UA51640C2 - Method for preventing establishment or reactivation of latent infection of herpes viruses - Google Patents

Abstract

A method for preventing the establishment or reactivation of latent infection of herpes viruses in humans which comprises administering to the human in need of such treatment, an effective amount of a compound of formula (A) or a bioprecursor, or a pharmaceutically acceptable salt, phosphate ester and/or acyl derivative of either of the foregoing. (А)

Description

Description of the invention

This invention relates to the treatment of latent infections caused by herpes viruses. As used herein, the term "treatment" includes prophylaxis where appropriate.

ER-A-141927 (Vespat Ogoir r.I.s.) discloses penciclovir, a compound of the formula (A): (A) 6)

M is | Mn

Zh i mosmn, 7 (Csnoi nosnyInsnyon and its salts, phosphate esters and acyl derivatives as antiviral compounds. Penciclovir sodium salt hydrate is disclosed in EP-A-216459 (Vespat (zgocr r.I.s.). Penciclovir and its antiviral activity is also described in the abstract of R. MII-5, p. 193 of the publication "Arvigasiv oi 14(i Ipi Sopodgezvi oi Misgobioiodu",

Mapspezieg, Epdiapa, 7-13 Zerietreg 1986 (Voua ei ai). with

Bioprecursors of the compound of the formula (A) that are active when taken orally are the compounds of the formula (B): o (c) x

M m | "c) "Zh Khri rya

I m smn, Te "- (SN); | ю но-сн, сН-сН, ОН 20 and their salts and derivatives determined by formula (A); where X is C1-6 alkyl, MNO or hydrogen. Compounds of the formula (B), in which X is a C.6 alkyl or MH2, are disclosed in EP-A-14927, and compounds of the formula (B), in which X is hydrogen, are disclosed in EPA-182024 (Veespat sgoyr r. 1.p.), are the preferred prodrugs. The best example of a compound of formula (B) is a compound in which X is hydrogen and in which two OH groups are in the form of an acetyl derivative, described in example 2 of EP-A-182024, hereinafter referred to as famciclovir.

Compounds of formulas (A) and (B) and their salts and derivatives are described as useful in the treatment of infections caused by herpes viruses such as Negrez zitriech type 2.

Previous work has shown that if antiviral treatment is delayed for more than a few hours after infection, then latency is established. If the latency of the infection is established, the infection may recur.

So far, it has been shown in mice that treatment with famciclovir can prevent the establishment of competent latency when the treatment begins 18 hours (first experiment) and up to 4 days (second experiment) after infection. At this time, it was also shown that latency can be prevented in an experiment on mice with a compromised immune system. A potential clinical advantage is that the patient can be treated with famciclovir within 4 days of exposure to prevent not only acute infection, but also the development of latency and thus avoid relapses. In addition, it is believed that there may be a slow natural loss of latently infected cells, and re-infection may be required to maintain the presence (F) of latently infected cells by establishing latency in new cells. Therefore, treatment is preferred

GI famciclovir over the long term (up to several years) may prevent new cells from becoming latently infected. Then the result will be a radical cure, and after that the patient will not have relapses.

Accordingly, the present invention provides a method of treating a latent infection caused by a herpes virus in humans, which comprises administering to a subject in need thereof an effective amount of a compound of formula (A): , OH or its bioprecursor, or a pharmaceutically acceptable salt, phosphate ester and/or acyl derivative t5 of any of the above-mentioned compounds.

The term "acyl derivative" is used herein to include any derivative of a compound of formula (A) wherein one or more acyl groups are present. Such derivatives are included as bioprecursors of compounds of formula (A) in addition to those derivatives that are biologically active in themselves.

The compound of formula (A) can be in one of the forms disclosed in ER-A-216459 (Vespat mountains r.I.s.).

Exemplary bioprecursors, pharmaceutically acceptable salts and derivatives are compounds described in the aforementioned European patents, the subject matter of which is incorporated herein by reference.

A particular compound of formula (B) of interest is 9-(4-acetoxy-3-acetoxymethylbut-1-yl)-2-aminopurine, known as famciclovir (FCV), a well-absorbed oral form of penciclovir. high school

The compound of formula (A), bioprecursors, salts and derivatives can be prepared as described in the above-mentioned European patents.

The compound, particularly famciclovir, can be administered parenterally to humans and can be formulated into a syrup, tablet, or capsule form. When it is made in the form of tablets, any pharmaceutical carrier suitable for obtaining such solid compositions can be used, for example, stearate. magnesium, starch, lactose, glucose, rice, flour and chalk. The compound may also be presented in the form of ingestible capsules, such as gelatin, containing the compound, or in the form of a syrup, solution or suspension. Suitable liquid pharmaceutical carriers include ethyl alcohol, glycerin, saline and water to which flavoring and coloring agents may be added to form a syrup. There are also long-term release dosage forms, for example, coated tablets that dissolve in the intestines.

For parenteral administration, liquid dosage forms are produced in the form of single doses containing the compound and a sterile carrier. The compound, depending on the carrier and concentration, can be either suspended or dissolved. Parenteral solutions are usually prepared by dissolving the compound in a carrier and filter-sterilizing before filling into either a suitable container or ampoule and sealing. It is desirable that - adjuvants such as local anesthetics, preservatives and buffer substances are also dissolved in the carrier. To increase stability, the composition can be frozen after filling the vessels, and the water can be removed under vacuum.

Parenteral suspensions are prepared in essentially the same manner, except that the compound is suspended in a carrier instead of dissolved and sterilized by exposure to ethylene oxide prior to suspension in a sterile carrier. pg 35 It is advisable to include a surface-active agent or a wetting agent in the composition to facilitate uniform distribution of the compound of the invention. - Preferred parenteral dosage forms include aqueous dosage forms using sterile

FU of water or saline with a pH of about 7.4 or greater, particularly containing penciclovir sodium hydrate. t» 50 As is usually accepted in practice, the compositions are usually accompanied by written or printed instructions for use in the corresponding medical treatment.

A suitable unit dose (dosage form) may contain from 50 mg to 1 g of active ingredient, for example 100 - 500 mg. Such doses may be administered 1-4 times a day, or more commonly, 2 or 3 times a day. An effective dose of the compound will generally be in the range of 0.2 to 40 mg per kg of body weight per day or, more typically, 10 to 20 mg/kg per day. In the case of famciclovir, a single dose is 125 mg,

GF) 250 mg, 500 mg or 750 mg, preferably 125 mg or 250 mg.

HF To prevent the formation of competent latency, treatment is preferably carried out as soon as possible after contact with the virus, preferably within 18 hours, although it is acceptable to start it within 4 days. The treatment period is usually 3-14 days, more usually 5-10 days, often 7 days.

For the treatment of an established recurrent disease, the treatment period is up to 5 years, for example, up to 1, 2, 3, 4 and 5 years.

The present invention also provides the possibility of using a compound of formula (A) or a bioprecursor, or a pharmaceutically acceptable salt, phosphate ester and/or acyl derivative of any of the specified compounds for the manufacture of a medicament for use in the treatment of latent infection caused by herpes 65 viruses. Such treatment may be carried out in the manner described hereinbefore.

The present invention further provides a pharmaceutical composition for use in the treatment of a latent infection caused by herpes viruses, which comprises an effective amount of a compound of formula (A) or a bioprecursor, or a pharmaceutically acceptable salt, phosphate ester and/or acyl derivative of any of the compounds , and a pharmaceutically acceptable carrier. Such compositions can be made in the same manner as described below.

The compound of formula (A) and its prodrugs exhibit a synergistic antiviral effect in combination with interferons; and therefore treatment using combined products including these two components for sequential or simultaneous administration by the same or different routes is covered by the scope of this invention. 70 The following results of animal studies illustrate the invention.

Studies on mice infected with NeM-1 virus

Each infection was created by inoculation into the earlobe of NZMU-1 (ZS16) mice and the effect of oral famciclovir on latent viral infection was investigated.

Female mice of VAI V/s (Vapiip apa Kipdtap, Kipoviop, Nyii, OK) were purchased at the age of 3-4 weeks and /5 Infected one week later. A virus suspension (10 μl) containing 5 x 104 b.u.e. was inoculated into the skin of the left earlobe. The thickness of the skin was measured every day in individual mice with the help of a screw micrometer (Mav ei a!I., 1980 9. Szep. Migoi. 48, 351 - 357). These mice were maintained for 3 (experiment 1) or 4 (experiment 2) months and then sacrificed. Trigeminal node and cervical dorsal node were removed and cultured together, those cultures showing viral replication were recorded as positive.

Experiment 1

In the first experiment, mice were treated within 18 hours and treatment was stopped on the 10th day after infection.

Of the 24 untreated control mice, 12 had a latent infection in the trigeminal ganglion (TG) and 20 had a latent infection in the cervical dorsal root ganglion (DCG). All 24 control mice showed either TG or DCG latency. None of the FCV-treated mice showed any latency.

Experiment 2

In the second experiment, antiviral treatment was started on days 2, 3, 4, and 5 after infection (p.i.) and stopped on day 10 p.i. The compounds were given with drinking water without restrictions at a concentration of mg/ml of zo (approximately 100 mg/kg/day).

The results are presented in the following table: - (Note: groups 1 and 2 received the same treatment courses, but the results were analyzed separately.) Ge

SHA

1) (group 2)

And J

(days) Twe/8 Nwe/8 Twe/8 Nwe/8 day 120 day 8

LPLP o lLplP 0 (pe 16) L/PTG i DKG (n - 8) L/PTG i DKG « 2 not with PE st NN PNT NN NO . piMYIE t NI NSS NO NO 2 po ET U U t PO

After four months, latent virus could be reactivated in explants of ganglia (ipsilateral and 1 contralateral trigeminal and dorsal root) from all 16 control mice. Latent virus was not reactivated from the ganglia of FCV-treated mice, with the exception of the ipsilateral ganglia, and only when the start of therapy was delayed until 4 days p.i. (2/16) or 5 days p.i. (6/16).

Ge) Similar results were obtained when the compounds were administered twice daily by gavage at 50 mg/kg per dose. f Experiment C 2 Mice were subjected to immunosuppression with cyclosporin A (CyA) from day -2 to day -10 (with day 0 being the day of infection). Groups of mice were: untreated (control) or treated with famciclovir orally at a dose of 50 mg/kg twice daily starting at 22 hours post-infection until 5.5 or 10.5 days. The ganglia were examined for reactivation of the infecting virus after 1 or 4 months, and the results are shown in the table below. yu rt t tv

GI (p-6) (p-6) (p-6) (p-6) life. 16|4,8, 3 o vv010101 o

DCG-dorsal root ganglion L/P-left/right

Experiments on mice infected with the NZM-2 virus

Each infection was created by inoculation into the earlobe of H5 M-2 (Vhu) mice and the effect of oral famciclovir on latent viral infection was investigated. Treatment consisted of 50 mg/kg twice a day for 5 days starting 22 hours after infection.

The table shows the number of mice/group with positive latent infection in the trigeminal or cervical dorsal root ganglia.

The number of mice with "ve ganglia/ (95, which gave at least one ve ganglion 9 the number of studied mice

Group Left Right / Left) Right trade CDK OO udk

T/G-triple

CAK-cervical dorsal root ganglion

Claims (5)

The formula of the invention 1. A method of hindering the establishment or reactivation of a latent infection caused by herpes viruses in humans, which includes the administration of a medicinal product, which is characterized by the fact that a medicinal product containing as an active component the compound of the formula (A) (А) І M / МН AH. sch ra Y MO sm, o (sleep); "c) zo / nHOe-CH,CH-CH.,OH" or its bioprecursor, or a pharmaceutically acceptable salt, phosphate ester and/or acyl derivative of any of the preceding compounds, and the specified medicinal product is administered at least 18 hours after infection 2. The method according to claim 1, which differs in that the latent infection is an infection caused by the virus "-- z5 herpes simplex type 1. C. The method of claim 1, wherein the latent infection is an infection caused by herpes simplex virus type 2. 4. The method according to claim 1, which differs in that the compound is famciclovir. 5. The method according to claim 1, which differs in that famciclovir is administered in a dose of 125 mg, 250 mg, 500 mg, 750 mg or "1 hour, two or three times a day. 20 dyn, dry r d -o s Official bulletin "Industrial Property". Book 1 "Inventions, useful models, topographies of integrated microcircuits", 2002, M 12, 15.12.2002. State Department of Intellectual Property of the Ministry of Education and Science of Ukraine. 1 - (o) Cheka" (42) name) 60 b5