GB2243549A - Medicament containing triclosan for treating gastrointestinal disorders - Google Patents

Medicament containing triclosan for treating gastrointestinal disorders Download PDF

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GB2243549A
GB2243549A GB9109439A GB9109439A GB2243549A GB 2243549 A GB2243549 A GB 2243549A GB 9109439 A GB9109439 A GB 9109439A GB 9109439 A GB9109439 A GB 9109439A GB 2243549 A GB2243549 A GB 2243549A
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Prior art keywords
triclosan
sodium
sustained release
helicobacter pylori
medicament
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GB2243549B (en
GB9109439D0 (en
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Peter William Dettmar
John Gareth Lloyd-Jones
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Reckitt Benckiser Healthcare UK Ltd
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Reckitt and Colman Products Ltd
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/0012Galenical forms characterised by the site of application
    • A61K9/0053Mouth and digestive tract, i.e. intraoral and peroral administration
    • A61K9/0065Forms with gastric retention, e.g. floating on gastric juice, adhering to gastric mucosa, expanding to prevent passage through the pylorus
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/075Ethers or acetals
    • A61K31/085Ethers or acetals having an ether linkage to aromatic ring nuclear carbon
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/0002Galenical forms characterised by the drug release technique; Application systems commanded by energy
    • A61K9/0007Effervescent
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/50Microcapsules having a gas, liquid or semi-solid filling; Solid microparticles or pellets surrounded by a distinct coating layer, e.g. coated microspheres, coated drug crystals
    • A61K9/5005Wall or coating material
    • A61K9/5021Organic macromolecular compounds
    • A61K9/5026Organic macromolecular compounds obtained by reactions only involving carbon-to-carbon unsaturated bonds, e.g. polyvinyl pyrrolidone, poly(meth)acrylates
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/50Microcapsules having a gas, liquid or semi-solid filling; Solid microparticles or pellets surrounded by a distinct coating layer, e.g. coated microspheres, coated drug crystals
    • A61K9/5005Wall or coating material
    • A61K9/5021Organic macromolecular compounds
    • A61K9/5036Polysaccharides, e.g. gums, alginate; Cyclodextrin
    • A61K9/5042Cellulose; Cellulose derivatives, e.g. phthalate or acetate succinate esters of hydroxypropyl methylcellulose
    • A61K9/5047Cellulose ethers containing no ester groups, e.g. hydroxypropyl methylcellulose

Abstract

The use of triclosan for the preparation of medicaments for the treatment of gastrointestinal disorders associated with Helicobacter pylori infections is disclosed. The medicaments may be in the form of powders, granules, spheroids or liquids, or in unit dosage form as capsules or tablets containing 1 to 100mg, preferably 10 to 60mg, of triclosan. The medicaments may also be in gastric sustained release form as raft forming tablets or liquids, optionally to be co-administered with a solid pharmaceutically acceptable carboxylic acid or acid salt, or as muco-adherent-coated granules or spheroids.

Description

1 PREPARATION OF A MEDICAMENT This invention relates to the preparation of
a medicament for the treatment of gastro intestinal disorders associated with Helicobacter pylori infections.
The relationship between peptic ulcer disease and gastr-itis has been recognised for several decades. The relationship between gastritis and infection with Helicobacter pXlori (formerly Campylobacter pylori), first demonstrated by Warren and Marshal in 1983, is now equally well established, see Vaira et al (Current Opinion in Gastroenterology 1989, 5: 817-823). Given this connection it is now being recognised that treatments of gastritis and peptic ulcer must be capable of removing the associated Helicobacter pylori infections.
A number of different treatment regimens have been proposed to treat Helicobacter pylori infections. European Patent applications No 206826 and 206627 (Marshall) describe the use of bismuth salts whilst EP 206625 (Marshall) and WO 88/05981 (Borody) describe the use of a combination of bismuth with a single antibiotic for the treatment of Helicobacter PZlori. However, bismuth alone achieves low (30 to 70%) initial clearance rates for Helicobacter -Pylori and recurrence of the infection approaches 100% by twelve months post therapy. Bismuth together with a single antibiotic, namely amoxicillin, appears to be relatively effective as a short term means of reducing the symptoms but it is now clear that the use of bismuth together with a single antibiotic frequently fails to eradicate the infection and has a high rate of reinfection (Rauws, Erik A. J. et al, Gastroenterology, 1988, 94: 33-40). WO 89/03219 (Burody) describes the use of a combination of bismuth, a first antimicrobial agent and a second antimicrobial agent. This treatment regimen is not only complicated and expensive but. still has unacceptably high ielapse rates.
A second approach to combination therapy uses histamine-H 2 receptor blocking anti-secretory agents. European Patent applications 282132 and 282131 (Proctor and Gamble) describe the use of H 2 antagonists in combination with bismuth or Camovlobacter inhibiting antimicrobial agents. This approach has still led to high relapse rates and may lead to many of the undesirable side effects of the individual treatment components.
Patent application No 219912 (Norwich Eaton) describes the use of nitrofurantoin as a monotherapy for the DroDhvlaxis of infectious treatment disoiders nastrointestinal or caused or mediated by Campylobacter-like organisms. This approach has been replaced in common practice by more complex duo or triple therapy.
There is still a requirement for an effective inonotherapy of gastrointestinal disorders associated with Helicobacter pylori.
We have now investigated the in vitro activity of various non-antibiotic antimicrobial agents versu Helicobacter pylori.
Triclosan (2-hydroxy-4,2 1 4 1- trichloro-diphenyl ether) is described and claimed, along with varLous formulations, in GB Patents '1022744, 1024022 and 1038185, published in 1966. Whilst G8 1022744 claims that triclosan may be used for "oral administration to disinfect the intestinal and urinary tracts" very few details are given, and no specific infections or conditions are mentioned. Since these patents were published Applicant is not aware of any publications suggesting the use of triclosan in the treatment of any gastrointestinal diseases, nor have there jo been any suggestions that triclosan may have activity against gastrointestinal infections with Helicobacter pylori' or any of the associated disease conditions.
According to the present invention there is provided the use of triclosan for the preparation of a medicament for the treatment of gastrointestinal disorders associated with Helicobacter pylori infections.
The effective oral dose of triclosan will depend upon the severity of the condition to be treated. Generally the dosage employed will fall within the range of 1 to 200mg and for most patients will fall within the range 10 to 100mg, for example 25mg. The frequency of dosing will again be dependent upon the severity of the condition to be treated and its sensitivity to the treatment, the dosing normally being up to three times a day.
The medicaments will be for oral administration and may be in the form of powders, granules, spheroids, tablets, capsules, solutions or suspensions.
For ease of administration and for accurac y in dosing, the medicament may be prepared in unit dosage forms. Thus in the case of powders, granules or spheroids they may be conveniently packed into sachets, each unit containing, from 1 to 100--ng (preferably 10 to 60mg) triclosan. In the case of tablets or capsules each unit will contain from 1 to 100mg (preferably 10 to 60mg) triclosan.
The medicament in the form of granules may be prepared by standard methods such as wet or dry granulation (slugging). They may be effervescent or non-effervescent to be mixed with a suitable quantity of water for administration as a drink. They may also be chewable granules.
The medicaments in the form of spheroids may be prepared by the following method. The triclosan and a carrier (for example microcrystaline cellulose) plus any other excipients are mixed with a sufficient quantity oil water to form a 'plastic' wet mass. The mass is extruded into cylinders of uniform diameter and equal length. The extrudates are rolled into spheres using a spheroniser and then dried, preferably in a fluid bed dryer.
The medicaments in the form of powders may be prepared by blending the triclosan and one or more pharmaceutically acceptable excipients such as bulking agents/diluents.
The medicaments in the form of tablets may be prepared by standard methods such as granulation or direct compression. They may be buffered and effervescent or non-effervescent.
The medicaments in the form of capsules may be prepared by standard methods such as filling powders, granules or spheroids into hard gelatine capsules or adding triclosan to melted pharmaceutically acceptable excipients before filling into capsules.
The medicaments in the form of solutions or suspensions may be prepared by mixing the components with a liquid such as water. Cunveniently the liquid formulations will contain 1 to 100mg of triclosan in 5 to 20m1. They may include pharmaceutically acceptable conventional excipients such as suspending agents, buffer systems etc. In order to.pr.otecb the medicaments against microbial 'deterioration it is preferable to include a preservative. A suitable system is a combination of methyl- and propylpara-hydroxybenzoate (methyl and propyl parabens).
The medicaments may also include one or more of a colourising, sweetening or flavouring agent.
In another aspect of the invention the medicaments may be formulated as gastric sustained release compositions, having prolonged residence time within the stomach and continuously releasing triclosan during that time. In this aspect the medicaments may be formulated so as to produce floating alginate rafts within the stomach, or as mucoadherant-coated granules or spheroids.
Medicaments formulated so as to produce floating alginate rafts within the stomach may be in solid single dosage form as tablets, or in liquid form.
In the form of tablets the alginate containing gastric sustained release compositions of triclosan will comprise is to BOOMg of alginic acid and/or a salt thereof, preferably a sodium, potassium or magnesium salt; 50 to 250mg of a sodium or potassium carbonate or bicarbonate salt; 1 to 100mg, preferably 10 to 60mg, triclosan; and optionally up to 100mg calcium carbonate. The compositions cnay also contain standard tableting excip1Lents known in the art, such as soluble fillers, binders, lubricants and flavours. The tablets may be produced by standard procedures such as direct compression or by wet or dry granulation followed by tablet compression.
In the form of liquids the alginate containing gastric sustained release compositions of triclosan will comprise an aqueous medium containing 0.1 to 2% w/v triclosan; 1 to 8 1% w/v sodium or potassium alginate; 1.3 to 6. 5% w/v sodium or potassium carbonate or bicarbonate salt; 0.5 to 4% calcium carbonate and optionally 0.3 to 1.7% w/v of a suspending agent, preferably carbomer. These liquid compositions may also contain standard excipients known in the art such as preservatives, flavouring and colouring agents. The alginate containing liquids may be produced by dispersing all of the ingredients except carbomer in water. if carbomer is used it will be added to the dispersion as a neutralised suspension in water.
When the alginate compositions described above come into contact with the, normally, acid conditions of the stomach the carbonate or bicarbonate salts produce effervescence, which aerates the raft structure formed by the alginates, causing it to float. It has, however, been 7 noted that in some patients suffering from Helibacter pylori infections the pH o1F the stomach contents may be elevated (possibly to as high as pH6) reducing effervescence and, consequently, reducing the ability of the rafts to float.
Floating rafts may still be formed in such patients however either by, in the case of tablet compositions, further including a pharmaceutically acceptable, solid carboxylic acid, or an acid salt thereof in a sufficient amount to neutralise between one quarter and all of the carbonate and/or bicarbonate of the composition; or, in the case o tablet or liquid. compositions, co-administering such.an aci or acid salt. A suitable acid is citric acid.
Mucoadherent-coated granules 01 spheroids Ti a y be produced by forming triclosan containing granules or is spheroids as described above, and coating them with one or more known mucoadherent polymers such as carboxymethylcelllulose or sodium carboxymethylcellulose, carbomer (especially carbomer 934P), tragacanth, sodium alginate, methylcellulose, hydroxyethylcellulose, poly (ethylene oxide) or hydroxypi.opylmethylcellulose. The coating may be carried out by any conventional technIque, for example spray coating. Once coated and dried the granules or spheroids may be filled into sachets or gelatine capsules or, if sufficiently robust microadherent coatings have been used, compressed to form tablets.
The invention is illustrated by the following examples. EXAMPLE 1 Tablet f A -preparation in the form of tablets according to the following formula was prepared Triclosan 200g Microcrystalline cellulose 1000g Magnesium stearate 6g The materials were blended together and compressed into tablets using 8mm diameter concave punches. Individual tablets had a weight of 301.5mg and contained 50mg triclosan.
EXAMPLE 2 Suspension A preparation in the form of a suspension was prepared according to the following formula Triclosan 1.0% w/v 3. 0 ',5G w/v 0.06% w/v 0.14% w/v Peppermint flavour 0.1% w/v Sodium saccharin 0.05% w/v Water to 100% The triclosan, parabens, flavouring and saccharin were dispersed in the bulk of the water. The sodium carboxymethylcellulose was added and stirred vigorously until dissolved. Water was added to bring the suspension to final volume and the^ suspension was mixed until it was homogenous.
EXAMPLE 3 Buffered tablets is Sodium carboxymethylcellulose Propy! parabens 'I.ethyl parabens A preparation in the form of buffered tablets was prepared according to the following formula Triclosan 50g Sodium carbonate 300g Hog 30g 5g The ingredients were blendeJ together and then compressed using 13mm diameter normal concave punches to a weight of 985mg. Each tablet contained 50mg of triclosan.
EXAMPLE 4 Capsules A preparation in the form of capsules was prepared according to the following formula Triclosan 150g Polyethyl glycol 6000 to 1050g The polyethylene glycol was melted and the triclosan added and stirred until dissolved. The melt was dosed appropriately sized hard gelatine capsules such that capsule contained 10, 50 or 100mg triclosan. EXAMPLE 5 Solution A preparation in the form of a solution was prepared according to the following formula Triclosan Propylene glycol Polyethylene glycol 300 Propyl paraben Microcrystalline cellulose Modified cellulose gum Magnesium stearate was i nto 20 each 1 % w/v 20% w/v 3% w/v 0.0375% w/v Example 5 (contd) Methyl paiaben 0.09% w/v Flavour qs Glycerol G to 100% The propylene glycol and polyethylene glycol were mixed and the triclosan was added and stirred until dissolved. The remaining ingredients were added and stirred until d'Lssolved.
EXAMPLE 6
Effervescent tablets A preparation in the form of prepared according to the following Tiiclosan Sodium carbonate Citric acid Sodium bicarbonate Sorbitol direct compression grade Maltodextrin 200g Peppermint flavour 50g Sodium saccharin 25g Magnesium stearate 10g The citric acid, sodium bicarbonate and 200g of the sorbitol were mixed in a planetary mixer and granulated with a small amount of water. The granules were dried in a fluid bed dryer and then passed through a 78Ogm mesh sieve. The remaining ingredients were added and blended together by tumble mixing. The mixture was compressed using 18mm effervescent tablets was f orinula Sog 1 00g 250g 400g 1 000g - 1 1 - punches to a final tablet weight of 208Sing.
contained 50mg triclosan.
EXAMPLE 7
Sachets A preparation in the f orm of sachets was prepared according to the following formula Triclosan 100g C "Cog Citric acid e_ Sodium bicarbonate 800g Each tablet codium carbonate d 0 0 g Sorbitol 7000g Sodium saccharin 100g Peppermint flavour 200g The ingredients were blended together and filled into sachets such that each sachet contained 50mg triclosan. EXAMPLE 8 Capsules A preparation in the form of capsules was prepared according to the following formula Triclosan 5g Microcrystalline cellulose 44g Talc (sterilised) 1g The powders were blended together and filled into appropiLatly sized hard gelatin capsules such that e a c,h capsule contained 10, 25 or 50mg triclosan.
EXAMPLE 9
Alqinate containinq tablets A gastric sustained release preparation in the form of - 12 alginate containing tablets was prepared according to the following formula per batch per tablet Triclosan Alginic acid FD (Protan) Sodium bicarbonate Calcium carbonate Mannitol 9 2000 680 320 6092 Magnesium stearate 100 Polyvinyl pyrrolidone (PVPk30) 400 Flavour peppermint Ferm 57.279 200 so Sodium saccharin a 2 All the ingredients other than the triclosan, magnesium stearate and the polyvinyl pyrrolidone were sieved and mixed in a planetary mixer. The polyvinyl pyrrolidone was dissolved in 2.7 litres of isopropyl alcohol and used to granulate the mixed powders. The granules were dried in a C. 1 i luid bed dryer at 700C for 30 minutes then sieved. The 20 triclosan and magnesium stearate were blended into the granules and the mixture was compressed using 25mm punches to a final tablet weight of 2.5g. Each tablet contained 50mg triclosan.
EXAMPLE 10 25 Alginate containing tablets A gastric sustained release preparation in the form of alginate containing tablets was prepared according to the following formula mg so 500 so 1523 25. 100 1 Triclosan Alginic acid LF-60 (Protan) Sodium bicarbonate Calcium carbonate Citric acid Mannitol Magnesium stearate 10.25 Flavour peppermint Ferm 57.279 20.45 Sodium-saccharin, 0'.80 All the ingredients with the exception of the citric acid and magnesium stearate were sieved and mixed in a planetary mixer at a low speed setting. 250ml of deionised water were then int3:oduced and the mixing speed increased, mixing continued for 3 minutes. The resultant granules were dried in an oven at 10011C for 40 minutes and then sieved. The citric acid and magnesium stearate were blended into the granules and the resultant mixture was compressed using 25mm punches to give 2.57g tablets each containing 50mg.triclosan.
EXAMPLE- 11
Alginate containing suspension A gastric sustained release preparation in the form of an alginate containing suspension was prepared according to the following formula per batch 9 20.45 204.70 69.60 32.75 69.60 623.50 per tablet mg
500 170 170 1523 per batch w/v 9 Triclosan 250 0.5 Carbomer 934P 325 0.65 Sodium alginate SF120 (Protan) 750 1.5 Sodium bicarbonate 1335 2.67 Calcium carbonate 800 1.6 Methyl paraben 200 0.4 Propyl paraben 30 0.06 20% Sodium hydroxide(w/v) approx 650 1.3 Deionised water to 50 L to 100% The carbomer- was fully dispersed in approximately 20 litres of the deionised water. 20% w/v sodium hydroxide was added to bring the pH to between 7.0 and 7.2. The sodium alginate was dispersed in a separate 20 litres of deionised water and the sodium bicarbonate, parabens and calcium carbonate were added and stirred until homogenous. The gelled, neutralised carbomer was added to the alginate dispersion and mixed until homogenous. The triclosan was added and mixed and the batch was adjusted to final volume with deionised water. EXAMPLE 12 Carbomer coated spheroids A gastric sustained release preparation in the form of capsules containing carbomer-coated spheroids was prepared according to the following formula procedure.
Spheroids were prepared according to the following formula per batch Microcrystalline cellulose Triclosan 25OOg 500g The powders were blended for 15 minutes, following which a total of 950ml of deionised water was added in aliquots whilst stirring continued at a slow speed. When the water had been incorporated the speed was increased for 2 minutes. The wet mass was extruded through a perforated screen of 1mm diameter holes using a Nice extruder (Nica Systems, Sweden). The wet extrudates were spheronised using a Nica spheroniser at 650rpi-ii for 5 minutes. The -spheroids were dried at 500C for 1 hour.
A coating suspension was produced according to the following formula Carbomer 934P Polyethylene glycol 6000 Citric acid Deionised water 60. Og 60. Og 56.25g 3000.00m1 The citric acid and polyethylene glycol were dispersed in 2250m1 of the deionised water. The carbomer was added and dispersed by stirring at 200Orpm. The solution was made to volume by the addition of the rest of the water.
The dried triclosan spheroids were coated with the coating suspension using an Aeromatic Strea 1 fluid bed system and a spray nozzle diameter of 1. 1 mm. All of the suspension was used to coat the 3Kg of cores.
The coated spheroids were dried and filled into hard gelatine capsules such that each capsule contained 25mg of triclosan.
EXAMPLE 13 Sodium carboxymethy1cellulose-coated spheroids A gastric sustained release preparation in the form of capsules containing sodium carboxymethylcellulose-coated 5 spheroids was produced according to the following procedure.
Triclosan containing spheroids were produced as described in Example 12. A coating suspension was produced following formula Sodium carboxymethy1cellulose 60g (low viscosity grade) Polyethylene glycol 6000 60g Deionised water 3000ml The sodium carboxymethy1cellulose and polyethylene glycol were sequentially dispersed in.22-400ml of the de'Lonised water by stirring at 20DOrpm. The solution was made up to volume by the addition of the rest of the water.
The triclosan cores were coated with the above suspension using the method of Example 12, all 3 litres of suspension were used for the 3Kg of cores.
The coated spheroids were dried and filled into hard gelatine capsules such that each capsule contained 25mg of triclosan.
The in vitro activities of a range of antimicrobial compounds versus Helicobacter pylori were determined by methods based on those of McNulty et al (Antimicrobial Agents and Chemotherapy, 28, 837- 838, 1985). The Minimum Inhibitory concentrations for 50% and 90% of the strains according to the A used (MIC50 and MIC90), versus each antimicrobial were determined using an agar dilution technique.
The MILC of an antimicrobial agent was defined as that concentration (in mg per litre of agar) at which less than 1 in 100 5 organisms produced visible colonies.
Helicobacter pylori strains were isolated from gastric antrum biopsy specimens taken at routine endoscopy during investigation of upper gastrointestinal symptoms. They were identified as Helicobacter pylori by their colonial morphology, gram stain appearance and positive rapid urease test. The organisms were stored in liquid nitrogen' before use and subcultured for testing by 48 hour incubation, at 370C under 10'IfO caibon dioxide in Tryptone Soya Broth (TSB, OXOID, UK) plus 5% horse serum (Tissue Culture Services, UK).
The first test procedure determined the effectiveness of a range of antimicrobial substances versus 16 to 10 Strains of Helicobacter pylori at neutral PH. Freshly prepared Isosensitest Agar of PH 7.2 (Oxoid, UK) supplemented with 10% saponinlysed horse blood was used to prepare a dilution series of each antimicrobial from which agar plates were produced. A multipoint inoculator (Den'Ley-Tech, UK) was used to deliver 1).0 of undiluted test culture to the surface of each plate in the dilution series to give approximately 10 6 cfu/spot. The plates were incubated for three days at -370C in a microaerobic atmosphere of 6% oxygen and 10% carbon dioxide.
Table 1 presents tes.t data for the twelve s-elected antimicrobial agents tested against HalicObacter pylori at neutral pH.
TABLE 1 presents P11C50 and MIC90 values of twelve anti microbial agenLs against eighteen isolates os Helicobacter pylori MIC (mg/1) MILC90 8 16 4 8 is 16 is is 32 32 Antimicrobial AQent Triclosan Tinidazole Cetalkonium Cl Cetyl pyridinium- Cl Clioquinol Hexetidine Dichlorphen Halquinol 4-Hexylresorcinol Hibitane PCM MIC50 1 0.5 2 a 16 16 16 16 32 32 Ranqe 0. 25-1 C 0.25-16 2 4 8-16 8-16 8-16 is 16-32 16-32 3 222 64 8-64 Guaiacol, 64 64 32-120^ From Table 1 it can be seen that triclosan with an MICSO of 1mg/1 and an MIC90 of Smg/1, and tinidazole with an MIC50 of 0. 5mg/1 and an MIC90 of 16mg/1, demonstrated the greatest activity of the twelve antimicrobial agents tested. A reported MIC90 for bismuth subcitrate at neutral pH is lsmg/1.
Three of the antimicrobial agents were selected for further evaluation over the pH range of 5 to 8, a range at which Helicobacter pylori survives. The threeselected 1 agents were triclosan, clioquinol (5-chloro-7-iodo-8 hydroxy-quinclone) and cetalkonium chloride. Tinidazole was rejected at this stage due to an observed bimodal distribution of MICs. Fifteen of eighteen isolates were sensitive with an MIC of less than 2mg/l, the other three strains demonstrating evidence of re5i5tance with an MIC of 16mg/l. This bimodal distribution has previously been reported with metronidazole, another imidazole. In the resistance to the nitro- ic) imidazoles can occur in many strains of Helicobacter pylori after only three- weeks treatment, therefore, this agent would not be recommended for the treatment of Helicobacter pylori associated gastrointestinal disorders.
The MIC90s of the three selected antimicrobial agents is were determined for sixteen to eighteen clinical isolates of Helicobacter pylori over the pH range 5 to 8. In the test procedure, Sorensens phosphate buffer (0.1M) was used to prepare the range of pH values 5, 5.5, 6, 6.5, 7, 7.5 and 8. Oxoid Columbia Agar Base (CM331) was added and the media autoclaved. After cooling to 500C, 7% Lysed Horse Blood (Tissue Culture Services, UK) was added and media at each pH was used to prepare a range of concentrations of the three selected test antimicrobial agents. To ensure pH stability, a surface pH electrode was used to monitor controi plates before, during and at the end of the three day microaerobic incubation.
The MIC90 was determined for each at each pH as described in the previous test procedure.
f clinical situation, acquired Tables 2-4 present the test data using the above test procedure. TABLE 2 - presents the effect of pH on the activity (MIC90 mg/1) of triclosan against sixteen isolates of Helicabacter pylori Range (ma/1) 0.06-0.25 0.06-1 0.12-2 2 0.12-4 2 0.03-4 2 0.06-4 8.0 2 0.06-2 From Table 2 it can be seen that the MIC90 for 15 triclosan was low at pH 5.0 and unaffected in the range pH 5.5 to B.O. TABLE 3 - presents the effect of pH on the activity (MIC90 mg/1) of clioquinol against sixteen isolates of Helicobacter pylari pH Value MIC90 (mg/l) 5.0 0.25 5.5 6.0 6.5 7.0 7.5 pH Value MIC90 (mg/l) Range (mg/l) 5.0 2 0.5-4 5.5 8 2-8 6.0 8 2-8 6.5 8 0.5-16 7.0 2 0.5-4 7.5 2 0.5-4 8.0 1 0.5-2 From Table 3 it can be seen that the activity of t clioquinol was only slightly affected by pH. The diFference would not be clinically important.
TABLE 4 - presents the effect of pH on the activity (MIC90 mg/1) of cetalkonium chloride against eighteen isolates of Helicobacter pylori pH Value MIC90 (mg/l) Range (mq/1) 0.5-2 0.5-2 1-4 2-4 3.0 5.3 6.0 6.5 7.0 4 2-4 7.5 4 1-4 8.0 2 1-8 Cetalkonium chloride was largely unaffected by pH over 15 the range 5 to 8.
1 2 2 4 Of the antimicrobial agents evaluated over a range of pH from 3 to 8, triclosan demonstrated the greatest activity with an MIC90 of 0.25mg/1 (range 0.06-0.25) at pH 5. The activity of the other two agents, clioquinol and cetalkonium chloride, demonstrated similar MIC90 activity profiles across the pH range.

Claims (14)

1. The use of triclosan for the preparation of a medicament for the treatment of gastrointestinal disorders associated with Helicobacter pylori infection.
2. Use according to Claim 1 characterised in that the medicament is in unit dosage form, in the form of powders, granules or spheroids packed into sachets, each unit containing from 1 to 100mg triclosan.
3. Use according to Claim 2 characterised in that each unit contains 10 to 60mg triclosan.
4. Use according to Claim 1 characterised in that the. medicament is in unit dosage form, in the form of tablets or capsules, each unit containing 1 to 100mg triclosan.
1
5. Use according to C.Laim 4 characterised in that each unit contains 10 to 60mg triclosan.
6. Use according to Claim 1 characterised in that the medicament is in the form of a liquid containing 1 to 100mg of triclosan in 5 to 20m1.
7. Use according to Claim 1 characterised in that the medicament is in the form of a gastric sustained release composition.
8. A gastric sustained release composition of triclosan for the treatment ol ga stro intestinal disorders associated with Helicobacter pylori infections in a solid unit dosage form comprising 200 to 600mg of alginic acid and/or a sodium, potassium or magnesium salt thereof; 50 to 250mg of a sodium or potassium carbonate or bicarbonate salt; 1 to 100mg triclosan; and optionally up to 100mg calcium 7 1 carbonate.
9. A composition as claimed in Claim 8 wherein each unit contains 10 to 60mg triclosan.
10. A composition as claimed in Claim 8 or Claim 9 further including a pharmaceutically acceptable solid carboxylic acid or an acid salt thereof; in a sufficient amount to neutralise between one quarter and all of the carbonate and/or bicarbonate of the composition.
11. A composition as claimed in Claim 10 wherein the acid is citric acid.
12. An aqueous gastric sustained release composition of triclosan for the treatment of gastrointestinal disorders associated with Helicobacter pylori, infections comprising 0. 1 to 2%a wj/v triclosan; 1 to 8% w/v sodium or potassium alginate; 1.3 to 6. 5 % W/v of a sodium or potassium carbonate or bicarbonate salt; 0.5 to 4%D w/v calcium carbonate; and optionally 0.3 to 1.7% w/v carbomer.
13. A gastric sustained release composition of triclosan XI lor the treatment of gastrointestinal disorders associated with Helicobacter pylori infections in the form of granules or spheroids comprising triclosan and optionally a pharmaceutically acceptable carrier, coated with a mucoadherent polymer such as carboxymethy1cellulose, sodium carboxymethylcellulose, carbomer, tragacanth, sodium alginate, methylcellulose, oxide) or hydroxypropylmethylcellulose.
14. A gastric sustained release composition of triclosan substantially as described in any one of Examples 9 to 13.
hydroxyethylcellulose, poly (ethylene Published 1991 at The Patent Office, Concept House, Cardiff Road. Newport, Gwent NP9 I RH. Further copies may be obtained from Sales Branch, Unit 6. Nine Mile Point. Cwrnfelinfach. Cross Keys, Newport. NP I 7HZ. Printed by Multiplex techniques ltd, St Mary Cray. Kent.
GB9109439A 1990-05-03 1991-05-01 Medicament containing triclosan for treating gastro-intestinal disorders Expired - Fee Related GB2243549B (en)

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CA2041400C (en) 2001-04-24
CA2041400A1 (en) 1991-11-04
DE69110969T2 (en) 1995-11-16
GB9010039D0 (en) 1990-06-27
GB9109439D0 (en) 1991-06-26
HK1007963A1 (en) 1999-04-30
EP0455475A2 (en) 1991-11-06
EP0455475B1 (en) 1995-07-05
IE911483A1 (en) 1991-11-06
AU645555B2 (en) 1994-01-20
AU7596891A (en) 1991-11-07
ZA912933B (en) 1992-01-29
NZ237904A (en) 1993-06-25
DK0455475T3 (en) 1995-10-30
DE69110969D1 (en) 1995-08-10
US5286492A (en) 1994-02-15
ATE124626T1 (en) 1995-07-15
IE65826B1 (en) 1995-11-15
EP0455475A3 (en) 1992-02-26

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