JPH10120569A - Preventive and therapeutic agent for eye disease - Google Patents
Preventive and therapeutic agent for eye diseaseInfo
- Publication number
- JPH10120569A JPH10120569A JP8277833A JP27783396A JPH10120569A JP H10120569 A JPH10120569 A JP H10120569A JP 8277833 A JP8277833 A JP 8277833A JP 27783396 A JP27783396 A JP 27783396A JP H10120569 A JPH10120569 A JP H10120569A
- Authority
- JP
- Japan
- Prior art keywords
- therapeutic agent
- preventive
- retinal
- lower alkylene
- eye
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
- Pending
Links
Abstract
Description
【0001】[0001]
【発明の属する技術分野】本発明は、1,4-(ジフェニ
ルアルキル)ピペラジン誘導体を有効成分とする眼疾
患、特に糖尿病性網膜症もしくは網膜血管閉塞症等の網
膜疾患または緑内障の予防または治療に有用な薬剤に関
するものである。The present invention relates to the prevention or treatment of ophthalmic diseases containing a 1,4- (diphenylalkyl) piperazine derivative as an active ingredient, particularly retinal diseases such as diabetic retinopathy or retinal vascular occlusion or glaucoma. It is about useful drugs.
【0002】[0002]
【従来の技術】網膜は視機能に関して重要な役割を果た
しており、この網膜に存在する網膜神経細胞は眼におけ
る情報伝達という重要な役割を担っている。網膜神経細
胞に障害が生じると情報伝達に異常を来たし、種々の眼
疾患を引き起こす。従って、網膜神経細胞を障害から保
護し、その正常な機能を維持させることは、眼疾患の予
防または治療法の一つとして重要である。2. Description of the Related Art The retina plays an important role in visual function, and retinal nerve cells present in the retina play an important role in information transmission in the eye. When retinal nerve cells are damaged, information transmission is abnormal and various eye diseases are caused. Therefore, protecting retinal nerve cells from damage and maintaining their normal function is important as one of preventive or therapeutic methods for eye diseases.
【0003】網膜神経細胞の障害は、種々の原因、例え
ば、糖尿病や網膜の虚血によって引き起こされる。その
結果、糖尿病性網膜症、網膜血管閉塞症、緑内障等の眼
疾患を引き起こす(眼科, 29, 311−318(19
87), 日眼会誌, 99, 1361−1376(199
5))。[0003] Retinal nerve cell damage is caused by a variety of causes, such as diabetes and retinal ischemia. As a result, eye diseases such as diabetic retinopathy, retinal vascular occlusion, and glaucoma are caused (Ophthalmology, 29 , 311-318 (19)
87), Journal of the Nikki Society, 99, 1361-1376 (199)
5)).
【0004】本発明の有効成分である1,4-(ジフェニ
ルアルキル)ピペラジン誘導体は、σ受容体に対し強い
親和性を有し、痴呆症、うつ病、精神分裂病、不安症等
の脳神経機能障害、免疫異常や内分泌異常に伴う疾患、
消化器系潰瘍等の治療剤として有用であることが報告さ
れている(特開平7-89949)。[0004] The 1,4- (diphenylalkyl) piperazine derivative, which is an active ingredient of the present invention, has a strong affinity for a sigma receptor, and has cerebral nerve functions such as dementia, depression, schizophrenia, and anxiety. Disorders, disorders associated with immune and endocrine disorders,
It has been reported that it is useful as a therapeutic agent for gastrointestinal ulcers and the like (JP-A-7-89949).
【0005】[0005]
【発明が解決しようとする課題】1,4-(ジフェニルア
ルキル)ピペラジン誘導体の眼疾患への応用研究は、未
だなされておらず、その眼における薬理作用の研究は非
常に興味のある課題である。The study of the application of 1,4- (diphenylalkyl) piperazine derivatives to eye diseases has not yet been made, and the study of pharmacological effects in the eyes is a very interesting subject. .
【0006】[0006]
【課題を解決するための手段】本発明者等は、1,4-
(ジフェニルアルキル)ピペラジン誘導体の新たな薬理
作用を見いだすべく鋭意研究を行ったところ、1,4-
(ジフェニルアルキル)ピペラジン誘導体が、網膜神経
細胞障害に対して用量依存的に保護作用を示すことを見
い出した。すなわち、1,4-(ジフェニルアルキル)ピ
ペラジン誘導体が、眼疾患、特に、糖尿病性網膜症、網
膜血管閉塞症等の網膜疾患や緑内障の予防または治療剤
として有用であることを見い出すに至った。Means for Solving the Problems The present inventors have made 1,4-
After diligent research to find new pharmacological effects of (diphenylalkyl) piperazine derivatives, 1,4-
It has been found that (diphenylalkyl) piperazine derivatives show a protective effect against retinal neuronal damage in a dose-dependent manner. That is, they have found that 1,4- (diphenylalkyl) piperazine derivatives are useful as agents for preventing or treating eye diseases, particularly retinal diseases such as diabetic retinopathy and retinal vascular occlusion, and glaucoma.
【0007】[0007]
【発明の実施の形態】本発明は、下記一般式[I]で示
される化合物またはその塩類を有効成分とする眼疾患の
予防または治療剤に関する。BEST MODE FOR CARRYING OUT THE INVENTION The present invention relates to a preventive or therapeutic agent for eye diseases comprising a compound represented by the following general formula [I] or a salt thereof as an active ingredient.
【0008】[0008]
【化3】 Embedded image
【0009】[式中、R1 は低級アルコキシ基を示す。
R2 は低級アルコキシ基を示す。Aは低級アルキレン基
を示す。Bは低級アルキレン基を示す。] 上記で規定した基をさらに詳細に説明する。低級アルコ
キシとはメトキシ基、エトキシ基、プロポキシ基、ブト
キシ基等の炭素原子が1〜6個の低級アルコキシを示
し、低級アルキレンとは、メチレン基、エチレン基、プ
ロピレン基、ブチレン基等の炭素原子が1〜6個の低級
アルキレンを示す。[Wherein, R 1 represents a lower alkoxy group.
R 2 represents a lower alkoxy group. A represents a lower alkylene group. B represents a lower alkylene group. The groups defined above will be described in more detail. Lower alkoxy refers to lower alkoxy having 1 to 6 carbon atoms such as methoxy group, ethoxy group, propoxy group and butoxy group, and lower alkylene refers to carbon atom such as methylene group, ethylene group, propylene group and butylene group. Represents 1 to 6 lower alkylenes.
【0010】上記の化合物において、好ましい例として
下記のものが挙げられる。Among the above compounds, preferred examples include the following.
【0011】・上記一般式[I]においてAが炭素数2
〜4個の低級アルキレンを示す化合物およびその塩類。In the above general formula [I], A represents 2 carbon atoms
Compounds having from 4 to 4 lower alkylenes and salts thereof.
【0012】・上記一般式[I]においてBが炭素数2
〜4個の低級アルキレンを示す化合物およびその塩類。In the above general formula [I], B is 2 carbon atoms
Compounds having from 4 to 4 lower alkylenes and salts thereof.
【0013】特に好ましい例として下記のものが挙げら
れる。Particularly preferred examples include the following.
【0014】・上記一般式[I]においてAが−(CH
2 )3 −で、Bが−(CH2 )2 −を示す化合物および
その塩類。In the above general formula [I], A is-(CH
2) 3 -, B is - (CH 2) 2 - compounds and salts thereof showing the.
【0015】・上記一般式[I]においてR1 およびR
2 がメトキシ基を示す化合物およびその塩類。In the above general formula [I], R 1 and R
Compounds wherein 2 represents a methoxy group and salts thereof.
【0016】特に好ましい化合物の具体例として下記式
[II]で示される1-[2-(3、4-ジメトキシフェニ
ル)エチル]-4-(3-フェニルプロピル)ピペラジ
ン、またはその塩類が挙げられる。Specific examples of particularly preferred compounds include 1- [2- (3,4-dimethoxyphenyl) ethyl] -4- (3-phenylpropyl) piperazine represented by the following formula [II] or salts thereof. .
【0017】[0017]
【化4】 Embedded image
【0018】上記の塩類とは、医薬として許容される塩
類であればよく、例えば塩酸塩、硫酸塩、リン酸塩、乳
酸塩、マレイン酸塩、フマル酸塩、シュウ酸塩等が挙げ
られる。また、上記化合物は水和物の形態をとっていて
もよい。The above salts may be pharmaceutically acceptable salts, and include, for example, hydrochloride, sulfate, phosphate, lactate, maleate, fumarate, oxalate and the like. Further, the above compound may be in the form of a hydrate.
【0019】本発明は網膜神経細胞の障害に起因する眼
疾患に広く適用できるものであるが、特に、糖尿病性網
膜症もしくは網膜血管閉塞症等の網膜疾患または緑内障
に有用である。The present invention can be widely applied to eye diseases caused by disorders of retinal nerve cells, and is particularly useful for retinal diseases such as diabetic retinopathy or retinal vascular occlusion or glaucoma.
【0020】網膜神経細胞の障害は、種々の原因により
惹起されるが、実験的疾患モデルとして、グルタミン酸
投与により誘発された網膜神経細胞障害モデルが報告さ
れている(Invest. Ophthalmol. Vis. Sci., 36, 2048-
2053(1995))。本発明者等は、このグルタミン酸誘発網
膜神経細胞障害モデルを用いて、1,4-(ジフェニルア
ルキル)ピペラジン誘導体の網膜神経細胞障害に対する
保護効果を調べた。詳細は、薬理試験の項で説明する
が、1,4-(ジフェニルアルキル)ピペラジン誘導体
は、優れた網膜神経細胞の保護効果を示し、網膜神経細
胞障害に起因する眼疾患、特に、糖尿病性網膜症、網膜
血管閉塞症または緑内障の予防または治療に有用である
ことが見い出された。Although retinal nerve cell damage is caused by various causes, a retinal nerve cell damage model induced by administration of glutamate has been reported as an experimental disease model (Invest. Ophthalmol. Vis. Sci. , 36 , 2048-
2053 (1995)). The present inventors examined the protective effect of a 1,4- (diphenylalkyl) piperazine derivative on retinal neuronal damage using this glutamic acid-induced retinal neuronal damage model. The details will be described in the section on pharmacological tests. However, 1,4- (diphenylalkyl) piperazine derivatives show an excellent protective effect on retinal nerve cells, and ocular diseases caused by retinal nerve cell damage, particularly diabetic retinal cells. Has been found to be useful in the prevention or treatment of retinopathy, retinal vascular occlusion or glaucoma.
【0021】薬物の投与剤型としては錠剤、カプセル
剤、顆粒剤等の経口剤、注射剤、点眼剤等が挙げられ、
それらの製剤は汎用される技術を用いて調製することが
できる。例えば、錠剤、カプセル剤、顆粒剤等の経口剤
は、必要に応じて、乳糖、デンプン、結晶セルロース、
植物油等の増量剤、ステアリン酸マグネシウム、タルク
等の滑沢剤、ヒドロキシプロピルセルロース、ポリビニ
ルピロリドン等の結合剤、カルボキシメチルセルロース
カルシウム等の崩壊剤、ヒドロキシプロピルメチルセル
ロース、マクロゴール、シリコン樹脂等のコーティング
剤、ゼラチン皮膜剤を用いて製剤化することができる。
また、点眼剤は、塩化ナトリウム、濃グリセリン等の等
張化剤、リン酸ナトリウム、酢酸ナトリウム等の緩衝化
剤、ポリオキシエチレンソルビタンモノオレート(以
下、ポリソルベート80とする。)、ステアリン酸ポリ
オキシル40、ポリオキシエチレン硬化ヒマシ油等の界
面活性剤、クエン酸ナトリウム、エデト酸ナトリウム等
の安定化剤、塩化ベンザルコニウム、パラベン等の防腐
剤等を必要に応じて用い製剤化することができる。点眼
剤のpHは眼科製剤に許容される範囲内にあればよい
が、4〜8の範囲が好ましい。Examples of the dosage form of the drug include oral preparations such as tablets, capsules and granules, injections, eye drops and the like.
These formulations can be prepared using commonly used techniques. For example, tablets, capsules, oral preparations such as granules, if necessary, lactose, starch, crystalline cellulose,
Extender such as vegetable oil, lubricating agent such as magnesium stearate, talc, binder such as hydroxypropylcellulose, polyvinylpyrrolidone, disintegrant such as calcium carboxymethylcellulose, coating agent such as hydroxypropylmethylcellulose, macrogol, silicone resin It can be formulated using a gelatin film agent.
Further, eye drops include isotonic agents such as sodium chloride and concentrated glycerin, buffering agents such as sodium phosphate and sodium acetate, polyoxyethylene sorbitan monooleate (hereinafter referred to as polysorbate 80), and polyoxyl 40 stearate. And a surfactant such as polyoxyethylene hydrogenated castor oil, a stabilizer such as sodium citrate and sodium edetate, and a preservative such as benzalkonium chloride and paraben, if necessary. The pH of the eye drops may be within the range acceptable for ophthalmic preparations, but is preferably in the range of 4 to 8.
【0022】投与量は症状、年齢、剤型等により適宜選
択されるが、経口剤であれば通常1日あたり1mg〜1
000mgを1回または数回に分け投与すればよく、点
眼剤であれば、0.001〜3%(w/v)のものを1
日1回〜数回点眼すればよい。The dosage is appropriately selected depending on the condition, age, dosage form and the like.
000 mg may be administered once or in several divided doses. For eye drops, 0.001 to 3% (w / v) may be administered in 1 dose.
It may be applied once to several times a day.
【0023】以下、実施例として薬理試験を示す。Hereinafter, a pharmacological test will be described as an example.
【0024】[0024]
【薬理試験】赤池等の報告(Invest. Ophthalmol. Vis.
Sci., 36, 2048-2053(1995))に準じてグルタミン酸誘
発ラット網膜神経細胞障害モデルを作成し、その障害モ
デルを用いて、上記文献記載の方法に準じ1,4−(ジ
フェニルアルキル)ピペラジン誘導体の網膜神経細胞の
保護効果を調べた。[Pharmacological test] Report by Akaike et al. (Invest. Ophthalmol. Vis.
Sci., 36 , 2048-2053 (1995)), a glutamate-induced rat retinal nerve cell injury model was prepared, and the injury model was used to produce 1,4- (diphenylalkyl) piperazine according to the method described in the above-mentioned literature. The protective effect of the derivative on retinal nerve cells was examined.
【0025】(実施例1) 1.培養網膜神経細胞の調製 (1) 妊娠17〜19日目の確定妊娠ラット(Wistar/S
T)より胎仔を摘出する。(Embodiment 1) Preparation of cultured retinal neurons (1) Confirmed pregnant rats (Wistar / S
Remove the fetus from T).
【0026】(2) 得られた胎仔より眼球を摘出する。(2) The eyeball is removed from the obtained fetus.
【0027】(3) 得られた眼球から顕微鏡下、網膜を摘
出する。(3) The retina is removed from the obtained eyeball under a microscope.
【0028】(4) 摘出した網膜を細断し、細胞懸濁液と
しウシ胎仔血清添加イーグルMEM培地で一週間培養す
る(培地の交換は2日毎に行う)。(4) The excised retina is cut into small pieces, and cultured as a cell suspension in Eagle MEM medium supplemented with fetal calf serum for one week (the medium is replaced every two days).
【0029】(5) 培養開始6日目にアラビノシトシン
(約10μM)を添加する。(5) On the 6th day from the start of the culture, arabinocytosine (about 10 μM) is added.
【0030】(6) 一週間経過後、ウシ胎仔血清添加イー
グルMEM培地をウマ血清添加イーグルMEM培地に交
換し培養する。(6) After one week, the Eagle MEM medium supplemented with fetal bovine serum is replaced with an Eagle MEM medium supplemented with horse serum, and cultured.
【0031】2.培養液の調製 イーグルMEM培地粉末(9400mg)、炭酸水素ナ
トリウム(2000mg)、L−グルタミン(290m
g)、ブドウ糖(1000mg)およびHEPES g
ood buffer(2380mg)をミリQ水に溶
解し1リットルとした後、95%O2 +5%CO2 混合
ガスを30分以上バブリングし、1NのNaOHでpH
を7.2に調整する。2. Preparation of culture solution Eagle MEM medium powder (9400 mg), sodium bicarbonate (2000 mg), L-glutamine (290 m
g), glucose (1000 mg) and HEPES g
After dissolving wood buffer (2380 mg) in milli-Q water to make 1 liter, bubbling 95% O 2 + 5% CO 2 mixed gas for 30 minutes or more, and pH with 1N NaOH.
Is adjusted to 7.2.
【0032】上記の様に調製した培養液を培養液Aとす
る。培養液Aに被験化合物を100μMの濃度になる様
に添加したものを培養液Bとする。培養液AにL−グル
タミン酸を500μMの濃度になる様に添加したものを
培養液Cとする。培養液Aに被験化合物(必要量)およ
びL−グルタミン酸を500μMの濃度になる様に添加
したものを培養液Dとする。The culture solution prepared as described above is referred to as a culture solution A. Culture solution B is prepared by adding a test compound to culture solution A to a concentration of 100 μM. Culture solution C was prepared by adding L-glutamic acid to culture solution A to a concentration of 500 μM. Culture solution A is prepared by adding a test compound (required amount) and L-glutamic acid to culture solution A to a concentration of 500 μM.
【0033】3.効果測定試験 (被験化合物添加群)培養網膜神経細胞を培養液B中で
5%CO2 雰囲気下、37℃で10分間インキュベート
した後、培養液Bを培養液Dに交換し5%CO2 雰囲気
下、37℃で10分間インキュベートした。さらに、培
養液Dを培養液Bに交換し5%CO2雰囲気下、37℃
で60分間インキュベートした。取り出した細胞を1.
5%トリパンブルー溶液で染色し、10%中性ホルマリ
ン溶液にて固定した後、顕微鏡下で生細胞数ならびに死
細胞数を測定した。3. Effect measurement test (Test compound addition group) After incubating the cultured retinal nerve cells in the culture solution B for 10 minutes at 37 ° C. in a 5% CO 2 atmosphere, the culture solution B is exchanged for the culture solution D, and a 5% CO 2 atmosphere Incubated at 37 ° C for 10 minutes. Further, the culture solution D was replaced with the culture solution B, and the mixture was heated at 37 ° C. in a 5% CO 2 atmosphere.
For 60 minutes. 1. Remove the removed cells
After staining with a 5% trypan blue solution and fixing with a 10% neutral formalin solution, the number of live cells and the number of dead cells were measured under a microscope.
【0034】(コントロール群)培養網膜神経細胞を培
養液A中で5%CO2 雰囲気下、37℃で10分間イン
キュベートした後、新しい培養液Aに交換し5%CO2
雰囲気下、37℃で10分間インキュベートした。さら
に、この培養液を新しい培養液Aに交換し5%CO2 雰
囲気下、37℃で60分間インキュベートした後、被験
化合物添加群と同様にして生細胞数ならびに死細胞数を
測定した。(Control group) Cultured retinal nerve cells were incubated in culture medium A at 37 ° C. for 10 minutes in a 5% CO 2 atmosphere, and then replaced with a new culture medium A and replaced with 5% CO 2.
Incubated at 37 ° C. for 10 minutes under an atmosphere. Further, this culture solution was replaced with a new culture solution A and incubated at 37 ° C. for 60 minutes in a 5% CO 2 atmosphere. Then, the number of viable cells and the number of dead cells were measured in the same manner as in the test compound addition group.
【0035】(グルタミン酸処置群)培養網膜神経細胞
を培養液A中で5%CO2 雰囲気下、37℃で10分間
インキュベートした後、培養液Aを培養液Cに交換し5
%CO2 雰囲気下、37℃で10分間インキュベートし
た。さらに、培養液Cを培養液Aに交換し5%CO2雰
囲気下、37℃で60分間インキュベートした後、被験
化合物添加群と同様にして生細胞数ならびに死細胞数を
測定した。(Glutamate-treated group) Cultured retinal nerve cells were incubated in culture medium A at 37 ° C. for 10 minutes in a 5% CO 2 atmosphere, and then culture medium A was replaced with culture medium C.
Incubation was carried out at 37 ° C. for 10 minutes in a% CO 2 atmosphere. Further, the culture solution C was exchanged for the culture solution A, and the mixture was incubated at 37 ° C. for 60 minutes in a 5% CO 2 atmosphere.
【0036】4.結果 被験化合物の例として下記式[III]で表される1−
[2−3,4−(ジメトキシフェニル)エチル]−4−
(3−フェニルプロピル)ピペラジン・二塩酸塩(以
下、化合物Aとする)を用い実験を行った結果を表1に
示す。4. Results As an example of the test compound, 1- represented by the following formula [III]
[2-3,4- (dimethoxyphenyl) ethyl] -4-
Table 1 shows the results of experiments conducted using (3-phenylpropyl) piperazine dihydrochloride (hereinafter, referred to as compound A).
【0037】[0037]
【化5】 Embedded image
【0038】網膜神経細胞の生存率を下記式に従って算
出した。The survival rate of retinal nerve cells was calculated according to the following equation.
【0039】生存率(%)=[生細胞数/(生細胞数+
死細胞数)]×100Survival rate (%) = [number of living cells / (number of living cells +
Dead cells)] x 100
【表1】 [Table 1]
【0040】5.考察 網膜神経細胞への影響は細胞の生存率を指標として評価
した。5. Discussion The effect on retinal nerve cells was evaluated using cell viability as an index.
【0041】表1に示したように、コントロール群では
網膜神経細胞の生存率は90.4%であったのに対し
て、L−グルタミン酸を加え10分間処置することによ
りその生存率は41.3%(グルタミン酸処置群)とな
り、L−グルタミン酸は網膜神経細胞に顕著な障害を引
き起こしている。一方、化合物Aを添加すると網膜神経
細胞の生存率は用量依存的に上昇し、100μMの濃度
では81.5%にまで達し、網膜神経細胞の障害を明ら
かに抑制した。As shown in Table 1, the survival rate of retinal nerve cells was 90.4% in the control group, whereas the survival rate was 41.10% by adding L-glutamic acid and treating for 10 minutes. 3% (glutamic acid treated group), L-glutamic acid causes significant damage to retinal nerve cells. On the other hand, when Compound A was added, the survival rate of retinal nerve cells increased in a dose-dependent manner, reaching 81.5% at a concentration of 100 μM, and clearly inhibited retinal nerve cell damage.
【0042】上記の結果から、化合物Aがグルタミン酸
により誘発される網膜神経細胞障害に対して優れた保護
および治療作用を有していることが明らかとなった。From the above results, it has been clarified that Compound A has excellent protective and therapeutic effects on retinal nerve cell damage induced by glutamate.
【0043】[0043]
【発明の効果】以上のことから、1,4−(ジフェニル
アルキル)ピペラジン誘導体は網膜神経細胞障害に対し
て優れた保護および治療作用を有しており、眼疾患、特
に、糖尿病性網膜症、網膜血管閉塞症等の網膜疾患や緑
内障の予防または治療剤として有用であることが認めら
れた。As described above, the 1,4- (diphenylalkyl) piperazine derivative has an excellent protective and therapeutic effect on retinal nerve cell damage, and is useful for eye diseases, particularly diabetic retinopathy. It was found to be useful as an agent for preventing or treating retinal diseases such as retinal vascular occlusion and glaucoma.
Claims (9)
フェニルアルキル)ピペラジン誘導体またはその塩類を
有効成分とする眼疾患予防または治療剤。 【化1】 [式中、R1 は低級アルコキシ基を示す。R2 は低級ア
ルコキシ基を示す。Aは低級アルキレン基を示す。Bは
低級アルキレン基を示す。]1. A prophylactic or therapeutic agent for ocular diseases comprising a 1,4- (diphenylalkyl) piperazine derivative represented by the following general formula [I] or a salt thereof as an active ingredient. Embedded image [Wherein, R 1 represents a lower alkoxy group. R 2 represents a lower alkoxy group. A represents a lower alkylene group. B represents a lower alkylene group. ]
ある請求項1記載の眼疾患予防または治療剤。2. The preventive or therapeutic agent for ophthalmic diseases according to claim 1, wherein A is lower alkylene having 2 to 4 carbon atoms.
ある請求項1記載の眼疾患予防または治療剤。3. The method according to claim 1, wherein B is lower alkylene having 2 to 4 carbon atoms.
2 )2 −である請求項1記載の眼疾患予防または治療
剤。4. A is — (CH 2 ) 3 — and B is — (CH
2 ) The agent for preventing or treating eye diseases according to claim 1, which is 2- .
項1記載の眼疾患予防または治療剤。5. The preventive or therapeutic agent for ophthalmic diseases according to claim 1, wherein R 1 and R 2 are methoxy groups.
の塩類を有効成分とする眼疾患予防または治療剤。 【化2】 6. A prophylactic or therapeutic agent for eye diseases comprising a compound represented by the following formula [II] or a salt thereof as an active ingredient: Embedded image
載の眼疾患予防または治療剤。7. The preventive or therapeutic agent for an eye disease according to claim 1, wherein the eye disease is a retinal disease.
管閉塞症である請求項7記載の眼疾患予防または治療
剤。8. The preventive or therapeutic agent for an ocular disease according to claim 7, wherein the retinal disease is diabetic retinopathy or retinal vascular occlusion.
の眼疾患予防または治療剤。9. The preventive or therapeutic agent for an eye disease according to claim 1, wherein the eye disease is glaucoma.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP8277833A JPH10120569A (en) | 1996-10-21 | 1996-10-21 | Preventive and therapeutic agent for eye disease |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP8277833A JPH10120569A (en) | 1996-10-21 | 1996-10-21 | Preventive and therapeutic agent for eye disease |
Publications (1)
| Publication Number | Publication Date |
|---|---|
| JPH10120569A true JPH10120569A (en) | 1998-05-12 |
Family
ID=17588909
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP8277833A Pending JPH10120569A (en) | 1996-10-21 | 1996-10-21 | Preventive and therapeutic agent for eye disease |
Country Status (1)
| Country | Link |
|---|---|
| JP (1) | JPH10120569A (en) |
Cited By (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| US6492369B2 (en) | 1998-11-09 | 2002-12-10 | Santen Pharmaceutical Co., Ltd. | Therapeutic agents for drug dependence |
-
1996
- 1996-10-21 JP JP8277833A patent/JPH10120569A/en active Pending
Cited By (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| US6492369B2 (en) | 1998-11-09 | 2002-12-10 | Santen Pharmaceutical Co., Ltd. | Therapeutic agents for drug dependence |
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