DE1667925A1 - drug - Google Patents

Description

PATENT ADVERTISER 8500 NUREMBERG,

DIPL.-ING. PR. BOOKS January 12, 1968

Re: Patent application in Germany Note: Messrs. TJnimed Inc., Morristown, New Jersey / USA

drug

The subject of the invention is the elimination of side effects occurring with normal administration in the case of orticosteroids (e.g. glycosteroids), which have proven to be valuable drugs in various diseases. the Elimination of these side effects, which are usual with normal administration, is achieved by simultaneously with the corticosteroid or shortly before or after, an effective amount of beta (2- or 4-pyridyl-alkyl) amine or administered a substance with a similar effect. It has been shown that - for reasons not yet completely have been clarified, but for which some theoretical explanation has been found - compounds such as beta (2- or 4-pyridil-alkyl) amines cause the corticosteroid as with normal administration and contributes to the relief of the disease, but without the known side effects appear.

The use of corticosteroids for many purposes, such as acute inflammation and allergic diseases of the Eyes, skin, mucous membrane, rheumatoid arthritis, bronchial agthma, ulcerative colitis and other diseases, the complete list of which would lead too far here has increased considerably in recent years. The frequent occurrence

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undesirable side effects when administering corticosteriods, e.g. hydrocortisone, in cases of illness however, has severely restricted the use of corticosteroids. Attempts have also been made to reduce the known undesirable side effects by developing various new steroid derivatives. However, since these new steroid derivatives led in some cases to an increased activity per molecule, the Efficacy per biological unit in relation to the biological basis essentially parallel to the side effects. So it has so far not been possible to eliminate or at least reduce the undesirable Side effects of the corticosteroids to find a satisfactory solution.

The known undesirable side effects associated with the use of corticosteroids include: Iatrogenic (or physician-induced) Cushing's Disease, sodium retention, potassium excretion associated with edema, hyp er t envision, hyperglkaemia, glycosuria etc. In many cases the side effects are so great that the continued administration of corticosteroids is no longer necessary However, the need for further administration would be urgently needed. Then you have calibrated often in such a way that one administered smaller amounts than were necessary, or that one often co-administered the treatment Corticosteroids completely stopped, although continuation of the treatment would have been advisable. It is now a success Finding a method by which the side effects of the corticosteroids are turned off by one at the same time with the corticosteroid, or shortly before or shortly after an additional agent administered. This invention Agent eliminates the known side effects without eliminating the desired effect of the corticosteroids

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or is restricted.

Accordingly, it is primarily on gate of the invention that Eliminate the side effects of administering corticosteroids to achieve the desired ones essential effects of the corticosteroids are preserved at the same time.

Another essential object of the invention is to provide a more superior drug that

it enables larger amounts of corticosteroids and the like

to be administered over longer periods of time without the known side effects occurring.

Further purposes and advantages of the invention are presented in the following description and in the claims.

The essence of the invention, then, is to find a method that involves administering corticosteroids without unwanted side effects made possible by one either at the same time as the corticosteroid or immediately before or after the administration of the corticosteroid at least one connection of the following groups:

Beta- (2-pyridyl-alkyl) -amines, beta- (4-pyridyl-alkyl) amines, 1- (2'-pyridyl) 2,3-cis or trans-dicarboxylic acid cycloutane, 1- (4 -'-pyridyl) -2,3-cis or trans-dicaruonic acid cyclobutane, Di-lower alkyl amides of alpha-picolinic acid, as well as their non-toxic acidic addition salts.

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The method according to the invention can be used for all corticosteroids and their derivatives which are used to heal inflammation and similar symptoms. Such steroids, which are only listed here as examples, can be: cortisone, including its derivatives, such as, for example, cortisone phosphate, etc., hydrocortisone and its derivatives, such as, for example, 21-sodium succinate, etc., prednisone, dexamethasone, ACTH, corticosterone, 11-dehydrocorticosterone, 11-deoxycorticosterone, aldosterone, etc. These corticosteroids are used to treat Addison ¹ disease, hypopituitarism, adrenal hyperphasia, such as rheumatoid arthritis, rheumatic mucus and rheumatic heart disease, allergies such as bronchial asthma, allergic vasomotor asthma Eyes, pulmonary fibrosis, sarcoid tumor, skin diseases and acute arthritic gout, etc. used.

The exact dose of the corticosteroid to be administered depends on the type of corticosteroid used and the disease to be cured. The invention is applicable to all effective amounts. For example, in the case of cortisone and oral administration, the dose can be 2.5 to 100 mg, for intramuscular administration 5 - 300 mg, for intravenous administration up to 100 mg, and for ointments for local treatment and for suspensions 0.5 - 2.5 96. In the treatment of cattle for acetonemia, the dose can be between 1.0 and 1.5 g i.d. m. amount. In the treatment from dogs for arthritis it can be between 25 and 75 mg when taken orally. When using Hydrocortisone the dose is generally 2/3 the dose of cortisone. For predison lies for achieving the containment Effect the oral dose at 20 to 60 mg per day, which can then be increased gradually until the optimal one

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Maintenance dose has been reached. When using dexamethasone, which is approximately 7 times as strong, than prednisolone and 20 to 35 times as strong as hydrocartisone, the dose is 0.5 to 1.5 mg orally, while a solution of $ 0.1 is appropriate for topical application. As already indicated above, the present one is Invention applicable to all effective doses and for all corticosteroids.

In accordance with the present invention, one means of the above Type (detailed examples are given below) f administered, either simultaneously with the corticosteroid or just before or after administration of the corticosteroid. For reasons that have not yet been clarified, the agent has the ability to prevent undesirable side effects of corticosteroid from occurring without the main effect of the corticosteroid is impaired. The application of the side effects preventive agent is preferably administered orally. The dose depends on the agent used and is different.

Preferably be used for the purposes of the invention, the following (mean: Beta-Pyrldyl-alkyl-amine, Beta4-pyridyl-alkyl-amine, and their non-toxic acid addition salts.

Most useful are those compounds which have a lower alkyl, such as methyl and / or ethyl, e.g. beta-2-pyridyl-ethyl-methyl-amine, Beta-4-pyridyl-ethylmethyl-amine, 1-2 pyridyl-2 methylamine-propane and their non-toxic acidic addition salts

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such as hydrochloride, tartrate, fumarate, gluconate, etc.

The beta-2 or 4-pyridyl amines are preferred given in doses of about 4 - 45 mg per day, but preferably in an amount of 12 mg - 45 mg per day. Advantageous a uniform dose of around 2-15 mg three to four times per day is given. These connections can be given either orally or by injection.

Other pyridylalkyl amines and pyridylalkyl amines acidic Addition salts are: 2- (2 '- (N, N-diethylamine) -ethyl) pyridine monofumarate; 2- (2'-N, -ethylamine) -ethyl) pyridine monofumarate; 2- (2 '- (amine) ethyl) pyridine monofumarate; 4- (2 '- (amine) ethyl) pyridine monofurmarate; 4- (2 '- (methylamine) ethyl) pyridine monofumarate; Beta (2-pyridyl) ethyl diethyl amine hydrochloride; 1- (1-pyridyl) -2-methylamine propane hydrochloride; and beta (2-pyridyl) ethylamine hydrochloride.

Of the pyridyl dicarboxylic acid cyclobutanes, the following are mentioned: 1- (2'-pyridyl) -2,3-trans dicarboxylic acid cyclobutane; 1- (4'-pyridyl) -2,3-trans dicarboxylic acid cyclobutane; 1- (2'-pyridyl) -2,3-cis dicarboxylic acid cyclobutane; and 1- (4'-pyridyl) -2,3-cis dicarboxylic acid cyclobutane;

From the Di-low. alkyl amides of alpha-picolinic acid are mentioned: diethylamide of alpha-picolinic acid, dimethylamide of alpha-picolinic acid, and of course theirs acidic addition salts such as hydrochloride, sulfate, etc. The dose generally used is around 0.1 1 mg three times a day

While the invention is not intended to be limited to any specific theory as to such as or

ORIGINAL

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why the undesirable side effects of the corticosteroid are prevented by the proposals according to the invention, Nevertheless, a theory should be set up in the following in the hope that the presentation will help encourage further research in this area.

It is believed that the action of the corticosteroids comes about through passive binding to microvascular smooth muscle cells and through interference with the anticonvulsant effects of histamine. Histamine is usually found in small amounts in smooth muscle cells. ä The generation of histamine is, however, achieved by strong stimuli either local or systemic nature (local or systemic nature). In general, there is an increase in histamine production when there is significant irritation (stress), such as; B. major injury, and then causes astringent substances such as adrenaline and noradrenaline to be released.

It could therefore be that the corticosteroid's intended counteraction against the increased histamine * production is the main function (essential stress function) of these hormones, the susceptibility to injuries in animals suffering from adrenaline deficiency and the wide variation in the requirement for the Corticosteroid effects (underly).

It therefore seems to be the case that the serious side effects of corticosteroid therapy by the tendency of these hormones to affect the microvascular muscles as a result of the Counteraction caused by the normal relaxation effects of the histamine. It follows that the corticosteroid

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the cappilar blood flow would diminish that tissue is malnourished and as a result diverse (widespread) abnormal reactions to the chemical processes in cells and other functions that cause the Cause side effects of corticosteroid therapy.

The agents according to the invention apparently counteract the tendency of the hormones, which consists in the capillary Decrease blood flow, while on the other hand increasing blood flow side effects of corticosteroid treatment prevented, but at the same time an interaction with the anti-inflammatory effect of the corticosteroid does not occur. It is also advantageous that the agents according to the invention only have a small amount Have toxicity and, more importantly, that they can be administered orally.

The following examples are provided for further explanation the invention. However, the scope of protection of the invention is not intended to be restricted by the exemplary embodiments cited will.

example 1

An injured adrenalectomized rat (a stressed adrenalectomized rat), which was exposed to parts of the adrenal gland 5 mg of hydrocortisone are injected. The increased closing time of the microvascular muscles of the Liver causes an abnormally rapid overflow of the open remaining capillaries. The process causes the activation of the metabolism of the over-nourished liver cells, whereby the general non-specific liver anabolic characteristics of the animal treated with the corticosteroid increases.

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Another rat prepared in this way was given the same dose of hydrocortisone and 1 mg of beta-2-pyridyl-methylethylene hydrochloride, Beta-histine hydrochloride is injected in physiological saline solution. It has been shown that despite the restoration the puncture (restoration) of the open and closed Sphincter muscles the extent of the side effects is significantly reduced.

Example 2

From the medicament according to the invention can also in f

Tablets are usually produced. Any tablet appropriately contains:

Cortisone 10 mg beta-2-pyridylethylmethyl-

Amine hydrochloride 5 g

Calcium Carbonate (q.s.) 200 mg

These tablets can be used for all purposes for which cortisone is also used when administered orally will. The full cortisone effect is reduced

There is a risk of side effects occurring (

Example 3;

Ampoules with a content of 10 cbcm can also be produced, with each cbcm containing 50 mg of hydrocortisone and 10 mg of 1-2-pyridyl-2-ethylmethylamine hydrochloride dissolved in a 0.9 # strength sodium chloride solution. The solution can be in all cases are used in which hydrocortisone is used for long periods of time without causing side effects,

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which usually comes with the use of hydrocortisone arise alone.

Example 4:

Other tablets can be made up as follows:

Prednisone 5 mg beta-2-pyrydil ethylamine

Hydrochloride 2 mg

lactose (q> s.) 250 mg.

The tablets mentioned can be used safely in all cases, (freely) in which the administration of prednisone appears to be indicated, but the occurrence of undesirable side effects of prednisone is considerably reduced.

Example 5:

A patient with acute inflammation of the mucous membranes received daily injections of 1-100 mg of cortisone acetate given intermuscularly. The patient was given twelve mg of beta-2-pyridyl-ethyl-diethylamine hydrochloride orally four times a day in tablet form. Even several weeks after the treatment, there were no undesirable side effects of cortisone shown.

Example 6;

Eye drops can, for example, have the following composition have per cubic centimeter:

Dexamethasone Sodium Phosphate 1mg

Beta-2-pyridyl-methylethylamine 2 mg

Hydrochloride

Sodium bisulfate (preservative) 0.32 #

Water for Injection (q.s.) 1 cc

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Example 7

An ointment can be composed as follows:

Hydrocortieone Acetate 25 mg

üeta-2-pyridyl methylethylamine
Hydrochloride 5 mg

mild, non-irritating ointment,
eg anhydrous lanolin, white petrolatum and mineral oil (qs «) 1g

This ointment can be applied topically to the skin, like for removal of local inflammation.

Of course, it is also possible to look at other uses and variations of the drug to find the invention without deviating from its essential properties, so that these too are within the scope of the following claims.

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Claims (1)

. Subject: Patent registration in Germany "Drug" Note: Messrs. Unimed Inc. Morristown, JMew «Jersey / USA Claims 1. Medicines for reducing the side effects arising from the administration of oorticosteroids, characterized in that this at least one compound of the following groups, namely .tfeta- (2-pyridyl-alkyl) -amines, beta- (4-pyridyl-alkyl> - amines, 1- (2 · -pyridyl) -2,3-cis-dicarboxylic acid cyclobutane, 1- {2 · -pyridyl) -2,3-trans-dicarboxylic acid cyclobutane, 1- (4'-pyridyl-2,3-ci3- dicarboxylic acid cyclobutane, 1- (4'-pyridyl) -2,3-trans-dicarboxylic acid cyclobutane, di-lower alkylamides of alpha ± "icolic acid, as well as their acidic non-toxic addition salts and a pharmaceutically acceptable basis. 2. Medicament according to claim 1, characterized in that the compound from the group of beta (2-pyridyl-lower alkyl) amines, the eta- (4-pyridyl-lower alkyl) amines is selected and their acidic non-toxic Contains addition salts. 3. Medicament according to claim 1 or 2, characterized in that the pharmaceutical base is suitable for oral administration is suitable. 4) Medicament according to claim 1 to 3, characterized in that the compound m a unit dose of approximately 2.50 mg. 109830 / 18A3 - 01 - 5β corticosteroid composition with reduced corticosteroids side effects, because it indicates that this composition consists of at least one member of the following groups, namely beta- (2-pyridyl-alkyl) amines, beta (4-pyridyl-alkyl-amines, 1 - (2 * -pyridyl ) -2,3-cis-diacid-cyclobutane, 1_ (2'-pyridyl) -2,3-trans-diacid-cyclo butanes, 1- (4 · -pyridyl) -2,3- cis-dicarboxylic acid cyclobutane, 1- (4'-pyridyl-2,3-trans-dicarDonic acid cyclobutane, di-lower alkylamides of alpha-picolinic acid and its acidic, non-toxic addition salts. 6. The composition according to claim 5, characterized in that the compound is a member from the group of beta (2-pyridyl-lower alkyl) amines, Beta (4 ~ pyridyl-lower alkyl) amines and acidic non-toxic addition salts is. 7. Composition according to claim 6, characterized in that that the effective compound, according to the invention, is present in an amount of about 2-15 mg. 8. Composition according to claim 7, characterized in that that it is in a form suitable for oral administration. j 9. Composition according to claim 5, characterized in that that it is in a form suitable for oral administration. 10. Composition according to claim 5, characterized in that that this is injectable, with the corticosteroid and the additional compound is distributed in an injectable liquid. -02- 109830/1843