CN105555268A - 阴离子性软隐形眼镜用眼科用组合物 - Google Patents
阴离子性软隐形眼镜用眼科用组合物 Download PDFInfo
- Publication number
- CN105555268A CN105555268A CN201480050791.7A CN201480050791A CN105555268A CN 105555268 A CN105555268 A CN 105555268A CN 201480050791 A CN201480050791 A CN 201480050791A CN 105555268 A CN105555268 A CN 105555268A
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- Prior art keywords
- anionic property
- scl
- pranoprofen
- salt
- ophthalmic composition
- Prior art date
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- 229960003101 pranoprofen Drugs 0.000 claims abstract description 86
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Classifications
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K31/00—Medicinal preparations containing organic active ingredients
- A61K31/33—Heterocyclic compounds
- A61K31/395—Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
- A61K31/435—Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with one nitrogen as the only ring hetero atom
- A61K31/4353—Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with one nitrogen as the only ring hetero atom ortho- or peri-condensed with heterocyclic ring systems
- A61K31/436—Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with one nitrogen as the only ring hetero atom ortho- or peri-condensed with heterocyclic ring systems the heterocyclic ring system containing a six-membered ring having oxygen as a ring hetero atom, e.g. rapamycin
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K31/00—Medicinal preparations containing organic active ingredients
- A61K31/185—Acids; Anhydrides, halides or salts thereof, e.g. sulfur acids, imidic, hydrazonic or hydroximic acids
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K31/00—Medicinal preparations containing organic active ingredients
- A61K31/21—Esters, e.g. nitroglycerine, selenocyanates
- A61K31/255—Esters, e.g. nitroglycerine, selenocyanates of sulfoxy acids or sulfur analogues thereof
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
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Abstract
本发明的目的是提供,在包含普拉洛芬和/或其盐的阴离子性SCL用眼科用组合物中,抑制普拉洛芬和/或其盐吸附至阴离子性SCL的技术。通过在包含普拉洛芬和/或其盐的阴离子性SCL用眼科用组合物中,含有牛磺酸和/或其盐,且将所述组合物的pH值设定为7.7以下,能够有效地抑制普拉洛芬和/或其盐吸附至阴离子性SCL。
Description
技术领域
本发明涉及能够抑制普拉洛芬和/或其盐吸附至阴离子性软隐形眼镜的阴离子性软隐形眼镜用眼科用组合物。此外,本发明涉及抑制普拉洛芬和/或其盐吸附至阴离子性软隐形眼镜的方法。
背景技术
近年来,开发了一次性、能够长期连续佩戴的软隐形眼镜(以下,有时简写为SCL),SCL佩戴者在增加。以往,作为SCL,开发了显示阴离子性、两性离子性、非离子性等各种表面特性的SCL,阴离子性SCL具有氧透过性优异、对角膜的负担少这样的优点,近年来被广泛使用。因此,为了提高阴离子性SCL佩戴者的便利性,要求能够在佩戴了阴离子性SCL的状态下使用的滴眼剂(阴离子性SCL用滴眼剂)。
对于SCL用滴眼剂,除了发挥所期望的药效以外,需要以不对SCL产生不良影响的方式进行制剂设计。特别是如果SCL用滴眼剂中的药物吸附于SCL,则导致眼镜的变形、使用感的降低等,进而有时变得不能对眼粘膜发挥所期望的药理效果,因此在SCL用滴眼剂的制剂设计上,抑制药物吸附至SCL成为特别重要的课题。此外,由于药物的吸附特性随着SCL的表面特性而变化,因此对于SCL用滴眼剂,需要与所应用的SCL的材料对应的制剂设计。
另一方面,普拉洛芬和/或其盐具有抑制成为炎症、疼痛的原因的前列腺素的生物合成的作用,在眼科领域中,以眼的充血、发痒等症状的缓和、睑缘炎、结膜炎、包括巩膜外层炎的巩膜炎、术后的炎症、前眼部葡萄膜炎等的预防或治疗为目的被广泛使用。关于包含普拉洛芬和/或其盐的SCL用滴眼剂的制剂技术,也有若干报道。例如,专利文献1中公开了含有维生素A类和牛磺酸的非离子性硅酮水凝胶隐形眼镜用眼科组合物能够抑制在非离子性硅酮水凝胶隐形眼镜表面的脂质吸附。然而,专利文献1中,没有研究关于普拉洛芬对SCL的吸附,而且没有公开可以适用于阴离子性SCL的技术。
此外,以往,也研究关于抑制药物对SCL的吸附的制剂技术。例如,专利文献2中公开了含有(A)选自具有仲氨基和/或叔氨基的胺及其盐的碱性药物、(B)选自氨基酸及其盐、酸性粘多糖及其盐以及环糊精中的1种或2种以上、且pH值为3.5~4.8的软隐形眼镜用组合物能够抑制碱性药物吸附至SCL。然而,在专利文献2中,没有形成任何关于抑制普拉洛芬吸附至阴离子性SCL的研究,而且必须将pH值设定为3.5~4.8,因此在制剂设计上的制约方面也存在问题。
现有技术文献
专利文献
专利文献1:日本特开2011-111425号公报
专利文献2:国际公开第2007/77783号
发明内容
发明所要解决的课题
以往,着眼于普拉洛芬和/或其盐,完全没有形成关于它们对阴离子性SCL的吸附特性的研究。在这样的状况下,本发明者确认了,与非离子性SCL相比,普拉洛芬和/或其盐对阴离子性SCL的吸附性高(参照后述的试验例1)。因此,为了将包含普拉洛芬和/或其盐的阴离子性SCL用眼科用组合物实用化,确立能够抑制普拉洛芬和/或其盐吸附至阴离子性SCL的制剂技术成为当务之急。
因此,本发明的目的在于,提供在包含普拉洛芬和/或其盐的阴离子性SCL用眼科用组合物中,抑制普拉洛芬和/或其盐吸附至阴离子性SCL的吸附的技术。
用于解决课题的方法
本发明者为了解决前述课题而进行了深入研究,结果发现,通过在包含普拉洛芬和/或其盐的阴离子性SCL用眼科用组合物中,使其含有牛磺酸和/或其盐、且将pH值设定为7.7以下,能够有效地抑制普拉洛芬和/或其盐吸附至阴离子性SCL。还发现,通过在前述阴离子性SCL用眼科用组合物中将pH值设定为5.5以上,能够实现澄清的外观性状。本发明是基于前述见解、进一步通过反复研究而完成的。
即,本发明提供下述公开的形式的发明。
项1.一种阴离子性软隐形眼镜用眼科用组合物,其特征在于,含有普拉洛芬和/或其可药用的盐、以及牛磺酸和/或其可药用的盐,且所述组合物的pH值为7.7以下。
项2.根据项1所述的阴离子性软隐形眼镜用眼科用组合物,pH值为5.5~7.7。
项3.根据项1或2所述的阴离子性软隐形眼镜用眼科用组合物,含有0.01~3w/v%的牛磺酸和/或其可药用的盐。
项4.根据项1~3中任一项所述的阴离子性软隐形眼镜用眼科用组合物,含有0.001~0.5w/v%的普拉洛芬和/或其可药用的盐。
项5.根据项1~4中任一项所述的阴离子性软隐形眼镜用眼科用组合物,是阴离子性软隐形眼镜用滴眼剂。
项6.一种抑制普拉洛芬和/或其可药用的盐吸附至阴离子性软隐形眼镜的方法,其特征在于,在包含普拉洛芬和/或其可药用的盐的阴离子性软隐形眼镜用眼科用组合物中,配合牛磺酸和/或其可药用的盐,且将pH值调节为7.7以下。
项7.下述液体制剂在阴离子性软隐形眼镜用眼科用组合物的制造中的应用,所述液体制剂含有普拉洛芬和/或其可药用的盐、以及牛磺酸和/或其可药用的盐,且所述液体制剂的pH值为7.7以下。
项8.一种抑制普拉洛芬和/或其可药用的盐吸附至阴离子性软隐形眼镜的方法,包含使下述液体制剂接触阴离子性软隐形眼镜的工序,所述液体制剂含有普拉洛芬和/或其可药用的盐、以及牛磺酸和/或其可药用的盐,且所述液体制剂pH值为7.7以下。
发明的效果
通过本发明的阴离子性SCL用眼科用组合物,能够抑制普拉洛芬和/或其盐吸附至阴离子性SCL,因此能够在不对阴离子性SCL产生不良影响的条件下有效地发挥普拉洛芬和/或其盐的药效。此外,通过本发明的阴离子性SCL用眼科用组合物,牛磺酸和/或其盐不仅发挥普拉洛芬和/或其盐对阴离子性SCL的吸附抑制作用,还发挥眼的新陈代谢促进作用,因此还能够联合普拉洛芬和/或其盐的药效,起到优异的眼病预防、恢复效果。
此外,通过将本发明的阴离子性SCL用眼科用组合物中的pH值设定为5.5以上,能够抑制普拉洛芬和/或其盐引起的白浊,能够提供呈现澄清的外观性状的阴离子性SCL用眼科用组合物。另外,在本说明书中,所谓“澄清”,是指没有因普拉洛芬和/或其盐而产生白浊的状态,不限于无色澄清,还包含由于其他含有成分而呈现颜色的有色澄清的概念。
具体实施方式
1.阴离子性SCL用眼科用组合物
本发明的阴离子性SCL用眼科用组合物的特征在于,含有普拉洛芬和/或其可药用的盐、以及牛磺酸和/或其可药用的盐,且所述组合物的pH值为7.7以下。以下对本发明的阴离子性SCL用眼科用组合物进行详述。另外,在本说明书中,所谓“阴离子性SCL用眼科用组合物”,表示在眼科领域中,以与阴离子性SCL接触的方式使用的组合物。此外,在本说明书中,各成分的浓度的单位“w/v%”表示质量对体积的百分率,与g/100mL含义相同。
本发明的阴离子性SCL用眼科用组合物含有普拉洛芬和/或其盐。所谓普拉洛芬,也称为α-甲基-5H-[1]苯并吡喃并[2,3-b]吡啶-7-乙酸,是在眼科领域中已知具有消炎作用的公知的化合物。
作为普拉洛芬的盐,作为可药用的限度,没有特别限制,可举出例如,钠盐、钾盐、钙盐、镁盐、铝盐等金属盐;三乙胺盐、二乙胺盐、吗啉盐、哌嗪盐等有机碱盐等。这些普拉洛芬的盐可以单独使用1种,此外也可以组合2种以上使用。
在本发明的阴离子性SCL用眼科用组合物中,可以从普拉洛芬及其盐中选择1种而单独使用,也可以组合2种以上来使用。普拉洛芬及其盐中,优选可举出普拉洛芬。
在本发明的阴离子性SCL用眼科用组合物中,普拉洛芬和/或其盐的浓度根据该阴离子性SCL用眼科用组合物的用途等进行适当设定,可举出例如,0.001~0.5w/v%,优选为0.01~0.2w/v%,更优选为0.01~0.1w/v%。
本发明的阴离子性SCL用眼科用组合物还含有牛磺酸和/或其盐。对于本发明的阴离子性SCL用眼科用组合物,通过使牛磺酸和/或其盐与前述普拉洛芬和/或其盐一起共存,能够抑制普拉洛芬和/或其盐吸附至阴离子性SCL。
牛磺酸也称为氨基乙基磺酸,化学名称为2-氨基乙磺酸。在眼科领域中,是也以促进眼的新陈代谢为目的等使用的公知的化合物。
作为牛磺酸的盐,作为可药用的限度,没有特别限制,可举出例如,钠盐、钾盐等碱金属盐等。这些牛磺酸的盐可以单独使用1种,此外也可以组合2种以上使用。
在本发明的阴离子性SCL用眼科用组合物中,可以从牛磺酸及其盐中选择1种单独使用,也可以组合2种以上使用。牛磺酸及其盐中,优选可举出牛磺酸。
在本发明的阴离子性SCL用眼科用组合物中,关于牛磺酸和/或其盐的浓度,可举出例如,0.01~3w/v%。特别是从更进一步有效地抑制普拉洛芬和/或其盐吸附至阴离子性SCL的观点出发,作为牛磺酸和/或其盐的浓度,可举出优选为0.1~3w/v%,更优选为0.1~1w/v%。
本发明的阴离子性SCL用眼科用组合物的pH值设定为7.7以下。本发明的阴离子性SCL用眼科用组合物中,通过使牛磺酸和/或其盐与前述普拉洛芬和/或其盐一起共存,且设定为这样的pH值范围,能够抑制普拉洛芬和/或其盐吸附至阴离子性SCL。
此外,如后述的试验例所示,在包含普拉洛芬和/或其盐的组合物中,确认了:如果pH值为4.5以下,则产生普拉洛芬和/或其盐引起的白浊;如果将pH值设定为5.5以上,则呈现澄清的外观性状。鉴于这一方面,作为本发明的阴离子性SCL用眼科用组合物的pH值,从在更进一步有效地抑制普拉洛芬和/或其盐吸附至阴离子性SCL的同时具备澄清的外观性状的观点出发,可优选举出5.5~7.7,更优选为6.5~7.7,进一步优选为6.5~7.4,最优选为6.5~7.0。
为了将本发明的阴离子性SCL用眼科用组合物的pH值调节到前述范围,只要在眼科用组合物中使用通常使用的pH调节剂、缓冲剂即可。作为pH调节剂,可举出例如,氢氧化钠、氢氧化钾等碱;乙酸、柠檬酸、盐酸、磷酸、酒石酸等酸。这些pH调节剂可以单独使用1种,此外可以组合2种以上来使用。此外,作为缓冲剂,可举出例如,磷酸缓冲剂、硼酸缓冲剂、柠檬酸缓冲剂、酒石酸缓冲剂、乙酸缓冲剂、氨基酸、氨丁三醇等。这些缓冲剂可以单独使用1种,此外可以组合2种以上来使用。
本发明的阴离子性SCL用眼科用组合物中,除了前述成分以外,可以根据需要含有普拉洛芬和/或其盐以外的药理成分。作为这样的药理成分,可举出例如,甘草酸二钾、尿囊素、ε-氨基己酸、溴芬酸、酮咯酸氨丁三醇、奈帕芬胺、盐酸小檗碱、硫酸小檗碱、薁磺酸钠、硫酸锌、乳酸锌、盐酸溶菌酶等消炎剂;马来酸氯苯那敏、盐酸苯海拉明等抗组胺剂;色甘酸钠、酮替芬富马酸盐、阿扎司特、氨来呫诺、吡嘧司特钾、曲尼司特、异丁司特等抗变态反应剂;诺氟沙星、氧氟沙星、洛美沙星、左氧氟沙星、庆大霉素、加替沙星等抗菌剂;抗坏血酸、黄素腺嘌呤二核苷酸钠、氰钴胺素、盐酸吡哆素、生育酚乙酸酯、视黄醇乙酸酯、视黄醇棕榈酸酯、泛醇、泛酸钙、泛酸钠等维生素类;天冬氨酸、硫酸软骨素钠等氨基酸类,新斯的明甲基硫酸盐等抗胆碱酯酶剂;萘甲唑啉、四氢唑啉、肾上腺素、麻黄碱、去氧肾上腺素、dl-甲基麻黄碱等血管收缩剂;透明质酸钠等角膜结膜上皮障碍治疗药;磺胺嘧啶、磺胺异唑、磺胺索嘧啶、磺胺二甲氧哒嗪、磺胺甲氧哒嗪、磺胺甲唑、磺胺乙二唑、磺胺托嘧啶、磺胺苯吡唑、磺胺脒、酞磺胺噻唑、琥珀磺胺噻唑等磺胺剂等。这里示例的化合物,作为可药用的限度,可以是盐的形态,此外也可以是其他的盐的形态。这些药理成分可以单独使用1种,此外也可以组合2种以上来使用。
关于这些药理成分的浓度,可以根据药理成分的种类、阴离子性SCL用眼科用组合物的用途等进行适当设定。
此外,本发明的阴离子性SCL用眼科用组合物中,除了前述成分以外,还可以根据需要含有等张剂、助溶剂、粘稠剂、螯合剂、清凉剂、防腐剂、稳定剂、表面活性剂等添加剂。
作为等张剂,可举出山梨糖醇、葡萄糖、甘露糖醇等糖类;甘油、丙二醇等多元醇类;氯化钠等盐类;硼酸等。这些等张剂可以单独使用1种,此外也可以组合2种以上来使用。
作为助溶剂,可举出例如,聚氧乙烯失水山梨糖醇单油酸酯、聚氧乙烯硬化蓖麻油、泰洛沙泊、普朗尼克(Pluronic)等非离子性表面活性剂;甘油、聚乙二醇(macrogol)等多元醇等。这些助溶剂可以单独使用1种,此外也可以组合2种以上来使用。
作为粘稠剂,可举出例如,聚乙烯基吡咯烷酮、聚乙二醇、聚乙烯醇、羧基乙烯基聚合物、黄原胶、硫酸软骨素钠、透明质酸钠等水溶性高分子;羟丙甲纤维素、羟乙基纤维素、甲基纤维素、羟丙基纤维素、羟丙基甲基纤维素、羧甲基纤维素钠等纤维素类等。这些粘稠剂可以单独使用1种,此外也可以组合2种以上来使用。
作为螯合剂,可举出例如,乙二胺四乙酸盐、柠檬酸或其盐等。这些螯合剂可以单独使用1种,此外也可以组合2种以上来使用。
作为清凉剂,可举出例如,l-薄荷醇、冰片、樟脑、桉树油等。这些清凉剂可以单独使用1种,此外也可以组合2种以上来使用。
作为防腐剂,可举出例如,山梨酸或其盐、苯甲酸或其盐、对羟基苯甲酸甲酯、对羟基苯甲酸乙酯、对羟基苯甲酸丙酯、氯丁醇、氯己定葡糖酸盐、硼酸、脱氢乙酸或其盐、苯扎氯铵、苄索氯铵、苯甲醇、氯化锌、对氯间二甲苯酚、氯甲酚、苯乙醇、泊利氯铵、硫柳汞、二丁基羟基甲苯等。这些防腐剂可以单独使用1种,此外也可以组合2种以上来使用。
作为稳定剂,可举出例如,聚乙烯基吡咯烷酮、亚硫酸盐、单乙醇胺、甘油、丙二醇、环糊精、葡聚糖、抗坏血酸、乙二胺四乙酸盐、生育酚、二丁基羟基甲苯等。这些稳定剂可以单独使用1种,此外也可以组合2种以上来使用。
作为表面活性剂,可举出例如,泰洛沙泊、聚氧乙烯硬化蓖麻油、聚氧乙烯聚氧丙烯嵌段共聚物、聚氧乙烯失水山梨糖醇脂肪酸酯、辛苯昔醇(octoxynol)等非离子性表面活性剂;烷基二氨基乙基甘氨酸、月桂基二甲基氨基乙酸甜菜碱等两性表面活性剂;烷基硫酸盐、N-酰基牛磺酸盐、聚氧乙烯烷基醚磷酸盐、聚氧乙烯烷基醚硫酸盐等阴离子表面活性剂;烷基吡啶盐、烷基胺盐等阳离子表面活性剂等。这些表面活性剂可以单独使用1种,此外也可以组合2种以上来使用。
关于这些添加剂的浓度,可以根据添加剂的种类、阴离子性SCL用眼科用组合物的用途等进行适当设定。
关于本发明的阴离子性SCL用眼科用组合物的制剂形态,只要是包含水作为基剂的液体制剂即可,例如可以是水溶液状、乳液状等中的任一种,但是优选可举出水溶液状。
对于本发明的阴离子性SCL用眼科用组合物,只要根据其用途,按照自身公知的调制法制造即可,例如,可以使用第十六版改正日本药典制剂总则中记载的方法来制造。
本发明的阴离子性SCL用眼科用组合物以如下形式使用:即使在阴离子性SCL佩戴中也能够滴眼的滴眼剂(阴离子性SCL用滴眼剂);即使在阴离子性SCL佩戴中也能够洗眼的洗眼剂(阴离子性SCL用洗眼剂);阴离子性SCL用佩戴液、阴离子性SCL用多功能护理液、阴离子性SCL用洗涤液、阴离子性SCL用保存液等隐形眼镜护理用品等。其中,可优选举出阴离子性SCL用滴眼剂、阴离子性SCL用洗眼剂,更优选阴离子性SCL用滴眼剂。
成为本发明的适用对象的阴离子性SCL,是将含有包含阴离子性基团的单体的聚合物作为构成材料的SCL。作为阴离子性SCL,可举出例如,将包含羧基、磺酸基、磷酸基等阴离子性基团的聚合物作为构成材料的SCL,更具体而言,可举出etafilconA、vifilconA、ocufilconD、methafilconA等材料的SCL。关于阴离子性SCL的材料,制法是公知的。
此外,成为本发明的适用对象的阴离子性SCL可以是高含水率的或低含水率的,可优选举出高含水率、即美国食品药品局(FDA)中分类为组IV(离子性单体1摩尔%以上,含水率50%以上)的SCL。
2.抑制普拉洛芬和/或其盐吸附至阴离子性SCL的方法(1)
此外,本发明提供抑制普拉洛芬和/或其盐吸附至阴离子性SCL的方法,其特征在于,在包含普拉洛芬和/或其可药用的盐的阴离子性SCL用眼科用组合物中配合牛磺酸和/或其可药用的盐,且将所述组合物的pH值调节为7.7以下。该吸附抑制方法在对阴离子性SCL用眼科用组合物赋予抑制普拉洛芬和/或其盐吸附至阴离子性SCL的作用方面是有用的。
在本发明的吸附抑制方法中,关于所使用的普拉洛芬和/或其可药用的盐的种类、浓度、牛磺酸和/或其可药用的盐的种类、浓度、阴离子性SCL用眼科用组合物的pH值、阴离子性SCL用眼科用组合物中所配合的药理成分、添加剂的种类、阴离子性SCL用眼科用组合物的制剂形态、用途、成为适用对象的阴离子性SCL的种类等,如前述“1.阴离子性SCL用眼科用组合物”栏中记载的那样。
3.抑制普拉洛芬和/或其盐吸附至阴离子性SCL的方法(2)
此外,本发明提供抑制普拉洛芬和/或其盐吸附至阴离子性SCL的方法,包含使下述液体制剂接触阴离子性SCL的工序,所述液体制剂含有普拉洛芬和/或其可药用的盐、以及牛磺酸和/或其可药用的盐,且所述液体制剂的pH值为7.7以下。
在本发明的吸附抑制方法中,关于所使用的普拉洛芬和/或其可药用的盐的种类、浓度、牛磺酸和/或其可药用的盐的种类、浓度、液体制剂的pH值、液体制剂中所配合的药理成分、添加剂的种类、液体制剂的制剂形态、用途、成为适用对象的阴离子性SCL的种类等,如前述“1.阴离子性SCL用眼科用组合物”栏中记载的那样。此外,在本发明的吸附抑制方法中,使前述液体制剂接触阴离子性SCL的方法只要根据该液体制剂的用途进行适当设定即可。例如,如果在前述液体制剂是滴眼剂的情况下,只要对佩戴了阴离子性SCL的眼滴加前述液体制剂即可。
实施例
以下举出实施例对本发明进行具体地说明,但是本发明不受这些任何限定。
试验例1
通过将表1所示的各成分用常法混合,来调制试验液。通过观察所得的各试验液的外观,并且测定浊度(660nm下的吸光度)来评价白浊的有无。
此外,将各试验液3mL放入小瓶中,在其中浸渍SCL1片,在25℃下振荡2小时以上。此外,将各试验液3mL放入小瓶中在不浸渍SCL的状态下,在25℃下振荡2小时以上。通过液相色谱测定振荡后各试验液中的普拉洛芬含量,按照下述式,算出普拉洛芬对SCL的吸附量。另外,如果在试验液中浸渍SCL的条件下进行振荡,则2小时以内普拉洛芬对SCL的吸附达到平衡状态,因此如果将振荡时间设定为2小时以上,则可以确认对普拉洛芬对SCL的吸附量的测定值无影响。
吸附于1片SCL的普拉洛芬量(μg)=(CC-CT)×V
CC:未浸渍SCL的试验液中的普拉洛芬含量(μg/mL)
CT:浸渍了SCL的试验液中的普拉洛芬含量(μg/mL)
V:试验中使用的试验液的量(mL)
另外,在本试验中,使用下述2种SCL,求出普拉洛芬在各SCL上的吸附量。
眼镜1:组IV、商品名“ワンデーアキュビュー(注册商标)”(ジョンソンエンドジョンソン株式会社制)、阴离子性、USAN名:etafilconA
眼镜2:硅酮水凝胶隐形眼镜、组I、商品名“エアオプティクス2ウィーク(注册商标)”(チバビジョン株式会社制)、USAN名:lotrafilconB
将所得结果示于表1。如比较例5的结果表明那样,确认了阴离子性SCL中普拉洛芬的吸附量多于非离子性硅酮水凝胶隐形眼镜。另一方面,在含有普拉洛芬和牛磺酸、且pH值为7.7以下的试验液(实施例1~3)中,可以显著地抑制普拉洛芬吸附至阴离子性SCL。与此相对,在pH值为8.0以上、且含有普拉洛芬和牛磺酸的试验液(比较例2和4)中,与不含有牛磺酸的情况相比,不仅不能抑制普拉洛芬吸附至阴离子性SCL,反而促进了普拉洛芬吸附至阴离子性SCL。以上的结果表明,通过与普拉洛芬一起含有牛磺酸和/或其盐、且pH值设定为7.7以下,可以抑制普拉洛芬吸附至阴离子性SCL。此外,在全部pH值为5.5以上的试验液中,显示未观察到白浊的澄清的外观性状。
[表1]
试验例2
通过将表2和表3所示的各成分用常法混合,来调制试验液。通过观察所得的各试验液的外观,并且测定浊度(660nm下的吸光度)来评价白浊的有无。此外,对于所得的各试验液,通过与前述试验例1同样的方法,测定普拉洛芬对阴离子性SCL的吸附量。
将所得的结果示于表2和表3。该结果确认了,通过在pH值5.5~7.7中,组合含有普拉洛芬和各种浓度的牛磺酸,可以抑制普拉洛芬吸附至阴离子性SCL。此外,在pH值5.5~7.7的全部的试验液中,显示未观察到白浊的澄清的外观性状。
[表2]
[表3]
试验例3
通过将表4所示的各成分用常法混合,来调制试验液。通过观察所得的各试验液的外观,并且测定浊度(660nm下的吸光度)来评价白浊的有无。
将所得结果示于表4。如表4表明那样,在pH值为4.5以下的情况下,在任一种包含普拉洛芬的试验液中,观察到白浊。根据上述试验例1和2的结果,明确了,通过与普拉洛芬一起含有牛磺酸和/或其盐、且将pH值设定为5.5以上,能够在呈现澄清的外观性状的同时抑制普拉洛芬吸附至阴离子性SCL。
[表4]
表中,各配合成分的配合量的单位是“w/v%”。
Claims (8)
1.一种阴离子性软隐形眼镜用眼科用组合物,其特征在于,含有普拉洛芬和/或其可药用的盐、以及牛磺酸和/或其可药用的盐,且所述组合物的pH值为7.7以下。
2.根据权利要求1所述的阴离子性软隐形眼镜用眼科用组合物,pH值为5.5~7.7。
3.根据权利要求1或2所述的阴离子性软隐形眼镜用眼科用组合物,含有0.01~3w/v%的牛磺酸和/或其可药用的盐。
4.根据权利要求1~3中任一项所述的阴离子性软隐形眼镜用眼科用组合物,含有0.001~0.5w/v%的普拉洛芬和/或其可药用的盐。
5.根据权利要求1~4中任一项所述的阴离子性软隐形眼镜用眼科用组合物,是阴离子性软隐形眼镜用滴眼剂。
6.一种抑制普拉洛芬和/或其可药用的盐吸附至阴离子性软隐形眼镜的方法,其特征在于,在含有普拉洛芬和/或其可药用的盐的阴离子性软隐形眼镜用眼科用组合物中,配合牛磺酸和/或其可药用的盐,且将pH值调节为7.7以下。
7.下述液体制剂在阴离子性软隐形眼镜用眼科用组合物的制造中的应用,所述液体制剂含有普拉洛芬和/或其可药用的盐、以及牛磺酸和/或其可药用的盐,且所述液体制剂的pH值为7.7以下。
8.一种抑制普拉洛芬和/或其可药用的盐吸附至阴离子性软隐形眼镜的方法,包含使下述液体制剂接触阴离子性软隐形眼镜的工序,所述液体制剂含有普拉洛芬和/或其可药用的盐、以及牛磺酸和/或其可药用的盐,且所述液体制剂的pH值为7.7以下。
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| JP2010143882A (ja) * | 2008-12-19 | 2010-07-01 | Rohto Pharmaceut Co Ltd | シリコーンハイドロゲルコンタクトレンズ用点眼剤 |
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