, and clindamycin topically.

However, the treatments carried out with these antibiotics have drawbacks. In particular, the appearance, in significant proportions, of strains of P. acnès resistant to clindamycin has been observed. This resistance is accompanied by cross resistance to erythromycin. At the same time, the emergence in patients treated with erythromycin of strains resistant to this antibiotic and also to clindamycin was noted; see for example W. Crawford, the Journal of
Investigative Dermatology, 72, 187-190 (1979). It has also been noted, in patients treated with clindamycin, the appearance of P.acnes strains resistant not only to clindamycin and to erythromycin, but also to tetracyclines; see C. Marin et al., Journal of the American Academy of
Dermatology, vol. 6, pages 902-908 (1982).

Similar observations have been made in patients treated with tetracycline; see James J. Leyden et al., Journal of the American
Academy of Dermatology, vol.8, pages 41-45 (1983).

We also know that synergistins are antibiotics, isolated from culture media of various strains of Streptomyces, consisting of the combination of two types of factors (A and B) belonging to the group of
Streptogramins and acting in synergy. Factors A have a structure close to that of macrolides and factors B are cyclic heptapeptides. Each of the factors, taken in isolation, has a bacteriostatic activity, but the association A + B has a bactericidal activity characterizing a synergistic effect.

It has now been discovered that antibiotics of the synergistin class have significant bacteriostatic and / or bactericidal activity with respect to P.acnes, including on strains resistant to other antibiotics. This discovery is all the more surprising since it was considered until now that synergistins were not usable in the treatment of acne. This is how in the case of the ointment
Staphylomycin, registered trademark for a synergistin of the Virginiamycin type, the manufacturer indicates that the use in the treatment of acne is excluded; see Vidal Dictionary (DVP, Paris, France) 1985 edition.

 The present invention therefore relates to the use of antibiotics from the synergistin class in the treatment of acne.

 In the present application, the expression "synergistin" or "antibiotic of the synergistin class" will denote a mixture of at least one streptogramin A and at least one streptogramin B.

 In other words, the subject of the invention is the use, in the treatment of acne, of the combination of at least one streptogramin A and at least one streptogramin B.

Among the streptogramins A, mention may in particular be made of virginiamycin M1, mikamycin A, pristinamycin II A or II B, and vernamycin A. Among streptogramins B, mention may be made of virginiamycin S, mikamycin B, pristinamycins IA , IB, IC, and vernamycins
B alpha, B beta, and B gamma.

It is of course possible to use the antibiotics of common name Virginiamycin (or Staphylomycin), Pristinamycin, Streptogramin or
Mikamycin, which consist of mixtures of streptogramins A and B.

Virginiamycin can be prepared according to the process described by
Somer et al., Antibiotics & Chemotherapy, 5, 632 (1955). It mainly consists of a mixture of virginiamycin M1 and virginiamycin S. The separation of virginiamycins M1 and S and the characterization of these two constituents are described for example by Vanderhaeghe et al., Antiobiotics & BR <
Chemotherapy, 7, 606 (1957); and Vanderhaeghe et al., J. Am. Chem. Soc., 82, 4414 (1960).

 Mikamycin can be prepared according to the method of French patent 1,349,946.

 The isolation and characterization of mikamycin A are described for example by Okabe, J. Antibiotics (Japan) Ser. A, 12, 89 (1959).

The isolation, properties and structure of mikamycin B are described, for example, by Watanabe et al., J. Antibiotics (Japan) Ser.A, 12, 112 (1959); 13, 57 (1960); 13, 291-293 (1960); 14, 14 (1961).

 Mikamycin A is identical to virginiamycin M1.

 Pristinamycin can be prepared according to the method of French patent 1,301,857.

Pristinamycin comprises on the one hand pristinamycins IA, IB and IC, and on the other hand pristinamycins II A and II B. The separation, structure and nomenclature of pristinamycins are described in particular by
Preud'homme et al., Bull. Soc. Chim. France, 585 (1968) and Crooy et al.,
J. Antibiot. 25, 371 (1972).

 Pristinamycin I A is identical to mikamycin B.

 Pristinamycin II A is identical to virginiamycin M1.

 Pristinamycin II B is 2 6, 26, 27-dihydrovirginiamycin M1.

 Vernamycins A and B can be prepared according to the method of US Patent 2,990,325. The structure of these products is described by Bodanszki et al., Antimicrobial Agent & Chemoterapy, 360 (1963). Vernamycins B include vernamycin B alpha (identical to mikamycin B), vernamycin B beta and vernamycin B gamma.

 Vernamycins B alpha, B beta and B gamma are identical respectively to pristinamycins I A, I B, and I C.

 Streptogramin (mixture of factors A and B) can be prepared according to the method of British patent 776,035.

 Synergistins are used in the treatment of acne in the form of compositions which can be administered topically, orally or rectally.

The topical route is the preferred route of administration. The pharmaceutical compositions for the topical route are, for example, in the form of ointments, tinctures, varnishes, ointments, powders, soaked pads, sprays or suspensions. These pharmaceutical forms are prepared according to the usual methods.

 For topical administration, these compositions generally contain, in an appropriate excipient or vehicle, 0.5 to 10% by weight of synergistin. For the oral or rectal route, they contain 0.0005 to 95% by weight of synergistin and in particular 85% for the oral route. In the case of prepared dressings (impregnated tissue, soaked tampons), the concentration of synergistin is generally 0.5 to 2% by weight.

 The respective proportions of factors A and B can vary from 10: 90 to 90: 10 by weight.

These pharmaceutical compositions can contain, in addition to the usual carriers, excipients or vehicles, additives such as
- a keratolytic agent such as salicylic acid, benzoyl peroxide or tretinoline; in the case of benzoyl peroxide, the association can be made at the time of use;
- an anti-fungal agent such as imidazole anti-fungals (econazole, miconazole), allylaminated anti-fungals, triazole anti-fungals, grizefuline, selenium sulfide, cyclopyroxolamine, etc ...

- a local anti-seborrheic agent such as progesterone,
S-carboxymethyl cysteine, S-benzyl cysteamine and its derivatives, known local antiandrogens
- And in the case of a composition for the oral route, an oral anti-androgenic agent, such as cyproterone acetate.

- other bacterial agents such as, for example, tioxolone;
- a non-steroidal anti-inflammatory agent, or zinc acetate.

 The compositions which can be used by the local route may also contain an agent promoting transcutaneous penetration such as methyl pyrrolidone or Laureth-4 (trademark for a polyoxyethylenated lauric acid containing 4 moles of ethylene oxide).

 The pharmaceutical compositions used according to the invention can also contain preserving agents, stabilizing agents, pH regulating agents, agents regulating the osmotic pressure, emulsifying agents, antioxidants, UV-A and UV-B filters, etc ...

 These compositions are used so as to locally administer 0.01 g to 0.1 g per day of active ingredient (synergistin) and to administer 1 to 4 g per day of active ingredient by oral route. The treatment is applied until healing. Treatment is generally well tolerated. However, some side effects have been reported after oral administration (nausea, gastric heaviness), and a few cases of sensitization during repeated applications of preparations for local use.

 A subject of the invention is also the use of a synergistin (as defined above) as an active ingredient in the preparation of anti-acne pharmaceutical compositions. These pharmaceutical compositions are used in the treatment of acne disorders such as polymorphic acne, post-drug acne, professional acne, cosmetic acne, senile acne and solar acne.

 Synergistins can also be used, to improve the appearance of the skin, in hygienic or cosmetic compositions for hygiene and care of the face and back, in particular in subjects suffering from mild acne disorders.

 The present invention therefore also relates to cosmetic compositions containing, in a suitable cosmetic carrier or vehicle, a synergistin as defined above.

 In cosmetic compositions, synergistin is present in concentrations which can vary between 0.0005 and 1% by weight.

 The supports or vehicles are in particular those which make it possible to present the composition in the form of lotions (foaming or not), gels, soaps, dermatological breads, creams, emulsions or milks for the face and the body. These cosmetic compositions are prepared and applied according to the usual methods.

 A subject of the invention is also the use as a hygienic or cosmetic agent intended for improving the appearance of acne-prone skin, of a synergistin as defined above.

 The following examples illustrate the invention without, however, limiting it.

EXAMPLE 1: Lotion
We prepared a lotion containing
Mikamycin A 2 g
Mikamycin B 2 g
isopropyl alcohol 85 g
water 10 g
propylene glycol 5 g
This lotion is applied 1 to 2 times a day on the lesions.

EXAMPLE 2: Cream
We prepared a fluid cream containing
Vernamycin A 2 g
Vernamycin B alpha 2 g
Tween 60 5 g
Span 60 2 g
ethyl alcohol 10 g
Miglyol 812 10 g
water qs 100 g
This cream is applied 1 to 2 times a day on the lesions.

 Tween 60 is a trademark for an oxyethylenated sorbitan monostearate containing 20 moles of ethylene oxide.

 Span 60 is a trademark for a sorbitan monostearate.

 Miglyol 812 is a trademark for a mixture of C8-C 12 saturated fatty acid triglycerides.

EXAMPLE 3 Gel
We prepared a skin gel containing
Virginiamycin M1 2 g
Mikamycin B 2 g
ethanol 20 g
Klucel HF 2 g
Water qs i0O g
This gel is applied 1 to 2 times a day on the lesions.

 Klucel HF is a trademark for a hydroxypropylcellulose.

EXAMPLE 4 Oral capsule
Capsules having the following composition were prepared
Pristinamycin II 1 g
Pristinamycin I 1 g
corn starch 0.060 g
lactose 0.300 g
The powder obtained is packaged in a gelule, the wall of which is
composed of gelatin, TiO2 and a preservative.

 This composition is administered 1 to 3 times a day with meals.

EXAMPLE 5: Cleansing milk
We have prepared a toilet milk for back, chest and face hygiene containing
Virginiamycin M1 0.25g
Virginiamycin S 0.25g
Cetostearyl alcohol 3.10g
Cetostearyl alcohol
oxyethylenated to 33 moles of oxide
ethylene 0.090g
Glycerol monostearate 1.00g
Sweet almond oil 6.00g
Silicone oil 1.00g
Glycerin 15.00g
Water qs 100.00g
This toilet milk is applied twice a day.

IN VITRO TESTS
The minimum inhibitory concentration (MIC) of various strains of P. acnes was studied, including reference strains and recent isolates collected by the National Anaerobic Reference Center (PASTEUR Institute).

Strains harboring known resistance characters to MLS (Macrolides-Lyncosamines-Streptogramines) were included (from the Center
National Anaerobic Reference Center or the National Reference Center for
Resistance - PASTEUR Institute).

 The boots, comprising an agar medium, are poured the day before the experiment and then put under anaerobic conditions. Incubation takes place at 370C in an anaerobic chamber.

 The culture medium used was the yeast meat (VL) medium supplemented with 1% sheep blood.

 Reading takes place at 6 p.m. and 48 a.m., with 2 boots per test.

The tests were carried out with pristinamycin IA (P1) from Rhône
Poulenc, pristinamycin IIB (P2) from Rhône-Poulenc, and the commercial antibiotic Pristinamycin (P) from Rhône-oulenc which is a mixture of the factors
P1 and P2, as well as with clindamycin (Cl) from Upjohn and erythromycin (Em) from Roussel-Uclaf.

The results (CMI in pglml) are summarized in the following Table I
TABLE I
Cl Em Pl P2 P strains
Pa 85-176 <0.06 <0.06 8 0.5 <0.06
Pa 85-219 <0.06 <0.06 8 0.5 <0.06
Pa 85-291 <0.06 <0.06 8 0.5 <0.06
Pa 85-307 <0.06 <0.06 16 0.5 <0.06
Pa 85-315 <0.06 <0.06 8 0.5 <0.06
Pa 85-316 <0.06 <0.06 8 0.5 <0.06
Pa 85-317 <0.06 <0.06 16 0.5 0.125
Pa 85-318 <0.06 <0.06 8 0.5 <0.06
Pa 85-319 0.5 0.125 8 32 0.25
Pa 85-411 0.25 <0.06 8 0.5 (0.06
Pa 85-484 0.5 <0.06 8 32 0.5
Pa 85-600 / 2 <0.06 <0.06 8 0.5 <0.06
Pa 85-640 <0.06 <0.06 8 0.5 <0.06
Pa 85-650 0.06 0.06 8 16 <0.06
Pa 85-663 0.125 <0.06 8 <0.06 <0.06
Pa 85-673 <0.06 <0.06 32 0.5 <0.06
Pa 85-725 <0.06 - 4> 128 32 2
Pa 85-729>128>128> 128 128 16
Pa 85-730 <0.06 0.06 16 1 <0.06
Pa 84-138 <0.06 0.06 16 0.5 <0.06
Pa 84-404 <0.06 0.06 16 0.5 <0.06
Pa 84-416 <0.06 <0.06 8 0 -. 5 <0.06
Pa 84-425 <0.06 <0.06 8 0.5 <0.06
Pa 5107 <0.06 4> 128 4 1
These results show
1) That on strains sensitive to erythromycin and clindamycin, the combination of the two synergistins is always at least as effective as erythromycin and clindamycin. In general, the MIC of synergistins with respect to sensitive strains is less than 0.06 pg / ml (first 8 strains in the table, 12th, 13th and 19th to 24th).

 2) In all cases (sensitive and resistant strains), synergy A + B is observed.

3) Regarding resistant strains
a) 2 strains resistant to lerythromycin (MIC 4pg / ml) are sensitive to the association pristinamycin '(IA + IIB).

 b) One strain (85.729) very resistant to clindamycin and to erythromycin (MIC 128 pg / ml) is only moderately resistant to pristinamycin (IA + IIB) (MIC 16pg / ml).

 c) A strain (85.725) resistant to erythromycin and moderately resistant to pristinamycin (IA + IIB) (MIC 2pg / ml) remains sensitive to clindamycin.

 In conclusion, the combination of pristinamycin (1A + IIB) appears to be as effective as erythromycin or clindamycin on sensitive strains and more effective than erythromycin on strains resistant to erythromycin. On the other hand, there does not seem to be any systematic cross-resistance between clindamycin and pristinamycin. Indeed, for the strain 85.663, pristinamycin is more effective than clindamycin, while it is the opposite for another strain (85.725).

In total, this study shows the superiority of Pristinamycin over Erythromycin. It shows an activity similar to that of the
Clindamycin. However, the absence of cross-resistance with this antibiotic shows that cases of resistance to Clindamycin can be treated with Pristinamycin (and vice versa).

Claims (13)

 1. Use of a synergistin as an active ingredient in the preparation of anti-acne pharmaceutical compositions which can be administered topically, orally or rectally, said synergistin consisting of at least one streptogramin A and at least one streptogramin B.  2. Use according to claim 1, characterized in that the relative proportions, by weight, of streptogramins A and B can vary from 10: 90 to 90: 10.  3. Use according to claim 1 or 2, characterized in that the streptogramin A is chosen from virginiamycin M1, mikamycin A, pristinamycin II A or II B and vernamycin A.  4. Use according to any one of the preceding claims, characterized in that the streptogramin B is chosen from virginiamycin S, mikamycin B, pristinamycins IA, IB, IC, and vernamycins B alpha, B beta, and B gamma.  5. Use according to claim 1 or 2, characterized in that said synergistin is chosen from Virginiamycin, Pristinamycin, Streptogramin and Mikamycin.  6. Use according to claim 1 or 2, characterized in that said synergistin is present, in said pharmaceutical compositions, administered topically, at a concentration between 0.5 and 10Z by weight.  7. Use according to claim 1 or 2, characterized in that said synergistin is present, in said pharmaceutical compositions, administrable by oral or rectal route at a concentration between 0.0005 and 95% by weight, and in particular 85% for the oral route.  8. Cosmetic composition characterized in that it contains, in a suitable cosmetic carrier or vehicle, from 0.0005 to 1% by weight of a synergistin constituted by a mixture of at least one streptogramin A and at least a streptogramin B.  9. Cosmetic composition according to claim 8, characterized in that the relative proportions of streptogramins A and B can vary from 10: 90 to 90: 10 by weight.  10. Cosmetic composition according to claim 8 or 9, characterized in that the streptogramin A is chosen from virginiamycin M1, mikamycin A, pristinamycins II A or II B and vernamycin A.  11. Cosmetic composition according to any one of claims 8 to 10, characterized in that said streptogramin B is chosen from virginiamycin S, pristinamycins IA, IB, IC, mikamycin B, and vernamycins B alpha, B beta and B gamma.  12. Cosmetic composition according to claim 8, characterized in that the said synergistin is chosen from Virginiamycin, the Pristinamycin, Streptogramin and Mikamycin.  13. Use as a hygienic or cosmetic agent intended to improve the appearance of acne-prone skin, of a synergistin consisting of at least one streptogramin A and at least one streptogramin B.