公开(公告)号：US20110223247A1

公开(公告)日：2011-09-15

申请号：US13126855

申请日：2009-11-06

申请人： Sang Yeob Park ,  Hojin Chung ,  Chaul Min Pai

发明人： Sang Yeob Park ,  Hojin Chung ,  Chaul Min Pai

IPC分类号： A61K9/58 ,  A61K9/00 ,  A61K9/22 ,  A61K9/54 ,  A61K31/445 ,  A61P25/00 ,  A61K9/56

CPC分类号： A61K9/0095 ,  A61K9/0056 ,  A61K9/5073 ,  A61K31/445

摘要： Disclosed is a pharmaceutical composition for release control comprising a plurality of particles for release control. The plurality of particles for release control comprise a core material containing methylphenidate and a polymer coating layer for release control formed on the core material. The plurality of particles for release control are divided into two or more groups based on the average thickness of the polymer coating layer for release control. The particle groups are identical in terms of the composition of the polymer in the polymer coating layer, but are different in terms of the average thickness of the coated layer. The pharmaceutical composition for release control according to the present invention may control the release pattern of methylphenidate contained in the core material as desired, and can be used as an oral formulation in a variety of forms such as orally disintegrating tablets, etc.

摘要翻译： 公开了一种用于释放控制的药物组合物，其包含多个用于释放控制的颗粒。 用于释放控制的多个颗粒包括含有哌甲酯的核心材料和用于在芯材上形成的用于释放控制的聚合物涂层。 用于释放控制的多个颗粒基于用于释放控制的聚合物涂层的平均厚度被分成两组或更多组。 在聚合物涂层中聚合物的组成方面，颗粒组是相同的，但是在涂层的平均厚度方面是不同的。 根据本发明的用于释放控制的药物组合物可以根据需要控制核心材料中所含的哌甲酯的释放模式，并且可以以各种形式如口腔崩解片等的口服制剂使用。

公开(公告)号：US08465768B2

公开(公告)日：2013-06-18

申请号：US13126855

申请日：2009-11-06

申请人： Sang Yeob Park ,  Hojin Chung ,  Chaul Min Pai

发明人： Sang Yeob Park ,  Hojin Chung ,  Chaul Min Pai

IPC分类号： A61K9/58

CPC分类号： A61K9/0095 ,  A61K9/0056 ,  A61K9/5073 ,  A61K31/445

摘要： Disclosed is a pharmaceutical composition for release control comprising a plurality of particles for release control. The plurality of particles for release control comprise a core material containing methylphenidate and a polymer coating layer for release control formed on the core material. The plurality of particles for release control are divided into two or more groups based on the average thickness of the polymer coating layer for release control. The particle groups are identical in terms of the composition of the polymer in the polymer coating layer, but are different in terms of the average thickness of the coated layer. The pharmaceutical composition for release control according to the present invention may control the release pattern of methylphenidate contained in the core material as desired, and can be used as an oral formulation in a variety of forms such as orally disintegrating tablets, etc.

摘要翻译： 公开了一种用于释放控制的药物组合物，其包含多个用于释放控制的颗粒。 用于释放控制的多个颗粒包括含有哌甲酯的核心材料和用于在芯材上形成的用于释放控制的聚合物涂层。 用于释放控制的多个颗粒基于用于释放控制的聚合物涂层的平均厚度被分成两组或更多组。 在聚合物涂层中聚合物的组成方面，颗粒组是相同的，但是在涂层的平均厚度方面是不同的。 根据本发明的用于释放控制的药物组合物可以根据需要控制核心材料中所含的哌甲酯的释放模式，并且可以以各种形式如口腔崩解片等的口服制剂使用。

公开(公告)号：US07749533B2

公开(公告)日：2010-07-06

申请号：US10841979

申请日：2004-05-07

申请人： Yourong Fu ,  Chaul Min Pai ,  Sang Yeob Park ,  Gun Seomoon ,  Kinam Park

发明人： Yourong Fu ,  Chaul Min Pai ,  Sang Yeob Park ,  Gun Seomoon ,  Kinam Park

IPC分类号： A61K9/20 ,  A61K9/16

CPC分类号： A61K9/0056

摘要： A fast-melting pharmaceutical tablet comprises a porous, plastic substance, a water penetration enhancer and a binder. One or more drugs can be incorporated into the formulation at different stages of the process so as to afford a pharmaceutically active tablet. Methods of making the pharmaceutical tablet entail combining the porous, plastic material, the water penetration enhancing agent, and the binder so as to form highly plastic granules, which are compressed into tablets. The resulting tablets dissolve rapidly in the mouth and have good hardness with low brittleness. The tablets are particularly valuable to those who have difficulty swallowing conventional pills.

摘要翻译： 快速熔化的药物片剂包括多孔塑料物质，水渗透增强剂和粘合剂。 可以在该方法的不同阶段将一种或多种药物并入制剂中，从而得到药用活性片剂。 制备药片的方法需要结合多孔，塑料，水渗透增强剂和粘合剂，以形成高度塑性的颗粒，将其压制成片剂。 所得片剂迅速溶于口中，硬度好，脆性低。 这些片剂对吞咽常规药丸有困难的人特别有价值。

公开(公告)号：US07273619B2

公开(公告)日：2007-09-25

申请号：US10414827

申请日：2003-04-15

申请人： Chaul Min Pai ,  Jin Deog Song ,  Joong Woong Cho

发明人： Chaul Min Pai ,  Jin Deog Song ,  Joong Woong Cho

IPC分类号： A61F13/00 ,  A61F15/16

CPC分类号： A61K9/0014 ,  A61K9/7023 ,  A61K31/00 ,  A61K31/46 ,  A61K47/10 ,  A61K47/14 ,  A61K47/18 ,  A61K47/38

摘要： The present invention relates to a transdermal composition of an antivomiting agent, and more particularly to a transdermal composition of an antivomiting agent which can minimize skin irritation by employing tropisetron as the antivomiting agent as well as by adjusting its pH to be in the range of 8 to 9 thus enhancing its rate of skin penetration thereby reducing the amount of a skin penetration enhancer used.

摘要翻译： 本发明涉及抗病毒剂的透皮组合物，更具体地说，涉及一种抗病毒剂的透皮组合物，其可以通过使用托烷司琼作为抗病毒剂，并通过将其pH调节至8范围内来最小化皮肤刺激 从而提高其皮肤渗透速率，从而减少使用的皮肤渗透增强剂的量。

公开(公告)号：US06413494B1

公开(公告)日：2002-07-02

申请号：US09318579

申请日：1999-05-25

申请人： Seung Seo Lee ,  Chang Baeg Lim ,  Chaul Min Pai ,  Sujung Lee ,  In Park ,  Moon Gun Seo ,  Heenam Park

发明人： Seung Seo Lee ,  Chang Baeg Lim ,  Chaul Min Pai ,  Sujung Lee ,  In Park ,  Moon Gun Seo ,  Heenam Park

IPC分类号： A61K4900

CPC分类号： A61K9/5078 ,  A61K9/286 ,  A61K9/4816 ,  A61K9/4891 ,  A61K9/5036 ,  C08L5/06 ,  Y10S514/96 ,  Y10S514/962 ,  C08L2666/02

摘要： A colonic drug delivery composition contains a first polysaccharide and a second polysaccharide wherein both polysaccharide are degradable by colonic enzymes and are mixed at a environmental pH of about 7 or above, without use of a cross-linking agent. A colon selective pharmaceutical composition and dosage form for oral delivery of a drug, diagnostic reagent, or mixture thereof includes the drug, diagnostic reagent, or mixture thereof in contact with the polysaccharide composition. A method of preparing such a colonic drug delivery composition and the colon selective pharmaceutical composition and dosage from are also disclosed.

摘要翻译： 结肠药物递送组合物包含第一多糖和第二多糖，其中两种多糖可通过结肠酶降解，并且在环境pH约为7或更高的条件下混合，而不使用交联剂。 用于口服递送药物，诊断试剂或其混合物的结肠选择性药物组合物和剂型包括与多糖组合物接触的药物，诊断试剂或其混合物。 还公开了制备这种结肠药物递送组合物和结肠选择性药物组合物和剂量的方法。

公开(公告)号：US07674767B2

公开(公告)日：2010-03-09

申请号：US10584449

申请日：2004-12-24

申请人： Chaul Min Pai ,  Mi Hong Min ,  Jun Seok Hwang ,  Kyung Mi Cho

发明人： Chaul Min Pai ,  Mi Hong Min ,  Jun Seok Hwang ,  Kyung Mi Cho

IPC分类号： A61K38/28 ,  A61K47/06 ,  C09D105/04

CPC分类号： A61K9/5123 ,  A61K9/08 ,  A61K9/146 ,  A61K9/5146 ,  A61K9/5192 ,  A61K31/545 ,  A61K31/66 ,  A61K31/727 ,  A61K38/1816 ,  A61K38/21 ,  A61K38/23 ,  A61K38/27 ,  A61K38/28 ,  A61K38/31 ,  A61K47/32 ,  A61K47/34 ,  A61K47/44

摘要： The present invention relates to an orally administrable composition containing nanoparticles with the particle size of 500 nm or less, comprising 0.1-30 weight % of a complex of a water-soluble drug and a counter-ion substance in which the charged water-soluble drug is bonded with the counter-ion substance, 0.5-80 weight % of a lipid, 0.5-80 weight % of a polymer, and 1-80 weight % of an emulsifier, wherein the weight ratio of said lipid and said polymer is in the range of 1:0.05-3, and a preparation method thereof. The composition of the present invention has high gastrointestinal absorption rate upon oral administration, and has high drug entrapping rate in the nanoparticle, and is also stable against lipases.

摘要翻译： 本发明涉及含有粒径为500nm以下的纳米粒子的可口服给药的组合物，其含有0.1-30重量％的水溶性药物和抗衡离子物质的复合物，其中带电的水溶性药物 与抗衡离子物质，0.5-80重量％的脂质，0.5-80重量％的聚合物和1-80重量％的乳化剂结合，其中所述脂质和所述聚合物的重量比在 范围为1：0.05-3，及其制备方法。 本发明的组合物在口服给药时具有高的胃肠吸收速率，并且在纳米颗粒中具有高的药物截留速率，并且对脂肪酶也是稳定的。

公开(公告)号：US5741511A

公开(公告)日：1998-04-21

申请号：US627805

申请日：1996-04-10

申请人： Hun Han Lee ,  Joong Woong Cho ,  Choul Young Kim ,  Chaul Min Pai ,  Jin Deog Song ,  Chul Min Park ,  Hye Jeong Yoon ,  Yoon Yeo ,  Jae Seung Paick

发明人： Hun Han Lee ,  Joong Woong Cho ,  Choul Young Kim ,  Chaul Min Pai ,  Jin Deog Song ,  Chul Min Park ,  Hye Jeong Yoon ,  Yoon Yeo ,  Jae Seung Paick

IPC分类号： A61M37/00 ,  A61F5/41 ,  A61F6/04 ,  A61K9/00 ,  A61K9/70 ,  A61F13/00 ,  A61F6/02

CPC分类号： A61K9/703 ,  A61F5/41 ,  A61F6/04 ,  A61K9/0034 ,  A61K9/7092 ,  Y10S602/901

摘要： The present invention is to provide a method and a transdermal drug delivery device for treating erectile dysfunction which comprises a patch containing pharmaceutically active ingredient and being directly apply to the male glans penis and its support and the rings for constricting the base part of the penis to aid the erection. The patch according to the present invention may be divided into two types, i.e. a cylinder type patch and a multi-reservoir type patch. The transdermal drug delivery patch device of the present invention is painless and safely to use and may be effectively produced and maintained erection of the penis without the adverse side effects and with a high degree of patient acceptability in the case of male impotence.

摘要翻译： 本发明提供一种用于治疗勃起功能障碍的方法和透皮药物递送装置，其包含含有药物活性成分的补片，并且直接应用于雄性龟头阴茎及其支撑体和用于收缩阴茎基部的环 帮助勃起。 根据本发明的贴片可以分为两种类型，即圆柱型贴片和多储器型贴片。 本发明的透皮药物递送贴片装置是无痛且安全使用的，并且可以有效地产生和维持阴茎的勃起而没有不利的副作用，并且在男性阳the的情况下具有高度的患者可接受性。

公开(公告)号：US5665428A

公开(公告)日：1997-09-09

申请号：US547962

申请日：1995-10-25

申请人： Younsik Cha ,  Young Kweon Choi ,  Chaul Min Pai

发明人： Younsik Cha ,  Young Kweon Choi ,  Chaul Min Pai

IPC分类号： A61K9/50 ,  A61K9/16 ,  A61K38/00 ,  A61K38/23 ,  A61K38/28 ,  A61K38/38 ,  A61K47/48 ,  B01J13/02 ,  B05D7/00

CPC分类号： A61K38/23 ,  A61K38/28 ,  A61K38/38 ,  A61K9/1647 ,  B01J13/02

摘要： Peptide/protein biodegradable drug delivery devices are prepared as microspheres without the use of solvents by a polymer melt process. A melt of thermostable polypeptides and an appropriate low melting block copolymer mixture is prepared and dispersed in an appropriate fluid medium such as air, water or an immiscible organic fluid without using any organic solvent to form microdroplets. The fluid medium is cooled to solidify the microdroplets into microspheres and then collected and purified or further processed as drug delivery devices. These biodegradable microspheres are suitable as implantable or injectable pharmaceutical formulations. Following administration as solid microspheres into the body of a warm blooded animal, the formulations absorb water from the body to form a hydrogel from which the polypeptide is released continuously over an extended period of time.

摘要翻译： 肽/蛋白质可生物降解的药物递送装置通过聚合物熔融方法制备为不使用溶剂的微球。 制备热稳定多肽和合适的低熔点嵌段共聚物混合物的熔体并将其分散在合适的流体介质如空气，水或不混溶的有机流体中，而不使用任何有机溶剂形成微滴。 将流体培养基冷却以将微滴固化成微球，然后收集并纯化或进一步加工为药物递送装置。 这些可生物降解的微球体适合作为可植入或可注射的药物制剂。 在作为固体微球体施用于温血动物的体内后，制剂吸收来自身体的水以形成水凝胶，多肽在延长的时间段内连续释放。