• Journal of Pharmaceutical Investigation
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• 제37권1호
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• pp.15-22
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• 2007

An oil-in-water solvent evaporation method was used to prepare the cyclosporin A (CyA)-loaded nanoparticles varying in poly (D,L-lactide-co-glycolide) (PLGA) polymer (RG 502H, RG 503H) and the amount of additive ethyl myristate (EM) or chitosan (CS). The particles were characterized for drug loading and entrapment efficiency by HPLC, surface morphology by scanning electron microscopy, particle size by dynamic light scattering and surface charge by Zetapotential. The results showed drug loadings ranging from 10.9% to 15.8% with high encapsulation efficiency (82.0-97.8%). SEM and DLS studies showed discrete and spherical particles with smooth surfaces and mean size ranging 257.6-721.7 nm. The additive EM or CS did not change the mean sizes of the nanoparticles, whereas by the coating effect of CS, the Zetapotential values of the CS-added nanoparticles were moved to the more positive direction as the amount of CS was increased. From the pharmacokinetic analysis, the nanoparticles formulations showed the higher bioavailability and MRT than $Neoral^{\circledR}$ While little adding effect of EM or CS was detected in pharmacokinetic profile when RG 503H was used as polymer carrier, more noticeable different pharmacokinetic behaviors could be observed in case of RC 502H. EM incorporation was found to elevate the $K_{el}$, whereas CS coating resulted in the decrease of F and $K_{el}$, which seems to be due to the function of CS as a barrier and a mucoadhesive coating.

• 대한치과보철학회지
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• 제54권2호
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• pp.120-125
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• 2016

목적: 본 연구는 in-vitro 상에서 recombinant human transforming growth factor-beta (rhTGF-${\beta}2$)와 poly(D,L-lactide-co-glycolide) (PLGA) 의 복합체를 티타늄 디스크 표면에 코팅하여, 생물학적으로 간엽줄기세포 증식에 미치는 영향을 조사하기 위해 시행되었다. 재료 및 방법: 양극산화 디스크에 일렉트로스프레이 코팅법을 이용하여 anodized 된 티타늄 디스크를 대조군으로 설정하고, rhTGF-${\beta}2$를 125 ng/ml와 500 ng/ml 농도로 코팅한 것을 실험군으로 하였다. 티타늄 디스크 표면에 분사된 복합체가 균일하게 분사되었는지 field-emission scanning electron microscopy (FE-SEM)을 통해 확인하였으며, atomic force microscope (AFM) test를 이용하여 rhTGF-${\beta}2$로 코팅한 디스크와 양극산화 디스크의 거칠기 차이를 확인하였다. 디스크 위에 간엽줄기세포 배양 후 1, 4, 7일에 세포증식 양상을 MTT (3-(4,5-dimethylthiazol-2-yl)-2,5 diphenyl-tetrazolium bromide) assay 검사를 통해 확인하였다. 결과: AFM 결과 대조군과 실험군에서 거칠기의 유의할만한 차이가 없었다 (P>.05). MTT 결과 7일차 배양 결과에서 125 ng/ml와 500 ng/ml PLGA/TGF-${\beta}2$처리된 그룹은 각각 평균 0.45와 0.48이였으며, 대조군은 평균 0.33으로 PLGA/TGF-${\beta}2$처리된 그룹에서 세포 증식이 더 활성화 되는 것을 확인할 수 있었다 (P<.05). 결론: rhTGF-${\beta}2$ 복합체를 electrospray법으로 코팅한 티타늄 표면에서 7일차에서 줄기간엽세포의 빠른 증식을 확인하였다. 또한 복합체 처리군의 농도가 증가할수록 높은 세포 성장 수치를 보였다.

• Macromolecular Research
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• 제11권4호
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• pp.207-223
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• 2003

For last five years, we are developing the novel local drug delivery devices using biodegradable polymers, especially polylactide (PLA) and poly(D,L-lactide-co-glycolide) (PLGA) due to its relatively good biocompatibility, easily controlled biodegradability, good processability and only FDA approved synthetic degradable polymers. The relationship between various kinds of drug [water soluble small molecule drugs: gentamicin sulfate (GS), fentanyl citrate (FC), BCNU, azidothymidine (AZT), pamidronate (ADP), $1,25(OH)_2$ vitamin $D_3$, water insoluble small molecule drugs: fentanyl, ipriflavone (IP) and nifedipine, and water soluble large peptide molecule drug: nerve growth factor (NGF), and Japanese encephalitis virus (JEV)], different types of geometrical devices [microspheres (MSs), microcapsule, nanoparticle, wafers, pellet, beads, multiple-layered beads, implants, fiber, scaffolds, and films], and pharmacological activity are proposed and discussed for the application of pharmaceutics and tissue engineering. Also, local drug delivery devices proposed in this work are introduced in view of preparation method, drug release behavior, biocompatibility, pharmacological effect, and animal studies. In conclusion, we can control the drug release profiles varying with the preparation, formulation and geometrical parameters. Moreover, any types of drug were successfully applicable to achieve linear sustained release from short period ($1{\sim}3$ days) to long period (over 2 months). It is very important to design a suitable formulation for the wanting period of bioactive molecules loaded in biodegradable polymers for the local delivery of drug. The drug release is affected by many factors such as hydrophilicity of drug, electric charge of drug, drug loading amount, polymer molecular weight, the monomer composition, the size of implants, the applied fabrication techniques, and so on. It is well known that the commercialization of new drug needs a lot of cost of money (average: over 10 million US dollar per one drug) and time (average: above 9 years) whereas the development of DDS and high effective generic drug might be need relatively low investment with a short time period. Also, one core technology of DDS can be applicable to many drugs for the market needs. From these reasons, the DDS research on potent generic drugs might be suitable for less risk and high return.

• Restorative Dentistry and Endodontics
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• 제29권6호
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• pp.548-552
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• 2004

본 연구는 제어방출형 근관소독제(CRD)로 부터 chlorhexidine (CHX)의 방출 속도를 제어하기 위한 3가지 polymer (chitosan, PMMA, PLGA) 의 코팅 효과를 평가하기 위함이다. 80번 paper point (Sure-EndoTM)에 20% CHX를 loading 한 후 각 군당 10개씩 4군으로 분류하였다: Group A: 폴리머를 코팅하지 않은 CRD prototype (control), Group B: chitosan-coated prototype, Group C: PMMA-coated prototype, Group D: PLGA-coated prototype. 모든 시편은 3 ml 증류수가 담긴 큐벳에 넣은 후 3, 6, 10, 20, 30, 40, 50분 마다, 1, 2, 3, 4, 5, 6시간마다 각각 10 μl 씩 채취하고, 1주일 후 다시 10 μl을 채취한 후 UV 흡광도를 이용하여 CHX의 방출 속도를 비교하였다. 실험결과 제어방출형 근관소독제로부터 CHX의 방출속도는 대조군, 키토산, PLGA, PMMA-군 순으로 천천히 일어났으며 PMMA군에서 가장 천천히 일어났다. 결론적으로 제어방출형 근관소독제 표면의 폴리머는 약물 (CHX) 방출속도를 효과적으로 제어하였다.