IE44404B1 - New niclosamide suspension formulations - Google Patents

New niclosamide suspension formulations

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Publication number
IE44404B1
IE44404B1 IE276876A IE276876A IE44404B1 IE 44404 B1 IE44404 B1 IE 44404B1 IE 276876 A IE276876 A IE 276876A IE 276876 A IE276876 A IE 276876A IE 44404 B1 IE44404 B1 IE 44404B1
Authority
IE
Ireland
Prior art keywords
suspension
niclosamide
compound
oil
suspension according
Prior art date
Application number
IE276876A
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IE44404L (en
Original Assignee
Bayer Ag
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
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Publication date
Priority claimed from DE2557617A external-priority patent/DE2557617C2/en
Application filed by Bayer Ag filed Critical Bayer Ag
Publication of IE44404L publication Critical patent/IE44404L/en
Publication of IE44404B1 publication Critical patent/IE44404B1/en

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Description

The present invention relates to formulations of niclosamide and of its salts suitable for medical administration.
Formulations of 2-hydroxy-5-2Ldichloro-4'-nitrobenzanilide (herein referred to as niclosamide), which is a substance having an anthelmintic action, and of its salts (in particular of the piperazine salt) have already been disclosed.
In this context it should be pointed out that niclosamide and its salts have hitherto generally been used as tablets and, particularly in veterinary medicine, as so-called wettable powders.
A wettable powder (abbreviation: WP) is understood as a powder which, before it is used, can easily be stirred in water to give a homogeneous, ready-to-use suspension.
In the formulations previously known, the active conpound niclosamide and its salts are generally employed in a micronised form (in this case, the maximum in the particle size distribution curve is between 2 and 50μ and especially between 2 and 20μ).
However, the previous formulations of niclosamide and of its salts had the disadvantage that they were either not immediately ready for use (wettable powders) and/or that a relatively large dose was necessary in order to achieve the same activity (tablet/wettable powders).
It has not yet been possible hitherto to prepare stable formulations of niclosamide and of its salts with a more finely ground or precipitated active compound (particle size about 1μ) in an aqueous medium. This is because it has been found, in general, that an undesirable growth in the particle size of the niclosamide or niclosamide salt particles takes place after a relatively short time and this prevents good resorption of the active compound. Thus, all commercially prepared aqueoqs suspension formulations exhibit crystals of 20u and larger. This growth in the particle size has been found hitherto when anhydrous niclosamide and niclosamide containing water of crystallisation, and also the niclosamide salts, were used.
According to the present invention we provide an oilbased suspension of niclosamide, or a salt thereof, in which at least 50 per cent of the particles of the niclosamide or its salt are smaller than 2μ. Preferably at least 50 per cent of the particles of niclosamide or its salt are smaller than 1μ.
The formulations of the invention display a particularly high anthelmintic activity and have a very high stability.
In this context it should be mentioned that resorption of the medicament from suspensions which are prepared with oily solvents can be improved or impaired, compared with that from an aqueous suspension.
Thus, for example, it has been reported that in the case of griseofulvin a corresponding oily suspension of the active compound gives better plasma concentrations of the active compound than does an aqueous suspension (see P.J.
Carrigan and T.R. Bates, I. Pharm. Sci. 62 (9), 1,476 (1973).
On the other hand, experiments showed that in most cases lower plasma concentrations of the active compound are obtained with an oily suspension, that is to say the resorption of the active compound which takes place is poorer than in the case of aqueous suspensions (in this context see, for example, Bntersuchungen beim Ampicillin (Experiments with - 3 44404 Ampicillin) K. Bauer, Bheinisches Arzteblatt No. 5/1975).
On the basis of the above, it is therefore to be regarded as surprising that the active compound niclosamide and its salts have such a good action in oily suspension and that finer grinding results in an improvement in fhe activity and, above all, the stability, these improvements being distinctly superior to those achieved with the micronised aqueous use form employed hitherto.
The invention also provides a method of combating ( including the prevention relief or cure cf) intestinal infection In non-human animals which comprises administering to the animals a suspension according to the invention.
The aotive compound which is used according to the invention, that is to say niclosamide (2-hydroxy-5,-2’~ dichloro-4'-nitrobenzanilide) and its use as an anthelmintic, especially as an agent for combating tapeworms, are, as has been stated, already known (see, for example, British Patent Specification No. 889,377). Moreover, salts of niolosamide and their use as anthelmintics are already known (with regard to the piperazine salt of niclosamide see, for example, German Patent No. 1,194,866, French Patent No. 1,509,908 and British Patent No. 966,074).
The formulations according to the invention comprise the active compound (niclosamide or a niclosamide salt), oily liquid excipients and, optionally, surface-active agents or emulsifiers.
The following can be used as the aotive compounds: anhydrcus niclosamide, niclosamide containing water of crystallisation, and niclosamide salts, especially the piperazine salt of niclosamide. - 4 44404 The preferred oily liquid excipients are physiologically acceptable oily liquid excipients in which the active compound is virtually insoluble. The following compounds are preferably employed according to the invention as liquid excipients: liquid paraffins, vegetable oils, for example sesame oil, groundnut oil, cotton seed oil, sunflower oil or olive oil, synthetic or partially synthetic oils, such as triglycerides of capric/caprylic acid, mixtures of triglycerides of saturated vegetable fatty acids of medium chain length, esters of fatty acids with fatty alcohols, such as oleic acid oleyl ester and oleic acid decyl ester, esters of a branched fatty acid of medium chain length with saturated fatty alcohols (0^-0^) and ethyl stearate. Further solvents, such as, for example, alcohols, (such as n- or iso-propanol, n-butanol or t-butanol) are optionally also added.
Examples of surface-active agents (comprising emulsifiers and wetting agents and frequently substances which at the same time promote resorption) are: 1. anionic surface-active agents, such as Na laurylsulphate, fatty alcohol ether sulphates and the monoethanolamine salt of mono-/di-alkyl-polyglycol-ether-orthophosphoric acid esters, 2. cationic surface-active agents, such as cetyltrimethylammonium chloride, 3. ampholytic surface-active agents, such as di-Na Nlauryl-p-iminodipropionate or lecithin, and 4. non-ionic surface-active agents, for example polyoxethylated castor oil, polyoxyethylated sorbitan monooleate, sorbitan monostearate, glycerol monostearate, polyoxyethylene stearate and alkylphenol polyglycol ethers. - 5 44404 The formulations according to the invention preferably contain the active compound (niclosamide or a niclosamide salt) in concentrations of from 2 to 60 per cent (weight/ volume) and most preferably from 5 to 20 per cent (weight/ volume).
The suspension formulations according to the invention preferably contain the liquid excipients in an amount of from 20 to 98 per cent (weight/volume) and preferably of from 80 to 95 per cent (weight/volume).
The suspension formulations according fo the invention preferably contain the surface-active agents (comprising emulsifiers and wetting agents) in an amount of from 0 to 50 per cent (weight/volume) and most preferably of from 1 to 20 per cent (weight/volume).
The auxiliaries according to the invention (liquid excipients and surface-active agents) are generally employed in the pure form for the preparation of the suspension formulations according to the invention.
In order to prepare the suspension formulations according to the· invention, the active compound (anhydrous niclosamide, niclosamide containing water of crystallisation, or a niclosamide salt, especially the piperazine ealt of niclosamide) is ground in the oily liquid excipient to the required particle size in a manner which is in itself known e.g. using ball mills, stirred ball mills or other suitable comminuting apparatus.
Preferably, in the proeess according to the invention, a so-called preconcentrate in which approximately 50 per cent of the particles should be ground to smaller than 2μ and preferably smaller than 1μ is first prepared. - 6 44404 A surface-active agent (wetting agent and/or emulsifier) is optionally added to this preconcentrate.
The concentrate which is now obtained is then preferably diluted with the liquid excipient to the desired use concentration.
The preferred sequence of process steps described above does not have to be strictly maintained. The sequence of process steps can be varied to a substantial extent. Moreover, it is also possible to employ a mixture of liquid excipients and/or surface-active agents for the preparation of the suspension formulations according to the invention.
The suspension formulations according to the invention are used in the same way as the previously known formulations of the same active compound (niclosamide or a salt of niclosamide) which has an anthelmintic action and, in particular, an action against tapeworms.
It is intended to demonstrate the preparation of the suspension formulations according to the invention by means of the examples which follow. However, these examples are intended to show only a few possibilities for the preparation of the suspension formulations according to the invention and not to have a restrictive effect. The symbol (S) designates a Registered Trade Mark.
Example 1 A 20% w A* concentrate of niclosamide containing water of crystallisation in paraffin of low viscosity·' is ground, in a high-speed stirred ball mill (for example of the Uni-mill,bead mill or sand mill type) to a particle size such that about 50% of the particles are smaller than 1μ. Glass beads with a diameter of 318 - 418μ are employed ae the grinding aid. 0.5% of lecithin ie added 444θ as the wetting agent. A 4% niclosamide weight/volume suspension in paraffin of low viscosity with a lecithin content of 3% is prepared from this concentrate by diluting with said paraffin and adding lecithin. A read5 to-use stable suspension which can be administered easily results.
Example 2 In the same way as in Example 1, a 20% strength suspension of niclosamide in sesame oil is ground. The concentrate is diluted to 10% niclosamide content with sesame oil, with the addition of 5% of polyoxyethylenesorbitan monooleate and 10% of n-butanol.
The formulation can be administered easily and in the case of moniezia infection of sheep is effective in a dose of 35 mg/kg. This is about half of the.dose of niclosamide which is otherwise customary.
Example 3 A niclosamide concentrate is prepared in the manner described in Example 1. After adding 5% of polyoxyethylene20 sorbitan monooleate, it is diluted to 10% weight of niclosamide/ volume with liquid paraffin of low viscosity.
The biological activity of the suspension formulations according to the invention was tested, compared with that of the previously known formulations of the same active compound.
In order to compare the activity of the formulation of Example 1 with that of a known formulation, an identical 4% strength suspension in which the maximum in the particle size distribution was at about 5 μwas prepared.
Example A Hymenolepsis nana - mice Animals infected experimentally with Hymenolepsis - 8 _ nana were treated orally after the prepatent period of the parasites had elapsed. The degree of efficacy of the formulation is determined by counting, after dissection, the worms which remained in the test animal, compared with the number in untreated control animals, and then calculating the percentage action.
Table relating to Example A z Preparation/formulation Daily dose oi Seduction in active com- parasites in pound in mg/kg per cent Oily suspension (liquid paraffin) 500 100 of sand mill-ground 250 100 niclosamide 100 96 Suspension of sand mill-ground 500 100 niclosamide in liquid paraffin, 250 100 with tiie addition of 0.5# of 100 93 lecithin, according to Example 1 Suspension of sand mill-ground 500 100 niclosamide In liquid paraffin, 250 99 with the addition of 0.5# of 100 94 polyoxyethylated sorbitan mono- oleate (Arlacel I'S'), prepared analogously to Example 3 Suspension of sand mill—ground 500 100 niclosamide in liquid paraffin, 250 100 with the addition of 3# of polyoxyethylated sorbitan monooleate (Arlaeel 1 ®), prepared analogously to Example 3 100 93 Untreated controls 0 Table relating to Example A Por comparison: tests with micronised niclosamide active compound (particle size distribution maximum about 5u)· Preparation/formulation Daily dose of Seduction in active com- parasites in pound in mg/kg per cent Oily suspension (liquid paraffin) 500 61 of micronised niclosamide 250 23 100 16 Suspension, of micronised niclos- 500 94 amide in liquid paraffin with 250 66 the addition of 5% of lecithin 100. 34 Suspension of micronised niclos- 500 99 amide in liquid paraffin with 250 91 addition of 3% of lecithin 100 47 Suspension of micronised niclos- 500 76 amide in. liquid paraffin with 250 49 ' the addition of 0.5$ of polyoxy- 100 0 ethylated sorbitan monooleate (Arlacel 1 ®) Suspension of micronised niclos- { 500 66 amide in liquid paraffin with 250 40 addition of 3$ of polyoxyethy- lated sorbitan monooleate (Arlacel I ®) 100 16 Untreated controls 0 Example Β 'Jaenia hydatigena/dogs Bogs infected experimentally with Taenia hydatigena were treated after the prepatent period of the parasites had elapsed. The active compound was administered orally. The degree of efficacy of the formulation employed was determined by counting, after dissection, the worms which remained in the! test animal, compared with the number in untreated control animals, and also by determining the number of parasite-free dogs relative to the total number of dogs treated with the particular dose and also by determining the average number of parasites per dog.
Table relating to Example B Average number of parasites per dog Formulation Dose in mg/kg Number of parasite-free dogs/ total number of dogs Piperazine salt of 2.0 5/10 0.8 (0-2) niclosamide in pul- 4.0 7/10 0.4 (0-2) verulent form 8.0 8/10 0.4 (0-2) (particle size distri- 16.0 10/10 0 bution maximum about 32.0 10/10 0 5μ) Sand mill-ground 0.25 3/10 1.3 (1*4) niclosamide suspended 0.5 6/10 0.7 (1-3) in liquid paraffin, 1.0 7/10 0.5 (1*2) according to the 2.0 10/10 0 invention 4.0 10/10 0 Untreated controls - 0/20 3.6 (1-4)

Claims (15)

CLAIMS:- /
1. An oil-based suspension of niclosamide (2-hydroxy5-2 , -dichioro-4 , -nitrobenzanilide) or a salt thereof in which least 50% of the particles of the said compound are smaller
2. A suspension according to claim 1 yzherein the said compound is in its anhydrous form.
3. A suspension according to claim 1 wherein the said compound is in a form which contains water of crystallisation. 10
4. A suspension according to claim 1, wherein the said compound is in the form of a piperazine salt.
5. A suspension according to any one of claims 1 to 4 including surface-active agent. 5 than 2μ. :
6. A suspension according to claim 5 wherein the surface 15 active agent comprises lecithin or a polyoxyethylated sorbitan monolaurate.
7. · A suspension according to claim 5 or claim 6 including up to 30% (weight/volume) of the surface active agent.
8. A suspension-according to any one of claims 1 to 7 20 wherein the oil base comprises a liquid paraffin or sesame oil.
9. A suspension according to any one of claims 1 to ψ comprising from 2 to 60% (weight/volume) of the said compound. 10. Suspension containing niclosamide according to claim 1 substantially as hereinbefore described in any one of the Examples. 16. An oil-based suspension of niclosamide when prepared by a process according to any one of claims 12 to 15·
10. A suspension according to any one of claims 1 to 9 25 wherein at least 50% of the particles of the said compound are smaller than 1μ.
11. An oil-based suspension substantially as hereinbefore described in any one of Examples 1 to 3·
12. A process for the preparation of a suspension according jQ to any one of claims 1 to 10 wherein anhydrous niclosamide, niclosamide containing water of crystallisation, or a niclosamide salt is ground in an oily liquid excipient, to an extent such that at least 50 per cent of the particles of active compound are smaller than 2 μ.
13. · A process according to claim 12 wherein a surface5 active agent is added to the suspension after grinding·
14. · A process according to claim 12 or claim 13 wherein the suspension is further diluted with the liquid excipient to a desired concentration· 15· A process for the preparation of an oil-based
15. 17· A method combating intestinal infection in non-human animals which comprises administering to the animals a suspension according to any one of claime 1 to 11 and 16.
IE276876A 1975-12-20 1976-12-17 New niclosamide suspension formulations IE44404B1 (en)

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
DE2557617A DE2557617C2 (en) 1975-01-02 1975-12-20 Process for the production of a glass substrate suitable for the manufacture of gas discharge boards, with electrical conductors attached thereto, in which a soldering glass is applied to the substrate and the substrate

Publications (2)

Publication Number Publication Date
IE44404L IE44404L (en) 1977-06-20
IE44404B1 true IE44404B1 (en) 1981-11-18

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Cited By (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN104430338A (en) * 2014-12-08 2015-03-25 江苏艾津农化有限责任公司 Niclosamide ethanolamine salt wettable powder as well as preparation method and application thereof
CN105394037A (en) * 2015-11-17 2016-03-16 镇江市疾病预防控制中心 Niclosamide ethanolamine self-emulsifying micro-emulsion and preparation method thereof

Cited By (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN104430338A (en) * 2014-12-08 2015-03-25 江苏艾津农化有限责任公司 Niclosamide ethanolamine salt wettable powder as well as preparation method and application thereof
CN105394037A (en) * 2015-11-17 2016-03-16 镇江市疾病预防控制中心 Niclosamide ethanolamine self-emulsifying micro-emulsion and preparation method thereof
CN105394037B (en) * 2015-11-17 2019-07-26 镇江市疾病预防控制中心 The agent of bayluscid self-emulsifying micro-emulsion and its preparation method

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IE44404L (en) 1977-06-20

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