• Journal of Pharmaceutical Investigation
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• 제26권1호
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• pp.13-22
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• 1996

Poly(D,L-lactic acid) (PLA) microspheres containing alprazolam(APZ) were prepared by a solvent-emulsion evaporation method and their release patterns were investigated in vitro. Various batches of microspheres with different size and drug content were obtained by changing the ratio of APZ to PLA, PLA concentration in the dispersed phase and stirring rate. Rod-like APZ crystals on microsphere surface, which were released rapidly and could act as a loading dose, were observed with increasing drug content. The release rate was increased with increase in drug contents and decrease in the molecular weight of PLA. The release rate of APZ for long-acting injectable delivery system in vitro, which would aid in predicting in vitro release profile, could be controlled by properly optimizing various factors affecting characteristics of microspheres.

• Journal of Pharmaceutical Investigation
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• 제24권4호
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• pp.257-263
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• 1994

The interpenetrating polymer networks (IPNs) of polyacrylic acid (PAA)-polyethylene glycol (PEG) were synthesized via crosslinking of PEG and simultaneous free radical polymerization of PAA. The equilibrium swelling of the IPNs matrices, ranged from 40% to 95%, was varied to a great extent as compared with PAA homopolymer due to the interpolymer interaction between PAA and PEG. The drug release kinetics of drug loaded matrices was significantly affected by the charge of drugs as well as interpolymer complexation.

• 폴리머
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• 제29권3호
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• pp.288-293
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• 2005

약물을 전달하기 위한 많은 방법들 중의 하나인 삼투압을 이용한 과립화는 타블렛 제형의 단점인 제조공정의 복잡함과 여러 문제점을 보완하기 위해 시도되었다. 유동층 코팅기로 제조된 삼투압을 이용한 과립은 물을 흡수하면 팽윤하는 시드층과 모델 약물인 니페디핀을 포함하는 약물층, 그리고 약물의 방출을 조절할 수 있는 반투막으로 구성되었다. 서로 다른 크기와 반투막의 두께는 각기 다른 양의 시드와 반투막 코팅액을 사용하여 얻을 수 있었다. 얻어진 과립은 각 코팅 단계에 따라서 서로 다른 모폴로지는 코팅되는 용액의 형태에 따라 다르게 나타났다. 과립의 크기가 클수록 방출은 지연되며, 이는 과립이 가지는 비표면적의 차이로 인한 것이라 사료된다. 또한 반투막의 두께가 두꺼울수록 약물의 방출이 지연되는데 이는 반투막이 두꺼울수록 물의 흡수가 늦어지는 것으로 추정된다 용출액의 약물 용해도는 약물의 방출에 큰 영향을 미쳐 용출액 선택의 중요성을 알 수 있었다. 이 실험을 통해 삼투압을 이용한 과립은 유동층 코팅을 이용하여 제조할 수 있었으며, 과립의 크기와 반투막의 두께, 돗출액에 따라 약물의 방출을 조절할수 있음을 확인하였다.

• 약학회지
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• 제31권1호
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• pp.25-32
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• 1987

The effect of loading dose, plasticiser and PVA molecular weight on naproxen release from hydrophilic polymer matrix was examined. Hydrophilic polymer matrix was prepared with PVA and PVP by adding glycerine as plasticiser. The release of naproxen from polymer matrix was determined in phosphate buffer medium. The release rate of naproxen from the polymer matrix increased as drug loading dose and plasticiser percentage increased. Raproxen released from the polymer matrix showed the time square root kinetics. Without changing the release-pattern, the release rate of naproxen could not be changed by varying molecular weight of PVA. Linearly released time range increased as drug loading dose increased, whereas decreased as plasticiser percentage increased up to 30%.

• 폴리머
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• 제34권2호
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• pp.172-177
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• 2010

최근 20년간 다양한 세포에서 파크리탁셀(PTX)의 효과에 관한 연구는 많이 있지만, 세포증식을 억제하기 위한 약물방출 동역학에 관한 연구는 거의 보고되지 않고 있다. 본 연구에서는 약물방출스텐트 (DES)에 적용하기 위해서 생분해성 고분자로부터 파크리탁셀의 방출거동을 고찰하였다. 다양한 생분해성 고분자인 poly(lactic acid-co-glycolic acid) (PLGA), poly-L-lactide(PLLA) 및 polycaprolactone(PCL)에 파크리탁셀의 함유량을 달리하여 필름을 제조한 후 약물방출 거동을 평가하였다. 약물방출은 8주 동안 이루어졌으며 FE-SEM을 통해 고분자의 분해정도를 관찰하였다. PCL의 생분해 속도는 가장 느리지만 파크리탁셀의 함량이 같을 경우 PCL로부터의 파크리탁셀 방출속도가 가장 빨랐으며 PLGA 그리고 PLLA 순서를 보였다. 이와 같은 결과를 바탕으로 PCL과 같이 유리전이온도($T_g$)가 낮은 고분자의 경우 체내에서 파크리탁셀과 같은 소수성 약물의 움직임이 용이하기 때문에 약물방출 속도가 빠를 수 있음을 제시하고 있다.

• Journal of Pharmaceutical Investigation
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• 제37권2호
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• pp.101-106
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• 2007

Venlafaxine, 1-[2-(dimethylamino)-1-(4-methoxyphenyl)ethyl] cyclohexanol hydrochloride is a novel, nontricyclic antidepressant. venlafaxine is a unique antidepressant that differs structurally from other currently available. The aim ot the study was to formulate sustained-release venlafaxine granules and assess their formulation variables. It consists of two layers, venlafaxine drug layer and sustained release coating layer and manufactured by fluidized bed process. The sustained release of drug could be increased by double-control rising various components in venlafaxine drug layer and sustained-release layer. The drug-containing granules were coated with cellulose acetate, cetyl alcohol and Eudragit RS along with plastisizer such as dibuthyl sebacate as an nano-pore former The release oi venlafaxine depended on the type of Eudragit such as RS, and RL used in the formulation of controlled release layer. These results obtained clearly suggest that the sustained release oral delivery system for venlafaxine could be designed with satisfying drug release profile approved.

• 한국산학기술학회논문지
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• 제11권7호
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• pp.2451-2458
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• 2010

고혈압 치료제인 카르베딜롤을 모델약물로 하여 새로운 서방성 방출 제어형 매트릭스 정제를 제조하기 위하여 소수성 서방성 부형제인 Compritol 888 ATO와 친수성 고분자인 hydroxypropyl methyl cellulose (HPMC) 또는 polyethylene oxide (PEO)를 이용하여 방출 제어형 매트릭스 정제를 제조하였다. 카르베딜롤 방출 제어형 매트릭스 정제의 제조 시 Compritol 888 ATO의 비율과 친수성 고분자의 종류 및 비율, hot melt coating coagglutination (HMCC) rocess의 적용 유무에 따른 카르베딜롤의 방출 양상을 위하여 용출시험기를 사용하여 pH 1.2의 인공위액과 pH 6.8의 인공장액에서 24시간 동안 $37^{\circ}C$, 50 rpm으로 용출시험을 실시하였다. 그 결과, HMCC process를 적용한 모든 제제가 약물의 방출 제어에 매우 효과적인 것을 확인하였다. 또한 소수성 서방성 부형제인 Compritol 888 ATO의 비율에 따라 약물의 방출 양상 및 시간이 기존 일반정제에 비하여 약 95%의 용출률을 나타내었으며 24시간까지 지연됨을 확인할 수 있었다.

• Journal of Pharmaceutical Investigation
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• 제38권2호
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• pp.105-110
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• 2008

Indapamide (4-chloro-N-(2-methyl-1-indolinyl)-3-sulfamoyl-benz-amide) is an oral antihypertensive diuretic agent indicated for the treatment of hypertensive. The diuretic and natriuretic effects are mainly due to the structure of o-chlorobenzenesulfonamide. The objective of this study was to formulate sustained release indapamide granules and assess their formulation variables. Granules were prepared by fluid bed coating method and consist of drug layer and membrane layer. The granules were coated with HPC and ethyl cellulose along with plasticizer dibuthyl sebacate. The release of indapamide depended on the type of Eudragit such as RS and NE 30 D used in the formulation controlled release layer. These results obtained clearly suggest that the sustained release oral delivery system for indapamide could be designed with satisfying drug release profile approved.

• 전기전자학회논문지
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• 제21권3호
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• pp.320-330
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• 2017

Porous nanosilica (PNS) has been identified as a potential candidate for controlled drug delivery. However, unmodified PNS-based carriers exhibited an initial release of loaded bioactive agents, which may limit their potential clinical applications. In this study, the surface of PNS was functionalized with adamantylamine (ADA) via disulfide bonds (-S-S-), PNS-S-S-ADA, which was then modified with cyclodextrin (CD)-heparin (Hep) (CD-Hep), PNS-S-S-CDH, for redox triggered rhodamine B (RhB) delivery. The obtained samples were then characterized by proton nuclear magnetic resonance ($^{1}H\;NMR$), Fourier transform infrared (FTIR), and transmission electron microscope (TEM). These results showed that PNS-S-S-CDH was successfully formed with spherical shape and average diameter of $45.64{\pm}2.33nm$. In addition, RhB was relatively encapsulated in the PNS-S-S-CDH (RhB@PNS-S-S-CDH) and slowly released up to 3 days. The release of RhB, in particular, was triggered due to the cleavage of -S-S- in the presence of dithiothreitol (DTT). It might be anticipated that the modified PNS can be used as redox-responsive drug delivery system in cancer therapy.

• 생체재료학회지
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• 제22권4호
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• pp.290-302
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• 2018

Background: The main purpose of drug delivery systems is to deliver the drugs at the appropriate concentration to the precise target site. Recently, the application of a thin film in the field of drug delivery has gained increasing interest because of its ability to safely load drugs and to release the drug in a controlled manner, which improves drug efficacy. Drug loading by the thin film can be done in various ways, depending on type of the drug, the area of exposure, and the purpose of drug delivery. Main text: This review summarizes the various methods used for preparing thin films with drugs via Layer-by-layer (LbL) assembly. Furthermore, additional functionalities of thin films using surface modification in drug delivery are briefly discussed. There are three types of methods for preparing a drug-carrying multilayered film using LbL assembly. First methods include approaches for direct loading of the drug into the pre-fabricated multilayer film. Second methods are preparing thin films using drugs as building blocks. Thirdly, the drugs are incorporated in the cargo so that the cargo itself can be used as the materials of the film. Conclusion: The appropriate designs of the drug-loaded film were produced in consideration of the release amounts and site of the desired drug. Furthermore, additional surface modification using the LbL technique enabled the preparation of effective drug delivery carriers with improved targeting effect. Therefore, the multilayer thin films fabricated by the LbL technique are a promising candidate for an ideal drug delivery system and the development possibilities of this technology are infinite.