Drug – bio-affecting and body treating compositions – Designated organic active ingredient containing – Peptide containing doai
Reexamination Certificate
2000-01-18
2001-12-11
Jarvis, William R. A. (Department: 1614)
Drug, bio-affecting and body treating compositions
Designated organic active ingredient containing
Peptide containing doai
C514S033000
Reexamination Certificate
active
06329339
ABSTRACT:
This application is a 371 of PCT/EP98/02,797, filed May 6, 1998.
This invention relates to a pharmaceutical antiviral composition comprising glycyrrhizic acid and at least one protein endowed with antiviral activity.
It is known that the Herpes Simplex Virus type 1 causes facial and oropharyngeal lesions (“Manual of Clinical Microbiology”, Murray, Baron, Pfaller, Tenover, Yolken, 6
th
edition, pages 876-883, American Society for Microbiology, Washington D.C., 1993).
In the past infections from Herpes Simplex Virus type 1 were treated with vidarabin (Goodman & Gilman, “Le basi farmacologiche della terapia”, Zanichelli, Bologna, 7
th
ed., page 1156, 1991) but this has been almost completely replaced by aciclovir (Goodman & Gilman, “The Pharmacological Basis of Therapeutics”, McGraw Hill Companies, 9
th
ed., chapter 50, page 1193, 1996; “Am. J. Med.”, 73, Suppl., 186-192, 1982 and “Clin. Pharmacokinet.”, 8, 187-201, 1983) because of its toxicity.
Currently, aciclovir is therefore the most used drug in the treatment of mouth and lip lesions (rash from fever) but its topical use often causes burning and irritation of mucous membranes. Moreover, aciclovir is fairly efficient when administered during the first infection, but is not very effective in the case of recurring infections, thus being non-resolutive and not preventing re-infection by Herpes Simplex Virus type 1.
Additionally, oral treatment has the disadvantage of causing side effects such as nausea, diarrhoea, itching, headaches, renal inadequacies and nephrotoxicity.
Therefore, there is still a real need for a drug which is active in the treatment of infections from Herpes Simplex Virus type 1 even in the case of recurring infections and which is free from side effects.
Indeed, it has also been known that glycyrrhizic acid shows a certain antiviral activity. At antiviral doses, it largely inhibits the synthesis of viral glycoproteins and only at very high doses does it also inhibit the cell glycoproteins synthesis. In fact while the action of the glycyrrhizic acid on the synthesis of proteins, both in normal cells and infected cells, is practically irrelevant even at doses of 4 mM, the synthesis of glyco-proteins shows a substantial difference in normal and infected cells. In fact, at the concentration of 0.5 mM (which inhibits 50% of viral replication) glycyrrhizic acid causes a reduction in the incorporation of glucosamine-H
3
of more than 10% in infected cells and no inhibition in normal cells. An increased dose of glycyrrhizic acid up to 1 mM, causes an 80%reduction of the virus, no inhibition of the synthesis of glyco-proteins in the control and a 20% reduction in the synthesis of glyco-protein in infected cells. At 4 mM, the synthesis of glyco-proteins in the normal cells is also slightly altered, but the production of the virus is inhibited by 99% (“L'Igiene Moderna”, Pompei R. and Marcialis M. A., 83, 385-391, 1985).
Furthermore, Table A shows the results of tests carried out treating cells infected by HSV1 with 8 mM glycyrrhizic acid. The infected cells have been kept in contact with the glycyrrhizic acid for 2 hours at 37° C. The experimental results given in the Table show that there is a strong decrease in infection at 12, 17 and 22 hours and that the cells retain their cellular integrity. The inhibition is of about 2 logarithms at 12 hours from the infection and 3 logarithms (99.9%) at 22 hours from infection (“Nature”, Pompei R. et al., 281, No. 5733, 689-690,1979).
TABLE A
Viral production (PFU*/ml) after the following hours
Hours
12
17
22
Control
3 × 10
6
5.4 × 10
6
2.6 × 10
7
Glycyrrhizic acid 8 mM
4.2 × 10
4
1.2 × 10
4
1.1 × 10
4
*PFU = plaque forming viral unit.
It is also known in the literature the antiviral activity and, more specifically, anti-herpetic (HSV1) activity of various types of lysozymes such as turkey lysosyme, human lysozyme, chicken lysozyme, denaturated (heat-inactivated) chicken lysozyme and chicken lysozyme digested with trypsin (“Current Microbiology”, Cisani et al., 10, 35-40, 1984).
Lysozymes are, in fact, enzymes which are widely spread in nature and cooperate in the defense of the organism against some infecting agents by causing or cooperating to the cleavage (i.e. lysis) thereof (“Mol. Cell. Biochem.”, Jolles et al., {grave over (63)}, 165-189, 1984; “Anticancer Res.”, Save et al., 9, 583-592, 1989).
Moreover, in the literature it is described the antiviral activity and, more particularly, the antiherpetic (HSV1) activity of lactoferrin (Fujihara T. and Hayashi H. “Lactoferrin inhibits herpes simplex virus type 1 (HSV1) infection to mouse cormea”, “Arch. Virol.”, 140, 1469-1472, 1995; Harmsen MC. et al. “Antiviral effects of plasma and milk protein: lactoferrin shows potent activity against both human immunodeficiency virus and human cytomegalovirus replication in vitro”, “J. Inf. Dis.”, 172, 380-388,1994).
It has now surprisingly been found that glycyrrhizic acid has a synergetic effect on the proteins endowed with antiviral activity.
Therefore, it is a first object of this invention to provide a pharmaceutical composition characterized in that it comprises glycyrrhizic acid and at least one protein having antiviral activity.
Preferably, the protein is selected from the group comprising the lysozymes and the lactoferrins.
Typical examples of lysozymes are turkey lysozyme, human lysozyme, chicken lysozyme, heat-inactivated chicken lysozyme and chicken lysozyme digested with trypsin. Preferably, the lysozyme is a chicken lysozyme or a human lysozyme.
Typical examples of lactoferrins are bovine and human lactoferrins.
Typically, the pharmaceutical composition of this invention is useful in the treatment of topical viral infections. Preferably, the virus is of a herpetic type. Even more preferably it is the Herpes Simplex Virus type 1 (HSV1).
Preferably, the pharmaceutical compositions of this invention are prepared in the form of suitable dosage forms. Examples of suitable dosage forms are creams, ointments and medicated plasters, for topical administration.
The dosage forms may also contain other conventional ingredients, such as: preservatives, stabilisers, surfactants, buffers, salts to regulate osmotic pressure, emulsifiers, sweeteners, colouring agents, flavouring agents and the like.
The amount of active ingredients in the pharmaceutical composition of this invention may vary within a wide range depending on known factors such as, for example, stage and severity of the infection, body weight of the patient, type of the dosage form, administration route, number of dosage forms administered per day and the efficacy of the active ingredients. However, the optimum amount will be determined readily and routinely by a person skilled in the art.
Preferably, the amount of glycyrrhizic acid, a lysozyme and/or a lactoferrin in the dosage form of this invention will be such that it ensures a daily administration of 0.25-8 mg/ml of glycyrrhizic acid, 0.5-10 mg/ml of lysozyme and/or 0.1-4 mg/ml of lactoferrin. Even more preferably, it will be such that it ensures a daily administration of 0.5-2 mg/ml of glycyrrhizic acid, 0.5-4 mg/kg of lysozyme and/or 0.25-1 mg/kg of lactoterrin. The dosage forms of the pharmaceutical composition of this invention may be prepared according to techniques which are well known to the pharmaceutical chemist, and comprise mixing, granulation, compression, dissolution and the like.
The following examples are intended to illustrate this invention without limiting it in any way.
The compounds used in the experiments were:
glycyrrhizic acid (as ammonium salt) supplied by FLUKA AG;
Herpes Simplex Virus type 1 supplied by the NIH, Rockville, Md.;
chicken lysozyme supplied by SIGMA;
lactoferrin supplied by SIGMA;
VERO cell from kidney of African green monkey from ICN FLOW, Costa Mesa, Calif.;
Eagle medium modified by Dulbecco (DMEM), added with calf foetal serum, inactivated for 30′ at 56° C., supplied by ICN FLOW, Costa Mesa, Calif.
REFERENCES:
Fukahori et al, Japanese Patents Abstracts,
Pinza Mario
Pompei Raffaello
Aziende Chimiche Riunite Angelini Francesco A.C.R.A.F. S.p.A.
Jarvis William R. A.
Oblon & Spivak, McClelland, Maier & Neustadt P.C.
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