DE2361488A1 - MANUFACTURE OF TRIPROPYL ACID DERIVATIVES AND THEIR USE IN MEDICAL AND ANIMAL MEDICAL PREPARATIONS - Google Patents

Description

Dipl.-Ing. P. WIRTH Dr. V. SCHMIED-KOWARZIK DIpL-lng. G. DANNENBERG Dr. P. WEINHOLD Dr. D. GUDEL

^{6 FRANK} ™ "ON THE MAIN

TELEPHONE COeill

287014 GH. ESCHENHEIMER STRASSE

Case Br. 102
Wd / Sch

XABAZ

39, avenue Pierre 1er de Serbie

P-75008 Paris

France.

Production of tripropyl acetic acid derivatives and their use in medical and veterinary preparations

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- 2 - 2361Α8δ

The present invention relates to tri-n-propyl acetic acid acid derivatives for use in the treatment of pathological mood swings. These derivatives have the general formula:

CH ₃ -CH ₂ -CH ₂

CH ₃ -CH ₂ -CH ₂

where T is the group NH ₂ or the group OM, in which M is an alkali metal, such as Li, Na or K, is.

These compounds can all be prepared by known methods for example, according to the following:

a) If Y is the group NH ₉ , tri-n-propylaceto-. nitrile under mild conditions in an acidic medium, preferably 7 sulfuric acid, hydrolyzed as described in J. Amer. Chem. Soc. 70 «3091 (1948) has been described.

b) If Y is the group OM, then a base becomes the formula

MOH,

wherein M has the abovementioned meaning with tri-n-propyl acetic acid implemented.

Another object of the present invention is therefore to provide a process for the preparation of the compounds of the above general formula.

The invention also relates to pharmaceutical or veterinary compositions used as essential Active ingredient at least one compound of the above general Formula contained in association with a suitable pharmaceutical carrier.

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Pharmacological experiments on laboratory animals have shown that the compounds of the general formula have properties, used in the treatment of pathological conditions caused by disorders of the central nervous system and disorders in the field of neuropsychiatry are very valuable. In these pharmacological experiments, which are described in detail below, it was found that the compounds of the general formula as Anticonvulsants, regulators of the central nervous system, Tranquilizers and potentizers for depressants of the central nervous system can be used.

In the course of further experiments with the inventive Compounds as regulating agents for the central nervous system were unexpectedly found to have these compounds a particularly valuable healing effect on pathological Exercise mood swings. In particular, the invention Compounds are extremely useful means of activating and disinhibiting patients, who suffer from serious apathy or communication difficulties known as apragmaticism and occur, for example, in certain types of schizophrenia.

All derivatives of the above general formula are known compounds insofar as they come under the general formula of British Patent No. 760 114, which relates to substances for reducing blood cholesterol. Moreover, wherein it is described as mild spasmolytisch is tri-n-propylacetamide in British Pat. No. 469,921, and in "Arch, for Experim. Pathology and Pharmacology", 186 (July / Sept _e 1937), wherein it from K _e Junkmann is described as weakly spasmolytic and somewhat stronger as a sleep aid _{9 in} particular. mentioned. Apart from the fact that the information on tri-n-propylacetamide regarding the dosage and the

* "variations of mood"

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Test criteria in these "two publications are not are very precise, it is not even remotely suggested by either of the two texts that the connections between the general formula the particular modes of action according to the invention can be attributed.

As for the effectiveness ascribed to the compounds of the general formula as a result of pharmacological tests It should be mentioned in particular that the use of the previously known neuroleptic agents and anti-depressants are accompanied by undesirable side effects, for example extrapyramidal disorders in the case of neuroleptic agents and complete mood reversals in the case of both types of agents. The invention In contrast, connections do not have these disadvantages. It has been found that their effects are already at doses occurs that are significantly lower than the dose that causes a behavioral disorder.

In the field of diseases requiring treatment with anticonvulsants make necessary, especially in the field of epilepsy, there are numerous preparations of indisputable Effectiveness. However, these substances often cause undesirable side effects, such as difficulty concentrating as well as "biological disorders, the most serious of which is hematological Are kind. Also, certain are known anticonvulsants toxic at relatively low doses, while others are only used to treat a single type of epilepsy are suitable. The compounds according to the invention do not have these disadvantages since they are relatively non-toxic and at the same time have diverse properties, whereby they are useful in treating a wide range of convulsive conditions.

As far as the tranquilizer effect is concerned, the invention Compounds do not have much better properties compared to the best known agents.

"" "409824/1151

wrote. However, it should be mentioned that the compounds of the invention in addition to the satisfactory Tranquilizer effects also include a wide range of neurotropic Have properties that exceed those of the known tranquilizers. -

Finally, it should be emphasized that, as already mentioned above, it was surprisingly found that the invention Compounds possess properties that are useful for the treatment of pathological mood swings and especially the treatment of severe apragma ti sinus are extremely valuable.

The following is a summary of the pharmacological tests carried out to determine the toxicity of the compounds of the invention and the presence of the various properties which, when combined, make the compounds valuable as anticonvulsants ₉ central nervous system regulators, muscle relaxants * tranquilizers and potentiators for central nervous system depressants.

1. Acute toxicity

The LDf-Q value was determined in mice by intraperitoneal administration determined according to the Karber and Behrens method. The following results were obtained for the preferred compounds according to the invention. -

Compound LDj-Q value in "mg / kg

Sodium tri-n-propyl acetate 327

Tri-n-propylacetamide. 340

what 20 ™ to 80 times the daily therapeutic Dose of compounds corresponds to,

* "myorelaxants"

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2j Neurotoxicity

The so-called "Rota Rod lest" (Boissier therapy 1958, XIII, pages 1074-1118) was used to determine the neurotoxicity. This test is used to determine the animals' ability to coordinate their movements. It is carried out with groups of 10 mice each weighing about 25 g. The compound to be investigated is administered to the animals in each group by the intraperitoneal route, in doses such that the next group receives a higher dose than the previous group. Thirty minutes after the administration, the mice are placed on a 4.8 cm diameter wooden roller rotating at a speed of 4 revolutions per minute for 2 minutes. The roller has a rough surface to prevent the animals from sliding off.

This can be used to determine the neurotoxic dose 50 (FTD 50), ie the dose of the compound at which half of the animals can no longer remain on the roller for a specified period of time.

With the preferred compounds of the invention gave the following results:

Compound NTD ₅₀ ~ value in mg / kg

Sodium tri-n-propyl acetate 120

Tri-n-propylacetamide 68

This attempt has a twofold value. Animal failure gives a very early indication of the slightest impairment of the neuromuscular punctures that cannot be determined by any other means. Second, this test is used to set of index numbers to compare results obtained with other behavior tests.

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5. Ant! Convulsive effectiveness

The anticonvulsant efficacy was first demonstrated by the procedure "in which seizures are induced by pentylenetetrazole, and thereafter tested by the maximum electric shock-induced seizure procedure. ■ '

a) Attack caused by pentylenetetrazole

The purpose of this experiment ₉ der'an mice is performed is to determine whether compounds of the invention, when administered prophylactically intraperitoneal route, some of the animals to protect against epileptic seizures in certain doses, by appropriate and before and certain doses of pentylenetetrazole can be caused which would be fatal in the absence of the compound according to the invention 100 io. The experiment was carried out on groups of 10 male OP 1 mice each weighing about 25 g. Each group of animals was administered a dose of the test compound by the intraperitoneal route which was higher than the dose of the previous group. Seven and a half minutes after the administration, 125 mg / kg of pentylenetetrazole was administered intraperitoneally to each animal. The experiment was repeated 15, 30, 45 and 60 minutes after administration of the compound to be examined, and the number of deaths was determined 3 hours after administration of the pentylenetetrazole. From these numbers, the effective dose 50 (EDc _Q value) was calculated, According to the method described by Litchfield and Wileoxon in J ₀ Pharmacol, 1938, 2, pages 192-216.

Bie with the preferred compounds of this invention obtained results are shown in the following table% '

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Table I.

link Time after administration 7 1/2
Min. 15 minutes. 30 min. 45 min. 60 min. Sodium tri-n-propyl
acetate, EDc- _n value in
mg / kg ⁵⁰
Tri-n-propylacetamide,
ED value in mg / kg 78 66
10 110
38 56 70

In the case of sodium tri-n-propyl acetate, there was no longer any relationship between efficacy and administered dose after 45 and 60 minutes, since the time of maximum efficacy of the compound was then already considerably exceeded and the efficacy had already decreased sharply. In the pail of tri-n-propylacetamide it was not possible _{to determine an ED 50} after 71/2 minutes, since the effectiveness of the compound was not yet evident at this point in time.

The index of activity of the compounds was also calculated by comparing the EDr- _Q value with the dose which is necessary to induce a hypnotic effect in 50 μl of the animals. This latter value is referred to as HD - called value ₀ or hypnotic dose 50, and the effectiveness index is through the break:

¹ ^ ₅ O

specified.

The potency indices for the preferred compounds as well for phenobarbital were as follows:

Sodium tri-n-propyl acetate tri-n-propyl acetamide Phenobarbi-fcal 409824/1151

1.8 9
3.3

These figures show that tri-n-propylacetamide is much more beneficial than phenobarbital, while sodium tri-n-propyl acetate is just as sedative as phenobarbital. Albeit sodium trin propyl acetate - has a considerable degree of effectiveness compared to its HDj-Q value, so it does not show the known disadvantages of barbiturates.

b) Seizure from maximum electric shock

This attack manifests itself in the mouse by stretching out the hind paws for 5 to 10 seconds. The same stretching out of the hind paws is observed in tonic-clonic seizures caused by chemical convulsants such as pentylenetetrazole or strychnine.

The experiment was carried out on groups of 10 mice each of breed OF 1, which weighed about 22 g. Various doses of the compound to be tested were administered intraperitoneally in such a way that each group received a higher dose than the previous one. Fifteen minutes later, each animal received an electric shock twice the threshold intensity (approximately 60 volts). It was determined the number of tonic seizures, and the ED ^ Q value, ie by 50 $> to protect the animals against tonic seizures, the dose of the test compound, which is required, was calculated.

The following results were obtained for the preferred compounds according to the invention and for phenobarbital:

Compound EDj- ₀ value in mg / kg

Sodium tri-n-propyl acetate 130

Tri-n-propylacetamide 82

Phenobarbital 78

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As in "the case of the experiment with evoked by pentylenetetrazole Seizures, the efficacy index was:

calculated, and the following results were obtained:

Sodium tri-n-propylaeetate 1.0

Tri-n-propylacetamide 1,3

Phenobarbital 1.3

These figures show that tri-n-propylacetamide, which does not have the disadvantages of barbiturates, has a level of effectiveness comparable to that of phenobarbital. It can also be seen that the effectiveness of sodium tri-n-propyl acetate, even if this has a lower effectiveness than phenobarbital, occurs at a dose which is far below its LD ^ Q value.

4. Muscle relaxing properties

The muscle-relaxing properties of the invention Connections were described by the traction test described by Courvoisier (Psychotropic Drugs, Milan 1957, pages 373-391) has been determined, and at the same time the anti-strychnine properties have been determined of these compounds noted.

a) traction test

With this test it is possible to determine the sense of balance as well as muscle tone and strength.

The test is carried out on groups of 10 male mice of breed OP 1, each weighing about 25 g. It consists in attaching the mice to a horizontally stretched wire

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Hang up goal paws. First it is observed how much time the animals in a comparison group "need to intercept, ie until they have brought at least one hind paw onto the wire. Each test group is then administered an intraperitoneal dose of the compound to be tested, a higher dose for each group dose than the previous one. it is then observed how many animals have lost 30 minutes after administration of the compound to the traction reflex, and it is the ED ^ calculated Q value, ie the dose of the test compound, the $ 50> of the animals to Causes loss of reflex.

To obtain an efficacy index number, the above is also used "Rota Rod Test" described, using for comparison two known muscle relaxants, namely diazepam and Mephenesin, can be used.

The following results were recorded:

Tri-n-pr'opyl-
acetamide Diazepam Mephenesin NTD ₅₀ value in the "Rota Rod Test "in mg / kg 68 3 100 ED ^ Q value in traction test in mg / kg 45 2.75 250 Effectiveness index:
NTD ₅₀ 1.5 1.1 0.4 ED ₅₀

These figures show a very favorable index of effectiveness for Tri-n-propylacetamide compared to the efficacy indices of two popular muscle relaxants. It even turns out that with tri-n-propylacetamide the muscular tensioning Dose is much further below the neurotoxic dose than im

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- 12 cases of the other two substances.

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b) antagonism to strychnine

Male mice of breed OP 1 weighing 22-24 g became by the intraperitoneal route with a compound of the invention treated.

Thirty minutes later, the animals were given a subcutaneous dose of 1.5 mg / kg of an aqueous solution of streaknine sulfate.

The number of deaths that occurred in the two hours after administration of the strychnine sulfate was recorded and the ED ^ value calculated. The EDj-Q value calculated for tri-n-propylacetamide was 65 mg / kg.

5. Hypnotic properties

The hypnotic properties of the compounds of the invention were determined by observing the postural reflex.

Male mice of breed OP 1 weighing about 25 g became divided into groups of 10 animals each. The animals in one group were given a higher dose of the compound to be investigated administered as the previous group.

Then the number of animals was determined to be different Time points after administration lost the reflex.

In this way, the HD ^ _Q - ¥ ert was determined at different times after administration, ie the dose of the compound to be investigated which resulted in the loss of the posture reflex at a certain time after administration in 50 # of the animals.

The results are shown in the following table:

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T a t e 1 1 e II

Compound time after administration

15 min. 30 min. 45 min. 60 min.

Sodium tri-n-propyl

fi f * f * * i "fl * t"

HD ₅₀ value in mg / kg 120 130 150 200

Tri-n-propylacetamide,

HD ₅₀ - ¥ ert in mg / kg 90 110 110 120

6. Tranquilizer properties

The tranquilizer properties of the compounds according to the invention were determined by the “chimney test”, the “evasion test ¹¹ and the“ hole-board test ”, which are described by Boissier in“ Med. Exp. "196O, 3, pages 81-84," Therapy ¹ . ¹ 1965, XX, pages 895-905 or in "Therapy", 1964, XIX, pages 571-589.

a) Chimney test

With the help of this test one can determine two groups of factors, namely neuromuscular factors (muscle strength, flexibility, coordination of movements) and psychological Factors (curiosity, fear, pluchin instinct).

The test was carried out on groups of 10 mice each weighing about 25 g weighed, carried out. The compound to be tested was administered intraperitoneally to the groups in such a way that one Each group received a higher dose than the previous group. The mice turned their heads one by one first inserted into a 30 cm long test tube, which was matched to the size of the mouse so that the animal could by backwards

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"Moved out of the glass in less than 30 seconds. The number of animals that could not do this was determined.

In this way, the ED, - ₀ value could be determined, ie the dose of the compound at which 50 % of the animals were unable to escape from the test tube within 30 seconds.

The preferred compounds according to the invention gave the following results:

Compound EDj-Q value in mg / kg

Sodium tri-n-propyl acetate 72

Tri-n-propylacetamide 32

This tranquilizer effect was achieved with only half the dose, which is necessary to make the neuromuscular punctures in the "Rota Rod Test".

b) evasion test

With this test it is possible to examine the urge to explore in mice. A parallel-piped, lidless plywood box is used, in which there is an inclined plane, also made of plywood, which is covered with a narrow scrap. There is a horizontal marking line on the inclined plane 2 cm below the point where the plane rests on the box wall. Dip's entire device is placed in an artificially lit room from which all high-pitched noises are kept away. Each time a mouse crosses the marker line in an upward direction is referred to as an "exit".

4/1151

The test was carried out with groups of 28 mice each weighing about 22 g weighed, carried out. The animals in each group received a dose of the test compound by intraperitoneal route, each group a larger dose than the previous group.

Thirty minutes after the compound was administered, the animals became placed in groups in the box and held for 10 seconds by a movable board on the bottom of the box. It was determined the average length of time after which the first "Exit" took place, as well as the total number of "Exits"

per group for one minute each and these observations continued for 5 minutes. The same information were also recorded for a control group that was not administered any compound. With the preferred according to the invention Connections gave the following results:

Table III

link Total number of Aus
kick per group 2 min. 3 min. 4 min. 5 min. Average
Time until Comparison
animals 1 min. 50 43 38 42 first Austre
th in seconds Sodium tri-
n-propyl
acetate
50 mg / kg 48 44 43 41 28 14th Sodium tri-
n-propyl
acetate
75 mg / kg 54 37 31 34 28 25th Tri-n-propyl
acetamide
10 mg / kg 44 37 27 26th 35 21 Tri-n-propyl
acetamide
50 mg / kg 46 43 38 31 25th 20th 40 49

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c) perforated board test

This test enables a quantitative determination of the mice's urge to explore in relation to their curiosity. The material used is a board 40 × 40 cm in size and 1.7 cm thick, in which 16 holes 3 cm in diameter have been cut. The board is placed on 4 legs that are as high as ¹ . (1.5 m) that the holes appear bottomless to the animals. The experiment is carried out in the greatest possible silence.

The test was carried out with groups of 10 male mice each of the breed OP 1, which weighed about 23 g. The animals each group was given a dose of the test compound by the intraperitoneal route, namely one group each a higher dose than the previous group. The comparison group did not find the compound under investigation administered.

Thirty minutes after the administration, the animals of each group were placed in the center of the board and the total number of holes explored per minute by each group was recorded for 5 minutes.

The results obtained with the preferred compounds according to the invention are shown in the following table:

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Table IV

link Total number of 2 min. * explored holes 4 min. 5 min. Comparison animals 1 min. 35 3 min. 43 33 ITa tr ium-tr in-
propyl acetate
50 mg / kg 32 13th 32 19th 17th Natriuin-tri-n-
propyl acetate
75 mg / kg 15th 6th 14th 1 7th Tri-n-propyl
aeetamid
10 mg / kg 2 28 3 35 27 Tri-n-propyl
acetamide
50 mg / kg 30th 10 23 6th 12th 8th 4th

The above results show that both sodium tri-n-propyl acetate as well as tri-n-propylacetamide the curiosity of the animals to decrease.

7. Neuroleptic properties

In all catalepsy experiments that were carried out on rats with the inventive Connections were made (crossing of homolateral paws, four corks test, parallel rod test ("parallel bars test"), negative results were obtained with doses slightly below the hypnotic Dose were.

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8. Potentiation of depressants for the central nervous system

Attempts have been made to reduce the potentiating effect of the compounds according to the invention to determine sodium pentobarbital and neuroleptic agents.

a) Sodium pentobarbital

Groups of 10 mice each from breed OP 1, weighing 22 - 24 g weighed, a dose of 50 mg / kg was given by the intraperitoneal route administered to the compound of interest. 30 minutes later a dose of 30 mg / kg sodium pentobarbital was followed by the same route administered. It was observed how much time passed on average until the animals fell asleep, and how long they slept on average. The combined effect of the two administered substances was compared with that Effect of a dose of 50 mg / kg of the same compound of the invention administered alone under the same conditions was, and with the effect of a dose of 30 mg / kg sodium pentobarbital, which was also administered alone under the same conditions.

With tri-n-propylacetamide the following results were obtained:

Table V

link Average
Time until
Fall asleep Average ti.
time of
Sleep Tri-n-propylacetamide
50 tng / kg
Sodium pentobarbital
30 mg / kg
Tri-n-propylacetamide
50 mg / kg
+ Sodium pentobarbital
30 mg / kg no mouse
slept
no mouse
slept
4 min. 45 sec. no mouse
slept
no mouse
slept
1 min. 37 sec.

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- 19 b) Potentiation of neuroleptic agents

For this experiment, groups of 10 mice each were bred OP 1s, which weighed 22-24 g, were used. One group was given a dose of 5 mg / kg of chlorpromazine, and another group was given administered a dose of 50 mg / kg of the compound to be tested. The results obtained were matched with the results of two other groups, who both also received a dose of 5 mg / kg chlorpromazine. 30 minutes later one of these latter groups became 10 rag / kg of the compound to be investigated and the other group 50 mg / kg of this Compound administered. In all cases the administration was by the intraperitoneal route.

With the compound according to the invention. Tri-n-propylacetainide was obtained get the following results:

Tabel

V I

link Cataleptic animals in $> Tri-n-propyl acetamide
50 mg / kg
Chlorproma ζ in
5 mg / kg
Tri-n-propylacetamide
10 mg / kg
+ Chlorpromazine
5 mg / kg
Tri-n-propylacetamide
50 mg / kg
+ Chlorpromazine
5 mg / kg no catalepsy "
no catalepsy
40
100 ^

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9. Antireserpine Efficacy

The antidepressants cancel or delay the sedative effect of reserpine, as was determined by experiments with ptosis in rats. Groups of 5 male rats of the breed GE 1, each weighing about 300 g, were administered a dose of 50 mg / kg of the compound to be tested by the intraperitoneal route. Thirty minutes later, 5 mg / kg reserpine was administered by the same route. It was observed how much time elapsed from the administration of the reserpine to the occurrence of the ptosis, the ptosis in each eye being rated according to the following scale:

0 = eyelids open

1 = eyelids 1/4 closed

2 = eyelids 1/2 closed

3 = eyelids 3/4 closed

4 = eyelids completely closed

For example, if an animal had a ptosis value of 1 in one eye and 2 in the other eye, it would be 1.5 rated.

The results obtained with tri-n-propylacetamide are shown in FIG Table below, with each result being the average of 10 measurements (5 animals, in each of which both eyes were assessed) represents:

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link P t o s i s 1 H. 2 hours. 3 hours. 4 hours 6 hours Comparison animals
Tri-n-propyla cetamide
10 mg / kg
Tri-n-propyla cetamide
20 mg / kg
Tri-n-propyla cetamide
30 mg / kg
Tri-n-propyla cetamide
40 mg / kg 0.6
0.2
0
4th
0
0 2.0
2.6
2.4
0.8
0.8 3.3
3.6
3.4
2.3
2.3 4.0
3.8
3.5
3.2
3.0 4.0
4.0
3.8
4.0
4.0

The therapeutic compositions according to the invention can be used in any suitable for human and animal medicine
Shape can be used. The administration units can, for example, in the form of optionally coated tablets,? Hard gelatin capsules, ampoules or syrup for oral administration, a sterile solution for parenteral administration and suppositories for rectal administration
are present.

Depending on the mode of administration chosen, the therapeutic compositions according to the invention comprise at least one
Compound of the formula I in combination with a suitable one
Carrier, the latter containing, for example, at least one of the following ingredients: talc, magnesium stearate,
Lactose, sucrose, carboxymethyl cellulose, starches,
Kaolin, levilite, cocoa butter.

The following examples serve to explain in more detail the preparation of the compounds according to the invention and of these containing therapeutic compositions.

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Example I. Preparation of tri-n-propylacetamide

a) Preparation of tri-n-propylacetonitrile

A solution of 123 g (3 mol) of acetonitrile and ΠΙΟ g (11.4 mol) of n-propyl bromide in 520 g of toluene was placed in a 4 liter flask equipped with a dropping funnel and a mechanical stirrer. The solution was ^{heated to 50 °} C. with stirring, after which a 90% suspension of 431 g of sodium amide in 775 g of toluene was slowly added through the dropping funnel over the course of 5 hours, taking care that the temperature was above 50 ⁰ C remained. During this process it was observed that the reflux temperature rose from 50 to 75 ⁰ C. The flask which had contained the sodium aramid suspension was then rinsed with 180 g of toluene. The reaction mixture was allowed to cool to room temperature and stirred for an additional 14 hours. Thereafter, the reaction mixture together with the rinsing liquid was gradually poured carefully into ice water containing 2000 g of purified water and 500 g of ice. The mixture was stirred for 30 minutes and the organic layer decanted and washed three times with 1 liter of water, after which the toluene was evaporated. The oily residue was distilled under reduced pressure (2 mm Hg), and the distillation fraction, which had a boiling point between 68 and 70 ^° C., was collected. 400 g of tri-n-propylacetonitrile were obtained, which corresponded to a yield of 80 % .

b) Production of tri-n-propylaoetamide

An 80 # aqueous solution of Added 550 g of sulfuric acid. While stirring, 110 g (0.66 mol) of tri-n-propylacetonitrile were added over the course of 20 minutes and at room temperature admitted. The temperature of the reaction mixture

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rose to 80 ^° C. and was increased to 105-110 ° C. for 6 hours. The solution was then ^{cooled to 10 °} C. and slowly poured into ice water (1000 g of purified water and 200 g of ice). As the solution was poured into the ice water, a dough-like precipitate gradually formed. As soon as the process was finished, the mixture was stirred for 15 minutes and the precipitate was separated by centrifugation and taken up twice in 350 g of ethyl ether. The ethereal solution was first washed twice with 200 g of water containing 10 % sodium bicarbonate and then washed twice with 250 g of water. The mixture was over 125 g for 24 hours. anhydrous sodium sulfate, after which the sodium sulfate was removed by centrifugation. The ether was then removed on a rotary evaporator to give an oil which crystallized into fine needles which were held under vacuum until they reached constant weight. In this way, 113 g of crude tri-n-propylacetamide were obtained, which corresponds to a yield of 92.6 $ . The crude product was then dissolved in 150 g of petroleum ether by heating. After dissolution, 1.15 g of "CECA WSL-Black" was added and the mixture was refluxed for 30 minutes. The additive was filtered off while the mixture was still hot. The filtrate was cooled for 3 hours at -15 ° C, after which the formed precipitate separated by centrifugation for 24 hours in a drying oven at 40 ⁰ C under a vacuum of 20 mm Hg was dried. 98.5 g of pure tri-n-propylacetamide were obtained, which corresponds to a yield of pure product of 87.1 % .

Example 2 Production of sodium tri-n-propyl acetate

a) Production of tri-n-propyl acetic acid

In a flask equipped with a dropping funnel, 480 g of distilled dioxane and then 80 g (0.432

A 0 9 8 2 UI 1 1 5 1

Mol) of tri-n-propylacetainide, which was dissolved by stirring, was added. A stream of dry hydrochloric acid gas was bubbled through the dioxane solution at room temperature for 20 minutes (ie a total of 100 g of hydrochloric acid gas). Upon completion of this process, 88 g (0.86 mol) of freshly distilled butyl nitrite were slowly added through the dropping funnel over a period of 2 hours. The temperature of the reaction medium rose from 31 to 43 ^° C., which made cooling in a water bath necessary. The solution was then for 2 hours at a temperature of 85 - 9O ⁰ O kept. The dioxane was then evaporated under reduced pressure of 20 rom Hg and a dough-like residue was obtained at room temperature. This residue was dissolved in 290 g of a 10 % aqueous solution of potassium hydroxide. The aqueous layer was decanted off and extracted twice with 75 g of ethyl ether. The potassium solution was acidified with 118 g of a 36% solution of hydrochloric acid (at 10-20 ° C.), after which the oily phase was decanted off. The aqueous phase was extracted twice with 75 g of ethyl ether, after which the oily phase and the ethereal extracts were combined. The ethereal solution was washed twice with 100 g of water and dried over 100 g of anhydrous sodium sulfate for 24 hours. The sodium sulfate was then removed by centrifugation. The ethyl ether was evaporated under atmospheric pressure and the residue recovered under 7 mm Hg. The fraction obtained had a boiling point of 126-128 ⁰ C and crystallized quickly. Was obtained in this way 61 g of crude tri-npropylessigsäure, which corresponds to a yield of fi 76th The crude product was then dissolved in 75 g of ethyl ether by heating. The ethereal solution was filtered off while it was hot, and the filtrate was kept at a temperature of -3O ⁰ C for 4 hours. The precipitate which formed was separated by centrifugation and dried in a desiccator for 6 hours under reduced pressure of 20 mm Hg. 46 g of pure tri-n-propyl acetic acid were obtained, which corresponds to a yield of 75.4 % of pure product and a total yield of 57.3%. Melting point: 67 ⁰ C.

U 0 9 8 2 k I 1 1 5 1

b) Production of sodium tri-n-propylaoetat ^{c Ό} '° ^c

Into a flask equipped with a dropping funnel and a mechanical stirrer, 30 g (0.161 mol) of pure tri-n-propylacetic acid, the preparation of which has been described above, and 75 g of toluene were placed. The mixture was stirred until completely dissolved, after which a hot solution of 6.45 g sodium hydroxide in 30 g methanol was added through the dropping funnel. To the resulting solution was added 1 g of CECA WSL-Black, after which the whole mixture was refluxed with stirring for 1 hour. The additive was then filtered off and the remaining mixture was distilled by gradually adding 88 g of toluene through the dropping funnel to prevent the mixture from turning into a solid. The distillation was stopped as soon as the temperature at the top of the column had reached 105 ^° C., after which the mixture was then cooled to room temperature. The resulting precipitate was separated off by centrifugation and rinsed twice with 20 g of acetone. Then it was dried in a rotary evaporator at 80 ^° C. for two hours, and then again at 105 ^° C. under atmospheric pressure for 4 hours in a ventilated drying oven. In this way, 30 g of sodium tri-n-propyl acetate were obtained, which corresponds to a yield of $ 89.5.

Example 3

Soft gelatin capsules were made according to known pharmaceutical processes manufactured with the following components:

component

Tri-n-propylacetamide. - '

talc
Magnesium stearate

. 167

409824 / ί151

Claims (1)

Claims; 1. Pharmaceutical or veterinary preparation, in particular for use as an anticonvulsant, regulating agent for the central nervous system, tranquilizer "or potentiating agent for depressants for the central nervous system or for the special treatment of pathological mood swings, characterized in that it is used as an active ingredient at least one derivative of the general formula: CH ₃ -CH ₂ -CH ₂ CH ₃ -CH ₂ -CH ₂ wherein Y is the group NH ₂ or the group OM, in which M is an alkali metal, optionally in conjunction with a pharmaceutical carrier, includes. 2. Preparation according to claim 1, characterized in that it is sodium tri-n-propyl acetate or tri-n-propyl acetamide as the active ingredient includes. Process for the preparation of tri-n-propyl acetic acid derivatives the general formula: CH ₃ -CH ₂ -CH ₂ CH ₃ -CH ₂ -CH ₂ wherein Y is the group NH ₂ or the group OM, in which M is an alkali metal, Α09824 / Γ151 characterized in that a) when Y is the group NH ₂ , tri-n-propylacetonitrile is hydrolyzed in an acidic medium, and b) if Y is the group OM, a base of the formula: MOH, wherein M has the abovementioned meaning with ir-n-propyl acetic acid is implemented. 4. The method according to claim 3, characterized in that sulfuric acid is used as the acidic medium for reaction a). 409824/1151