JP6966667B2 - Aqueous ophthalmic composition containing diquafosol or a salt thereof, and polyvinylpyrrolidone. - Google Patents

Description

The present invention relates to an aqueous ophthalmic composition containing diquafosol or a salt thereof, and polyvinylpyrrolidone.

Diquafosol is P ^1, P 4 ^- di purine receptor agonists, also known as (uridine-5 ') tetraphosphate or Up4U, has a lacrimation promoting action, the axis Aho Sol sodium salts thereof "Jikuasu ^{( It is used for the treatment of dry eye as "registered trademark)} ophthalmic solution 3%" (hereinafter, ^{also referred to as "Diquafosol (registered trademark)} ophthalmic solution") (Patent No. 365207 (Patent Document 1), Diquafosol ^{(registered trademark).} Ophthalmic solution 3% Attachment (Non-Patent Document 1)). The ^{dosage of Diquas (registered trademark)} ophthalmic solution is usually 1 drop at a time, 6 times a day (Non-Patent Document 1), but sufficient therapeutic effect can be obtained even if it is used at a predetermined dosage. There are also patients with no severe dry eye. Furthermore, in daily life, it is difficult to apply eye drops regularly and frequently, so there are some patients who do not obtain the expected effects due to poor eye drop adherence. In addition, although it is rare, there are some patients who complain of side effects such as eye irritation due to the use of ^{Diquas (registered trademark) ophthalmic solution (Non-Patent Document 1).}

As an attempt to search for a new therapeutic agent for dry eye having a higher tear volume increasing effect, it is known to use diquafosol or a salt thereof in combination with an existing therapeutic agent for dry eye. Japanese Unexamined Patent Publication No. 2012-07780 (Patent Document 2) discloses that tear secretion is synergistically promoted by the combined use of diquafosol or a salt thereof and hyaluronic acid as a therapeutic agent for dry eye. .. Japanese Unexamined Patent Publication No. 2015-160826 (Patent Document 3) discloses that tear secretion is synergistically promoted by the combined use of diquafosol or a salt thereof and rebamipide, which is a therapeutic agent for dry eye.

Japanese Patent No. 36527707 Japanese Unexamined Patent Publication No. 2012-07780 Japanese Patent Application Laid-Open No. 2015-160826

Diquas (registered trademark) ophthalmic solution 3% Package insert

It is an interesting subject to provide an aqueous ophthalmic composition capable of reducing side effects such as eye irritation while enhancing the medicinal effect of diquafosol or a salt thereof.

As a result of diligent research, the present inventors have found that an aqueous ophthalmic composition containing diquafosol or a salt thereof and polyvinylpyrrolidone (hereinafter, also referred to as “the present composition”) significantly improves the fluorescein staining score, that is, It was found that it showed a remarkable effect of improving corneal epithelial damage, and it was clarified that polyvinylpyrrolidone enhances the medicinal effect of diquafosol or a salt thereof. In addition, the inventors have found that the present composition, which has a certain viscosity by containing polyvinylpyrrolidone having a certain K value, has a smaller number of instillations than ^{the existing Diquas (registered trademark) ophthalmic solution.} It has also been found that it has a therapeutic effect equal to or higher than that of Diquas ^{(registered trademark) ophthalmic solution.} It was also found that this composition showed high viable cell activity and was highly safe for the keratoconjunctival epithelium. It was also found that this composition does not show neurostimulation and can further improve the feeling of instillation of eye drops. Furthermore, it was also found that even if the present composition contains a silver salt, the silver salt is stable, and the present composition having the silver salt exhibits an excellent preservative effect.

That is, the present invention relates to the following.
(1) An aqueous ophthalmic composition containing diquafosol or a salt thereof, and polyvinylpyrrolidone.

(2) The aqueous ophthalmic composition according to (1), which further contains a silver salt.
(3) The aqueous ophthalmic composition according to (2), wherein the silver salt contains silver nitrate.

(4) The aqueous ophthalmic composition according to any one of (1) to (3) for the prevention or treatment of dry eye.

(5) The aqueous ophthalmic composition according to (4), which contains sodium diquafosol at a concentration of 1 to 5% (w / v) and polyvinylpyrrolidone having a K value of more than 30 to 120 or less.

(6) The aqueous ophthalmic composition according to (4), which contains sodium diquafosol at a concentration of 3% (w / v) and polyvinylpyrrolidone having a K value of more than 30 to 120 or less.

(7) The aqueous ophthalmic composition according to (4), which contains diquafosol sodium at a concentration of 1 to 5% (w / v) and has a viscosity of 1.5 to 30 mPa · s at 25 ° C.

(8) The aqueous ophthalmic composition according to (4), which contains diquafosol sodium at a concentration of 3% (w / v) and has a viscosity of 1.5 to 30 mPa · s at 25 ° C.

(9) The aqueous ophthalmic composition according to any one of (5) to (8), which is used so as to be instilled 2 to 4 times a day.

(10) The aqueous ophthalmic composition according to any one of (5) to (8), which is used so as to be administered by eye drops three times a day.

(11) The aqueous ophthalmic composition according to (9) or (10), which is used so as to be administered by eye drops at a time of 1 to 2 drops.

(12) An ophthalmic pharmaceutical product, wherein 0.1 to 1 mL of the aqueous ophthalmic composition according to (1) is filled in a unit dose type eye drop container.

(13) An ophthalmic pharmaceutical product, wherein 0.3 to 0.5 mL of the aqueous ophthalmic composition according to (1) is filled in a unit dose type eye drop container.

(14) An ophthalmic pharmaceutical product, wherein 1 to 10 mL of the aqueous ophthalmic composition according to any one of (1) to (3) is filled in a multi-dose type eye drop container.

(15) An ophthalmic pharmaceutical product, wherein 5 mL of the aqueous ophthalmic composition according to any one of (1) to (3) is filled in a multi-dose type eye drop container.

(16) An ophthalmic pharmaceutical product, wherein 1 to 10 mL of the aqueous ophthalmic composition according to (1) is filled in a PFMD container.

(17) An ophthalmic pharmaceutical product, wherein 5 mL of the aqueous ophthalmic composition according to (1) is filled in a PFMD container.

(18) The ophthalmic pharmaceutical product according to any one of (12) to (17) for the prevention or treatment of dry eye.

(19) The ophthalmic pharmaceutical use according to (18), wherein the aqueous ophthalmic composition contains diquafosol sodium at a concentration of 1 to 5% (w / v) and polyvinylpyrrolidone having a K value of more than 30 to 120 or less. product.

(20) The ophthalmic pharmaceutical product according to (18), wherein the aqueous ophthalmic composition contains diquafosol sodium at a concentration of 3% (w / v) and polyvinylpyrrolidone having a K value of more than 30 to 120 or less.

(21) The ophthalmic drug according to (18), wherein the aqueous composition contains 1 to 5% (w / v) of sodium diquafosol and has a viscosity of 1.5 to 30 mPa · s at 25 ° C. Product for.

(22) The ophthalmic pharmaceutical product according to (18), wherein the aqueous composition contains diquafosol sodium at a concentration of 3% (w / v) and has a viscosity of 1.5 to 30 mPa · s at 25 ° C. ..

(23) The ophthalmic pharmaceutical product according to any one of (19) to (22), which is used so as to be administered by eye drops 2 to 4 times a day.

(24) The ophthalmic pharmaceutical product according to any one of (19) to (22), which is used so as to be administered by eye drops three times a day.

(25) The ophthalmic pharmaceutical product according to (23) or (24), which is used so as to be administered by eye drops at a time of 1 to 2 drops.

(26) The aqueous ophthalmic composition according to any one of (1) to (4), which comprises polyvinylpyrrolidone having a K value of 17 or more.

(27) The aqueous ophthalmic composition according to any one of (1) to (4), which comprises polyvinylpyrrolidone having a K value of 17 to 120.

(28) The aqueous ophthalmic composition according to any one of (1) to (4), which comprises polyvinylpyrrolidone having a K value of more than 30 to 120 or less.

(29) The aqueous ophthalmic composition according to any one of (1) to (4), which comprises polyvinylpyrrolidone having a K value of 90.

(30) The aqueous ophthalmic composition according to any one of (1) to (11), wherein the concentration of polyvinylpyrrolidone is 0.001% (w / v) or more.

(31) The aqueous ophthalmic composition according to any one of (1) to (4), wherein the concentration of the diquafosol or a salt thereof is 0.0001 to 10% (w / v).

(32) The aqueous ophthalmic composition according to any one of (1) to (4), wherein the concentration of the diquafosol or a salt thereof is 0.01 to 5% (w / v).

(33) The aqueous ophthalmic composition according to any one of (1) to (4), wherein the concentration of the diquafosol or a salt thereof is 1 to 5% (w / v).

(34) The aqueous ophthalmic composition according to any one of (1) to (4), wherein the concentration of the diquafosol or a salt thereof is 3% (w / v).

(35) The aqueous ophthalmic composition according to any one of (1) to (11), wherein the pH of the aqueous ophthalmic composition is in the range of 6 to 8.

(36) The aqueous ophthalmic composition according to any one of (1) to (11), wherein the pH of the aqueous ophthalmic composition is in the range of 7 to 8.

(37) The aqueous ophthalmic composition according to any one of (1) to (11), wherein the aqueous ophthalmic composition is a sterile aqueous ophthalmic solution.

(38) The aqueous ophthalmic composition according to any one of (1) to (11), which can be stored at room temperature.

(39) The aqueous ophthalmic composition according to any one of (1) to (6), wherein the aqueous ophthalmic composition has a viscosity of 1.5 to 30 mPa · s at 25 ° C.

(40) The aqueous ophthalmic composition according to any one of (1) to (4), wherein the salt of the diquafosol is diquafosol sodium.

(41) A 3% (w / v) concentration of diquafosol sodium having a K value of 90, characterized in that it is used so as to be administered by instillation of 1 to 2 drops at a time, 2 to 4 times a day. An aqueous ophthalmic composition for the prevention or treatment of dry eye, containing polyvinylpyrrolidone and silver nitrate.

(42) Concentrations of diquafosol sodium, polyvinylpyrrolidone and silver nitrate at a concentration of 3% (w / v), characterized in that they are used by instilling 1 to 2 drops at a time, 2 to 4 times a day. An aqueous ophthalmic composition for the prevention or treatment of dry eye, which is contained and has a viscosity of 3 to 30 mPa · s at 25 ° C..

(43) The aqueous ophthalmic composition according to (41) or (42), which is used so as to be administered by eye drops three times a day.

(44) A dry ophthalmic composition containing 0.1 to 1 mL of an aqueous ophthalmic composition containing diquafosol sodium at a concentration of 3% (w / v) and polyvinylpyrrolidone having a K value of 90 was filled in a unit dose type eye drop container. An ophthalmic pharmaceutical product for the prevention or treatment of eye, characterized in that the aqueous ophthalmic composition is instilled 1 to 2 drops at a time, 2 to 4 times a day. , Ophthalmic pharmaceutical products.

(45) Prevention or treatment of dry eye in which 0.1 to 1 mL of an aqueous ophthalmic composition containing diquafosol sodium and polyvinylpyrrolidone at a concentration of 3% (w / v) is filled in a unit dose type eye drop container. The aqueous ophthalmic composition has a viscosity of 3 to 30 mPa · s at 25 ° C., and is administered by instillation at 1 to 2 drops at a time, 2 to 4 times a day. An ophthalmic pharmaceutical product, characterized in that it is used in such a manner.

(46) A dry eye in which 1 to 10 mL of an aqueous ophthalmic composition containing diquafosol sodium at a concentration of 3% (w / v) and polyvinylpyrrolidone having a K value of 90 is filled in a multidose eye drop container. An ophthalmic pharmaceutical product for prophylaxis or treatment, characterized in that the aqueous ophthalmic composition is used to be administered by eye drops 1 to 2 drops at a time, 2 to 4 times a day. Pharmaceutical products.

(47) For prevention or treatment of dry eye, 1 to 10 mL of an aqueous ophthalmic composition containing diquafosol sodium and polyvinylpyrrolidone at a concentration of 3% (w / v) was filled in a multidose eye drop container. The aqueous ophthalmic composition has a viscosity of 3 to 30 mPa · s at 25 ° C., and is administered by instillation at 1 to 2 drops at a time, 2 to 4 times a day. An ophthalmic pharmaceutical product characterized by being used in.

(48) Prevention or treatment of dry eye in which 1-10 mL of an aqueous ophthalmic composition containing diquafosol sodium at a concentration of 3% (w / v) and polyvinylpyrrolidone having a K value of 90 was filled in a PFMD container. A product for ophthalmic medicine, characterized in that the aqueous ophthalmic composition is used by instillation 1 to 2 drops at a time, 2 to 4 times a day. ..

(49) An ophthalmic drug for the prevention or treatment of dry eye, in which 1 to 10 mL of an aqueous ophthalmic composition containing diquafosol sodium and polyvinylpyrrolidone at a concentration of 3% (w / v) is filled in a PFMD container. The aqueous ophthalmic composition has a viscosity of 3 to 30 mPa · s at 25 ° C., and is used so as to be administered by instillation at 1 to 2 drops at a time, 2 to 4 times a day. An ophthalmic pharmaceutical product characterized by this.

(50) The ophthalmic pharmaceutical product according to any one of (44) to (49), which is used so as to be administered by eye drops three times a day.

(51) The ophthalmic pharmaceutical product according to any one of (46) or (47), further containing silver nitrate.

The present invention also relates to the following.
(A-1) A method for treating dry eye, which comprises administering 1 to 2 drops of an aqueous ophthalmic composition filled in a unit dose type eye drop container to a patient once to 2 to 4 times a day. The aqueous ophthalmic composition contains 3% (w / v) concentration of diquafosol sodium and polyvinylpyrrolidone having a K value of 90, and the unit dose type eye drop container contains the aqueous ophthalmic composition 0.1. A method for treating dry eye, which is filled with ~ 1 mL.

(A-2) A method for treating dry eye, which comprises administering 1 to 2 drops of an aqueous ophthalmic composition filled in a unit dose type eye drop container to a patient once to 2 to 4 times a day. The aqueous ophthalmic composition contains 3% (w / v) concentrations of diquafosol sodium and polyvinylpyrrolidone, has a viscosity of 3 to 30 mPa · s at 25 ° C., and is contained in the unit dose type eye drop container. A method for treating dry eye, which is filled with 0.1 to 1 mL of the aqueous ophthalmic composition.

(A-3) A method for treating dry eye, which comprises administering 1 to 2 drops of an aqueous ophthalmic composition filled in a multidose type eye drop container to a patient once to 2 to 4 times a day. The aqueous ophthalmic composition contains 3% (w / v) concentration of diquafosol sodium and polyvinylpyrrolidone having a K value of 90, and the multidose type eye drop container contains 1 to 10 mL of the aqueous ophthalmic composition. A method of treating dry eye that is filled with.

(A-4) A method for treating dry eye, which comprises administering 1 to 2 drops of an aqueous ophthalmic composition filled in a multi-dose type eye drop container to a patient once to 2 to 4 times a day. The aqueous ophthalmic composition contains 3% (w / v) concentrations of diquafosol sodium and polyvinylpyrrolidone, has a viscosity of 3 to 30 mPa · s at 25 ° C., and the multidose type eye drop container has a viscosity of 3 to 30 mPa · s. A method for treating dry eye, which is filled with 1 to 10 mL of the aqueous ophthalmic composition.

(A-5) A method for treating dry eye, which comprises administering 1 to 2 drops of an aqueous ophthalmic composition filled in a PFMD container to a patient at a time, 2 to 4 times a day, and the above-mentioned aqueous ophthalmology. The composition contains 3% (w / v) concentration of diquafosol sodium and polyvinylpyrrolidone having a K value of 90, and the PFMD container is filled with 1 to 10 mL of the aqueous ophthalmic composition. How to treat dry eye.

(A-6) A method for treating dry eye, which comprises administering 1 to 2 drops of an aqueous ophthalmic composition filled in a PFMD container to a patient at a time, 2 to 4 times a day, and the above-mentioned aqueous ophthalmology. The composition for use contains 3% (w / v) concentrations of sodium diquafosol and polyvinylpyrrolidone, has a viscosity of 3 to 30 mPa · s at 25 ° C., and the PFMD container contains the aqueous ophthalmic composition. A method for treating dry eye, which is filled with 1 to 10 mL of the substance.

(A-7) The dry according to any one of (A-1) to (A-6), which comprises administering 1 to 2 drops of the aqueous ophthalmic composition to a patient by eye drops three times a day. How to treat eye.

(B-1) An ophthalmic pharmaceutical product containing 0.1 to 1 mL of an aqueous ophthalmic composition used for the prevention or treatment of dry eye in a unit dose type eye drop container, wherein the aqueous ophthalmic composition is It contains 3% (w / v) concentration of diquafosol sodium and polyvinylpyrrolidone having a K value of 90, and is characterized by being used to be administered by instillation 1 to 2 drops at a time, 2 to 4 times a day. An ophthalmic pharmaceutical product.

(B-2) An ophthalmic pharmaceutical product containing 0.1 to 1 mL of an aqueous ophthalmic composition used for the prevention or treatment of dry eye in a unit dose type eye drop container, wherein the aqueous ophthalmic composition is It contains 3% (w / v) concentration of diquafosol sodium and polyvinylpyrrolidone, has a viscosity of 3 to 30 mPa · s at 25 ° C., and is administered by eye drops 1 to 2 drops at a time, 2 to 4 times a day. An ophthalmic pharmaceutical product, characterized in that it is used as such.

(B-3) An ophthalmic pharmaceutical product in which 1 to 10 mL of an aqueous ophthalmic composition used for prevention or treatment of dry eye is filled in a multidose type eye drop container, and the aqueous ophthalmic composition is 3%. It contains (w / v) concentration of diquafosol sodium and polyvinylpyrrolidone having a K value of 90, and is characterized in that it is used so as to be administered by eye drops 1 to 2 drops at a time, 2 to 4 times a day. , Ophthalmic pharmaceutical products.

(B-4) An ophthalmic pharmaceutical product in which 1 to 10 mL of an aqueous ophthalmic composition used for prevention or treatment of dry eye is filled in a multidose type eye drop container, and the aqueous ophthalmic composition is 3%. It contains (w / v) concentrations of diquafosol sodium and polyvinylpyrrolidone, has a viscosity of 3 to 30 mPa · s at 25 ° C., and is administered by eye drops 1 to 2 drops at a time, 2 to 4 times a day. An ophthalmic pharmaceutical product, characterized in that it is used in an ophthalmic manner.

(B-5) An ophthalmic pharmaceutical product containing 1 to 10 mL of an aqueous ophthalmic composition used for the prevention or treatment of dry eye in a PFMD container, wherein the aqueous ophthalmic composition is 3% (w / w / v) An ophthalmic drug comprising diquafosol sodium at a concentration of 90 and polyvinylpyrrolidone having a K value of 90, which is used to be administered by instillation 1 to 2 drops at a time, 2 to 4 times a day. Product for.

(B-6) An ophthalmic pharmaceutical product containing 1 to 10 mL of an aqueous ophthalmic composition used for the prevention or treatment of dry eye in a PFMD container, wherein the aqueous ophthalmic composition is 3% (w / w / It contains v) concentrations of diquafosol sodium and polyvinylpyrrolidone, has a viscosity of 3 to 30 mPa · s at 25 ° C., and is administered by instillation at 1 to 2 drops at a time, 2 to 4 times a day. An ophthalmic pharmaceutical product characterized by being used.

(B-7) Any of (B-1) to (B-6), wherein the aqueous ophthalmic composition is used by instilling 1 to 2 drops at a time, 3 times a day. The ophthalmic pharmaceutical product according to 1.

(C-1) Aqueous ophthalmic composition containing 3% (w / v) concentration of diquafosol sodium and polyvinylpyrrolidone having a K value of 90 for producing a drug for the prevention or treatment of dry eye. In the use of a substance, 0.1 to 1 mL of the aqueous ophthalmic composition is filled in a unit dose type eye drop container and used so as to be administered by instillation 1 to 2 drops at a time, 2 to 4 times a day. The use of aqueous ophthalmic compositions.

(C-2) Contains 3% (w / v) concentrations of diquafosol sodium and polyvinylpyrrolidone for producing a drug for the prevention or treatment of dry eye, and 3 to 30 mPa · s at 25 ° C. In the use of an aqueous ophthalmic composition having the above viscosity, 0.1 to 1 mL of the aqueous ophthalmic composition is filled in a unit dose type eye drop container, and 1 to 2 drops at a time are instilled 2 to 4 times a day. Use of an aqueous ophthalmic composition, characterized in that it is used to be administered.

(C-3) Aqueous ophthalmic composition containing 3% (w / v) concentration of diquafosol sodium and polyvinylpyrrolidone having a K value of 90 for producing a drug for the prevention or treatment of dry eye. The present invention is characterized in that 1 to 10 mL of the aqueous ophthalmic composition is filled in a multi-dose type eye drop container and used so as to be instilled 1 to 2 drops at a time, 2 to 4 times a day. Use of an aqueous ophthalmic composition.

(C-4) Containing 3% (w / v) concentrations of diquafosol sodium and polyvinylpyrrolidone for producing a drug for the prevention or treatment of dry eye, 3 to 30 mPa · s at 25 ° C. In the use of an aqueous ophthalmic composition having the above viscosity, 1 to 10 mL of the aqueous ophthalmic composition is filled in a multi-dose type eye drop container, and 1 to 2 drops at a time are instilled 2 to 4 times a day. Use of an aqueous ophthalmic composition, characterized in that it is used in such a manner.

(C-5) Aqueous ophthalmic composition containing 3% (w / v) concentration of diquafosol sodium and polyvinylpyrrolidone having a K value of 90 for producing a drug for the prevention or treatment of dry eye. The use of the substance is characterized in that 1 to 10 mL of the aqueous ophthalmic composition is filled in a PFMD container and used so as to be instilled 1 to 2 drops at a time and 2 to 4 times a day. Use of aqueous ophthalmic compositions.

(C-6) Containing 3% (w / v) concentrations of diquafosol sodium and polyvinylpyrrolidone for producing a drug for the prevention or treatment of dry eye, and 3-30 mPa · at 25 ° C. In the use of an aqueous ophthalmic composition having a viscosity of s, 1 to 10 mL of the aqueous ophthalmic composition is filled in a PFMD container, and 1 to 2 drops at a time are instilled 2 to 4 times a day. Use of an aqueous ophthalmic composition, characterized in that it is used in.

(C-7) Any of (C-1) to (C-6), wherein the aqueous ophthalmic composition is used by instilling 1 to 2 drops at a time, 3 times a day. Use of the aqueous ophthalmic composition according to 1.

(D-1) A method for imparting a preservative effect to an aqueous ophthalmic composition containing diquafosol or a salt thereof, and polyvinylpyrrolidone, which comprises incorporating a silver salt in the aqueous ophthalmic composition. ..

(D-2) A method for maintaining the preservative efficacy of an aqueous ophthalmic composition containing diquafosol or a salt thereof, and polyvinylpyrrolidone, which comprises incorporating a silver salt in the aqueous ophthalmic composition. ..

In addition, each configuration of the present invention can be arbitrarily selected and combined with two or more.

Since this composition has a high tear volume increasing effect, a stronger dry eye therapeutic effect is expected as compared with the case of instillation of ^{existing Diquas (registered trademark) ophthalmic solution.} Therefore, it is also expected that the present composition exerts the same or higher dry eye therapeutic effect at a lower concentration than the ^{existing Diquas (registered trademark) ophthalmic solution.} In addition, the existing Diquas ^{(registered trademark)} ophthalmic solution needs to be instilled 6 times a day, and there are some patients who do not obtain the expected effect due to poor eye drop adherence, but polyvinylpyrrolidone having a certain K value. the compositions which led to have a constant viscosity by containing the existing Jikuasu ^® existing Jikuasu a smaller eye number than eye drops ^{(registered trademark)} ophthalmic solution equal to or more therapeutic effects It is expected that the eye drop adherence will be improved.

Furthermore, it is expected that this composition exhibits high viable cell activity, is highly safe for the keratoconjunctival epithelium, does not exhibit neurostimulation, and can improve the feeling of instillation of eye drops.

Further, even if the present composition contains a silver salt, the silver salt is stable and exhibits excellent preservative effect.

It is a graph which shows the fluorescein staining score of a cornea. It is a figure which shows the result of the cytotoxicity test by a corneal epithelial cell. It is a figure which shows the maximum fluorescence intensity (RFUmax) after the addition of diquafosol sodium.

The present invention will be described in more detail.
As used herein, "(w / v)%" means the mass (g) of the target component contained in 100 mL of the aqueous ophthalmic composition of the present invention.

As used herein, "PVP" means polyvinylpyrrolidone.
As used herein, "HEC" means hydroxyethyl cellulose.

As used herein, "CMC-Na" means sodium carboxymethyl cellulose.

As used herein, "HPMC" means hydroxypropylmethylcellulose.

As used herein, "CVP" means a carboxyvinyl polymer.
As used herein, "diquafosol ophthalmic solution" means an aqueous ophthalmic solution containing diquafosol or a salt thereof.

As used herein, "diquafosol sodium ophthalmic solution" means an aqueous ophthalmic solution containing diquafosol sodium.

"Diquafosol" is a compound represented by the following chemical structural formula.

The "salt of diquafosol" is not particularly limited as long as it is a pharmaceutically acceptable salt, and is a metal salt with lithium, sodium, potassium, calcium, magnesium, zinc, etc .; hydrochloric acid, hydrobromic acid, hydrogen iodide. , Salts with inorganic acids such as nitrate, sulfuric acid, phosphoric acid; acetic acid, fumaric acid, maleic acid, succinic acid, citric acid, tartaric acid, adipic acid, gluconic acid, glucoheptic acid, glucuronic acid, terephthalic acid, methanesulfonic acid, Lactic acid, horse uric acid, 1,2-ethandisulfonic acid, isetionic acid, lactobionic acid, oleic acid, pamoic acid, polygalacturonic acid, stearic acid, tannic acid, trifluoromethanesulfonic acid, benzenesulfonic acid, p-toluenesulfonic acid, Salts with organic acids such as lauryl sulfate, methyl sulfate, naphthalene sulfonic acid, sulfosalicylic acid; quaternary ammonium salts with methyl bromide, methyl iodide, etc .; with halogen ions such as bromine ion, chlorine ion, iodine ion Salt; Salt with ammonia; Triethylenediamine, 2-aminoethanol, 2,2-iminobis (ethanol), 1-deoxy-1- (methylamino) -2-D-sorbitol, 2-amino-2- (hydroxymethyl) ) -1,3-Propanediol, procaine, salts with organic amines such as N, N-bis (phenylmethyl) -1,2-ethanediamine and the like.

In the present invention, "diquafosol or a salt thereof" also includes a hydrate and an organic solvate of diquafosol (free form) or a salt thereof.

If polymorphs and polymorphs (crystal polymorphs) are present in "diquafosol or salts thereof", those polymorphs and polymorphs (polymorphs) are also within the scope of the present invention. include. Here, the crystal polymorph group (crystal polymorph system) is an individual crystal shape and its process at each stage when the crystal shape changes due to conditions and conditions such as production, crystallization, and storage of those crystals. Means the whole.

The "diquafosol or salt thereof" of the present invention is preferably a sodium salt of diquafosol, and a diquafosol tetrasodium salt represented by the following chemical structural formula (also simply referred to as "diquafosol sodium" in the present specification) is particularly preferable. preferable.

Diquafosol or a salt thereof can be produced by the method disclosed in JP-A-2001-510484.

The present composition may contain an active ingredient other than diquafosol or a salt thereof, or diquafosol or a salt thereof may be contained as the only active ingredient.

In the present invention, the concentration of diquafosol or a salt thereof is not particularly limited, but is preferably 0.0001 to 10% (w / v), for example, 0.001 to 5% (w / v). ), More preferably 0.01 to 5% (w / v), even more preferably 0.1 to 5% (w / v), and 1 to 5% (w / v). It is more preferably w / v), and particularly preferably 3% (w / v). More specifically, 0.001% (w / v), 0.002% (w / v), 0.003% (w / v), 0.004% (w / v), 0.005%. (W / v), 0.006% (w / v), 0.007% (w / v), 0.008% (w / v), 0.009% (w / v), 0.01% (W / v), 0.02% (w / v), 0.03% (w / v), 0.04% (w / v), 0.05% (w / v), 0.06% (W / v), 0.07% (w / v), 0.08% (w / v), 0.09% (w / v), 0.1% (w / v), 0.2% (W / v), 0.3% (w / v), 0.4% (w / v), 0.5% (w / v), 0.6% (w / v), 0.7% (W / v), 0.8% (w / v), 0.9% (w / v), 1% (w / v), 1.5% (w / v), 2% (w / v) ), 2.5% (w / v), 3% (w / v), 3.5% (w / v), 4% (w / v), 4.5% (w / v) or 5% (W / v) is preferable.

In the present invention, "polyvinylpyrrolidone" is a polymer compound obtained by polymerizing N-vinyl-2-pyrrolidone, and is generally used as a thickening agent. Polyvinylpyrrolidone is also called povidone. The K value of polyvinylpyrrolidone used in the present invention is preferably 17 or more, more preferably 17 to 120, still more preferably 25 to 120, still more preferably 30 to 120, still more preferably more than 30 to 120 or less, and more preferably 40. ~ 120 is even more preferable, 60 to 120 is particularly preferable, 60 to 90 is particularly preferable, and 90 is even more preferable. For example, polyvinylpyrrolidone K17, polyvinylpyrrolidone K25, polyvinylpyrrolidone K30, polyvinylpyrrolidone K40, polyvinylpyrrolidone K50, polyvinylpyrrolidone K60, polyvinylpyrrolidone K70, polyvinylpyrrolidone K80, polyvinylpyrrolidone K85, polyvinylpyrrolidone K90, polyvinylpyrrolidone K120 and the like can be mentioned. The K value of polyvinylpyrrolidone is a viscosity characteristic value that correlates with the molecular weight, and is a numerical value calculated by applying the relative viscosity value (25 ° C.) measured by a capillary viscometer to the following Fikenscher equation (1). be.

In the formula (1), η _rel is the relative viscosity of the polyvinylpyrrolidone aqueous solution with respect to water, and c is the polyvinylpyrrolidone concentration (%) in the polyvinylpyrrolidone aqueous solution.

Here, since the K value is 90 to 108% of the displayed K value according to the description regarding the K value of the 17th revised Japanese Pharmacopoeia "Povidon", for example, "K90" is the above formula. The viscosity characteristic value (K value) calculated by applying to (1) is in the range of 81 to 97.2.

In the present invention, polyvinylpyrrolidone may be used alone, or two or more kinds of polyvinylpyrrolidones having different K values may be used in any combination.

In the present invention, the concentration of polyvinylpyrrolidone is not particularly limited, but is, for example, 0.001% (w / v) or more, preferably 0.001 to 10% (w / v), and more preferably 0. 0.01 to 10% (w / v), more preferably 0.05 to 10% (w / v), even more preferably 0.1 to 10% (w / v), and even more preferably 0.1 to 5. % (W / v), particularly preferably 1 to 5% (w / v).

The composition may be further supplemented with pharmaceutically acceptable preservatives as needed. For example, silver salts such as silver nitrate, benzalkonium chloride, benzalkonium bromide, benzethonium chloride, chlorhexidine gluconate, boric acid, borosand, sorbic acid, potassium sorbate, methyl paraoxybenzoate, propyl paraoxybenzoate, Examples thereof include chlorobutanol, polydronium chloride, and polyhexanide hydrochloride.

As is clear from the test results described later, since the present composition containing a silver salt has an excellent preservative effect, a preferable preservative in the present invention is a silver salt. Examples of silver salts include silver nitrate, silver sulfate, silver chloride, silver bromide, silver oxide, silver acetate, silver carbonate, silver citrate, silver lactate, silver phosphate, silver oxalate, silver thiosulfate, and protein silver. However, silver nitrate is preferable.

In the present invention, the concentration of the silver salt is not particularly limited, and is not particularly limited as long as it is in the range of 0.00000001 to 1% (w / v), for example. Specifically, the lower limit is, for example, 0.00000001% (w / v) or more, 0.000000001% (w / v) or more, 0.000001% (w / v) or more, 0.0000025%. (W / v) or more, 0.000004% (w / v) or more, 0.000005% (w / v) or more, 0.000008% (w / v) or more, 0.00001% (w / v) or more , 0.000016% (w / v) or more, 0.000025% (w / v) or more, 0.00004% (w / v) or more, 0.00005% (w / v) or more, 0.00008% ( It is preferably w / v) or more, or 0.0001% (w / v) or more. The upper limit is, for example, 1% (w / v) or less, 0.5% (w / v) or less, 0.1% (w / v) or less, 0.05% (w / v) or less. Hereinafter, 0.01% (w / v) or less, 0.005% (w / v) or less, or 0.001% (w / v) or less is preferable.

In addition to the above-mentioned polyvinylpyrrolidone and preservatives, pharmaceutically acceptable additives can be further added to the present composition, if necessary. For example, buffering agents such as sodium phosphate, sodium hydrogen phosphate, sodium hydrogen phosphate hydrate, sodium dihydrogen phosphate, sodium acetate, epsilon-aminocaproic acid; calcium chloride, sodium chloride, potassium chloride, concentrated glycerin, etc. Isotonic agents; stabilizers such as sodium edetate, sodium edetate hydrate, citrate hydrate, sodium citrate hydrate; surfactants such as polysorbate; antioxidants such as ascorbic acid; A thickening agent (also referred to as a thickener) such as hydroxyethyl cellulose and hydroxypropylmethyl cellulose; a pH adjuster such as hydrochloric acid and sodium hydroxide can be selected and added as necessary. These additives may be used alone or in any combination of two or more. The present composition may not contain a cellulosic polymer which is a thickening agent such as hydroxyethyl cellulose and hydroxypropylmethyl cellulose.

The pH of the composition is not limited to a specific value as long as it is within a pharmaceutically acceptable range. However, the pH of the composition is preferably 8 or less, more preferably in the range of 4-8, even more preferably in the range of 5-8, even more preferably in the range of 6-8, and even more preferably in the range of 7-8. , Particularly preferably in the vicinity of 7. More specifically, for example, pH 6.0, 6.1, 6.2, 6.3, 6.4, 6.5, 6.6, 6.7, 6.8, 6.9, 7. 0, 7.1, 7.2, 7.3, 7.4, 7.5, 7.6, 7.7, 7.8, 7.9, and 8.0 are preferred, 7.0, 7 More preferably, 1.1, 7.2, 7.3, 7.4, 7.5, 7.6, 7.7, 7.8, 7.9, and 8.0.

In the present invention, the "ophthalmic composition" refers to a composition for use in the prevention and / or treatment of eye diseases and the like. Examples of the dosage form include eye drops, eye ointments, injections, ointments (for example, which can be administered to the skin of the eyelids), and the like, and eye drops are preferable. Here, eye drops are synonymous with eye drops or eye drops, and eye drops for contact lenses are also included in the definition of eye drops.

In the present invention, the "aqueous ophthalmic composition" is an aqueous ophthalmic composition using water as a solvent (base), and more preferably an aqueous eye drop.

The present composition may be a soluble eye drop or a suspension type eye drop depending on the properties and contents of the active ingredient and the additive.

The present composition is preferably a sterile aqueous ophthalmic solution. Here, sterility means a state in which microorganisms are killed or removed, and specifically, for example, a state in which the preservation efficacy test standard described in the 17th revised Japanese Pharmacopoeia is met.

The composition is preferably storable at room temperature.
The viscosity of the present composition is not particularly limited as long as it is within a pharmaceutically acceptable range, but is preferably in the range of 1 to 500 mPa · s, more preferably more than 1.4 to 100 mPa · s or less. Within the range of, more preferably within the range of 1.5 to 100 mPa · s, even more preferably within the range of 1.5 to 50 mPa · s, even more preferably within the range of 1.5 to 30 mPa · s, even more preferably. Is in the range of 1.5 to 20 mPa · s, more preferably in the range of 1.5 to 10 mPa · s, more preferably in the range of 2 to 10 mPa · s, and particularly preferably in the range of 3 to 10 mPa · s. , More particularly preferably within the range of 5 to 10 mPa · s, and even more particularly preferably within the range of 7 to 10 mPa · s. The viscosity of the present composition is in the range of 1.5 to 30 mPa · s, preferably in the range of 2 to 30 mPa · s, more preferably in the range of 3 to 30 mPa · s, and further preferably in the range of 5 to 30 mPa · s. It can also be adjusted to be within the range of, particularly preferably within the range of 7 to 30 mPa · s. As the lower limit of the viscosity of the present composition, for example, 1 mPa · s or more, 1.5 mPa · s or more, 2 mPa · s or more, 3 mPa · s or more, 5 mPa · s or more, or 7 mPa · s or more is preferable. Further, as the upper limit value, for example, 500 mPa · s or less, 100 mPa · s or less, 50 mPa · s or less, 30 mPa · s or less, 20 mPa · s or less, or 10 mPa · s or less is preferable. The viscosity of the composition is measured with a rotational viscometer (25 ° C; ^{shear rate of 50s -1).}

The osmotic pressure of the present composition is not limited to a specific value as long as it is within a pharmaceutically acceptable range. However, the osmotic pressure of the composition is preferably 2 or less, more preferably in the range of 0.5 to 2, still more preferably in the range of 0.7 to 1.6, still more preferably in the range of 0.8 to 1.4. The range of, particularly preferably 0.9 to 1.2.

The present composition can be filled in an airtight container, specifically, an eye drop container and stored. Examples of the eye drop container filled with the present composition include a “multi-dose type eye drop container” or a “unit dose type eye drop container”.

In the present invention, the "ophthalmic pharmaceutical product" refers to a product for ophthalmic pharmaceuticals in which the present composition is filled in an eye drop container. Here, examples of the "ophthalmic pharmaceutical product" include eye drop products. The definition of each term in the "ophthalmic pharmaceutical product" of the present invention is the same as the definition of each term in the "composition".

In the present invention, the "multi-dose type instillation container" is an instillation container provided with a container main body and a cap that can be attached to the container main body, and the cap can be freely opened and resealed. Say that. The multi-dose type eye drop container usually contains a plurality of doses of eye drops for use for a certain period of time. When the composition does not contain a preservative such as benzalkonium chloride, the composition may be contained in a PFMD (Preservative Free Multi Dose) container. The filling amount of the present composition to be filled in the multi-dose type eye drop container or PFMD container is, for example, preferably 1 to 20 mL, more preferably 1 to 15 mL, further preferably 1 to 10 mL, and 2.5 to 10 mL. Even more preferable, 5 mL is particularly preferable.

On the other hand, the "unit-dose type eye drop container" is an eye drop for the purpose of having a cap fused and sealed at the bottle mouth and breaking and opening the fused portion between the cap and the bottle-shaped main body at the time of use. It refers to a container. The unit dose type eye drop container contains eye drops for one or several uses. In general, the eye drop liquid contained in the unit dose type eye drop container does not contain a preservative such as benzalkonium chloride. The filling amount of the present composition to be filled in the unit dose type instillation container is, for example, preferably 0.1 to 1 mL, more preferably 0.1 to 0.5 mL, still more preferably 0.3 mL to 0.5 mL. , 0.3 mL or 0.4 mL is particularly preferred.

The usage of this composition can be appropriately changed according to the dosage form, the severity of the patient's symptoms to be administered, age, weight, judgment of the doctor, etc., but for example, when eye drops are selected as the dosage form. A single dose of 1 to 5 drops, preferably 1 to 3 drops, more preferably 1 to 2 drops, particularly preferably 1 drop, 1 to 6 times a day, preferably 1 to 4 times a day, more preferably. It can be administered by eye drops 2 to 4 times a day, more preferably 3 times a day, daily to weekly. Here, more specifically, for example, the number of eye drops is preferably 6 times a day, 5 times a day, 4 times a day, 3 times a day, 2 times a day or once a day, 6 times a day. 4 times a day, 3 times a day or 2 times a day is more preferable, 4 times a day, 3 times a day or 2 times a day is more preferable, and 3 times a day is particularly preferable.

When the concentration of diquafosol or a salt thereof in the present composition is 3% (w / v), a single dose of 1 to 5 drops, preferably 1 to 3 drops, more preferably 1 to 2 drops, particularly preferably. 1 drop 6 times a day, 5 times a day, 4 times a day, 3 times a day, 2 times a day or once a day, preferably 6 times a day, 4 times a day, 3 times a day It can be administered by eye drops once or twice a day, more preferably four times a day or three times a day, and particularly preferably three times a day.

Further, one drop is preferably 10 to 50 μL, more preferably 20 to 50 μL, and particularly preferably 40 to 50 μL.

This composition is used for the prevention or treatment of dry eye, and is effective as a preventive or therapeutic agent for dry eye. Dry eye is defined as "a chronic disease of tears and keratoconjunctival epithelium caused by various factors and is accompanied by eye discomfort and visual abnormalities", and keratoconjunctivitis sicca (KCS) is included in dry eye. .. In the present invention, the occurrence of dry eye symptoms caused by wearing soft contact lenses is also included in dry eye.

Dry eye symptoms include subjective symptoms such as dry eyes, discomfort, eye fatigue, dullness, dullness, eye pain, and blurred vision (blurred vision), as well as other symptoms such as congestion and keratoconjunctival epithelial disorders. Findings are also included. In the present invention, "prevention or treatment of dry eye" also includes improvement of the above-mentioned subjective symptoms and / or objective findings.

There are many unclear points about the etiology of dry eye, but Sjogren's syndrome; congenital anhidrosis; sarcoidosis; graft-versus-host disease (GVHD: Graft Versus Host Disease) by bone marrow transplantation; blepharitis of the eye; Stevens Johnson syndrome Lacrimal obstruction caused by tracoma, etc .; Diabetes; Decreased reflex secretion caused by LASIK (LASIK: -assisted) in Situ Graft-versus); Mybohm gland dysfunction; Caused by blepharitis, etc. It has been reported that the cause is a decrease in the oil layer; blink failure or blepharitis caused by eye protrusion, rabbit eye, etc .; decreased mutin secretion from embryo cells; VDT (Visual Display Thermals) work and the like.

In addition, the present composition can be instilled in the eyes of a dry eye patient wearing soft contact lenses. Here, instilling eye drops into the eyes of a dry eye patient wearing a soft contact lens means that the eye drops are instilled while the soft contact lens is worn on the cortex of the dry eye patient.

The results of pharmacological tests and examples of pharmaceutical products are shown below, but these are for a better understanding of the present invention and do not limit the scope of the present invention.

[Test 1]
Using normal male white rabbits, the time course of tear volume after instillation of this composition was evaluated.

(Sample preparation method)
Eye drops 1:
Ophthalmic solution 1 was prepared according to the prescription table shown in Table 1. That is, sodium diquafosol (9 g), sodium hydrogen phosphate hydrate (0.6 g), sodium edetate hydrate (0.03 g) and sodium chloride (1.35 g) were dissolved in sterile purified water. A 6-fold concentrated solution was obtained as 50 mL. Further, after mixing 10 mL of the 6-fold concentrated solution and 5 mL of sterilized purified water, a pH adjuster was appropriately added to adjust the pH to 7, and sterilized purified water was added to make 20 mL, and a 3-fold concentrated solution was obtained. PVP K90 (4 g) was dissolved in sterilized purified water to make the total amount 100 g, and then high-pressure steam sterilization (121 ° C. for 20 minutes) to obtain a 4.00% (w / w) PVP K90 solution. Add 4 mL of 3-fold concentrated solution to 6.0 g of 4.00% (w / w) PVP K90 solution, add sterile purified water to adjust the total volume to 12 mL, and then add a pH adjuster as appropriate to adjust the pH to 7. Therefore, ophthalmic solution 1 was prepared.

Eye drops 2:
Ophthalmic solution 2 was prepared according to the prescription table shown in Table 1. That is, sodium diquafosol (9 g), sodium hydrogen phosphate hydrate (0.6 g), sodium edetate hydrate (0.03 g) and sodium chloride (1.35 g) were dissolved in sterile purified water. A 6-fold concentrated solution was obtained as 50 mL. After mixing 10 mL of 6-fold concentrated liquid and 5 mL of sterile purified water, dissolve PVP K30 (1.2 g), adjust the pH to 7 by appropriately adding a pH adjuster, and add sterile purified water to make 20 mL. A 3-fold concentrated solution was obtained. Ophthalmic solution 2 was prepared by adding sterile purified water to 4 mL of a 3-fold concentrated solution to adjust the total volume to 12 mL, and then appropriately adding a pH regulator to adjust the pH to 7.

Eye drops 3:
Ophthalmic solution 3 was prepared according to the prescription table shown in Table 1. That is, sodium diquafosol (9 g), sodium hydrogen phosphate hydrate (0.6 g), sodium edetate hydrate (0.03 g) and sodium chloride (1.35 g) were dissolved in sterile purified water. A 6-fold concentrated solution was obtained as 50 mL. Further, after mixing 10 mL of the 6-fold concentrated solution and 5 mL of sterilized purified water, a pH adjuster was appropriately added to adjust the pH to 7, and sterilized purified water was added to make 20 mL, and a 3-fold concentrated solution was obtained. Hydroxyethyl cellulose (15 g) was dissolved in 1500 mL of sterilized purified water and sterilized by high pressure steam (121 ° C. for 20 minutes) to obtain a 1.00% (w / w) hydroxyethyl cellulose solution. Add 4 mL of 3-fold concentrated solution to 3.6 g of 1.00% (w / w) hydroxyethyl cellulose solution, add sterile purified water to adjust the total volume to 12 mL, and then add a pH adjuster as appropriate to adjust the pH to 7. As a result, ophthalmic solution 3 was prepared.

Eye drops 4:
Ophthalmic solution 4 was prepared according to the prescription table shown in Table 1. That is, sodium diquafosol (9 g), sodium hydrogen phosphate hydrate (0.6 g), sodium edetate hydrate (0.03 g) and sodium chloride (1.35 g) were dissolved in sterile purified water. A 6-fold concentrated solution was obtained as 50 mL. Further, after mixing 10 mL of the 6-fold concentrated solution and 5 mL of sterilized purified water, a pH adjuster was appropriately added to adjust the pH to 7, and sterilized purified water was added to make 20 mL, and a 3-fold concentrated solution was obtained. An ophthalmic solution 4 was prepared by adding sterile purified water to 4 mL of a 3-fold concentrated solution to adjust the total volume to 12 mL, and then appropriately adding a pH regulator to adjust the pH to 7.

Eye drops 5:
Ophthalmic solution 5 was prepared according to the prescription table shown in Table 1. That is, sodium diquafosol (18 g), sodium hydrogen phosphate hydrate (1.2 g), and sodium edetate hydrate (0.06 g) were dissolved in sterile purified water to obtain a 6-fold concentrated solution as 100 mL. rice field. After mixing 2.5 mL of 6-fold concentrated solution and 5 mL of sterile purified water, dissolve PVP K60 45% aqueous solution (0.67 g) and sodium chloride (0.068 g), and then add a pH adjuster as appropriate to adjust the pH. Ophthalmic solution 5 was prepared by adjusting to 7 and adding sterile purified water to make 15 mL.

The viscosities of the prepared ophthalmic solutions 1 to 5 are the 17th revised Japanese Pharmacy, 2.53 viscosity measuring method, the second rotational viscometer method, 2.1.3 conical-flat plate type rotational viscometer (cone). It was measured according to the method described in (Plate type viscometer). Specifically, Kinexus pro + (manufactured by Malvern) was used, and the measurement conditions were set as follows. (Measurement condition)
Rotor angle: 1 °
Rotor diameter: 50 mm
Sample volume: 0.57 mL
Measurement temperature: 25 ° C
Shear velocity: 50s ^-1
Measurement time: The viscosity was measured every 2 seconds, and the average value for 1 minute was taken as the viscosity.

(Test method and drug administration method)
Normal male white rabbits (16 animals and 32 eyes in total) were instilled with Benokiseal ^{(registered trademark)} ophthalmic solution 0.4% (manufactured by Santen Pharmaceutical Co., Ltd.) and subjected to local anesthesia. Three minutes later, a Sylmel test paper (manufactured by AYUMI Pharmaceutical Corporation) was inserted into the lower eyelid, and one minute after the insertion, the paper was removed and the length of the wet portion (tear volume) was read. This was used as the previous value. Next, each eye drop 1 to 5 was instilled once (4 animals in a group, 8 eyes, only eye drops 4 in 12 animals, 24 eyes). Three minutes before inserting the Sylmel test paper (manufactured by AYUMI Pharmaceutical Corporation) into the lower eyelid, ^{0.4% of Benokiseal (registered trademark)} ophthalmic solution (manufactured by Santen Pharmaceutical Corporation) was instilled and local anesthesia was applied. Each ophthalmic solution 60 minutes after instillation, a Sylmel test paper (manufactured by AYUMI Pharmaceutical Corporation) was inserted into the lower eyelid, and 1 minute after the insertion, it was withdrawn and the length of the wet portion (tear volume) was read.

(Evaluation method)
Ophthalmic solution The change in tear volume before and after instillation was calculated as Δtear volume (mm / min).

(Test results)
The amount of Δtear fluid (mm / min) 60 minutes after instillation is shown in Tables 1 and 2 (each value is the average value of 8 eyes, but only the instillation 4 is the average value of 24 eyes). In addition, the tear volume increasing effect of this composition was evaluated according to the following criteria.
+++: ΔTear volume (mm / min) 60 minutes after instillation is 4 mm / min or more
++: ΔTear volume (mm / min) 60 minutes after instillation is 1 mm / min or more and less than 4 mm / min
+: ΔTear volume (mm / min) 60 minutes after instillation is more than 0 mm / min or less than 1 mm / min.
-: The amount of Δtear (mm / min) 60 minutes after instillation is 0 mm / min or less.

As shown in the results of Table 1 above, the eye drops containing PVP K30 (eye drops 2) did not have the same effect of increasing the amount of tears 60 minutes after instillation as the eye drops not containing it (eye drops 4). rice field. In addition, HEC is generally used as a thickener, but the eye drops containing HEC (eye drops 3) have a relatively high viscosity, but like the eye drops 4, 60 minutes after instillation. No effect of increasing the amount of tears was observed. On the other hand, the eye drops containing PVP K90 (eye drops 1) showed an extremely higher tear volume increasing effect than the eye drops 2 to 4.

As shown in the results of Table 2 above, even when the K value of PVP was 60, the eye drops containing PVP (eye drops 5) had a high tear volume increasing effect.

(Discussion)
Polyvinylpyrrolidone increased the viscosity of an aqueous composition containing diquafosol or a salt thereof, and enhanced the medicinal effect of diquafosol or a salt thereof, especially when polyvinylpyrrolidone having a K value of more than 30 is added or polyvinylpyrrolidone is added. It was shown that the medicinal effect of diquafosol or a salt thereof is significantly enhanced when the viscosity of the aqueous composition exceeds 1.4.

[Test 2]
Rat exorbital lacrimal gland extraction model is widely used as a model for evaluating the therapeutic effect of corneal epithelial disorders caused by dry eye, also, it is also utilized as a model for evaluating the therapeutic effect of P2Y ₂ receptor agonist (Invest. Ophthalmol. Vis. Sci., 42 (1), 96-100 (2001)). Using the dry eye model, it was examined whether or not the improvement effect of corneal epithelial damage could be obtained by instillation of this composition.

(How to make a dry eye model)
Using male SD rats, a rat extraorbital lacrimal gland resection model was prepared according to the method of Fujihara et al. (Invest. Opthalmol. Vis. Sci., 42 (1), 96-100 (2001)). That is, after general anesthesia was administered by administration of somnopentil, the extraorbital lacrimal gland was removed to induce corneal epithelial damage.

(Sample preparation method)
Eye drops A:
Sodium hydrogen phosphate hydrate (0.2 g), sodium edetate hydrate (0.01 g), sodium chloride (0.45 g), silver nitrate (0.00004 g), polyvinylpyrrolidone K90 (2 g), diquafosol Sodium (3 g) was dissolved in sterile purified water to make 100 mL, and a pH adjuster (q.s.) was added to make pH 7.5.

Eye drops B:
Sterilized purified water containing sodium hydrogen phosphate hydrate (0.2 g), sodium edetate hydrate (0.01 g), sodium chloride (0.45 g), silver nitrate (0.00004 g), and polyvinylpyrrolidone K90 (4 g). The pH was adjusted to 100 mL, and a pH adjuster (q.s.) was added to adjust the pH to 7.5.

Eye drops X:
As the eye drops X, "Diquas ^{(registered trademark)} eye drops 3%" (manufactured by Santen Pharmaceutical Co., Ltd.) used as a therapeutic agent for dry eye was used. Ophthalmic solution X contains 30 mg of diquafosol sodium as an active ingredient in 1 mL of water, and as additives, potassium chloride, sodium chloride, chlorhexizing gluconate solution, sodium hydrogen phosphate hydrate, sodium edetate hydrate. , Contains a pH adjuster.

The viscosities of the prepared ophthalmic solutions A, B and X are the 17th revised Japanese Pharmacy, 2.53 viscosity measuring method, the second rotational viscometer method, 2.1.3 conical-plate type rotational viscometer. The measurement was performed according to the method described in (Cone plate type viscometer). Specifically, Kinexus pro + (manufactured by Malvern) was used, and the measurement conditions were set as follows.
(Measurement condition)
Rotor angle: 1 °
Rotor diameter: 50 mm
Sample volume: 0.57 mL
Measurement temperature: 25 ° C
Shear velocity: 50s ^-1
Measurement time: The viscosity was measured every 2 seconds, and the average value for 1 minute was taken as the viscosity.

The measured viscosities of each eye drop were as follows.
Eye drops A: 7.9 mPa · s
Eye drops B: 28.0 mPa · s
Eye drops X: 0.9 mPa · s
(Test method and drug administration method)
Eye drop A, eye drop B, and eye drop X were administered to the rat in which the corneal epithelial disorder was induced as follows.
-Eye drop A, 3 times a day administration group: Eye drops A were instilled into both eyes 3 times a day for 4 weeks. (6 animals in a group, 12 eyes)
-Eye drop B, 3 times a day administration group: Eye drops B were instilled into both eyes 3 times a day for 4 weeks. (6 animals in a group, 12 eyes)
-Eye drop X, 6 times a day administration group: Eye drops X were instilled into both eyes 6 times a day for 4 weeks. (6 animals in a group, 12 eyes)
The rats that did not induce the corneal epithelial disorder and had no eye drops for 4 weeks were included in the non-eye drop group (4 animals in a group, 8 eyes).

Four weeks after the start of instillation, the damaged part of the cornea was stained with fluorescein, and corneal epithelial damage was determined according to the method of Murakami et al. (New Ophthalmology, 21 (1), 87-90 (2004)). That is, the degree of staining with fluorescein was scored for each of the upper part, the middle part, and the lower part of the cornea according to the following criteria, and the average value of the total of those scores was calculated. In addition, 0.5 was set as an intermediate value between each score of 0, 1, 2, and 3.

(criterion)
0: Not dyed,
1: Staining is sparse, and the dotted stains are separated.
2: The staining is moderate, and a part of the punctate stained part is adjacent.
3: The staining is dense, and the dotted staining portions are adjacent to each other.

(result)
FIG. 1 shows a graph of the calculated fluorescein staining scores of each group. The score is the average value + standard error of each of 8 or 12 cases.

As is clear from FIG. 1, in the group in which the eye drops A was administered three times a day, an improvement in the fluorescein staining score was observed from 2 weeks after the start of the instillation as compared with the administration of the eye drops B three times a day. In the group in which the instillation X was administered 6 times a day, an improvement in the fluorescein staining score was observed 4 weeks after the start of the instillation as compared with the administration of the instillation B 3 times a day. Four weeks after instillation, the group in which ophthalmic solution A was administered three times a day and the group in which ophthalmic solution X was administered six times a day showed similar effects.

(Discussion)
Ophthalmic solution X is used as "Diquas ^{(registered trademark)} ophthalmic solution 3%" for the treatment of dry eye, and the number of instillations is 6 times a day. It was clarified that this composition to which polyvinylpyrrolidone K90 was added had a sufficient therapeutic effect on dry eye by instillation three times a day, and particularly two weeks after the start of instillation, "Diquas ^{(registered trademark)} instillation was performed. The therapeutic effect of "Liquid 3%" surpassing that of instillation 6 times a day was observed. Accordingly, the composition has been shown to exhibit the existing Jikuasu ^® ophthalmic solution equal to or more therapeutic effects in a small eye number than the existing Jikuasu ^® ophthalmic solution. In particular, considering the test results of Test 1, the present composition to which polyvinylpyrrolidone having a K value of more than 30 is added, or the present composition having a viscosity of more than 1.4 due to the addition of polyvinylpyrrolidone, 2 to 2 per day. It was suggested that 4 times instillation had the same or better therapeutic effect as 6 times a day ^{instillation of the existing "Diquas (registered trademark) ophthalmic solution 3%".}

[Test 3]
In order to investigate the effect of this composition on corneal epithelial cells, a test was conducted on the cytotoxicity of corneal epithelial cells.

(Sample preparation method)
Eye drops Y, C and D were prepared according to the formulations shown in Table 3.

Eye drops Y:
An eye drop of Ophthalmic Solution Y was prepared according to the formulation shown in Table 3. Specifically, sodium hydrogen phosphate hydrate (0.2 g), sodium edetate hydrate (0.01 g), sodium chloride (0.45 g), silver nitrate (0.00004 g), sodium diquafosol ( 3 g) was dissolved in sterile purified water to make 100 mL, and a pH adjuster (q.s.) was added to make pH 7.5.

Eye drops C and D:
According to the prescription shown in Table 3, each eye drop C and D was prepared in the same manner as the eye drop Y.

The viscosities of the prepared ophthalmic solutions Y, C and D are the 17th revised Japanese Pharmacy, 2.53 viscosity measurement method, the second rotational viscometer method, 2.1.3 conical-plate type rotational viscometer. The measurement was performed according to the method described in (Cone plate type viscometer). Specifically, Kinexus pro + (manufactured by Malvern) was used, and the measurement conditions were set as follows.
(Measurement condition)
Rotor angle: 1 °
Rotor diameter: 50 mm
Sample volume: 0.57 mL
Measurement temperature: 25 ° C
Shear velocity: 50s ^-1
Measurement time: The viscosity was measured every 2 seconds, and the average value for 1 minute was taken as the viscosity.

(Test method)
SV40 immortalized human corneal epithelial cells (HCE-T: RIKEN, Bioresource Center, Cell No .: RCB2280) were seeded in 96-well plates (1 × 10 ⁴ cells / well) and 10% FBS-containing D-MEM / The cells were cultured in F12 medium for 1 day. The next day, after exchanging the medium with eye drops Y, eye drops C or eye drops D, the corneal epithelial cells were cultured for 5, 10 and 15 minutes. The cell proliferation assay kit (manufactured by Promega, catalog number: G3580) was used to measure the viable cell activity (corresponding to the absorbance at 490 nm).

(result)
The test results are shown in FIG.

As is clear from FIG. 2, the diquafosol ophthalmic solution (eye drops C and D) containing polyvinylpyrrolidone maintained a high survival rate in immortalized human corneal epithelial cells even after 15 minutes of culture. On the other hand, the survival rate of diquafosol ophthalmic solution (eye drop Y) containing no polyvinylpyrrolidone decreased with time.

(Discussion)
Diquafosol ophthalmic solution containing polyvinylpyrrolidone shows high viable cell activity in cultured immortalized human corneal epithelial cells, so that it is safer for corneal conjunctival epithelium and unstable corneal epithelium such as dry eye. It is useful for use in various diseases.

[Test 4]
The irritation of diquafosol sodium to peripheral nerves in the presence of PVP was investigated.

(Sample preparation method)
Prescription solution 1:
The prescription solution 1 was prepared according to the prescription table shown in Table 4. That is, sodium chloride (8.5 g) and sodium hydrogen phosphate hydrate (2 g) were dissolved in sterile purified water, a pH adjuster was added, the pH was adjusted to 7.5, and the total volume was adjusted to 100 mL. A 10-fold buffer was obtained. PVP K30 (16 g) was dissolved in sterile purified water to adjust the total volume to 200 mL to obtain an 8% PVP K30 aqueous solution. 2 mL of 10-fold buffer and 5 mL of 8% PVP K30 aqueous solution were weighed, the total volume was adjusted to 20 mL with sterile purified water, and the pH was adjusted to 7.5 using a pH adjuster to obtain a prescription solution 1.

Prescription solution 2:
The prescription solution 2 was prepared according to the prescription table shown in Table 4. That is, sodium chloride (8.5 g) and sodium hydrogen phosphate hydrate (2 g) were dissolved in sterile purified water, a pH adjuster was added, the pH was adjusted to 7.5, and the total volume was adjusted to 100 mL. A 10-fold buffer was obtained. 2 mL of 10-fold buffer and PVP K90 (0.4 g) were dissolved in sterile purified water, the pH was adjusted to 7.5 using a pH adjuster, and the total volume was 20 mL to obtain prescription solution 2.

Prescription solution 3:
The prescription solution 3 was prepared according to the prescription table shown in Table 4. That is, sodium chloride (8.5 g) and sodium hydrogen phosphate hydrate (2 g) were dissolved in sterile purified water, a pH adjuster was added, the pH was adjusted to 7.5, and the total volume was adjusted to 100 mL. A 10-fold buffer was obtained. Add 2 mL of 10-fold buffer and sodium chondroitin sulfate (0.06 g) to sterile purified water, adjust the pH to 7.5 using a pH adjuster, confirm dissolution, and adjust the total volume to 20 mL. I got 3.

Prescription liquid 4-6:
According to the prescription table shown in Table 4, prescription liquids 4 to 6 were prepared in the same manner as the prescription liquid 3.

(Test method)
Cultured peripheral nerve cells (rat dorsal root ganglion neurons, purchased from Lonza Japan) were incubated in a buffer containing intracellular calcium-indicating fluorescent dye (FLIPR Calcium 6 Assay Kit, Molecular Devices). 40% of the total buffer solution was replaced with each of the above prescription solutions. The non-stimulation group and the stimulation control group were similarly treated with a buffer solution instead of the prescription solution. After allowing to stand at room temperature, the fluorescence measurement of the calcium indicator dye over time was started using a fluorescent plate reader. Sodium diquafosol (final concentration: 0.3%) was added 60 seconds after the start, and the measurement of fluorescence intensity was continued.

(Evaluation method)
The maximum fluorescence intensity (RFUmax) after the addition was calculated with the fluorescence intensity (RFU) immediately before the addition of diquafosol sodium as 100%.

(Test results)
The results are shown in FIG. In the stimulus control group and prescription solutions 3 to 6, RFU increased after the addition of diquafosol sodium, and RFUmax of 103.5% or more was recorded. On the other hand, RFUmax was less than 101% in each group of prescription solutions 1 and 2 containing PVP.

(Discussion)
Peripheral nerve cells that receive some kind of stimulus generate action potentials and become excited, and the stimulus signals converted into action potentials are then transmitted to the central nervous system. The action potential is a change in cell membrane potential caused by the intracellular influx of cations including calcium ions. Therefore, an increase in the calcium ion concentration in a nerve cell is widely used experimentally as an index showing an excited state of a nerve cell. When peripheral nerve cells were exposed to diquafosol sodium, the fluorescence intensity of intracellular calcium ions was rapidly increased, indicating that the nerve cells received diquafosol sodium as a stimulus and became excited. Similar stimulus responses were observed in each group of polymer formulation solutions 3 to 6 containing no PVP as a comparative example, and each polymer of chondroitin sodium sulfate, HPMC, CVP and CMC-Na was neurostimulated with diquafosol sodium. It had no effect on sex. On the other hand, under the prescription solutions 1 and 2 containing PVP, no increase in the intracellular calcium ion signal after the addition of diquafosol sodium was shown. That is, it was suggested that diquafosol sodium coexisting with PVP did not show neurostimulation, and that the addition of PVP improved the comfort of diquafosol sodium ophthalmic solution.

[Test 5]
The effect of this composition on the stability of preservatives was investigated.

(Sample preparation method)
Eye drops 6:
Ophthalmic solution 6 was prepared according to the formulation shown in Table 5. Specifically, sodium diquafosol (3 g), chlorhexidine sulconate (0.0025 g), hydroxyethyl cellulose (0.2 g), sodium hydrogen phosphate hydrate (0.2 g), sodium edetate hydrate. (0.01 g) and sodium chloride (0.45 g) were dissolved in water to make 100 mL, and a pH adjuster (q.s.) was added to make pH 7.5.

Eye drops 7-10:
According to the prescription shown in Table 5, eye drops 7 to 10 were prepared in the same manner as the eye drops 6.

(Test method)
The content of chlorhexidine gluconate when the eye drops 6 and 7 were stored at 60 ° C. for up to 4 weeks, respectively, was quantified by using high performance liquid chromatography (HPLC), and the residual ratio (%) was calculated. The content of chlorhexidine gluconate when the eye drops 8 and 9 were stored at 60 ° C. for up to 2 weeks was quantified by using high performance liquid chromatography (HPLC), and the residual rate (%) was calculated. .. The silver nitrate content when the ophthalmic solution 10 was stored at 60 ° C. for up to 4 weeks was quantified using high frequency inductively coupled plasma emission spectroscopy (ICP-AES), and the residual rate (%) was calculated.

(Test results)
The results of the stability test are shown in Table 6.

(Discussion)
In an aqueous ophthalmic composition containing diquafosol or a salt thereof and polyvinylpyrrolidone (the present composition), when chlorhexidine gluconate was contained as an antiseptic, the residual rate was significantly reduced (eye drops 7-9). .. On the other hand, when silver nitrate, which is a silver salt, was contained as a preservative, the residual rate was high (eye drops 10). From the above, it was shown that this composition destabilizes chlorhexidine gluconate while stabilizing silver salt.

[Test 6]
The preservation effect of this composition containing a silver salt was examined.

(Sample preparation method)
Eye drops 11:
Ophthalmic solution 11 was prepared according to the formulation shown in Table 7. Specifically, sodium diquafosol (3 g), silver nitrate (0.00008 g), sodium hydrogen phosphate hydrate (0.2 g), sodium edetate hydrate (0.01 g), polyvinylpyrrolidone K30 (2 g). ), Concentrated glycerin (1.2 g) and hydroxyethyl cellulose (0.25 g) were dissolved in sterile purified water to make 100 mL, and a pH adjuster (q.s.) was added to make pH 7.5.

Eye drops 12 to 15:
According to the prescription shown in Table 7, each eye drop of the eye drops 12 to 15 was prepared in the same manner as the eye drop 11.

(Test method)
The storage efficacy test was conducted in accordance with the 17th revised Japanese Pharmacopoeia's storage efficacy test method. In this test, E. coli (E. coli), Pseudomonas aeruginosa (P. aeruginosa), Staphylococcus aureus (S. aureus), Candida albicans (Candida albicans), and Candida albicans (Candida albicans) were used as test bacteria. ..

(Test results)
The test results are shown in Table 8.

The test results in Table 8 show how much the viable cell count at the time of the test decreased compared to the number of inoculated bacteria by log reduction. For example, in the case of "1", the viable cell count at the time of the test is shown. Shows that the number of inoculated bacteria has decreased to 10%.

As shown in Table 8, it was shown that this composition containing a silver salt conforms to the preservation efficacy test standard of the Japanese Pharmacopoeia.

(Discussion)
From the above results, it was shown that the present composition containing a silver salt has an excellent preservative effect.

[Test 7]
Using normal male white rabbits, the time course of tear volume was evaluated 90 minutes after instillation of this composition.

(Sample preparation method)
Eye drops 16:
As the ophthalmic solution 16, sodium hydrogen phosphate hydrate (0.2 g), sodium edetate hydrate (0.01 g), sodium chloride (0.45 g), silver nitrate (0.00004 g), polyvinylpyrrolidone K90 (2 g). ), Sodium diquafosol (3 g) was dissolved in sterile purified water to make 100 mL, and a pH adjuster (q.s.) was added to make pH 7.5.

Eye drops 17:
As the eye drops 17, "Diquas ^{(registered trademark)} eye drops 3%" (manufactured by Santen Pharmaceutical Co., Ltd.), which is used as a therapeutic agent for dry eye, was used. The ophthalmic solution 17 contains 30 mg of diquafosol sodium as an active ingredient in 1 mL of water, and as additives, potassium chloride, sodium chloride, chlorhexzing gluconate solution, sodium hydrogen phosphate hydrate, sodium edetate hydrate. , Contains a pH adjuster.

(Test method and drug administration method)
Normal male white rabbits (12 animals and 24 eyes in total) were instilled with Benokiseal ^{(registered trademark)} ophthalmic solution 0.4% (manufactured by Santen Pharmaceutical Co., Ltd.) and subjected to local anesthesia. Three minutes later, a Sylmel test paper (manufactured by AYUMI Pharmaceutical Corporation) was inserted into the lower eyelid, and one minute after the insertion, the paper was removed and the length of the wet portion (tear volume) was read. This was used as the previous value. Next, each eye drop 16 and 17 was instilled once (6 animals in a group, 12 eyes). Three minutes before inserting the Sylmel test paper (manufactured by AYUMI Pharmaceutical Corporation) into the lower eyelid, ^{0.4% of Benokiseal (registered trademark)} ophthalmic solution (manufactured by Santen Pharmaceutical Corporation) was instilled and local anesthesia was applied. 90 minutes after each ophthalmic solution was instilled, a Sylmel test paper (manufactured by AYUMI Pharmaceutical Corporation) was inserted into the lower eyelid, and 1 minute after the insertion, it was withdrawn and the length of the wet portion (tear volume) was read.

(Evaluation method)
Ophthalmic solution The change in tear volume before and after instillation was calculated as Δtear volume (mm / min).

(Test results)
Table 9 shows the amount of Δtear fluid (mm / min) 90 minutes after instillation (each value is an average value of 12 eyes). In addition, the tear volume increasing effect of this composition was evaluated according to the following criteria.
+++: ΔTear volume (mm / min) 90 minutes after instillation is 4 mm / min or more
++: ΔTear volume (mm / min) 90 minutes after instillation is 1 mm / min or more and less than 4 mm / min
+: The amount of Δtear (mm / min) 90 minutes after instillation is more than 0 mm / min or less than 1 mm / min.
-: The amount of Δtear (mm / min) 90 minutes after instillation is 0 mm / min or less.

As shown in the results of Table 9 above, this composition showed a high tear volume increasing effect even 90 minutes after instillation.

[Test 8]
The preservation effect of this composition containing a silver salt was examined.

(Sample preparation method)
Eye drops 18:
Ophthalmic solution 18 was prepared according to the formulation shown in Table 10. Specifically, sodium diquafosol (3 g), silver nitrate (0.00003 g), sodium hydrogen phosphate hydrate (0.2 g), sodium edetate hydrate (0.01 g), polyvinylpyrrolidone K90 (2 g). ), Sodium chloride (0.45 g) was dissolved in sterile purified water to make 100 mL, and a pH adjuster (q.s.) was added to make pH 7.0.

Eye drops 19:
The eye drops 19 were prepared in the same manner as the eye drops 18 according to the prescription shown in Table 10.

(Test method)
The storage efficacy test was conducted in accordance with the 17th revised Japanese Pharmacopoeia's storage efficacy test method. In this test, E. coli (E. coli), Pseudomonas aeruginosa (P. aeruginosa), Staphylococcus aureus (S. aureus), Candida albicans (Candida albicans), and Candida albicans (Candida albicans) were used as test bacteria. ..

(Test results)
The test results are shown in Table 11.

The test results in Table 11 show how much the viable cell count at the time of the test decreased compared to the number of inoculated bacteria by log reduction. For example, in the case of "1", the viable cell count at the time of the test is shown. Shows that the number of inoculated bacteria has decreased to 10%.

As shown in Table 11, it was shown that the composition containing silver salt, with or without EDTA, conforms to the storage efficacy test standards of the Japanese Pharmacopoeia.

(Discussion)
From the above results, it was shown that the present composition containing a silver salt has an excellent preservative effect.

[Test 9]
The preservation effect of this composition containing a silver salt was examined.

(Sample preparation method)
Eye drops 20:
Ophthalmic solution 20 was prepared according to the formulation shown in Table 12. Specifically, sodium diquafosol (3 g), silver nitrate (0.00004 g), sodium hydrogen phosphate hydrate (0.2 g), sodium edetate hydrate (0.01 g), polyvinylpyrrolidone K90 (2 g). ), Sodium chloride (0.45 g) was dissolved in sterile purified water to make 100 mL, and a pH adjuster (q.s.) was added to make pH 7.5.

Eye drops 21-23:
According to the prescription shown in Table 12, each eye drop of the eye drops 21 to 23 was prepared in the same manner as the eye drop 20.

(Test method)
The storage efficacy test was conducted in accordance with the 17th revised Japanese Pharmacopoeia's storage efficacy test method. In this test, E. coli (E. coli), Pseudomonas aeruginosa (P. aeruginosa), Staphylococcus aureus (S. aureus), Candida albicans (Candida albicans), and Candida albicans (Candida albicans) were used as test bacteria. ..

(Test results)
The test results are shown in Table 13.

The test results in Table 13 show how much the viable cell count at the time of the test decreased compared to the number of inoculated bacteria by log reduction. For example, in the case of "1", the viable cell count at the time of the test is shown. Shows that the number of inoculated bacteria has decreased to 10%.

As shown in Table 13, the composition containing silver salt, with or without EDTA, was shown to meet the Japanese Pharmacopoeia's preservation efficacy test standards. In addition, it was shown that ophthalmic solutions containing silver phosphate and silver chloride as silver salts also meet the preservation efficacy test standards of the Japanese Pharmacopoeia.

(Discussion)
From the above results, it was shown that the present composition containing a silver salt has an excellent preservative effect.

[Test 10]
The effect of this composition on the stability of preservatives was investigated.

(Sample preparation method)
Eye drops 24:
Sodium diquafosol (3 g), sodium edetate hydrate (0.01 g), sodium hydrogen phosphate hydrate (0.2 g), sodium chloride (0.45 g), polyvinylpyrrolidone K90 (2 g), silver nitrate ( 0.00004 g) was dissolved in water to make 100 mL, and a pH adjuster (q.s.) was added to make the pH 7.5, and an ophthalmic solution 24 was prepared.

(Test method)
The content of silver nitrate when the ophthalmic solution 24 was stored at 40 ° C. for up to 6 months was quantified using high frequency inductively coupled plasma emission spectroscopy (ICP-AES), and the residual rate (%) was calculated.

(Test results)
The results of the stability test are shown in Table 14.

(Discussion)
When silver nitrate, which is a silver salt, was contained as a preservative, the residual rate was high. From the above, it was shown that the silver salt is stable in this composition.

[Example of pharmaceutical product]
The agent of the present invention will be described in more detail with reference to pharmaceutical examples, but the present invention is not limited to these pharmaceutical examples.

(Prescription Example 1: Sterile aqueous ophthalmic solution (3% (w / v)))
Diquafosol sodium 3g in 100mL
Sodium hydrogen phosphate hydrate 0.01-0.5 g
Sodium chloride 0.01-1g
Sodium edetate hydrate 0.0001-0.1g
Polyvinylpyrrolidone K90 0.0001-10g
pH regulator Appropriate amount Add diquafosol sodium and other components to the purified water, and mix them well to prepare the above eye drops. 1 to 10 mL of the above ophthalmic solution can be filled in a multi-dose type eye drop container or a PFMD container to produce an ophthalmic pharmaceutical product. Further, 0.1 to 1 mL of the above ophthalmic solution can be filled in a unit dose type eye drop container to produce an ophthalmic pharmaceutical product. The above eye drops can be stored at room temperature.

(Prescription Example 2: Sterile aqueous ophthalmic solution (3% (w / v)))
Diquafosol sodium 3g in 100mL
Sodium hydrogen phosphate hydrate 0.01-0.5 g
Sodium chloride 0.01-1g
Sodium edetate hydrate 0.0001-0.1g
Polyvinylpyrrolidone K60 0.0001-10g
pH regulator Appropriate amount Add diquafosol sodium and other components to the purified water, and mix them well to prepare the above eye drops. 1 to 10 mL of the above ophthalmic solution can be filled in a multi-dose type eye drop container or a PFMD container to produce an ophthalmic pharmaceutical product. Further, 0.1 to 1 mL of the above ophthalmic solution can be filled in a unit dose type eye drop container to produce an ophthalmic pharmaceutical product. The above eye drops can be stored at room temperature.

(Prescription Example 3: Sterile aqueous ophthalmic solution (3% (w / v)))
Diquafosol sodium 3g in 100mL
Sodium hydrogen phosphate hydrate 0.01-0.5 g
Sodium chloride 0.01-1g
Sodium edetate hydrate 0.0001-0.1g
Polyvinylpyrrolidone K40 0.0001-10g
pH regulator Appropriate amount Add diquafosol sodium and other components to the purified water, and mix them well to prepare the above eye drops. 1 to 10 mL of the above ophthalmic solution can be filled in a multi-dose type eye drop container or a PFMD container to produce an ophthalmic pharmaceutical product. Further, 0.1 to 1 mL of the above ophthalmic solution can be filled in a unit dose type eye drop container to produce an ophthalmic pharmaceutical product. The above eye drops can be stored at room temperature.

(Prescription Example 4: Sterile aqueous ophthalmic solution (3% (w / v)))
Diquafosol sodium 3g in 100mL
Sodium hydrogen phosphate hydrate 0.01-0.5 g
Sodium chloride 0.01-1g
Sodium edetate hydrate 0.0001-0.1g
Polyvinylpyrrolidone K90 0.0001-10g
Silver nitrate 0.00000001 ~ 1g
pH regulator Appropriate amount Add diquafosol sodium and other components to the purified water, and mix them well to prepare the above eye drops. A multi-dose type eye drop container can be filled with 1 to 10 mL of the above eye drop solution to produce an ophthalmic pharmaceutical product. The above eye drops can be stored at room temperature.

(Prescription Example 5: Sterile aqueous ophthalmic solution (3% (w / v)))
Diquafosol sodium 3g in 100mL
Sodium hydrogen phosphate hydrate 0.01-0.5 g
Sodium chloride 0.01-1g
Sodium edetate hydrate 0.0001-0.1g
Polyvinylpyrrolidone K60 0.0001-10g
Silver nitrate 0.00000001 ~ 1g
pH regulator Appropriate amount Add diquafosol sodium and other components to the purified water, and mix them well to prepare the above eye drops. A multi-dose type eye drop container can be filled with 1 to 10 mL of the above eye drop solution to produce an ophthalmic pharmaceutical product. The above eye drops can be stored at room temperature.

(Prescription Example 6: Sterile aqueous ophthalmic solution (3% (w / v)))
Diquafosol sodium 3g in 100mL
Sodium hydrogen phosphate hydrate 0.01-0.5 g
Sodium chloride 0.01-1g
Sodium edetate hydrate 0.0001-0.1g
Polyvinylpyrrolidone K40 0.0001-10g
Silver nitrate 0.00000001 ~ 1g
pH regulator Appropriate amount Add diquafosol sodium and other components to the purified water, and mix them well to prepare the above eye drops. A multi-dose type eye drop container can be filled with 1 to 10 mL of the above eye drop solution to produce an ophthalmic pharmaceutical product. The above eye drops can be stored at room temperature.

(Prescription Example 7: Sterile aqueous ophthalmic solution (3% (w / v)))
Diquafosol sodium 3g in 100mL
Sodium hydrogen phosphate hydrate 0.01-0.5 g
Sodium chloride 0.01-1g
Polyvinylpyrrolidone K90 0.0001-10g
pH regulator Appropriate amount Add diquafosol sodium and other components to the sterile purified solution and mix them well to prepare the above eye drops. 1 to 10 mL of the above ophthalmic solution can be filled in a multi-dose type eye drop container or a PFMD container to produce an ophthalmic pharmaceutical product. Further, 0.1 to 1 mL of the above ophthalmic solution can be filled in a unit dose type eye drop container to produce an ophthalmic pharmaceutical product. The above eye drops can be stored at room temperature.

(Prescription Example 8: Sterile aqueous ophthalmic solution (3% (w / v)))
Diquafosol sodium 3g in 100mL
Sodium hydrogen phosphate hydrate 0.01-0.5 g
Sodium chloride 0.01-1g
Polyvinylpyrrolidone K60 0.0001-10g
pH regulator Appropriate amount Add diquafosol sodium and other components to the purified water, and mix them well to prepare the above eye drops. 1 to 10 mL of the above ophthalmic solution can be filled in a multi-dose type eye drop container or a PFMD container to produce an ophthalmic pharmaceutical product. Further, 0.1 to 1 mL of the above ophthalmic solution can be filled in a unit dose type eye drop container to produce an ophthalmic pharmaceutical product. The above eye drops can be stored at room temperature.

(Prescription Example 9: Aseptic aqueous ophthalmic solution (3% (w / v)))
Diquafosol sodium 3g in 100mL
Sodium hydrogen phosphate hydrate 0.01-0.5 g
Sodium chloride 0.01-1g
Polyvinylpyrrolidone K40 0.0001-10g
pH regulator Appropriate amount Add diquafosol sodium and other components to the purified water, and mix them well to prepare the above eye drops. 1 to 10 mL of the above ophthalmic solution can be filled in a multi-dose type eye drop container or a PFMD container to produce an ophthalmic pharmaceutical product. Further, 0.1 to 1 mL of the above ophthalmic solution can be filled in a unit dose type eye drop container to produce an ophthalmic pharmaceutical product. The above eye drops can be stored at room temperature.

(Prescription Example 10: Sterile aqueous ophthalmic solution (3% (w / v)))
Diquafosol sodium 3g in 100mL
Sodium hydrogen phosphate hydrate 0.01-0.5 g
Sodium chloride 0.01-1g
Polyvinylpyrrolidone K90 0.0001-10g
Silver nitrate 0.00000001 ~ 1g
pH regulator Appropriate amount Add diquafosol sodium and other components to the purified water, and mix them well to prepare the above eye drops. A multi-dose type eye drop container can be filled with 1 to 10 mL of the above eye drop solution to produce an ophthalmic pharmaceutical product. The above eye drops can be stored at room temperature.

(Prescription Example 11: Aseptic aqueous ophthalmic solution (3% (w / v)))
Diquafosol sodium 3g in 100mL
Sodium hydrogen phosphate hydrate 0.01-0.5 g
Sodium chloride 0.01-1g
Polyvinylpyrrolidone K60 0.0001-10g
Silver nitrate 0.00000001 ~ 1g
pH regulator Appropriate amount Add diquafosol sodium and other components to the purified water, and mix them well to prepare the above eye drops. A multi-dose type eye drop container can be filled with 1 to 10 mL of the above eye drop solution to produce an ophthalmic pharmaceutical product. The above eye drops can be stored at room temperature.

(Prescription Example 12: Sterile aqueous ophthalmic solution (3% (w / v)))
Diquafosol sodium 3g in 100mL
Sodium hydrogen phosphate hydrate 0.01-0.5 g
Sodium chloride 0.01-1g
Polyvinylpyrrolidone K40 0.0001-10g
Silver nitrate 0.00000001 ~ 1g
pH regulator Appropriate amount Add diquafosol sodium and other components to the purified water, and mix them well to prepare the above eye drops. A multi-dose type eye drop container can be filled with 1 to 10 mL of the above eye drop solution to produce an ophthalmic pharmaceutical product. The above eye drops can be stored at room temperature.

(Prescription Example 13: Sterile aqueous ophthalmic solution (3% (w / v)))
Diquafosol sodium 3g in 100mL
Sodium hydrogen phosphate hydrate 0.01-0.5 g
Sodium chloride 0.01-1g
Citric acid hydrate 0.0001-0.1g
Polyvinylpyrrolidone K90 0.0001-10g
pH regulator Appropriate amount Add diquafosol sodium and other components to the purified water, and mix them well to prepare the above eye drops. 1 to 10 mL of the above ophthalmic solution can be filled in a multi-dose type eye drop container or a PFMD container to produce an ophthalmic pharmaceutical product. Further, 0.1 to 1 mL of the above ophthalmic solution can be filled in a unit dose type eye drop container to produce an ophthalmic pharmaceutical product. The above eye drops can be stored at room temperature.

(Prescription Example 14: Aseptic aqueous ophthalmic solution (3% (w / v)))
Diquafosol sodium 3g in 100mL
Sodium hydrogen phosphate hydrate 0.01-0.5 g
Sodium chloride 0.01-1g
Citric acid hydrate 0.0001-0.1g
Polyvinylpyrrolidone K90 0.0001-10g
Silver nitrate 0.00000001 ~ 1g
pH regulator Appropriate amount Add diquafosol sodium and other components to the purified water, and mix them well to prepare the above eye drops. A multi-dose type eye drop container can be filled with 1 to 10 mL of the above eye drop solution to produce an ophthalmic pharmaceutical product. The above eye drops can be stored at room temperature.

Existing Jikuasu ^® ophthalmic solution has to be instilled 6 times a day, but there severe dry eye patients who do not provide a sufficient therapeutic effect can be used with default Dosage. In addition, there are some patients who do not get the expected effect due to poor eye drop adherence. This composition ^{has a stronger dry eye therapeutic effect than the existing Diquas (registered trademark)} ophthalmic solution, and is expected to improve eye drop adherence by reducing the number of instillations. It is also expected that this composition exerts the same or higher dry eye therapeutic effect at a lower concentration than the ^{existing Diquas (registered trademark) ophthalmic solution.}

Furthermore, it is expected that this composition exhibits high viable cell activity, is highly safe for the keratoconjunctival epithelium, does not exhibit neurostimulation, and can improve the feeling of instillation of eye drops.

Further, even if the present composition contains a silver salt, the silver salt is stable and exhibits excellent preservative effect.

Claims (45)

An aqueous ophthalmic composition for preventing or treating dry eye, which contains diquafosol or a salt thereof and polyvinylpyrrolidone filled in a multi-dose type eye drop container, and the filling amount of the aqueous ophthalmic composition is 1 to 1. 10 mL of aqueous ophthalmic composition. The aqueous ophthalmic composition according to claim 1, further comprising a silver salt. The aqueous ophthalmic composition according to claim 2, wherein the silver salt contains silver nitrate. Axis Aho Sol sodium and K values of the concentration of 1~5% (w / v) contains greater than 30 to 120 the following polyvinyl pyrrolidone, aqueous ophthalmic composition of claim 1. 3% Axis Aho Sol sodium and K values of the concentration of (w / v) contains greater than 30 to 120 the following polyvinyl pyrrolidone, aqueous ophthalmic composition of claim 1. The aqueous ophthalmic composition according to claim 1, which contains 1 to 5% (w / v) of sodium diquafosol and has a viscosity of 1.5 to 30 mPa · s at 25 ° C. The aqueous ophthalmic composition according to claim 1, which contains diquafosol sodium at a concentration of 3% (w / v) and has a viscosity of 1.5 to 30 mPa · s at 25 ° C. The aqueous ophthalmic composition according to any one of claims 1 to 7 , wherein the composition is used so as to be administered by eye drops 2 to 4 times a day. The aqueous ophthalmic composition according to any one of claims 1 to 7 , wherein the composition is used so as to be administered by eye drops three times a day. The aqueous ophthalmic composition according to claim 8 or 9 , wherein the composition is used so as to be administered by eye drops at a time of 1 to 2 drops. An ophthalmic pharmaceutical product for the prevention or treatment of dry eye, wherein 1 to 10 mL of an aqueous ophthalmic composition containing diquafosol or a salt thereof and polyvinylpyrrolidone is filled in a multidose type eye drop container. An ophthalmic pharmaceutical product for the prevention or treatment of dry eye, wherein 5 mL of an aqueous ophthalmic composition containing diquafosol or a salt thereof and polyvinylpyrrolidone is filled in a multidose type eye drop container. An ophthalmic pharmaceutical product for the prevention or treatment of dry eye, wherein 1 to 10 mL of an aqueous ophthalmic composition containing diquafosol or a salt thereof and polyvinylpyrrolidone is filled in a PFMD container. An ophthalmic pharmaceutical product for the prevention or treatment of dry eye, wherein 5 mL of an aqueous ophthalmic composition containing diquafosol or a salt thereof and polyvinylpyrrolidone is filled in a PFMD container. 13. Ophthalmic pharmaceutical products. The ophthalmology according to any one of claims 11 to 14, wherein the aqueous ophthalmic composition contains diquafosol sodium at a concentration of 3% (w / v) and polyvinylpyrrolidone having a K value of more than 30 to 120 or less. Medicinal product. Aqueous composition containing Axis Aho Sol sodium concentration of 1~5% (w / v), has a viscosity of 1.5~30mPa · s at 25 ° C., to any one of claims 11 to 14 The listed ophthalmic pharmaceutical products. The one according to any one of claims 11 to 14, wherein the aqueous composition contains 3% (w / v) concentration of diquafosol sodium and has a viscosity of 1.5 to 30 mPa · s at 25 ° C. Ophthalmic pharmaceutical products. The ophthalmic pharmaceutical product according to any one of claims 11 to 18 , wherein the product is used so as to be administered by eye drops 2 to 4 times a day. The ophthalmic pharmaceutical product according to any one of claims 11 to 18 , wherein the product is used so as to be administered by eye drops three times a day. The ophthalmic pharmaceutical product according to claim 19 or 20 , wherein the product is used so as to be administered by eye drops at a time of 1 to 2 drops. The aqueous ophthalmic composition according to any one of claims 1 to 3 , which comprises polyvinylpyrrolidone having a K value of 17 or more. The aqueous ophthalmic composition according to any one of claims 1 to 3 , which comprises polyvinylpyrrolidone having a K value of 17 to 120. The aqueous ophthalmic composition according to any one of claims 1 to 3 , which comprises polyvinylpyrrolidone having a K value of more than 30 to 120 or less. The aqueous ophthalmic composition according to any one of claims 1 to 3 , which comprises polyvinylpyrrolidone having a K value of 90. The aqueous ophthalmic composition according to any one of claims 1 to 10 , wherein the concentration of polyvinylpyrrolidone is 0.001% (w / v) or more. The aqueous ophthalmic composition according to any one of claims 1 to 3 , wherein the concentration of the diquafosol or a salt thereof is 0.0001 to 10% (w / v). The aqueous ophthalmic composition according to any one of claims 1 to 3 , wherein the concentration of the diquafosol or a salt thereof is 0.01 to 5% (w / v). The aqueous ophthalmic composition according to any one of claims 1 to 3 , wherein the concentration of the diquafosol or a salt thereof is 1 to 5% (w / v). The aqueous ophthalmic composition according to any one of claims 1 to 3 , wherein the concentration of the diquafosol or a salt thereof is 3% (w / v). The aqueous ophthalmic composition according to any one of claims 1 to 10 , wherein the pH of the aqueous ophthalmic composition is in the range of 6 to 8. The aqueous ophthalmic composition according to any one of claims 1 to 10 , wherein the pH of the aqueous ophthalmic composition is in the range of 7 to 8. The aqueous ophthalmic composition according to any one of claims 1 to 10 , wherein the aqueous ophthalmic composition is a sterile aqueous ophthalmic solution. The aqueous ophthalmic composition according to any one of claims 1 to 10 , which can be stored at room temperature. The aqueous ophthalmic composition according to any one of claims 1 to 5 , wherein the aqueous ophthalmic composition has a viscosity of 1.5 to 30 mPa · s at 25 ° C. The aqueous ophthalmic composition according to any one of claims 1 to 3, wherein the salt of diquafosol is diquafosol sodium. Diquafosol sodium at a concentration of 3% (w / v), polyvinylpyrrolidone with a K value of 90 and An aqueous ophthalmic composition containing silver nitrate for the prevention or treatment of dry eye. It contains 1 to 2 drops of diquafosol sodium, polyvinylpyrrolidone and silver nitrate at a concentration of 3% (w / v), characterized in that it is used to be administered by eye drops 2 to 4 times a day. An aqueous ophthalmic composition for the prevention or treatment of dry eye, the aqueous ophthalmic composition having a viscosity of 3 to 30 mPa · s at 25 ° C. The aqueous ophthalmic composition according to claim 37 or 38 , which is used so as to be administered by eye drops three times a day. Prevention or treatment of dry eye in which 1-10 mL of an aqueous ophthalmic composition containing 3% (w / v) concentration of diquafosol sodium and polyvinylpyrrolidone with a K value of 90 was filled in a multidose eye drop container. An ophthalmic pharmaceutical product for, wherein the aqueous ophthalmic composition is used to be administered by eye drops 1 to 2 drops at a time, 2 to 4 times a day. .. An ophthalmic drug for the prevention or treatment of dry eye, in which 1 to 10 mL of an aqueous ophthalmic composition containing diquafosol sodium and polyvinylpyrrolidone at a concentration of 3% (w / v) is filled in a multidose eye drop container. It is a product for use, and the aqueous ophthalmic composition has a viscosity of 3 to 30 mPa · s at 25 ° C., and is used so as to be instilled 1 to 2 drops at a time and 2 to 4 times a day. An ophthalmic pharmaceutical product characterized by this. 1-10 mL of an aqueous ophthalmic composition containing diquafosol sodium at a concentration of 3% (w / v) and polyvinylpyrrolidone with a K value of 90 was filled in a PFMD container for the prevention or treatment of dry eye. An ophthalmic pharmaceutical product, characterized in that the aqueous ophthalmic composition is used by instillation at 1 to 2 drops at a time, 2 to 4 times a day. An ophthalmic pharmaceutical product for the prevention or treatment of dry eye, in which 1-10 mL of an aqueous ophthalmic composition containing diquafosol sodium and polyvinylpyrrolidone at a concentration of 3% (w / v) is filled in a PFMD container. The aqueous ophthalmic composition has a viscosity of 3 to 30 mPa · s at 25 ° C., and is characterized in that it is used so as to be administered by eye drops 1 to 2 drops at a time and 2 to 4 times a day. An ophthalmic pharmaceutical product. The ophthalmic pharmaceutical product according to any one of claims 40 to 43 , which is used so as to be administered by eye drops three times a day. The ophthalmic pharmaceutical product according to claim 40 or 41 , further comprising silver nitrate.

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