CN1313753A - 皮肤与组织护理和/或治疗制剂 - Google Patents
皮肤与组织护理和/或治疗制剂 Download PDFInfo
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- CN1313753A CN1313753A CN99809842A CN99809842A CN1313753A CN 1313753 A CN1313753 A CN 1313753A CN 99809842 A CN99809842 A CN 99809842A CN 99809842 A CN99809842 A CN 99809842A CN 1313753 A CN1313753 A CN 1313753A
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Abstract
本发明涉及皮肤与组织护理和/或治疗制剂。确切地说,本发明涉及用于组织损害表现及后果的护理、保护和预防和用于皮肤与组织的治疗的制剂,其中所述制剂包含至少一种选自碱金属盐和碱土金属盐和其它矿物质的盐,其特征在于它含有至少一种氨基酸和氧化锌和/或无机过氧化物。任选地,本发明制剂可以另外含有收敛剂、粘结与粘合剂、湿润剂、精油、tego-甜菜碱、辅助性植物物质(例如表儿茶素)、不饱和脂肪酸、脂质体、维生素、微量元素和抗真菌和/或抗微生物组分。
Description
本发明涉及皮肤与组织护理和/或治疗制剂。本发明尤其涉及用于组织损害表现及后果的护理、保护和预防和用于皮肤与组织的治疗的制剂,其中所述制剂包含至少一种选自碱金属盐、碱土金属盐和其它矿物质的盐,其特征在于它含有至少一种氨基酸和氧化锌和/或无机过氧化物,优选为过氧化镁或过氧化钠。任选地,本发明制剂可以另外含有收敛剂、粘结与粘合剂、湿润剂、精油、tego(含苯酚-甲醛树脂牛皮纸)-甜菜碱、辅助性植物物质(例如表儿茶素)、不饱和脂肪酸、脂质体、维生素、微量元素和抗真菌和/或抗微生物组分。
天然养分是细胞和机体的健康所必需的。它们能够供养和再生皮肤,以及促进细胞的代谢和供氧。养分供应的广泛意义在皮肤护理、美容和皮肤医学领域中也变得越来越重要。激素水平改变、素质、不均衡与不正当的饮食和不健康的习惯(尤其是吸烟和缺乏锻炼)会引起典型的皮肤表现,例如组织改变、组织变形和细胞代谢障碍。有目的的养分供应可协调代谢,因此带来自然的细胞生理平衡。
众所周知,维生素、矿物质和微量元素是皮肤养分供应所不可缺少的。由氨基酸构成的蛋白质是细胞和内源性活性物质(例如酶和某些激素)的重要组成部分。对健康和功效来说,多不饱和脂肪酸、辅助性植物物质(例如类黄酮和表儿茶素)和脂质体一般变得越来越重要。维生素、矿物质和微量元素、多不饱和脂肪酸和生物活性植物物质(例如类黄酮)是必需的代谢调节剂和皮肤健康的保护性养分。
维生素是必需的营养成分,对异养生物的正常功能来说,必须得到供应,或多或少地带有强制性,相当于必需品,因为它们只能从外部来源或在环境(millieu)因素(例如肠内菌丛)的影响下获得。它们的特殊的生物催化作用是以代替进行代谢消耗的酶的活性基团为基础的。从科学角度来说,已知例如B族维生素在中间代谢中起到辅酶的作用,维生素C、E和β-胡萝卜素主要起抗氧化剂的作用。由不充分的供应或吸收、肠内菌丛紊乱或代谢紊乱、抗维生素作用或消耗增加所导致的缺乏会引起维生素缺少和维生素缺乏。
此外,矿物质和微量元素是必需的代谢调节剂。锌、镁和B族维生素是高性能的元素,因为它们可激活酶,因此可进行碳水化合物、脂肪和蛋白质物质的代谢。硅对皮肤的稳定性和养护具有有利作用。此外,科学上无可争辩的是,锌对免疫系统和皮肤代谢具有必需的功能。
多不饱和脂肪酸含有亚油酸和α-与γ-亚麻酸,它们在代谢中是生物活性调节剂(例如二十碳化合物和前列腺素)的重要起始物质,确保代谢中的健康平衡。目前,二十碳化合物和前列腺素也称为组织激素,它们对健康的稳定作用受到科学家们的广泛关注。多不饱和脂肪酸对健康皮肤功能以及炎症过程的有利影响是已知的。此外,还已知ω-3-脂肪酸(二十碳五烯酸、α-亚麻酸)和ω-6-脂肪酸(亚油酸,γ-亚麻酸)类型的多不饱和脂肪酸对神经性皮炎和牛皮癣以及负荷诱发的再生过程具有有利作用。所谓的辅助性植物物质(在专业科学中也称为生物活性植物物质)对健康的重要性现在也受到关注。生物类黄酮有效地支持维生素C关于耐受力、血管壁和结缔组织的作用,也算在这些天然植物物质中。此外,还已知生物类黄酮具有抗氧化剂的性质,因此它们协同补充维生素C、E和β-胡萝卜素的作用。
关于生物合成方面,氨基酸分为必需的、半必需的和非必需的氨基酸。除了作为蛋白质的组成部分以外,氨基酸还是生物学上有效化合物的前体。氨基酸例如参见L.Stryer,生物化学(Biochemie),Spektrum Akademischer Verlag,Oxford,1994和吕姆普化学百科全书(Roempp Lexikon Chemie),editor J.Falbe,M.Regitz,关键词“氨基酸”,Thieme Verlag,1996以及引用在这里的参考文献。
脂质体是被单层或多层磷脂双膜所包围的粒子,在内部含水相中可以加载亲水性药物分子。利用它们作为药物载体,可以实现活性物质的选择性局部富集和活性物质的延迟释放。
商业上可得到大量用于治疗和预防霉菌的、微生物的、病理的和其它组织损害表现及后果、组织改变、组织变形和细胞代谢障碍以及对人组织造成的其它形式损害的制剂。例如各种治疗皮肤和结缔组织问题的治疗手段。不过,很多这些制剂的成功是不可靠的,因为这些制剂不能到达受损害的细胞和/或作用于受损害的细胞。此外,很多商业上可得到的产品没有采取科学家们所发现的活性机理,在该机理中以天然方式为细胞补充矿物质,并刺激代谢以重新建立细胞的天然内部压力,使细胞体积正常化,并持续地转移和分泌脂质和废物。
DE-OS-19622708描述了用于局部和肠胃外体内用药的植物生物学制剂,用于预防、护理和治疗各种病理后果和其它内源性与外源性后果、改变和疾病,以及用于维持、恢复和重新建立动物和人器官和软组织中的内环境稳定,其特征在于它含有下列组分:
(a)一种或多种含有离子的组分和矿物盐,
(b)一种或多种收敛组分、一种或多种粘结剂、湿润剂和一种或多种精油,和
(c)可选的一种或多种植物提取物、胶凝剂、酸结合剂、透明质酸酶或其它适当组分,含量在0.01与20%之间。该制剂任选地含有金盏花、金缕梅或其它顺势医疗组分、氨基酸、酶、维生素、电解质、染剂、蜡、乳化剂、淀粉、凡士林、石蜡、油、酸、脂肪、植物混合物与提取物、尿素、硫酸盐化合物等。该专利申请既没有公开氨基酸的例子,也没有在实施例中使用氨基酸。
本发明的目的是提供皮肤与组织的护理和/或治疗制剂,该制剂的突出之处在于快速的作用、优异的耐受性、广泛的应用范围和特别强的深度作用。特别是该制剂应可用于组织损害表现及后果的护理、保护、预防和用于皮肤与组织的治疗。根据本发明的制剂应采取这样的研究成果,离子通过离子通道扩散进入细胞内空间,并改善细胞内的微循环。
通过提供包含下列组分的组合物以达到本发明的目的:
(a)至少一种选自碱金属盐与碱土金属盐和其它矿物质的盐,
其特征在于它含有
(b)至少一种氨基酸,和
(c)氧化锌和/或无机过氧化物。
优选地,组合物的组分(c)采用氧化锌、过氧化镁或过氧化钠。
在优选的实施方式中,本发明制剂可以在每种情况下彼此独立地另外包含至少一种收敛剂、湿润剂、精油、tego-甜菜碱、辅助性植物物质(例如类黄酮和表儿茶素)、不饱和脂肪酸、脂质体、维生素、微量元素和抗真菌与抗微生物组分。此外,还可以包含常用的载体和助剂以及粘结与粘合剂和常用的溶剂。在优选的实施方式中,本发明制剂是通过直接在作用部位上用药加以局部使用的。
本发明制剂采取这样的新的研究成果,离子通过离子通道扩散进入细胞内空间。据此,矿物盐离子穿透皮肤上层,深入皮下组织、结缔组织和脂肪细胞的细胞内部。本发明制剂尤其采用这样的原理,利用由制剂活性物质的组合所产生的高渗透压,在细胞内部与细胞外部之间进行离子交换。不过在该过程中,氨基酸扮演了重要角色,它们帮助离子更有效地克服细胞膜的天然屏障以到达细胞内部的实际作用部位。
即使细胞关于离子活性的功能受到限制,本发明组合物仍然是特别有效的。特别是当离子活性受到限制时,氨基酸充当额外的物质载体,该物质的渗入是细胞内活性所必须的,目的是在此发挥功能。已经发现,与盐的使用相比,氨基酸与氧化锌和/或无机过氧化物的组合改善细胞内微循环。这种改善作用是可以观察和生物测量到的。如果仅使用盐,那么细胞内微循环的增加在约1.5小时后突然降回至原始值。当使用包含氨基酸与氧化锌和/或无机过氧化物的组合的组合物时,与盐的使用相比,微循环的改善作用更强、更连续、持续时间更长,并缓慢地接近原始值。这使物质更好地渗入细胞,更好地在细胞内分布,由此增加了协同效应。
此外,与单独的盐形成对照,盐与氨基酸的组合对皮肤生理机能具有更积极的作用。特别是影响皮肤的保湿因子、pH值和sebometry。当盐与氨基酸结合使用时,盐比没有氨基酸时更有效地渗入细胞,因为氨基酸在一方面是细胞膜的钥匙,另一方面支持和提高离子通道的活化作用。
碱金属盐和碱土金属盐和其它矿物质是代谢所必需的调节剂。本发明中,可以使用所有已知的碱金属盐和碱土金属盐和其它矿物质,它们也可以是微量元素。可以用在本发明中的碱金属盐和碱土金属盐和矿物质的优选代表是钠、钾、镁、钙、硅、锌、锰、铜、铁、氟、氯、溴、碘和磷。优选的微量元素是偶然的微量元素,例如银、金、铝、钡、铋、镉、铬、镍、铅、锡、钛和钒,和必需的微量元素,例如铬、钴、铜、氟、铁、碘、锰、钼和硒,它们例如以酶、色蛋白和激素成分的形式存在。本发明制剂中碱金属盐和碱土金属盐和其它矿物质的量优选为10至90重量百分率,更优选为20至85重量百分率,具体在可局部用药的制剂中,优选为10至30重量百分率,更优选为10至25重量百分率,以制剂中全部组分的总和计,因所需的渗透效果而异。碱金属盐和碱土金属盐和其它矿物质以常用的盐化合物或有机化合物的形式加入。例如,钠、钾和镁优选以它们的氯化物盐的形式加入,钠和钙优选以磷酸盐的形式加入。
任选地用在本发明中的收敛剂包含为此常用的化合物。优选用作收敛剂的是单宁、金缕梅、大黄、拉坦尼(Ratanhia)和鼠尾草。本发明中收敛剂的量优选为0至30重量百分率,更优选为1至25重量百分率,以制剂中全部组分的总和计。收敛剂优选以纯的形式加入。
本发明中,可以任选地使用常用的湿润剂。优选的湿润剂是甘油、芦荟、胶原、脱酰胺胶原、胶原水解物、弹性蛋白水解物、玻璃粘液溶液(Hyalomuccoloesung)、纤维刺激素、PN73、Q10、水、翠叶芦荟胶、茶提取物、常春藤提取物(Hedera Helix)、母菊(春黄菊)油和丁二醇。本发明制剂中湿润剂的量优选为0至70重量百分率,更优选为5至50重量百分率,以制剂中全部组分的总和计。
此外,本发明制剂可以任选地包含常用的精油。优选的精油是春黄菊、熏衣草、迷迭香、樟脑、山松、薄荷、茶树和桉树的油。本发明制剂中精油的量优选为0至70重量百分率,更优选为3至50重量百分率,以制剂中全部组分的总和计。精油优选以纯的形式或提取物的形式或冷榨和热榨油的形式加入。
本发明制剂可以含有所有已知的氨基酸和氨基酸衍生物。优选的氨基酸和氨基酸衍生物是丙氨酸、苯丙氨酸、半胱氨酸、胱氨酸、脯氨酸、酪氨酸、丝氨酸、组氨酸、甘氨酸、亮氨酸、异亮氨酸、缬氨酸、色氨酸、精氨酸、赖氨酸、天冬酰胺和谷氨酰胺。特别地使用胱氨酸、半胱氨酸、脯氨酸、丝氨酸、组氨酸、枸杞碱、亮氨酸、异亮氨酸、缬氨酸、酪氨酸、精氨酸、赖氨酸、天冬酰胺和谷氨酰胺。尤其优选的是胱氨酸、组氨酸、甘氨酸、亮氨酸、缬氨酸、精氨酸、赖氨酸和谷氨酰胺。可以使用氨基酸的D-型、DL-型和L-型,其中L-型是优选的。氨基酸衍生物的例子是N-乙酰化形式,例如N-乙酰-L-谷氨酰胺、N-乙酰-L-酪氨酸和N-乙酰-DL-色氨酸。氨基酸和氨基酸衍生物可以单独或以混合物形式使用。本发明制剂中氨基酸和氨基酸衍生物的量优选为0.1至40重量百分率,更优选为0.2至30重量百分率,最优选为0.2至15重量百分率,以制剂中全部组分的总和计。氨基酸和它们的衍生物优选以纯的形式加入。
本发明制剂进而以氧化锌和/或无机过氧化物的存在为特征。无机过氧化物优选采用过氧化锌、过氧化钠、过氧化钾、过氧化钙或过氧化镁。氧化锌和/或无机过氧化物例如可用于调节渗透压。令人惊奇地是,与单用过氧化镁相比,氨基酸与氧化锌和/或无机过氧化物的组合具有特别好的作用。本发明制剂中氧化锌和无机过氧化物的总量优选为0.5至50重量百分率,更优选为1.5至40重量百分率,以制剂中全部组分的总和计。如果局部用药的话,无机过氧化物的量应当优选为不大于10重量百分率,更优选为不大于6重量百分率,最优选为不大于3重量百分率,如果内部用药的话,则优选为不大于20重量百分率,更优选为不大于15重量百分率。氧化锌和无机过氧化物优选以纯的形式加入。
任选地,本发明制剂中可以另外存在tego-甜菜碱。本发明制剂中tego-甜菜碱的量优选为0至25重量百分率,更优选为1至20重量百分率,最优选为5至10重量百分率,以制剂中全部组分的总和计。
任选地,本发明制剂可以含有所有已知的生物活性植物物质,也叫辅助性植物物质。用在本发明中的辅助性植物物质尤其包含类胡萝卜素、植物甾醇、皂甙、多元酚、类黄酮、萜烯、植物雌激素、硫化物、肌醇六磷酸和食纤维质。上述生物活性植物物质中,用在本发明中的尤其是多元酚、类黄酮和生物类黄酮。天然来源的生物类黄酮是本发明制剂尤其优选的。生物活性植物物质在优选的制剂实施方式中的含量优选为0至75重量百分率,更优选为2至50重量百分率,以制剂中全部组分的总和计。优选的生物类黄酮天然来源是蔬菜,例如豆类、胡萝卜、番茄、花椰菜和辣椒、玉米、芝麻、柑橘果实、绿茶和红茶、圣约翰草、葡萄等。生物活性植物物质优选以提取物的形式加入。
任选地,本发明制剂中可以另外使用所有已知的不饱和脂肪酸。优选地使用包括在植物油和动物油(例如鱼油)中的不饱和脂肪酸。植物来源的多不饱和脂肪酸是重要的代谢调节剂(二十碳化合物和前列腺素)所必需的前体。本发明制剂中不饱和脂肪酸的量优选为0至70重量百分率,更优选为2至45重量百分率,以制剂中全部组分的总和计。不饱和脂肪酸优选的纯植物来源的例子是晚樱油、亚麻油、橄榄油、麦胚油、豆油、向日葵油、琉璃苣油、南瓜子油和红醋栗种子的油。不饱和脂肪酸优选以冷榨油的形式加入。
任选地,本发明制剂进而可以另外含有常用的脂质体、卵磷脂和lipodermine。脂质体是重要的,因为它们控制维生素A和维生素E的释放。藉此方式这些维生素可以长时间加以利用。本发明制剂中脂质体、卵磷脂或lipodermine的量优选为0至30重量百分率,更优选为2至20重量百分率,以制剂中全部组分的总和计。
任选地,本发明制剂可以另外包含表儿茶素,优选是从绿茶中获得的。表儿茶素可以延缓细胞的老化。此外,它们是重要的辅助物质,能够支持维生素等微量养分的作用。制剂中表儿茶素的量优选为0至60重量百分率,更优选为2至30重量百分率,以制剂中全部组分的总和计。表儿茶素优选以纯的形式或提取物的形式加入。
任选地,本发明制剂可以另外包含所有已知的典型维生素和维生素原。特别优选用在制剂中的是维生素A、B族维生素、维生素C、D、E和β-胡萝卜素。本发明制剂中维生素的量优选为0至75重量百分率,更优选为5至50重量百分率,以制剂中全部组分的总和计。维生素以提取物的天然形式和合成形式(例如B-维生素)加入,由此维生素的作用上的差异与该事实无关。
任选地,本发明制剂可以另外包含抗真菌和抗微生物组分。可以向本发明制剂中加入抗生素、抑菌剂、皮质甾类、可的松类、硝酸益康唑、地塞米松、羟基苯甲酸盐等。制剂中抗真菌和抗微生物组分的量优选为0至60重量百分率,最优选为2至30重量百分率,以制剂中全部组分的总和计。
任选地,本发明制剂可以包含所有已知的助剂、添加剂与载体物质、常用的粘结与粘合剂和溶剂。优选的例子是乳脂、未氢化的、部分氢化的或氢化的豆脂、豆油、核桃脂、甘油、明胶、果胶、卵磷脂、β-胡萝卜素、山梨醇溶液、氧化铁、二氧化钛、染剂、脂肪、蜡、乳化剂(例如Pentafarm Ltd.,CH的IRICALMIN)、聚硅氧烷、聚乙烯、聚山梨酮(polysorbitone)、(甲基)丙烯酰基化合物、滑石、dragantum、黄原胶、淀粉、凡士林、葡萄糖、糖精、石蜡、酸、防腐剂和芳香剂。可使用果胶作为粘结剂和粘合剂。上述物质和试剂以常用量使用,例如,果胶最多为10重量百分率,以制剂中全部组分的总和计。
本发明制剂可以按照本领域技术人员公知的方式加以制备,例如将活性成分与适当的,无毒的、惰性的、药学上可接受的固体或液体载体物质和可选的常用添加剂、助剂和溶剂一起制成盖仑给药剂型。制造软膏和霜剂等盖仑给药剂型的方法例如描述于H.Sucker,B.Fuchs,P.Speiser,“制药技术”(“PharmazeutischeTechnologie”)第2版(1991),Georg Thieme Verlag Stuttgart;R.Voigt,“制药技术教科书”(“Lehrbuch der pharmazeutischenTechnologie”),Thieme Verlag,1976。对本发明制剂来说,所有已知的用药剂型都是可能的。优选的用药剂型是霜剂、软膏、糊剂、乳剂、洗剂、流体、溶液、凝胶、粉末、喷雾剂、明胶剂、泡沫等。内部用药剂型例如胶囊剂、片剂、包衣片、口服液和注射液,例如皮下注射。作为用药剂型,缓释形式也是可能的。
原则上,所有已知的用药方式对本发明制剂来说都是可能的。最优选的是局部用药,例如将相应的用药剂型施用于皮肤,例如涂抹、摩搓、轻轻地摩擦、喷雾、轻拍等。用药也可以是软膏绷带或皮下注射的形式。本发明制剂每天可以施用一次或多次,可以历经较短和较长时间。不过,每日剂量和每天的用药频率因各发明制剂的配方而异。
根据配方的不同,本发明制剂适合作为营养补充剂、化妆品或药物组合物,优选为局部化妆品或局部药物组合物,施用于哺乳动物的皮肤与组织上,例如用于组织损害表现与后果的护理、保护和预防,用于皮肤与组织的治疗。根据配方的不同,它们在优选的实施方式中特别可用于所有的皮肤刺激(例如皮肤生理机能紊乱、晒伤)、蜂窝织炎、皱纹、痤疮、疱疹、牛皮癣、神经性皮炎、臭氧损害、灼伤、腐蚀性灼伤、细胞代谢紊乱和其它有组织液、脂肪与其它细胞产物及细胞分解代谢产物蓄积的改变,例如增厚、水肿、血肿,此外例如可用于痔、风湿病、关节病和皮肤癌。该制剂也可以用于粘膜,例如胃和肠道粘膜。
本发明通过实施例加以进一步阐述。
实施例1
按常用方法制备根据本发明的制剂,具有下列组分:
氧化锌 8wt%
过氧化钠 3wt%
磷酸钠 10wt%
磷酸钙 6wt%
氯化钙 5wt%
精氨酸 7wt%
亮氨酸 8wt%
天冬酰胺 5.5wt%
缬氨酸 2wt%
金缕梅 1wt%
单宁 3wt%
果胶 1wt%
tego-甜菜碱 2wt%
维生素A 1wt%
维生素E 1.5wt%
β-胡萝卜素 0.5wt%
胶原 1.5wt%
芦荟 2wt%
橄榄油 2wt%
类胡萝卜素 2wt%
明胶 1wt%
脂质体 2wt%
纯净水,加至 100wt%
将上例组合物施用于被试者的一条腿。对另一条腿施用对照物(安慰剂;对照腿)。检查结果总结如下:
作为上述发明配方的急性反应,发现微循环增加。约50分钟后,之后观察到微循环显著改善,约100分钟后达到最大增加。约120分钟之后观察到显著有效期。在对照腿上,观察到微循环没有变化。作为由本发明配方的用药所导致的进一步反应,可以观察到治疗腿上脂肪层减少了,而对照腿上没有改变。通过这些检查显示,本发明制剂能够显著改善微循环,减少脂肪层。
实施例2
量(wt%)天冬酰胺 0.30亮氨酸 0.20缬氨酸 0.30精氨酸 0.20过氧化锌 0.50磷酸钙 4.50磷酸钠 3.50透明氧化锌 2.00氯化钙 4.00硫酸镁 3.00蒸馏水 62.90金缕梅 2.50tego-甜菜碱 2.00山梨醇 6.00迷迭香油 0.30薄荷醇 0.30绿茶粉 1.00常春藤/问荆/藻/绿茶 5.00黄原胶 1.50
上述发明制剂按常用方法制备。
首先,测量被试者特定皮肤区域上的微循环。然后,在该皮肤区域轻轻地摩擦实施例2配方。然后立即测量微循环,然后每半小时测量一次,共计4小时。以通量单位测量微循环。将测量结果对时间作图。将包含盐和过氧化镁的商业上可得到的产品象本发明制剂一样施用于另一块皮肤区域,与之相比,当使用包含某些氨基酸与氧化锌和过氧化锌的组合的本发明配方时,观察到微循环上升较早,维持较高水平,历经较长时间,平缓恢复至原始值要晚得多。在相应的测量点上,与商业产品相比的改善作用在7与15%之间。结果显示,本发明配方与商业产品相比,具有提高了的系统和协同效果。
实施例3
按常用方法制备根据本发明的制剂,具有下列组分:
量(wt%)蒸馏水 71.15磷酸钙 1.50亮氨酸 0.20缬氨酸 0.30精氨酸 0.20天冬酰胺 0.30过氧化锌 0.25磷酸钠 1.50透明氧化锌 3.00Karion FP液 4.00Neo Dragold液 0.30氯化钙 1.50硫酸镁 2.50绿茶粉 2.00金盏花 3.00
金缕梅 2.50
圣约翰草 3.00
芳香剂1677 0.30
澳大利亚茶树油 1.00
黄原胶 1.50
实施例4按常用方法制备根据本发明的制剂,具有下列组分:
量(wt%)
蒸馏水 66.70
透明氧化锌 2.00
磷酸钠 3.00
天冬酰胺 0.05
磷酸钙 3.50
氯化钙 3.50
亮氨酸 0.20
硫酸镁 3.00
过氧化锌 0.30
tego-甜菜碱 2.00
金缕梅 2.50
山梨醇 5.00
YLANG-YLANG油Ⅱ 0.10
莲花芳香剂-精油混合物 0.10
薄荷醇 0.05
绿茶粉 0.50
IRICALMIN 3.00
GLYCODERM 3.00
黄原胶 1.50
在进一步应用中,观察到该配方对皮肤的老化、弹性、水分、皱纹形成和绷紧性方面都具有显著积极的效果。
Claims (16)
1.包含下列组分的制剂:
(a)至少一种选自碱金属盐、碱土金属盐和其它矿物质的盐,
其特征在于它含有
(b)至少一种氨基酸,和
(c)氧化锌和/或无机过氧化物。
2.根据权利要求1的制剂,其特征在于它另外包含tego-甜菜碱。
3.根据权利要求1或2的制剂,其特征在于它另外包含至少一种辅助性植物物质和/或至少一种表儿茶素。
4.根据权利要求1至3任意一项的制剂,其特征在于它另外包含至少一种不饱和脂肪酸和/或至少一种微量元素。
5.根据权利要求1至4任意一项的制剂,其特征在于它另外包含至少一种脂质体和/或至少一种维生素。
6.根据权利要求1至5任意一项的制剂,其特征在于它另外包含至少一种收敛剂和/或至少一种湿润剂和/或至少一种精油。
7.根据权利要求1至6任意一项的制剂,其特征在于它另外包含抗真菌和/或抗微生物组分。
8.根据权利要求1至7任意一项的制剂,其特征在于它另外包含至少一种选自载体物质、助剂、添加剂、粘结剂、粘合剂和溶剂的组分。
9.根据权利要求1至8任意一项的制剂,包含下列组分:
(a)10至90wt%的盐,选自碱金属盐、碱土金属盐和其它矿物质,
其特征在于,它包含
(b)0.1至40wt%的氨基酸,和
(c)总量为0.5至50wt%的氧化锌和无机过氧化物,以制剂中全部组分的总和计。
10.根据权利要求1至9任意一项的制剂,包含下列组分:
(a)至少一种金属盐,选自钠、钾、镁、钙、硅、锌、锰、铜、铁、氟、氯、溴、碘和磷,
其特征在于它含有
(b)至少一种氨基酸或氨基酸衍生物,选自胱氨酸、半胱氨酸、脯氨酸、丝氨酸、组氨酸、甘氨酸、亮氨酸、异亮氨酸、缬氨酸、酪氨酸、精氨酸、赖氨酸、天冬酰胺和谷氨酰胺,和
(d)氧化锌和/或无机过氧化物。
11.根据权利要求1至10任意一项的制剂,其特征在于该无机过氧化物是过氧化锌、过氧化钠、过氧化钾、过氧化钙或过氧化镁。
12.根据权利要求1至11任意一项的制剂的用途,用于局部用药。
13.根据权利要求12的制剂的用途,用作化妆品。
14.根据权利要求12的制剂的用途,用作药物组合物。
15.根据权利要求1至11任意一项的制剂作为药物组合物的用途。
16.根据权利要求1至11任意一项的制剂作为营养补充剂的用途。
Applications Claiming Priority (2)
Application Number | Priority Date | Filing Date | Title |
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DE19831798A DE19831798A1 (de) | 1998-07-15 | 1998-07-15 | Mittel zur Pflege und/oder Behandlung von Haut und Gewebe |
DE19831798.0 | 1998-07-15 |
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CN1313753A true CN1313753A (zh) | 2001-09-19 |
CN1201723C CN1201723C (zh) | 2005-05-18 |
Family
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EP (2) | EP1639991A3 (zh) |
JP (1) | JP3917370B2 (zh) |
KR (1) | KR100542606B1 (zh) |
CN (1) | CN1201723C (zh) |
AT (1) | ATE308968T1 (zh) |
AU (1) | AU761947B2 (zh) |
BR (1) | BR9912821A (zh) |
CA (1) | CA2337772C (zh) |
DE (3) | DE19831798A1 (zh) |
DK (1) | DK1096918T3 (zh) |
ES (1) | ES2252976T3 (zh) |
HK (1) | HK1037958A1 (zh) |
HU (1) | HUP0103236A2 (zh) |
IL (1) | IL140889A0 (zh) |
NO (1) | NO20010220L (zh) |
PL (1) | PL345689A1 (zh) |
WO (1) | WO2000003689A2 (zh) |
ZA (1) | ZA200101244B (zh) |
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1998
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- 1999-07-15 DK DK99947221T patent/DK1096918T3/da active
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Cited By (6)
Publication number | Priority date | Publication date | Assignee | Title |
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CN104173232A (zh) * | 2014-08-06 | 2014-12-03 | 金玲 | 一种提升肌肤抵抗力并修复微损肌肤的美容液制作方法 |
CN104189000A (zh) * | 2014-09-12 | 2014-12-10 | 朴荣范 | 外伤药液及其制备方法 |
CN107205463A (zh) * | 2015-02-11 | 2017-09-26 | 雀巢产品技术援助有限公司 | 维生素a组合物 |
US11109615B2 (en) | 2015-02-11 | 2021-09-07 | Societe Des Produits Nestle S.A. | Vitamin A composition |
CN105901703A (zh) * | 2016-04-19 | 2016-08-31 | 上海海洋大学 | 一种用于烧伤患者的海洋生物型肠内营养制剂 |
CN105901703B (zh) * | 2016-04-19 | 2020-03-10 | 上海海洋大学 | 一种用于烧伤患者的海洋生物型肠内营养制剂 |
Also Published As
Publication number | Publication date |
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NO20010220D0 (no) | 2001-01-12 |
CA2337772C (en) | 2009-06-09 |
HUP0103236A2 (hu) | 2002-02-28 |
DK1096918T3 (da) | 2006-01-09 |
EP1639991A3 (de) | 2007-09-05 |
CN1201723C (zh) | 2005-05-18 |
AU6077899A (en) | 2000-02-07 |
KR100542606B1 (ko) | 2006-01-11 |
PL345689A1 (en) | 2002-01-02 |
DE59912774D1 (de) | 2005-12-15 |
CA2337772A1 (en) | 2000-01-27 |
KR20010070965A (ko) | 2001-07-28 |
JP3917370B2 (ja) | 2007-05-23 |
JP2002520348A (ja) | 2002-07-09 |
DE19831798A1 (de) | 2000-01-27 |
ATE308968T1 (de) | 2005-11-15 |
AU761947B2 (en) | 2003-06-12 |
EP1096918A2 (de) | 2001-05-09 |
WO2000003689A2 (de) | 2000-01-27 |
EP1639991A2 (de) | 2006-03-29 |
IL140889A0 (en) | 2002-02-10 |
ZA200101244B (en) | 2003-05-14 |
HK1037958A1 (en) | 2002-03-01 |
ES2252976T3 (es) | 2006-05-16 |
EP1096918B1 (de) | 2005-11-09 |
NO20010220L (no) | 2001-03-13 |
WO2000003689A3 (de) | 2000-04-20 |
DE19981295D2 (de) | 2001-08-30 |
BR9912821A (pt) | 2001-05-02 |
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