JPH10513177A - Use of melatonin for the treatment of patients with drug addiction - Google Patents

Abstract

  (57) [Summary] Melatonin is more likely to relieve symptoms in patients with multidrug addiction to the drug or patients with symptoms of dependence, tolerance, or addiction to benzodiazepines, or administration of benzodiazepines And for the manufacture of a medicament for the prevention of the onset of a patient with symptoms of dependence, tolerance and addiction to the benzodiazepines mentioned above. The present invention relates to a formulation for achieving the above object, comprising at least one diluent, carrier or adjuvant, and benzodiazepines and melatonin as active ingredients.

Description

DETAILED DESCRIPTION OF THE INVENTION               Use of melatonin for the treatment of patients with drug addiction   The present invention relates to the treatment of patients who are dependent, tolerant and addictive to benzodiazepines. Used in the manufacture of a medicament for or for the prevention or treatment of patients with multidrug addiction And formulations used for such treatments.   Benzodiazepine dependence uses benzodiazepines to induce sleep. Insomnia patients, and to reduce anxiety and cramps during the course of drug withdrawal It frequently occurs in people with addictive drugs who regularly use zodiazepine. Also, benzodiaze Long-term administration of pin (long half-life of benzodiazepine) may induce tolerance There is also. Resistance was elicited when increasing the amount of use had no effect. However, the mechanism of its induction is unknown. In addition, suddenly these drugs The "rebound" or "withdrawal" phenomenon that often occurs after discontinuing use of Recognized and eventually leads to addiction (Greenblatt, D.J, Shader, R.I., Dr. ug Metab. Rev., 1987, 8: 13-28). Use of psychotherapy drugs in 1990 According to the U.S. National Family Survey, about 8% of hypnotic users It is usual to gradually increase the combined dose during use, and Has increased by 25% since 1979. This survey shows that 2.6% of the population (2.4% in the 1979 survey) account for benzodiazepines It was revealed that he was using a series of hypnotics. Judging from this number, It is estimated that 560,000 patients have any drug resistance or dependence I have. This figure includes non-therapeutic and non-social use and multidrug abuse. Not. Patients who are dependent on benzodiazepine-type hypnotics immediately start using the drug No effective new ways to stop it have yet been reported, It is a major obstacle to the rehabilitation and recovery of drug addicts.   Melatonin is an indole-induced hormone produced by the pineal gland at night. Yes, mainly involved in mediating the circadian sleep-wake cycle and regular sleep It is well known that there are. Melatonin boosts benzodiazepine efficacy There is some evidence (eg, Cardinali, D.P. et al, Adv. Biochem. Psychopharm., 1986, 42: 155-164; Acuna Castroveijo, D., et. al, J. Pineal Res., 1986, 3: 101-101; Niles, L.P. et al. Neural Transm. 70: 117-124). Melatonin also exerts an anxiety effect of diazepam in mice (Guardiola-Lemaitre, B, et al, Pha ramacol. Biochem. Behav., 1992, 41, 405-4080). On the other hand, benzodiazepines In humans and certain animals, melatonin synthesis and its secretion by GABA (cancer) Aminobutyric acid) induction (McIntyre I.M. et al, Biol. Psychi at., 1988, 24: 105-108), and in humans, benzodiazepines are Has the effect of suppressing the increase in the number of nights, which is the disorder of the circadian melatonin rhythm. (Kabuto, M. et al, Endocr. Japon. , 1986, 33, 405-414). In addition, long-term treatment with oxazepam can Alters the circadian variability of nocturnal melatonin receptor levels in the brain of rats This has not been found in pinealectomized animals (Anis, Y.e. t al, J. et al. Neural Transm., 1992, 89: 155-166).   By co-administering melatonin with benzodiazepines, (1) Weakens patient dependence, addiction, and tolerance to zodiazepines; Even in patients diagnosed as having a potential need for diazepines, Patient at a stage where the disease has not yet occurred), preventing the actual onset of such symptoms It was surprising that was discovered in the present invention.                               Description of the invention   In one aspect, the invention relates to a multidrug addicted patient or benzodiazepi To treat patients with addictive, resistant, or addictive symptoms, or However, administration of benzodiazepines is likely to reduce symptoms. For the treatment of patients diagnosed on the floor, the benzodiazepines were Manufacture of drugs to prevent the onset of patients with dependent, resistant and addictive symptoms The use of melatonin is provided.   In yet another aspect, the invention relates to a multidrug addicted patient or benzodiazepine To treat patients with addiction, resistance, or addictive symptoms to the drug, or Diagnosis is that the administration of nzodiazepines tends to alleviate symptoms. Dependence on benzodiazepines for the treatment of affected patients Used to prevent the development of patients with resistant, addictive symptoms, at least One diluent, carrier or adjuvant, and benzodiazepines as active ingredients A formulation comprising a drug and melatonin is provided.   The above drugs are preparations that can be administered orally, rectally, parenterally, and transdermally. Also contains one type of diluent, carrier and adjuvant, and at least one of the following features: A formulation with one. That is, (i) a unit dosage form, in which each (Ii) the amount of melatonin contained in the dose is in the range of 0.0025 to 100 mg; A controlled release formulation, wherein the melatonin contained therein is preferably predetermined (Iii) at least one melatonin being released at a controlled rate Receptor modifier and / or melatonin profile modifier Including In addition, the above drug, and the preparation according to the present invention, alprazolam , Chlordiazepoxide, chlorazepat, diazepam, flunitrazepam, Lulazepam, Harazepam, Lorazepam, Oxazepam, Prazepam, Temazepam Benzodiazepines consisting of at least one of triazolam Including at least. In addition, at least one of the above benzodiazepines The formulation containing also has one or more of the above characteristics (i), (ii), (iii) You.   The present invention relates to multidrug addiction patients or benzodiazepines If applied to the treatment of patients with addictive symptoms, at least Administer nzodiazepines to reduce at least one symptom Coadminister melatonin in an amount that is effective.   In specific embodiments of such treatments, benzodiazepines or mela Formulation in which any one of tonin can be administered orally, rectally, parenterally, or transdermally Wherein the dosage form comprises at least one diluent, carrier, and adjuvant. further The benzodiazepines and melatonin were separately formulated and administered separately. Or a single formulation containing both.   The dose of melatonin should be considered for co-administration with one or more benzodiazepines. Total or individual doses should be within the range of 0.01 to 10 mg per day. It is effective and the dosage form is a controlled release formulation. As an example, 1-2 mg of mela Tonin may be administered at night in the form of a controlled release formulation. Melatonin, melatonin Receptor Modifier or Melatonin Profile Modifier It may be administered in the beginning. Examples of melatonin receptor modifiers include oxa There are short-acting benzodiazepines such as Zepam, Examples of feel modifiers include benzodiazepines, beta blockers, There are serotonin uptake inhibitors. Instead of using profile modifiers In addition, or in addition, patients may be administered before, after or during melatonin administration. The melatonin profile may be modified by exposure to light.   The benzodiazepines described here are symptoms of addiction, tolerance, and addiction Is the cause of the In the present invention, a prejudice for such general properties Eliminating, for example, alprazolam, chlordiazepoxide, Chlorazepat, diazepam, flunitrazepam, flurazepam, halazepam, b One of Lazepam, Oxazepam, Prazepam, Temazepam, Triazolam The above can be used as such a drug.   Another alternative for applying the present invention to the treatment of conditions as described above. In one embodiment, the above-mentioned benzodiazepine is administered continuously continuously first, Melatonin, which was already accepted by the patient before starting the treatment Is administered in substantially the same amount as the daily dose of The invention can be used to treat such conditions In yet another embodiment where applicable, the benzodiazepines described above The systemic drug is administered in combination with melatonin, in which case the daily dose of melatonin is Than the amount of melatonin already accepted by the patient before starting treatment for Make it reduced on the floor. In this embodiment, the reduction is stepwise. Daily dose, for example, until a predetermined stable dose is reached. Or continuously until the dose of the benzodiazepine reaches zero. Give.   When the content of the present invention is used for preventive purposes, that is, benzodiazepines For patients who have been clinically diagnosed as having symptoms that are likely to be reduced by administration of At the same time, symptoms of dependence, tolerance and addiction to benzodiazepines An effective amount of a benzodiazepiate to alleviate the condition in the prevention of the development of certain patients Administer at least one such symptom at the same time A melatonin in an effective amount alone is also co-administered. Treatment of patients with the above conditions The various examples above applied to the prevention of onset at the same time apply to Exceptions are made where they cannot be applied for reasons that are self-evident. For example, In this example, treatment with benzodiazepines is absolutely essential and Clearly reduce the dose of benzodiazepines to zero This is the case. However, it may not be reduced in special cases determined by a doctor. Would.   However, for certain special purposes, benzodiazepines have been Not only can you use it in combination with melatonin at the daily dose you used Conventionally, a daily dose is administered to alleviate the above-mentioned symptoms. It is also within the scope of the prophylactic application of the present invention to administer smaller doses. You.   As explained above, the scope of the present invention covers at least one benzodiaze Formulations containing pin drugs and melatonin are included. Benzodiazepines are usually It is administered 1 to 4 times a day. In that case, the dose of concomitant melatonin per day is 0.01-100 mg, mainly administered at night. The two drugs are administered separately. When given, the dosage of benzodiazepines is preferably No.   Thus, the formulations according to the invention are in unit dose form, each dose unit comprising Preferably, the melato is administered in an amount between 0.0025 and 100 mg. It preferably contains nin.   The table below shows the benzodiazepines used for adults with the aforementioned symptoms. It shows the dose of the pharmacologic agent. Storage, half-life, dosage form, and children and infants See Goodman & Gilman, Therapeutic Drug Pharmacology, for more information on The Pharmacological Basis of Therapeutics ", 1985, 7th edition (Mac Millan Publishing's quote on the use of benzodiazepines (eg For example, see pages 352 and 437). All of these citations are referenced in this patent. See the reference.   The preparation method and release profile of the formulation according to the present invention are as follows.   (A) 2 mg / tablet, melatonin (Biosynth Co., Switzerland) and acrylic resin The carrier (Rohm Pharma) Eudragit RS100 (Edragit RS100) (Formulation S R-Ms) or Eudragit RSPO (formulation SR-Mf) After dry-mixing the powder material consisting of other components as shown separately, Compressed at 2.5 tonnes in a punch. In the case of the formulation SR-Ms, Hydragit RS100 48.8%, lactose 50%, melatonin 1. 2%, the component in the case of the formulation SR-Mf contains 35.3% of Euradit RSPO, Lactose 16.7%, calcium hydrogen phosphide 41.4%, talc 1.3 %, Magnesium stearate 4% and melatonin 1.3%. Formulation SR -Ms and SR-Mf are both sustained-release preparations.   The conventional formulation (RM) is prepared in the same manner as the formulation SR-Mf described above. However, lactose is used instead of Eudragit as a carrier.   (B) First, the release profile of the tablets described in (a) above was measured at 37 ° C. Dissolve melatonin from tablets in distilled water,In vitro(in in vitro). Table A shows the results. The amount of melatonin dissolved at each interval time is expressed in% (average of 6 tablets). Value).   (C) the SR-Mf tablet prepared as described in section (a) above;In vivo(in  vivo) The profile at which circulating melatonin levels become undetectable At 10 o'clock, a healthy male (36 years old) was administered the tablet twice orally and observed. Me Of ratoninIn vivo(in vivo) Is the major release of melatonin in urine The metabolite 6-sulfatoxymelatonin was assayed by radioimmunoassay. Quantified. The amount of 6-sulfatoxymelatonin in urine is the amount of the hormone in the blood Is fairly accurate. Table B shows the results, as a percentage of the total amount of melatonin administered. The quantified melatonin is shown by% (average value of 2 tablets).   As shown in Table A, the release of melatonin in vitro was dependent on the initial release of melatonin. Because of the well-known phenomenon that the active ingredient is absorbed into the tissue during the phase It is noteworthy that the resulting in vivo release profile is similar That is.   The amount of melatonin contained in the sustained release preparation was changed to, for example, 0.5, 1, 5 mg / tablet. In this case, the same release pattern was observed with 2 mg / tablet melatonin. The result is obtained.   Melatonin analogs with functions substantially similar to melatonin in the human body It is well known to those skilled in the art that quality is available, but such analogs Obviously, it is chemically equivalent to the melatonin used in the invention.   According to the present invention, one or more benzodiazepines are provided in an amount as described above, It may be included in the above-mentioned preparations.   The following examples illustrate the invention in more detail.                                   Example 1   Long-term combination administration of benzodiazepines and melatonin, Effects on benzodiazepine and benzodiazepine receptors and melamines that reverse these effects The ability of tonin was examined. Male rats in a bright environment for 14 hours every day, 10 hours in dark environment (bright environment from 5 o'clock, under cool white fluorescent lighting) It was kept at 24 ± 2 ° C. Food and drinking water were provided ad libitum. Rat ( (2 months after birth) were divided into 4 groups, each group having 5 animals. Of the first group (CON) Rats were injected intraperitoneally with vehicle (200 μl saline) daily at 14:00 Fired. Group 2 (VAL) rats were given diazepa daily at 14:00. (1 mg in 200 μl of vehicle; Roche) was injected intraperitoneally. Third group (MEL) Rats were injected daily with vehicle at 14:00 and this group contained melatonin. Drinking water (1 liter of 4 mg dissolved in 100 μl of ethanol) Diluted in water). Group 4 (VAL / MEL) rats daily at 14:00 Azepam (1 mg in 200 μl excipient) was injected and this group contained melatonin. Water was also given (1 liter of 4 mg dissolved in 100 μl ethanol). Diluted to Torr). The test was stopped after 21 days and the rats were weighed. VA The average weight of the L group (274 ± 20 g) and the VAL / MEL group (239 ± 30 g) was C. Less than body weight of ON group (292 ± 30 g) or MEL group (285 ± 30 g) Turned out to be small.   The next day, he was decapitated at 18-19.00 (at this time, in the medulla pons in the brain) 2-¹²⁵I-iodmelatonin is at its maximum). Take out the brain quickly, Laud on, M. and Zisapel, N., FEBS Lett, 1986, 197: 9-12, Prepare synaptosoml pellets and prepare melatonin receptor An evaluation was performed. For benzodiazepine receptors, see Amiri, Z. et al., Brain Res. , 1991, 553: 155-158,^ThreeH-flunitrazepam (^ThreeH-FNZ) When^ThreeIt was evaluated by measuring the binding of H-RO.15-1788. Binding parameters Was calculated from the equilibrium binding data. The Bmax value is 2− in the saturated state.¹²⁵ 1-iodmelatonin,^ThreeH-FNZ or^ThreeSpecific conclusion of H-RO-15-1788 The Kd value indicates the apparent dissociation constant. Binding parameters in different groups Data comparisons are analyzed for variance, followed by Student News for various comparisons. Performed by the Mann Carl test. If P <0.05, there was a significant difference. 3 Daily injection of diazepam into male rats over a week (1 mg i.p at 16.00) 2 in the medulla pons in the brain¹²⁵The concentration of I-iodomelatonin binding site was significantly Decreased (Table 1), but had no significant effect on benzodiazepine binding ( Table 2). If Melatonin Receptors Are Involved in Controlling the Sleep-Wake Cycle These results indicate that long-term administration of benzodiazepines And a subsequent decrease in bioactivity.   Melatonin administered orally with drinking water for 3 weeks is found in the medulla pons in the brain. To^ThreeAlthough the binding of H-RO.15-1788 was significantly enhanced (Tables 2 and 3), 2-¹²⁵ There was no effect on I-iodomelatonin binding. Benzodiazepine binding concentration The increase in apparent Kd values in the medulla and intramedullary pons by melatonin treatment was Matches the previously observed increase in the rat cortex and is mediated by opioid peptides (Gomar, M.D. et al, Neuroendocrinology 1993, 4 : 987-990). In addition, this enhanced binding is also seen in animals treated with diazepam The fact that melatonin and benzodiazepine This indicates that there is no conflict between.   The daily administration of both diazepam and melatonin allows the cerebral medulla pons To^ThreeIt enhances the binding of H-RO.15-1788 while simultaneously −¹²⁵Reverses the inhibitory effect of diazepam induction on I-iodomelatonin binding (Tables 1 and 2). These results are surprising, but As previously reported (Anis, Y. et al, hamster brain Melatonin binding site in: effect of melatonin, Molec. Cell. Endocrinol., 19 89, 67: 121 128; Oaknin-Bendahan, S, et al, J. Mol. Basic Clin. Physiol. Pharm acol., 1992, 3: 253-268)) or, as confirmed in this study, Whether nin is injected in the morning or night or orally in drinking water In most brain regions, including the intramedullary pontine, the concentration of melatonin binding sites and The reason is that it does not affect the daily fluctuation of the concentration. Furthermore, pineal gland cutting Removal affects phase position (Oaknin-Bendahan et al., 1992, ibid) , 2-¹²⁵Does not exclude daily variation in I-iodomelatonin binding sites. Therefore, changes in melatonin binding site concentration are dependent on melatonin receptor self-regulation. It is not for adjustment.   In the cerebral cortex, melatonin is^ThreeH-RO.15-1788 and^ThreeH-FN Z bonds were slightly reduced. In addition, diazepam treatment^ThreeH-RO ・ 15-17 88 and^ThreeNo significant effect on H-FNZ binding but melatonin-mediated binding Reduction was prevented (Tables 2, 3). First of all, we can see from these data: The effects of melatonin at the benzodiazepine binding site are Localization rather than promotion, and second, melatonin replacement therapy Neutralizes the harmful effects of long-term administration of benzodiazepines It is.   Table 1 shows rats treated with diazepam and / or melatonin and such treatments. In synaptosome preparations obtained from the medulla pontine region of rats without trauma^{12 Five} The equilibrium binding parameters of the I-iodomelatonin binding site were determined using Kd values (nM) and Bmax Values (μmol / mg protein) are shown as the mean and standard deviation, respectively. In Table 1, numerical values with the same letter have no significant difference between them. (The same applies to Tables 2 and 3 below).   Table 2 shows the rats treated with diazepam and / or melatonin and their treatment. In synaptosome preparations obtained from the medulla pontine region of untreated rats^ThreeH -The equilibrium binding parameters of the RO-15-1788 binding site were determined using the Kd value (nM) and x-value (μmol / mg protein), expressed as the mean and standard deviation You.   Table 3 shows that diazepam or melatonin in rat cerebral cortical membranes^ThreeH-FNZ When^ThreeThe effect on H-RO · 15-1788 binding was determined by the Kd value (nM) and Bmax value (μm). (mol / mg protein).                                   Example 2   In this example, melatonin promotes rapid cessation of benzodiazepine resistance I will explain the surprising effect of this. The subject is a 43-year-old woman with two children Humans have suffered from insomnia with frequent severe migraine headaches for 10 years. A thorough neurological evaluation was negative. No psychiatric or other problems Was. In the last few years, biofeedback and relaxation methods, as well as benzodiazepi Patients who had been treated with cancer drugs, tricyclic antidepressants and neurotherapies No improvement was seen. In the previous year, he used 4-8mg of lorazepam every night .   Significant pathological symptoms even after thorough psychological evaluation performed at the sleep laboratory of Tel Aviv University No condition was observed. Bedtime sleep using a small device on your wrist Sleep-Activate an actigraph trace that automatically monitors the pattern Sleep quality was assessed. Record traces for 3 consecutive days, low efficiency, long sleep latency Disturbed sleep patterns such as a late wake and many awakenings were noted. Every 3 hours (3 Urine collected at 6 hours) and can be used as an indicator of endocrine secretion of plasma melatonin. 6-Sulfatoxymelatonin, a novel melatonin metabolite, was quantified. So Results show that 6-sulfatoxymelatonin secretion levels were lower than those of the same age. , Indicating that no typical circadian rhythm was observed (Table 4).   Tablets containing 1mg melatonin for the treatment of deficiency or disorder of melatonin rhythm Of controlled release melatonin preparations (Neurim Pharmaceuticals, Israel) Oral administration was started. One tablet was administered daily at 8:30 pm. Until then drink every night Patients were instructed to reduce the number of benzodiazepines they had. Surprisingly , On the second day after the administration of the above melatonin preparation, the patient was treated with benzodiazepine hypnosis. He stopped using the drug altogether and noticed a marked improvement in insomnia. In addition, for headaches It was gradually subsided. After 3 weeks of treatment, actigraph As a result, a marked improvement in sleep patterns was observed.   Two weeks after discontinuation of treatment, urine was again collected every 3 hours (36 hours) and -Sulfatoxymelatonin was quantified. What can be seen from the results (Table 4) Indicates that the amount of 6-sulfatoxymelatonin in urine increases quantitatively and a clear nocturnal peak It is showing that. After 5 months of follow-up, this patient Quality can be maintained normally and the headache is completely cured . However, after stopping treatment for 6 months, the quality of sleep deteriorated and melatonin treatment was stopped. Resumed.   In this case report, treatment with melatonin has shown that quality of life is benzodiazepine-based. Demonstrating that it can be a breakthrough for many patients who are exacerbated by sleep-adding addiction I have. In addition, exogenous melatonin administration may be resistant to benzodiazepines. To serve as a fast, asymptomatic, withdrawal method for a patient Indicates that it can be done.                                   Example 3   This example illustrates the use of melatonite in the treatment of insomnia in benzodiazepine-dependent patients. This shows the effect of long-term administration of the drug.   80-year-old man Y. L. And a 73-year-old woman E. L. Have been volunteering for many years Insomnia and / or frequent awakening at night, and once awake, She has suffered from the difficulty of sleeping. 6 which is urinary metabolite of melatonin -By quantifying sulfatoxymelatonin, the melatonin content of both patients It turned out to be less secreted. Both patients received 1-2 mg of flunitrase daily before going to bed. He was taking Pam orally.   The dose of flunitrazepam to each patient was gradually reduced, and at the same time melatonin (release Oral administration of flunitraze for 2 months in a controlled dosage form Removed from Pam. Even after the end of that period, each patient will receive the same dosage form of melato Nin continued to be administered at the same dose for approximately two years.   Each patient had better sleep and was better able to subjectively improve sleep quality. I admitted that. In particular, patient E. L. First stopped taking flunitrazepam Improved sleep quality at the early stages of the disease. L. Then, in the second week of the complete suspension, Various effects were recognized. In all patients, stop taking flunitrazepam. Early in the day, fatigue during the day was reduced, and melatonin Admitted that there was no fatigue and no fuss. Side effects were observed in all patients Was not.                                   Example 4   This example demonstrates long-term use of benzodiazepines in a randomized, double-blind, cross-over study. Explains the Effect of Melatonin Replacement Therapy for Improving Sleep in Elderly Patients It is.   Subjects were eight men and five women with an average age of 78 (standard deviation = 9.7) Group, all using a variety of benzodiazepines to induce sleep. Patient with long-term insomnia. Collect urine every 4 hours for 15 hours, Nocturnal secretion of 6-sulfatoxymelatonin, a key urinary metabolite, was It was quantified again. Urine analysis of these patients showed that 6-sulfatoxymelatonin Secreted in small amounts and delayed (a young adult secreted 25 μg / min.). , Whereas these patients had less than 14 μg overnight). This test Protocol consists of two treatment periods (one period is three weeks). A one-week wash-out period is provided during the period. This During the treatment period, patients receive 2 mg of controlled release melatonin tablets or placebo. Either of them was orally administered 2 hours before going to bed. Melatonin treatment for 5 patients It continued for two months after the initial test period.   At the end of each treatment, the patient's sleep was monitored by an actigraph attached to the wrist. It was evaluated three consecutive nights. For each subject, record movements Analyzed using algorithms, sleep latency, sleep efficiency, total sleep time, sensation after falling asleep The number of times of awakening and awakening was determined as an average of three nights. Six Wilcoxun marks The Merck Rank Test (Wilcoxon matched-pairs signed-ranks analyzes) There is a statistically significant difference in sleep parameters between treatment cycle ranks for tonin and placebo. It turned out to be. Table 5 shows the results.   Based on the above results, melatonin replacement therapy uses benzodiazepines Improve sleep onset and duration in elderly people with low endogenous melatonin secretion Conclusion. The effect of melatonin treatment increases with time, This suggests that a restructuring of the circadian mechanism is taking place.

[Procedure for Amendment] Article 184-8, Paragraph 1 of the Patent Act [Date of Submission] February 19, 1997 [Content of Amendment] By administering melatonin in combination with benzodiazepines, (1) patients receiving benzodiazepines Even in patients diagnosed as having a potential for addiction, addiction, tolerance, and (2) a need for a benzodiazepine drug (patients who have not yet developed symptoms), the actual It was surprising that the present invention was found to be able to prevent the onset. Cited Prior Art Approval EP-A-513 702 describes the use of melatonin and its derivatives, optionally in the presence of benzodiazepines, in the treatment of sleep disorders and as a medicament before anesthesia. According to this description, benzodiazepines can be administered at relatively low doses, and such administration of benzodiazepines has effects associated with administration of benzodiazepines at high doses or over a long period of time (changes in sleep rhythms). , Counter-operation, and resistance). However, the description states that doses of 10 mg or less of melatonin or its derivatives can be used for the above purpose, and that melatonin already shows dependence, tolerance and addiction to benzodiazepines. It is not described as being effective in patients. EP-A-518468 briefly describes controlled release formulations that release melatonin according to a profile similar to that in human plasma with a normal endogenous melatonin profile. It also states that preparations optionally containing a melatonin receptor profile modifier, such as oxazepam, are useful for treating diseases associated with melatonin deficiency and abnormal melatonin secretion, such as sudden infant death syndrome and migraine. . However, it does not suggest the use of melatonin in the prevention and treatment of addiction to benzodiazepines. In dialog file supplier PHIND.AN00302794,13-03-92, for example, in insomnia patients after discontinuation of benzodiazepine dosing, indole-3-pyruvate (IPA) increases sleep time and reduces Such effects have been reported to be mediated primarily by increased melatonin turnover in the pineal gland. However, this report does not suggest the use of melatonin in the prevention and treatment of addiction to benzodiazepines. DESCRIPTION OF THE INVENTION The present invention is directed to treating addiction to benzodiazepines in multidrug addiction patients or patients with addiction, tolerance, and addictive symptoms to benzodiazepines, or alleviating symptoms with administration of benzodiazepines Melatonin in the manufacture of a medicament for the treatment of a patient who is clinically diagnosed as being susceptible to the condition, while at the same time preventing the onset of a patient having dependence, tolerance, and addictive symptoms to the benzodiazepines. The use, wherein the medicament comprises at least a therapeutically effective amount of melatonin, the amount of which is used to treat a patient clinically diagnosed as having a condition that is likely to be alleviated by administration of a benzodiazepine drug. In this case, the daily dose is in the range of 0.01 to 100 mg, and the drug is a sustained-release preparation. Use of melatonin in the manufacture of a medicament, comprising up to 5 mg melatonin. Thus, the formulations according to the invention are in unit dose form, each unit dose preferably being administered at night and preferably containing an amount of melatonin in the range of 0.0025 to 100 mg. The following table shows the dosage of benzodiazepines used for adults with the above-mentioned symptoms. For more information on storage, half-life, dosage forms, and dosages for children and infants, see Goodman & Gilman, The Pharmacological Basis of Therapeutics, 1985, 7th Edition ( See Mac Millan Publishing), citing the use of benzodiazepines (eg, pages 352, 437). The preparation method and release profile of the formulation according to the present invention are as follows. (A) 2 mg / tablet Melatonin (Biosynth Co., Switzerland) and Eudragit RS100 (trade name: Eudragit RS100) which is an acrylic resin carrier (Rohm Pharma) (formulation SR-Ms) or Eudragit RSPO (trade name: Eudragit RSPO) (Formulation SR-Mf) A powder material composed of other components as shown separately from the above was dry-mixed, and then placed in a 7 mm cylindrical punch and compressed at 2540 kg (2.5 tons). In the case of the formulation SR-Ms, Euradit RS100 (trade name) is 48. In the case of 8%, 50% lactose, 1.2% melatonin, and formulation SR-Mf, the components of Eudragit RSPO (trade name) are 36.3%, lactose is 16.7%, and calcium hydrogen phosphide is 41. 0.4%, talc 1.3%, magnesium stearate 4%, melatonin 1.3%. The preparations SR-Ms and SR-Mf are both sustained-release preparations. The conventional preparation (RM) is prepared in the same manner as in the preparation SR-Mf described above, but using lactose instead of Eudragit (trade name) as a carrier. Claims 1. To treat addiction to benzodiazepines in patients with multidrug addiction or who have symptoms of dependence, tolerance, or addiction to benzodiazepines, or that benzodiazepines tend to alleviate the symptoms clinically. The use of melatonin in the manufacture of a medicament for the treatment of a diagnosed patient, while at the same time preventing the onset of a patient with symptoms of dependence, tolerance, addiction to said benzodiazepines, said medicament comprising: Contains at least the therapeutically effective amount of melatonin, the amount per day in the case of treatment of a patient clinically diagnosed as being in a condition that is likely to be alleviated by administration of a benzodiazepine drug. The dosage is in the range of 0.01 to 100 mg, and the drug is a sustained-release preparation, and 5 mg or less of melatonin. Use of melatonin in the manufacture of a medicament, including. 2. Use of melatonin according to claim 1 in the manufacture of a medicament for the treatment of addiction to benzodiazepines in patients with multidrug addiction or patients with symptoms of dependence, tolerance and addiction to benzodiazepines. 3. 3. The use according to claim 2, wherein said medicament is a sustained release formulation and contains no more than 5 mg melatonin. 4. For the treatment of patients clinically diagnosed as being in a state where symptoms are likely to be alleviated by administration of benzodiazepines, at the same time, onset of dependence, tolerance, addiction symptoms to the above benzodiazepines The use of melatonin in the manufacture of a sustained release medicament for the prevention of melatonin, said medicament comprising at least said therapeutically effective amount of melatonin, the amount of which may be in the range of 0.01 to 0.01 mg / day. Use of melatonin according to claim 1 in the range of 100 mg. 5. The use according to any one of claims 1 to 4, wherein said medicament is a formulation capable of oral, rectal, parenteral and transdermal administration and comprises at least one diluent, carrier or adjuvant. 6. When the above-mentioned preparation is (i) a unit dose dosage form and not a sustained release preparation, the amount of melatonin contained in each unit dose is in the range of 0.0025 to 100 mg, and if the preparation is a sustained release preparation, (Ii) if it is a sustained-release preparation, it is a controlled-release preparation, and the melatonin contained therein is released at a predetermined controlled rate; 6. Use according to claim 5, characterized in that it comprises at least one of (iii) at least one melatonin receptor modifier and / or melatonin profile modifier. 7. The formulation comprises at least one benzodiazepine drug, wherein the benzodiazepine drug is preferably alprazolam, chlordiazepoxide, chlorazepat, diazepam, flunitrazepam, flurazepam, halazepam, lorazepam, oxazepam, prazepam, temazepam, triazolam. 7. Use according to any of the preceding claims, comprising at least one of the above. 8. The treatment includes co-administration of a benzodiazepine and a melatonin, wherein the benzodiazepine is gradually increased in a daily dose until a predetermined stable daily dose can be achieved. The use according to any one of claims 1 to 7, which is administered while reducing the weight. 9. The treatment includes co-administration of a benzodiazepine and melatonin, wherein the benzodiazepine is administered in gradually decreasing daily doses until the patient is ready to completely withdraw from the benzodiazepine. Use according to any one of claims 1 to 7.

────────────────────────────────────────────────── ─── Continuation of front page    (81) Designated countries EP (AT, BE, CH, DE, DK, ES, FR, GB, GR, IE, IT, LU, M C, NL, PT, SE), OA (BF, BJ, CF, CG , CI, CM, GA, GN, ML, MR, NE, SN, TD, TG), AP (KE, LS, MW, SD, SZ, U G), UA (AZ, BY, KG, KZ, RU, TJ, TM ), AL, AM, AT, AU, AZ, BB, BG, BR , BY, CA, CH, CN, CZ, DE, DK, EE, ES, FI, GB, GE, HU, IS, JP, KE, K G, KP, KR, KZ, LK, LR, LS, LT, LU , LV, MD, MG, MK, MN, MW, MX, NO, NZ, PL, PT, RO, RU, SD, SE, SG, S I, SK, TJ, TM, TR, TT, UA, UG, US , UZ, VN

Claims (1)

[Claims]   1. Dependence, tolerance, preference for multidrug addiction patients or benzodiazepines To treat patients with addictive symptoms or to administer benzodiazepines For the treatment of patients who are clinically diagnosed as being in a condition where symptoms are likely to be reduced, At the same time, dependence, tolerance, and addictive symptoms on the benzodiazepines Use of melatonin in the manufacture of a medicament for preventing the onset of a patient.   2. The above drug is a preparation that can be administered orally, rectally, parenterally, or transdermally. Use according to claim 1, which comprises at least one diluent, carrier or adjuvant.   3. The above-mentioned preparation is (i) a dosage form having a unit dose, and a medicament contained in each unit dose. The amount of ratonin is in the range of 0.0025-100 mg; (Ii) a controlled release formulation wherein the melatonin contained therein is preferably predetermined A dosage form that is released at a controlled rate, (Iii) at least one melatonin receptor modifier and / or mela Including the Tonin Profile Modifier, 3. Use according to claim 2, having at least one of the following characteristics:   4. 3. The formulation of claim 2 wherein the formulation comprises at least one benzodiazepine drug. Is the use described in 3.   5. The benzodiazepines are alprazolam, chlordiazepoxy Do, chlorazepat, diazepam, flunitrazepam, flurazepam, halazepam , Lorazepam, Oxazepam, Prazepam, Temazepam, Triazolam 5. Use according to claim 4, comprising at least one.   6. Dependence, tolerance, preference for multidrug addiction patients or benzodiazepines To treat patients with addictive symptoms or to administer benzodiazepines At the same time, for the treatment of patients who are diagnosed Patients with dependence, tolerance and addictive symptoms to the aforementioned benzodiazepines At least one diluent, carrier or supplement used to prevent the Auxiliaries and products containing benzodiazepines and melatonin as active ingredients Agent.   7. Oral, rectal, parenteral, transdermal administration is possible, and the formulation is i) The dosage form is a unit dosage, and the amount of melatonin contained in each unit dosage is Being in the range of 0.0025-100 mg, (Ii) a controlled release formulation wherein the melatonin contained therein is preferably predetermined Released at a controlled rate, (Iii) at least one melatonin receptor modifier and / or mela Including the Tonin Profile Modifier, The formulation of claim 6, having at least one of the following characteristics:   8. The benzodiazepines are alprazolam, chlordiazepoxy Do, chlorazepat, diazepam, flunitrazepam, flurazepam, halazepam , Lorazepam, Oxazepam, Prazepam, Temazepam, Triazolam The preparation according to claim 6, comprising at least one.