JP2009084253A - Prophylactic and/or therapeutic drug for headache - Google Patents

Abstract

<P>PROBLEM TO BE SOLVED: To provide a new prophylactic and/or therapeutic drug for headache, which is effective in patients who cannot get sufficient results by taking existing therapeutic drugs for headache. <P>SOLUTION: Administration of a thyroid hormone at a dose lower than that prescribed for hypothyroidism effectively can relieve headache by shortening the time to onset of actions of the existing drugs or reducing the occurrence of, eliminating, etc., headache attacks in patients who cannot achieve sufficient results by taking the existing therapeutic drugs for headache. When combined with the use of the existing prophylactic and/or therapeutic drug for headache, the administration of the thyroid hormone can reduce doses of the existing drugs. <P>COPYRIGHT: (C)2009,JPO&INPIT

Description

  The present invention relates to a preventive and / or therapeutic agent for headache comprising thyroid hormone as an active ingredient.

  Headache is a general term for deep pain in the head. Headache is a common physical complaint that many people experience. Most of them are migraines, cluster headaches and tension headaches, most of the chronic headaches are functional headaches, including tension headaches, migraines and a mixture of both. Some of them are strongly influenced by psychological and social factors in addition to constitutional predisposition. These headaches are functional headaches that develop due to stress, mental tension or muscle tone, and are thought to be caused by reduced blood circulation in the brain, dilatation of cerebral blood vessels, and inflammation around them.

  According to an epidemiological survey, about 8 million Japanese are suffering from migraine headaches, more common among women than men. In the case of migraine, the pain lasts several hours to several days. The exact pathogenesis of migraine is still unclear, but the blood vessel theory that the headache is caused by the constriction and dilation of blood vessels has been considered. In addition, neural theory based on excessive excitability of vascular cells in the cerebral cortex and trigeminal neurovascular theory that emphasizes the relationship between the trigeminal nerve and blood vessels are shown. From previous studies, at least for the development of migraine, neurogenic inflammation that depends on local hypervascular permeability through platelet activation, vasoconstriction and dilation, and release of neuropeptides from the trigeminal nerve Is considered to be one cause.

  Also, as a cause of headache, secondary headache that develops due to brain or body disease can be mentioned. For example, migraine may occur in children, but secondary headache causes include, for example, sinusitis, hypothyroidism, pituitary tumor (Ratke's cyst), hyperthyroidism, etc. However, the headache observed in these diseases is not truly a migraine.

Many therapeutic agents for headache are commercially available, and examples include aspirin and ibuprofen. As a treatment for migraine, NSAIDs such as aspirin and naproxen are taken in mild cases. If NSAIDs have not been effective in the past or have moderate or more severe headaches, a triptan preparation (Imigrant ^(R) (Glaxo (SmithKline Co., Ltd.)) and Ergotamine (Cafe Lugot ^(R) (Novartis Pharma Co., Ltd.)). However, for headache treatment drugs, there is a problem that there are responders that are effective after taking and non-responsive non-responders that are not sufficient.

  Thyroid hormone is produced in thyroid follicular cells. There are two types of thyroid hormone, thyroxine (T4) and triiodothyronine (T3). As for thyroid hormone, when thyroid stimulating hormone (TSH) secreted from the pituitary gland binds to TSH receptor (TSH receptor) of the thyroid cell membrane, synthesis and secretion of thyroid hormone (T4, T3) are performed by the stimulation. T4 and T3 secreted in the blood act on the pituitary gland and act to suppress the secretion of TSH. More follicular cells secrete T4 into the blood than T3, and T4 is converted to T3 in the liver and kidney. Most of T4 and T3 in the blood flow in the blood in a state of being bound to thyroid hormone binding protein, but a part thereof becomes active thyroid hormones as free hormones (FT4, FT3) and acts throughout the body.

  There is a report analyzing the relationship between thyroid dysfunction and headaches for over 28,000 people (Non-Patent Document 2). Here, as a result of analysis from various fields, when the reference value of TSH is 0.2 to 4 mU / L, when TSH is a high value (10 mU / L or more), headache is not a problem. However, those who endured headaches tended to have a slightly lower TSH. However, no relationship between the amount of thyroid hormone in the blood and headache has been reported.

As thyroid hormone preparations, dried thyroid derived from natural products (retioid ^(R) (Daiichi Sankyo Co., Ltd.), dried thyroid (Merck Pharmaceutical Co., Ltd.)) and the like are commercially available. Moreover, levothyroxine sodium (Tyrazine ^(R) (Asuka Pharmaceutical Co., Ltd.)) is also sold as a synthetic thyroxine. These thyroid hormone preparations have been applied to hypothyroidism or diseases associated with hypothyroidism. There are reports on pharmaceutical preparations containing levothyroxine, but none mentions the relationship with headache (Patent Documents 1 and 2).
http://kodomo.e-zyosei.com/ Eur J Neurol .; 8 (6), 693-9 (2001) JP 2002-284679 A JP-T-2006-525234

  It is an object of the present invention to provide a novel preventive and / or therapeutic agent for headaches that effectively acts even on patients who cannot obtain sufficient effects with existing therapeutic agents for headaches.

  In order to solve the above problems, the present inventors focused on the relationship between the amount of serum free thyroid hormone and the effectiveness of existing headache drugs, and as a result of intensive studies, when free T4 is somewhat low, In some cases, the effect of headache medicine was not sufficient. Therefore, when thyroid hormone is administered at a lower dose than prescribed for hypothyroidism, headaches are effectively improved even for patients who are not fully effective with existing treatments for headache It was confirmed.

That is, this invention consists of the following.
1. A preventive and / or therapeutic agent for headache, comprising thyroid hormone as an active ingredient.
2. 2. The preventive and / or therapeutic agent according to item 1, wherein the thyroid hormone is thyroxine.
3. 3. The preventive and / or therapeutic agent according to item 2, wherein the thyroxine is levothyroxine sodium.
4). 4. The preventive and / or therapeutic agent according to any one of items 1 to 3, wherein the dose of thyroid hormone as an active ingredient is 0.5 to 5 μg / kg / day.
5). 5. The preventive and / or therapeutic agent according to item 4 above, wherein the dose of thyroid hormone as an active ingredient is 1 to 3 μg / kg / day.
6). 6. The preventive and / or therapeutic agent according to any one of 1 to 5 above, which is used in combination with an existing preventive and / or therapeutic agent for headache.
7). 7. The preventive and / or therapeutic agent according to any one of 1 to 6 above, wherein the headache is migraine, cluster headache and / or tension-type headache.

  According to the preventive and / or therapeutic agent for headache of the present invention, effects such as shortening of the onset time, reduction of the number of headache attacks, elimination, etc. can be achieved for patients who cannot obtain sufficient effects with existing therapeutic agents for headache. Headache is improved. The preventive and / or therapeutic agent for headache of the present invention contains thyroid hormone as an active ingredient, but the preventive and / or therapeutic agent used for the improvement of headache has a smaller thyroid than the dose prescribed for hypothyroidism. The effect of a headache is obtained with the dose of the hormone. In addition, when used in combination with an existing preventive and / or therapeutic agent for headache, the dose of the existing drug can be reduced. Since levothyroxine sodium already marketed as a hypothyroid drug can be administered to infants, it can be used as a highly safe headache prevention and / or treatment for infants. is there.

In the present invention, the thyroid hormone contained as an active ingredient includes, for example, levothyroxine and its sodium salt, liothyronine and its sodium salt, and dried thyroid, among which levothyroxine sodium is particularly preferably used. The thyroid hormone may be derived from a natural product or may be obtained by synthesis. For example, commercially available thyroid hormone agents, specifically dry thyroid derived from natural products (retioid ^(R) (Daiichi Sankyo Co., Ltd.), dry thyroid (Merck Pharmaceutical Co., Ltd.)), and levo, which is a synthetic thyroxine And thyroxine sodium (Tyrazine ^(R) (Asuka Pharmaceutical Co., Ltd.)). Among these, in the case of synthetic thyroxine compared to the natural product-derived thyroid gland, it is considered that it can be used more effectively because there are few impurities. More preferably, levothyroxine sodium is highly safe and effective in that it is also used for infants.

  The agent for preventing and / or treating headache comprising the thyroid hormone of the present invention as an active ingredient can be formulated together with a pharmaceutically acceptable inorganic compound. Examples of the pharmaceutically acceptable inorganic compound include sodium bicarbonate, sodium carbonate, sodium hydrogen phosphate, calcium carbonate, calcium phosphate, calcium hydrogen phosphate, calcium silicate, magnesium oxide, magnesium hydroxide, synthetic aluminum silicate, Potassium iodide etc. are mentioned. In the present invention, among these inorganic stabilizers, sodium carbonate, sodium hydrogen phosphate, calcium carbonate, calcium silicate, magnesium oxide, magnesium hydroxide, or synthetic aluminum silicate may be mentioned. These compounds can be used as a stabilizer for thyroid hormone, and can be used alone or in combination of two or more.

  The agent for preventing and / or treating headache of the present invention generally includes tablets, powders, granules, pills, capsules, suppositories and the like, and in particular, tablets, capsules, powders or granules. preferable. Additives that can be used in these preparations include, in addition to the above inorganic stabilizers, for example, excipients, disintegrants, binders, lubricants, colorants, coating agents, corrigents, etc. These additives can be appropriately selected and used at the time of formulation.

  Here, examples of the excipient include lactose, glucose, D-mannitol, anhydrous calcium hydrogen phosphate, starch, and sucrose.

  Examples of the disintegrant include carboxymethylcellulose, carboxymethylcellulose calcium, croscarmellose sodium, crospovidone, starch, partially pregelatinized starch, and low-substituted hydroxypropylcellulose.

  Examples of the binder include hydroxypropyl cellulose, ethyl cellulose, gum arabic, starch, partially pregelatinized starch, polyvinyl pyrrolidone, and polyvinyl alcohol.

  Examples of the lubricant include magnesium stearate, calcium stearate, talc, hydrous silicon dioxide, and hardened oil.

  Examples of the colorant include iron sesquioxide, yellow iron sesquioxide, titanium oxide, and tar dye.

  Examples of the coating agent include purified sucrose, hydroxypropylmethylcellulose, hydroxypropylcellulose, methylcellulose, ethylcellulose, polyvinylpyrrolidone and the like.

  Examples of the corrigent include citric acid, aspartame, ascorbic acid, menthol and the like.

  In the present invention, the dose of thyroid hormone as an active ingredient is 0.5 to 5 μg / kg, preferably 1 to 3 μg / kg per day. For example, levothyroxine sodium is already on the market as a drug for infant hypothyroidism, and its dosage is 10 μg / kg / day for infants and 5 μg / kg / day for premature infants. When used as an agent for preventing and / or treating headache according to the present invention, it is safe because it can be used at a lower dose than the amount used.

  The headache in the agent for preventing and / or treating headache of the present invention is not particularly limited, and examples thereof include migraine, cluster headache and / or tension-type headache, and particularly preferably migraine. The headache in the prophylactic and / or therapeutic agent for headache of the present invention is suitably used particularly for a headache of a patient who cannot obtain a sufficient effect after taking it with an existing therapeutic agent for headache. For example, an ergotamine combination drug is prescribed as a migraine treatment, but this drug may not be effective unless it is taken when migraine is mild. In recent years, triptan preparations have shown improvement in severe headaches, but eletriptan and sumatriptan have different effects, and prescribing these drugs rarely causes heart disease-like symptoms. Side effects such as being seen may occur. In addition, even in cases where the effect has been recognized, a phenomenon that the effect is lost is recognized, which is a clinical problem.

  The preventive and / or therapeutic agent for headache according to the present invention is effective for headache in patients whose free T4 is low and sufficient effects cannot be obtained after taking with existing therapeutic agents for headache. Even in cases where the effects of existing treatments for headache have been confirmed, the phenomenon of ineffectiveness has been observed, which is also effective in cases that are clinically problematic. Furthermore, although the reference value of the TSH value is recognized as 0.2 to 4 mU / L, it is considered that the TSH value is effective even for patients having 2 mU / L or less. Moreover, it can be effectively used for a headache of a patient who cannot obtain a sufficient effect after taking it with an existing therapeutic agent for headache, regardless of the measured value of free T4 or TSH.

  Whether or not an effect is obtained within 60 minutes after administration of a therapeutic agent for headaches, as will be described in Examples below, regarding the relationship between the values of free T4 and free T3 and the effectiveness of existing therapeutic agents for headaches As a result of evaluation, it was confirmed that there are many cases where the effectiveness is low when the free T4 in the serum is 0.87 ± 0.07 ng / dl compared to 1.08 ± 0.10 ng / dl. . Although the reference value of free T4 varies depending on the facility, it is certified as 0.97 to 1.7 ng / dl in the inventor's facility. When a drug containing the thyroid hormone of the present invention was administered to a patient with low efficacy as confirmed above, a reduction or disappearance of a headache attack was observed. For example, in the case where no effect was observed with lomerizine hydrochloride, the number of migraine headaches was 12-16 times / month, but when the drug containing the thyroid hormone of the present invention was administered, it was reduced to 4-1 times / month. There are also examples. In addition, when an existing headache therapeutic agent is prescribed after administration of a drug containing thyroid hormone of the present invention, there is an example in which the time until the effect of the existing headache therapeutic agent is recognized is reduced to a quarter or less. is there.

  In the present invention, the existing preventive and / or therapeutic agent for headache is not particularly limited as long as it is already marketed or scheduled to be marketed. For example, it is a migraine drug. Examples include triptan-based preparations, ergotamine preparations, and lomerizine hydrochloride preparations. Moreover, aspirin, ibuprofen, etc. may be sufficient.

  Among the existing preventive and / or therapeutic agents for headaches, the migraine preventive drug lomerizine hydrochloride is said to act on the serotonin receptor 5-HT2A, and the triptan agent is said to act on 5-HT1B / 1D. The cause of the inability to obtain sufficient effects after taking existing headache prevention and / or treatment agents has not been fully elucidated, but one of the causes is the reception of serotonin due to stress and abuse of existing drugs. It may be mentioned that the sensitivity to the body is reduced. On the other hand, T3 (triiodothyronine) has been reported to enhance the action of serotonin and enhance the action of antidepressants (Life Sci .; 58, 1551-9 (1996)). T3 has been reported to act on 5-HT1B and 5-HT2A of the setronin receptor (J Neurosci Methods; 140, 133-9 (2004), Neuroendocrinology; 69, 453-9 (1999)). Among the thyroid hormone preparations, for example, levothyroxine sodium is a synthetic T4 and is converted into T3 in vivo, so that the converted T3 acts on the serotonin receptor and stimulates the serotonin receptor, thereby causing headache. It is possible that improvements have been made. However, further studies are awaited on the mechanism by which thyroid hormone acts as an active ingredient to prevent and / or treat headache.

  The agent for preventing and / or treating headache according to the present invention may be used alone or optionally in combination with existing preventive and / or therapeutic agents for headache. The present invention also encompasses a preventive and / or therapeutic agent for headache that is used in combination with existing preventive and / or therapeutic agents for headache. When used together, it is expected to have an excellent effect on existing preventive and / or therapeutic drugs for headaches, and it is also expected to reduce the dose of existing preventive and / or therapeutic drugs for headaches it can.

  Examples of the present invention will be described below in more detail, but the present invention is not limited to these, and various applications are possible without departing from the technical idea of the present invention. It is.

Example 1
For 77 migraine patients, the effectiveness of the therapeutic agent for triptan-type migraine was evaluated based on whether or not the effect appeared within 60 minutes. As a result, 37 effective cases (high response cases) were found. There were 40 cases with poor (low / no reaction) cases. As a result of measuring free T4 for these patients, the average value of the high response cases was 1.08 ± 0.10 ng / dl, whereas the average value of the low response cases was 0.87 ± 0. 0.07 ng / dl, showing a significant difference (FIG. 1). On the other hand, the free T3 was also measured in the same manner. As a result, the average value of the high reaction example was 2.52 ± 0.37 pg / ml, whereas the average value of the low / no reaction example was 2.37 ± 0. .33 pg / ml and no significant difference was observed (FIG. 1).

Among the above, levothyroxine sodium tablet Tyrazine ^(R) S25 (manufactured by Asuka Pharmaceutical Co., Ltd.) 0.2 to 0.25 tablets for 29 patients with low / no response and low free T4 When administered, migraine attacks were reduced or eliminated.
Moreover, Imigran ^(R) tablet 50, which is a therapeutic agent for triptan-type migraine, was administered in accordance with a normal prescription, and the time until it was confirmed to be effective (effect onset time) was measured. As a result, it was 78.3 ± 17.7 minutes before administration of Tyrazine ^(R) S25, but significantly decreased to 61.2 ± 10.7 minutes after administration (FIG. 2).

(Example 2)
Of migraine patients, in cases where the effect against lomerizine hydrochloride agent is a migraine prophylactic drugs was not observed at all (29 cases), but migraine attacks count was 12 to 16 times / month, Chirajin ^{( R) When} 0.2 to 0.25 tablets of S25 (manufactured by Asuka Pharmaceutical Co., Ltd.) were administered, the number of migraine attacks decreased to 4 to 1 per month.

  As described above in detail, the agent for preventing and / or treating headache of the present invention is effective because it effectively improves headache even for patients who are not sufficiently effective with existing therapeutic agents for headache. It can be used as a new drug. In addition, when used in combination with an existing preventive and / or therapeutic agent for headache, the dose of the existing drug can be reduced. Furthermore, since levothyroxine sodium already marketed as a drug for hypothyroidism can be administered to infants, it is a safer and / or therapeutic agent for headaches that is highly safe for infants and pregnant women. Is available as

It is a figure which shows the relationship between the effectiveness of a triptan headache therapeutic drug, and free thyroid hormone (T3, T4). Example 1 It is a figure which shows the effect expression time of the triptan headache therapeutic agent before and after thyroid hormone administration with respect to a low and unresponsive example. Example 1

Claims (7)

A preventive and / or therapeutic agent for headache, comprising thyroid hormone as an active ingredient. The prophylactic and / or therapeutic agent according to claim 1, wherein the thyroid hormone is thyroxine. The prophylactic and / or therapeutic agent according to claim 2, wherein the thyroxine is levothyroxine sodium. The preventive and / or therapeutic agent according to any one of claims 1 to 3, wherein the dose of thyroid hormone as an active ingredient is 0.5 to 5 µg / kg / day. The preventive and / or therapeutic agent according to claim 4, wherein the dose of thyroid hormone as an active ingredient is 1 to 3 µg / kg / day. The prophylactic and / or therapeutic agent according to any one of claims 1 to 5, which is used in combination with an existing prophylactic and / or therapeutic agent for headache. The preventive and / or therapeutic agent according to any one of claims 1 to 6, wherein the headache is migraine, cluster headache and / or tension-type headache.

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