US20110098359A1 - Compositions and Methods for Treatment of Glaucoma - Google Patents

Compositions and Methods for Treatment of Glaucoma Download PDF

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US20110098359A1
US20110098359A1 US12/672,475 US67247508A US2011098359A1 US 20110098359 A1 US20110098359 A1 US 20110098359A1 US 67247508 A US67247508 A US 67247508A US 2011098359 A1 US2011098359 A1 US 2011098359A1
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paracetamol
glaucoma
treatment
administered
patient
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David Meyer
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Stellenbosch University
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/16Amides, e.g. hydroxamic acids
    • A61K31/165Amides, e.g. hydroxamic acids having aromatic rings, e.g. colchicine, atenolol, progabide
    • A61K31/167Amides, e.g. hydroxamic acids having aromatic rings, e.g. colchicine, atenolol, progabide having the nitrogen of a carboxamide group directly attached to the aromatic ring, e.g. lidocaine, paracetamol
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P27/00Drugs for disorders of the senses
    • A61P27/02Ophthalmic agents
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P27/00Drugs for disorders of the senses
    • A61P27/02Ophthalmic agents
    • A61P27/06Antiglaucoma agents or miotics

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  • This invention relates to medicament, more specifically to a medicament for use in the treatment of glaucoma.
  • Glaucoma is a well-known eye disorder characterised by abnormally high pressure within the eyeball that leads to loss of retinal ganglion cells in a characteristic pattern of optic neuropathy. Although raised intraocular pressure is a significant risk factor for developing glaucoma, there is no set threshold for intraocular pressure that causes glaucoma. Nerve damage may occur at a relatively low pressure in some patients, while others may have high eye pressure for years and yet never develop damage. Glaucoma affects one in two hundred people aged fifty and younger, and one in ten over the age of eighty.
  • glaucoma leads to permanent damage of the optic nerve and resultant visual field loss, causing impaired vision and sometimes blindness.
  • the loss of visual field often occurs gradually over a long time and may only be recognized when it is already quite advanced.
  • Cannabis, or marijuana is known to reduce the intraocular pressure.
  • Cannabis, or marijuana is known to reduce the intraocular pressure.
  • the widespread use of cannabis as an illegal recreational substance as well as its side effects have limited its application for treating the intraocular pressure in glaucoma.
  • paracetamol for use in a method of treating glaucoma, which method comprises administering to a patient in need of such treatment an effective amount of paracetamol (also known as acetaminophen).
  • the paracetamol to be administered in the form of an ophthalmic solution; for the solution to contain between 0.1 to 5% of paracetamol; and for one to two drops of the solution to be administered to each eye 4 to 6 hourly.
  • the paracetamol to be administered to a patient in oral format 4 to 6 hourly.
  • the invention further provides an ophthalmic solution including as its active ingredient paracetamol.
  • the solution to include paracetamol in the range 0.1 to 5%; and for the solution to further include one or more of the following excipients: hydroxypropylmethylcellulose, benzalconium chloride, polyacrylic acid; and Teargel®.
  • the invention also provides for the use of paracetamol in the manufacture of a medicament for use in a method of treating glaucoma which method comprises administering to a patient in need of such treatment an effective amount of paracetamol.
  • the invention still further provides a method of treating glaucoma which includes administering to a patient in need thereof an effective amount of paracetamol.
  • Further features of the invention provide for the method to include the oral administration of paracetamol, alternately the ophthalmic administration of paracetamol to a patient.
  • the invention yet further provides a package which includes at least one dose of paracetamol in an amount effective for the treatment of glaucoma and instructions for the use thereof in a treatment for glaucoma.
  • the at least one dose to be suitable for oral administration, alternately suitable for ophthalmic administration.
  • FIG. 1 is a two-dimensional line graph showing mean flux values of paracetamol in aqueous solution (0.1%) and Teargel® (0.1%) across human and rabbit corneas where bars represent the standard error of the mean.
  • CB1 receptor is expressed in the central nervous system, eye and numerous other tissues and has been recognized as an important therapeutic target for glaucoma. It is suspected that it is through this pathway that paracetamol acts to reduce intra-ocular pressure.
  • an ophthalmic solution was proposed as the preferable manner of delivering an effective amount of paracetamol to the eye in a glaucoma patient.
  • 1 mg/ml (0.1%) solution of paracetamol in phosphate corneas In more than 2000 corneal penetration experiments it has been demonstrated that paracetamol does penetrate the cornea well. Corneal penetration is statistically significantly improved when the paracetamol is suspended in polyacrylic acid gel.
  • HIV human immunodeficiency virus
  • rabbit corneas were obtained from 6 freshly slaughtered rabbits (Country Lane Nursery Farm, Kraaifontein, Cape Town, South Africa). Excised corneas were immediately placed in McCarey-Kaufman solution and transported to a laboratory within 6 hours.
  • the McCarey-Kaufman solution consisted of a stock solution of Medium 199 (Sigma Chemical Company, St.
  • tissue specimens were thawed at room temperature in phosphate buffered saline (PBS, pH 7.4). Although some damage may have occurred on a cellular level, the processes of freezing, storage, and thawing were demonstrated to have no adverse effects on the permeability characteristics of corneal tissues in 2 previous studies (Van der Bijl et al., 2001; Van der Bijl et al., 2002).
  • PBS phosphate buffered saline
  • corneas were very carefully cut, so as not to damage either the endo- or epithelial surfaces, into 4-mm 2 sections and mounted in flow-through diffusion cells (exposed areas, 0.039 cm2) as previously described (Van der Bijl et al., 1997; Van der Bijl et al., 1998; Van der Bijl et al., 2000).
  • Each experiment using the paracetamol solution was repeated six times for the human and rabbit corneas, respectively.
  • tissue disks were equilibrated for 10 minutes with PBS (pH 7.4) at 20° C. in both the donor and receiver compartments of the diffusion cells.
  • the PBS was removed from the donor compartment and replaced with 1.0 mL of PBS, containing 1 mg/mL (0.1%) paracetamol in PBS at pH 7.4 (w/v) or else 1 mg/mL (0.1%) paracetamol in a commercially available artificial tear gel i.e. Teargel® liquid gel (Restan Laboratories, Bryanston, South Africa).
  • Teargel® liquid gel Restan Laboratories, Bryanston, South Africa.
  • the latter is a highly viscous clear gel, with an extended tear film break-up time.
  • the gel after its addition to the donor chamber, was capped completely with a tight-fitting teflon disc and 1 mL of PBS deposited on top of the disc.
  • the PBS did not, in any way, mix with the gel, but was simply used to prevent dessication of the gel during the 24-hour experiment.
  • Each gram of the latter gel contains 2 mg of polyacrylic acid and cetrimide 0.01% m/m as a preservative.
  • PBS at 20° C. was pumped through the receiving chambers at a rate of 1.5 ml/h with a ISMATEC® 16 Channel High precision tubing pump and collected, by means of a ISCO Retriever IV fraction collector, at 2-h intervals for 24 h.
  • the permeability studies were performed under sink conditions, i.e. at the completion of each run the concentration of paracetamol solution in the acceptor chamber never reached 10% of that in the donor compartment.
  • Paracetamol containing samples were collected in appropriate sampling tubes of the fraction collector. Samples were analyzed at the Division of Pharmacology, Faculty of Health Sciences, Whybosch University by HPLC with UV detection. The collected fractions were analyzed directly after completion of the respective experiment for their paracetamol content.
  • Q indicates quantity of substance crossing membrane (in ng); A, membrane area exposed (in cm 2 ); and t, time of exposure (in minutes).
  • Non-linear regression analyses (third order polynomials) were performed using a GraphPad Prism, Version 4, 2003 computer programme. An F test was used to compare entire curves. A t-test at steady state, was also performed for comparative purposes. A significance level of 5% was used for all tests and comparisons.
  • Permeant-containing effluent samples collected from the acceptor compartments of the perfusion apparatus over the 2-hour sampling intervals, were analyzed using an Hewlett Packard 1100 series high-performance binary liquid chromatograph (Agilent Technologies, Waldbronn, Germany) equipped with an Agilent Eclipse (XDB-C18) Zorbax analytical column (3.5- ⁇ m particle size), 150 ⁇ 4.6 mm (ID). The latter column was preceded by a 30 ⁇ 2.1-mm (ID) 018 guard column (40- ⁇ m particle size). The temperature was maintained at 40° C. and a flow rate of 1.0 mL/min was used for the entire run.
  • the mobile phase consisted of a mixture of 2 solvents, A (50 mol/L KH 2 PO 4 , pH 5.4) and B (acetonitrile-isopropanol, 4:1 vol/vol).
  • A 50 mol/L KH 2 PO 4 , pH 5.4
  • B acetonitrile-isopropanol, 4:1 vol/vol.
  • Three isocratic mixtures of A:B were used in sequential order as follows: firstly for 0 to 1.0 min: 90% Solvent A/10% Solvent B; secondly for 1 to 4.0 min: Linear gradient to 70% Solvent A/30% Solvent B, thirdly for 4.10 mins: return to use of 90% Solvent A/10% Solvent B.
  • En equilibration time of 2.5 min was used for 90% Solvent A/30% Solvent B.
  • FIG. 1 Mean flux values for 0.1% paracetamol in aqueous solution (PBS) and Teargel (TG) across the frozen/thawed rabbit and human cornea versus time are shown in FIG. 1 .
  • the diffusion rates of paracetamol (in both PBS and TG) across human comeas were higher in the first few hours of the diffusion experiment than the values found across rabbit corneas. Steady state was also reached much earlier for paracetamol diffusion across human corneas. Teargel as a soluent did not affect the diffusion rate of paracetamol across human corneas as the graphs are nearly identical. Teargel does, however, increase the diffusion rate of paracetamol across rabbit comeas.
  • the invention provides a promising breakthrough in the treatment of glaucoma. This is particularly so for paracetamol in an ophthalmic solution which shows good corneal permeability of paracetamol. This has the benefits of the paracetamol acting directly on to have a direct effect on the therapeutic targets for glaucoma as well as reducing its effects on the hepatic and renal systems.
  • doses of paracetamol which are effective in the treatment of glaucoma will be packaged together with instructions for the use thereof in the treatment of this condition.
  • Such doses could be intended for oral administration and could consist of one or more tablets, capsules or the like.
  • the doses could be intended for ophthalmic administration and could be provided by one or more containers of a suitable ophthalmic solution intended for single or repeated use.

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Abstract

A new use for paracetamol in a method of treating glaucoma, which method comprises administering to a patient in need of such treatment 500 mg to 1000 mg of paracetamol in oral format 4 to 6 hourly. An ophthalmic solution is also provided containing between 0.1 to 5% of paracetamol which is administered as one to two drops in each eye 4 to 6 hourly. The ophthalmic solution further includes one or more of the following excipients: hydroxypropylmethylcellulose, benzalconium chloride, polyacrylic acid such as Teargel®.

Description

    FIELD OF THE INVENTION
  • This invention relates to medicament, more specifically to a medicament for use in the treatment of glaucoma.
    • BACKGROUND TO THE INVENTION
  • Glaucoma is a well-known eye disorder characterised by abnormally high pressure within the eyeball that leads to loss of retinal ganglion cells in a characteristic pattern of optic neuropathy. Although raised intraocular pressure is a significant risk factor for developing glaucoma, there is no set threshold for intraocular pressure that causes glaucoma. Nerve damage may occur at a relatively low pressure in some patients, while others may have high eye pressure for years and yet never develop damage. Glaucoma affects one in two hundred people aged fifty and younger, and one in ten over the age of eighty.
  • If not treated, however, glaucoma leads to permanent damage of the optic nerve and resultant visual field loss, causing impaired vision and sometimes blindness. The loss of visual field often occurs gradually over a long time and may only be recognized when it is already quite advanced.
  • Several drugs with different mechanisms of action are currently available for the treatment of glaucoma, each with a specific mechanism of action and efficacy or tolerability. New molecules and mechanisms of action are the subject of much research. Cannabis, or marijuana, is known to reduce the intraocular pressure. However, the widespread use of cannabis as an illegal recreational substance as well as its side effects have limited its application for treating the intraocular pressure in glaucoma.
    • OBJECT OF THE INVENTION
  • It is an object of this invention to provide a medicament for use in the treatment of glaucoma.
    • SUMMARY OF THE INVENTION
  • In accordance with this invention there is provided paracetamol for use in a method of treating glaucoma, which method comprises administering to a patient in need of such treatment an effective amount of paracetamol (also known as acetaminophen).
  • According to one aspect of the invention there is provided for the paracetamol to be administered in the form of an ophthalmic solution; for the solution to contain between 0.1 to 5% of paracetamol; and for one to two drops of the solution to be administered to each eye 4 to 6 hourly.
  • According to a second aspect of the invention there is provided for the paracetamol to be administered to a patient in oral format 4 to 6 hourly.
  • The invention further provides an ophthalmic solution including as its active ingredient paracetamol.
  • Further features of the invention provide for the solution to include paracetamol in the range 0.1 to 5%; and for the solution to further include one or more of the following excipients: hydroxypropylmethylcellulose, benzalconium chloride, polyacrylic acid; and Teargel®.
  • The invention also provides for the use of paracetamol in the manufacture of a medicament for use in a method of treating glaucoma which method comprises administering to a patient in need of such treatment an effective amount of paracetamol.
  • The invention still further provides a method of treating glaucoma which includes administering to a patient in need thereof an effective amount of paracetamol.
  • Further features of the invention provide for the method to include the oral administration of paracetamol, alternately the ophthalmic administration of paracetamol to a patient.
  • The invention yet further provides a package which includes at least one dose of paracetamol in an amount effective for the treatment of glaucoma and instructions for the use thereof in a treatment for glaucoma.
  • Further features of the invention provide for the at least one dose to be suitable for oral administration, alternately suitable for ophthalmic administration.
    • BRIEF DESCRIPTION OF THE DRAWINGS
  • The invention will be described, by way of example only, with reference to FIG. 1 which is a two-dimensional line graph showing mean flux values of paracetamol in aqueous solution (0.1%) and Teargel® (0.1%) across human and rabbit corneas where bars represent the standard error of the mean.
    •  DETAILED DESCRIPTION WITH REFERENCE TO THE DRAWINGS Treatment of Patients with Glaucoma
  • In initial trials, 1000 mg of paracetamol was administered orally 4 to 6 hourly to several patients with glaucoma. In all cases the intra-ocular pressure reduction was in the order of 30% after 24 to 48 hours. This compares well with the pressure lowering effect of currently available commercial preparations.
  • Extrapolating from this test, it appears that a dosage in the range of 500 to 1000 mg should be sufficient to treat glaucoma. Whilst such doses every 4 to 6 hours have been shown to be effective, it is possible that this frequency could be reduced.
  • Although the mechanism of action in the present application is not fully understood it is suspected that it is through paracetamol's indirect activation of cannabinoid CB1 receptors. The CB1 receptor is expressed in the central nervous system, eye and numerous other tissues and has been recognized as an important therapeutic target for glaucoma. It is suspected that it is through this pathway that paracetamol acts to reduce intra-ocular pressure.
  • Given the effects of paracetamol on the hepatic and renal systems, an ophthalmic solution was proposed as the preferable manner of delivering an effective amount of paracetamol to the eye in a glaucoma patient.
  • An ophthalmic solution was made up as follows: 1 mg/ml (0.1%) solution of paracetamol in phosphate buffered saline (pH=7.4) was used for half of the experiments and 1 mg/ml (0.1%) solution of paracetamol in phosphate corneas. In more than 2000 corneal penetration experiments it has been demonstrated that paracetamol does penetrate the cornea well. Corneal penetration is statistically significantly improved when the paracetamol is suspended in polyacrylic acid gel. These tests were conducted in the following manner.
    • Materials and Methods Cornea Specimens
  • Harvested donor comeas, which were deemed unsuitable for transplantation because of infections such as hepatitis B and human immunodeficiency virus (HIV), were obtained from The Eye Bank Foundation of South Africa Observatory from 6 patients (mean age±SD, 35±12 years; range, 24-65 years). In addition, rabbit corneas were obtained from 6 freshly slaughtered rabbits (Country Lane Nursery Farm, Kraaifontein, Cape Town, South Africa). Excised corneas were immediately placed in McCarey-Kaufman solution and transported to a laboratory within 6 hours. The McCarey-Kaufman solution consisted of a stock solution of Medium 199 (Sigma Chemical Company, St. Louis, Mo., U.S.A.) to which sodium bicarbonate, as well as 25 mM of HEPES and 5% dextran, was added before using the solution for the transport of corneal specimens. On arrival in the laboratory, the corneas were hemisected. One half was used immediately, and the other half was snap-frozen in liquid nitrogen and stored at −85° C. for no longer than 6 months before use. At least one piece of corneal tissue from each specimen was placed in formalin and retained for histologic examination.
  • No specimens were obtained in which there was clinical evidence of any corneal disease or pathology that might have influenced the permeability characteristics of the cornea. The study was approved by the Ethics Committee of the Faculty of Health Sciences, University of Stellenbosch and the Tygerberg Academic Hospital in Cape Town, South Africa.
    • Permeability Experiments and Histology
  • Before each permeability experiment, tissue specimens were thawed at room temperature in phosphate buffered saline (PBS, pH 7.4). Although some damage may have occurred on a cellular level, the processes of freezing, storage, and thawing were demonstrated to have no adverse effects on the permeability characteristics of corneal tissues in 2 previous studies (Van der Bijl et al., 2001; Van der Bijl et al., 2002). Thereafter, corneas were very carefully cut, so as not to damage either the endo- or epithelial surfaces, into 4-mm2 sections and mounted in flow-through diffusion cells (exposed areas, 0.039 cm2) as previously described (Van der Bijl et al., 1997; Van der Bijl et al., 1998; Van der Bijl et al., 2000). Each experiment using the paracetamol solution was repeated six times for the human and rabbit corneas, respectively. Before commencing each permeability experiment, tissue disks were equilibrated for 10 minutes with PBS (pH 7.4) at 20° C. in both the donor and receiver compartments of the diffusion cells.
  • Following equilibration, the PBS was removed from the donor compartment and replaced with 1.0 mL of PBS, containing 1 mg/mL (0.1%) paracetamol in PBS at pH 7.4 (w/v) or else 1 mg/mL (0.1%) paracetamol in a commercially available artificial tear gel i.e. Teargel® liquid gel (Restan Laboratories, Bryanston, South Africa). The latter is a highly viscous clear gel, with an extended tear film break-up time. The gel, after its addition to the donor chamber, was capped completely with a tight-fitting teflon disc and 1 mL of PBS deposited on top of the disc. The PBS did not, in any way, mix with the gel, but was simply used to prevent dessication of the gel during the 24-hour experiment. Each gram of the latter gel contains 2 mg of polyacrylic acid and cetrimide 0.01% m/m as a preservative. PBS at 20° C. was pumped through the receiving chambers at a rate of 1.5 ml/h with a ISMATEC® 16 Channel High precision tubing pump and collected, by means of a ISCO Retriever IV fraction collector, at 2-h intervals for 24 h. The permeability studies were performed under sink conditions, i.e. at the completion of each run the concentration of paracetamol solution in the acceptor chamber never reached 10% of that in the donor compartment. Paracetamol containing samples were collected in appropriate sampling tubes of the fraction collector. Samples were analyzed at the Division of Pharmacology, Faculty of Health Sciences, Stellenbosch University by HPLC with UV detection. The collected fractions were analyzed directly after completion of the respective experiment for their paracetamol content.
    • Calculation of Flux Values
  • Flux (J) values across membranes were calculated by means of the relationship

  • J=Q/A×t(ng×cm−2×min−1)
  • where Q indicates quantity of substance crossing membrane (in ng); A, membrane area exposed (in cm2); and t, time of exposure (in minutes).
    • Steady State Kinetics
  • When no statistically significant differences (p<0.05; analysis of variance and Duncan's multiple range test) between flux values were obtained over at least two consecutive time intervals, a steady state (equilibrium kinetics) was assumed to have been reached for a particular corneal specimen.
    • Statistical Analysis
  • Non-linear regression analyses (third order polynomials) were performed using a GraphPad Prism, Version 4, 2003 computer programme. An F test was used to compare entire curves. A t-test at steady state, was also performed for comparative purposes. A significance level of 5% was used for all tests and comparisons.
    • HPLC Detection of Paracetamol
  • Permeant-containing effluent samples, collected from the acceptor compartments of the perfusion apparatus over the 2-hour sampling intervals, were analyzed using an Hewlett Packard 1100 series high-performance binary liquid chromatograph (Agilent Technologies, Waldbronn, Germany) equipped with an Agilent Eclipse (XDB-C18) Zorbax analytical column (3.5-μm particle size), 150×4.6 mm (ID). The latter column was preceded by a 30×2.1-mm (ID) 018 guard column (40-μm particle size). The temperature was maintained at 40° C. and a flow rate of 1.0 mL/min was used for the entire run. The mobile phase consisted of a mixture of 2 solvents, A (50 mol/L KH2PO4, pH 5.4) and B (acetonitrile-isopropanol, 4:1 vol/vol). Three isocratic mixtures of A:B were used in sequential order as follows: firstly for 0 to 1.0 min: 90% Solvent A/10% Solvent B; secondly for 1 to 4.0 min: Linear gradient to 70% Solvent A/30% Solvent B, thirdly for 4.10 mins: return to use of 90% Solvent A/10% Solvent B. En equilibration time of 2.5 min was used for 90% Solvent A/30% Solvent B. All reagents used for the mobile phase were HPLC grade (Burdick & Jackson, Honeywell International Inc, Muskegon, Mich.), and all inorganic solvents were filtered through a 0.45-μm filter. Deionized water was used for preparing all aqueous standard and buffer solutions. Aliquots (15 μL) from each fraction sample were injected directly onto the column. Since no extraction procedure was required, it was unnecessary to determine recovery rates. Paracetamol was detected at 245 nm (retention time, 3.45 mins), while the total run time was set at 5.0 minutes. Recording and integration of peaks were performed by means of an Agilent Chem. Station. Spiked standards over the expected concentration range of 250 ng/ml to 4000 ng/ml (4.0 μg/ml) were randomly included in each batch on a variable wave Detector (Agilent, Waldbonn, Germany). Calibration was linear over the entire concentration range (R2=0.9999).
    • Results Permeability Experiments
  • Mean flux values for 0.1% paracetamol in aqueous solution (PBS) and Teargel (TG) across the frozen/thawed rabbit and human cornea versus time are shown in FIG. 1. The diffusion rates of paracetamol (in both PBS and TG) across human comeas were higher in the first few hours of the diffusion experiment than the values found across rabbit corneas. Steady state was also reached much earlier for paracetamol diffusion across human corneas. Teargel as a soluent did not affect the diffusion rate of paracetamol across human corneas as the graphs are nearly identical. Teargel does, however, increase the diffusion rate of paracetamol across rabbit comeas.
  • Statistically significant differences (P<0.05) were obtained when whole curves are compared using an F-test (3rd degree polynomial) between the steady-state flux values of: paracetamol (TG) and paracetamol (in PBS) across rabbit corneas (P<0.0001); paracetamol (in PBS) across rabbit and human corneas (P<0.0001); and paracetamol (TG) across rabbit and human comeas (P=0.0095). No statistically significant differences were found for paracetamol (TG) and paracetamol (in PBS) across human comeas (P=0.9939).
  • For paracetamol from 0.1% paracetamol in PBS, steady-state flux values were 774±30 ng·cm−2·min−1 and 870±76 ng·cm−2·min−1 across rabbit and human cornea respectively (FIG. 1). For paracetamol from 0.1% paracetamol in TG, steady-state flux values were 860±39 ng·cm−2·min−1 and 860±33 ng·cm−2·min−1 across rabbit and human cornea respectively (FIG. 1).
    • CONCLUSIONS
  • As paracetamol has been safely used in humans for more than 100 years and its effects on the body are well known, the invention provides a promising breakthrough in the treatment of glaucoma. This is particularly so for paracetamol in an ophthalmic solution which shows good corneal permeability of paracetamol. This has the benefits of the paracetamol acting directly on to have a direct effect on the therapeutic targets for glaucoma as well as reducing its effects on the hepatic and renal systems.
  • It is envisaged that doses of paracetamol which are effective in the treatment of glaucoma will be packaged together with instructions for the use thereof in the treatment of this condition. Such doses could be intended for oral administration and could consist of one or more tablets, capsules or the like. Alternately the doses could be intended for ophthalmic administration and could be provided by one or more containers of a suitable ophthalmic solution intended for single or repeated use.
  • It will be appreciated that many other embodiments of the invention exist which fall within the scope of the invention, particularly as regards dosage forms and therapeutic regimens.
    • REFERENCES
    • Van der Bijl P, van Eyk A D, Meyer D. Effects of three penetration enhancers on transcorneal permeation of cyclosporine. Cornea. 2001; 20:505-508.
    • Van der Bijl P, Engelbrecht A H, van Eyk A D, et al. Comparative permeability of human and rabbit comeas to cyclosporin and tritiated water. J Ocul Pharmacol Ther. 2002; 18:419-427.
    • Van der Bijl P, Thompson I O C, Squier Calif. Comparative permeability of human vaginal and buccal mucosa. Eur J Oral Sci 1997; 105:571-5.
    • Van der BO P, Van Eyk A D, Thompson I O C. Diffusion rates of vasopressin through human vaginal and buccal mucosa. Eur J Oral Sci 1998; 106:958-62.
    • Van der Bijl P, Penkler L, Van Eyk A D. Permeation of sumatriptan through human vaginal and buccal mucosa. Headache 2000; 40: 137-41.

Claims (19)

1. Paracetamol for use in a method of treating glaucoma, which method comprises administering to a patient in need of such treatment an effective amount of paracetamol.
2. Paracetamol according to claim 1 wherein the effective amount of paracetamol is between 500 mg and 1000 mg.
3. Paracetamol according to either claim 1 or 2 wherein the paracetamol is administered to the patient in an oral format.
4. Paracetamol according to claim 1 wherein the paracetamol is administered to the patient in the form of an ophthalmic solution.
5. Paracetamol according to claim 4 wherein the ophthalmic solution contains between 0.1 and 5% of paracetamol.
6. Paracetamol according to either claim 4 or 5 wherein the paracetamol is administered as one to two drops of the solution to each eye 4 to 6 hourly.
7. An ophthalmic solution including as its active ingredient paracetamol.
8. An ophthalmic solution according to claim 7 wherein the paracetamol is present in the range of 0.1 to 5%.
9. The use of paracetamol in the manufacture of a medicament for use in a method of treating glaucoma which method comprises administering to a patient in need of such treatment an effective amount of paracetamol.
10. The use according to either claim 9 wherein the paracetamol is administered to the patient in an oral format.
11. The use according to claim 10 wherein the paracetamol is administered to the patient in the form of an ophthalmic solution.
12. The use according to claim 11 wherein the ophthalmic solution contains between 0.1 and 5% of paracetamol.
13. The use according to either claim 12 wherein the paracetamol is administered as one to two drops of the solution to each eye 4 to 6 hourly.
14. A method of treatment of glaucoma which includes administering to a patient in need thereof an effective amount of paracetamol.
15. A method as claimed in claim 14 wherein the paracetamol is administered orally.
16. A method as claimed in claim 14 wherein the paracetamol is administered ophthalmically.
17. A package which includes at least one dose of paracetamol in an amount effective for the treatment of glaucoma and instructions for the use thereof in a treatment for glaucoma.
18. A package as claimed in claim 17 wherein the at least one dose of paracetamol is suitable for oral administration.
19. A package as claimed in claim 17 wherein the at least one dose of paracetamol is suitable for ophthalmic administration.
US12/672,475 2007-08-07 2008-07-30 Compositions and Methods for Treatment of Glaucoma Abandoned US20110098359A1 (en)

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Citations (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US6316025B1 (en) * 1997-03-05 2001-11-13 Smithkline Beecham Plc Swallow tablet comprising paracetamol
US20060074086A1 (en) * 2004-10-05 2006-04-06 Adolor Corporation Phenyl derivatives and methods of use

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FR2646773B1 (en) * 1989-05-12 1994-05-13 Chauvin Sa Laboratoire PHARMACEUTICAL COMPOSITION BASED ON PARACETAMOL
IT1313579B1 (en) * 1999-07-30 2002-09-09 Acraf PARACETAMOL-BASED LIQUID PHARMACEUTICAL COMPOSITION.
US20030185892A1 (en) 2001-08-17 2003-10-02 Bell Steve J. D. Intraocular delivery compositions and methods

Patent Citations (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US6316025B1 (en) * 1997-03-05 2001-11-13 Smithkline Beecham Plc Swallow tablet comprising paracetamol
US20060074086A1 (en) * 2004-10-05 2006-04-06 Adolor Corporation Phenyl derivatives and methods of use

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ZA201001530B (en) 2010-10-27
US20140045946A1 (en) 2014-02-13
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CN101815513A (en) 2010-08-25
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WO2009019555A2 (en) 2009-02-12
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EP2203165A4 (en) 2011-10-05
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