• 한국미생물·생명공학회지
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• 제28권4호
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• pp.223-227
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• 2000

A novel two-step acetone treatment method was developed to enhance the enantioselectivity of Candida rugosa lipase (CRL) toward the hydrolysis of racemic naproxen methyl ester. The acetone-teated CRL was considerably more enantioselective than the crude CRL, yielding an enantiomeric excess of 98~100%. The crude and acetone-treated CRLs were subjected to anion exchange chromatography, and their chromatography profiles were compared. In consequence, both chromatography profiles were found to be almost identical, resulting in two separate lipase peaks (lipase A and B). The lipase B, which is known to be less enantioselective, was treated with acetone using a two-step treatment method. The enantioselectivity of acetone-treated lipase B was dramatically increased, yielding an enantiomeric excess of 99%.

• 약학회지
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• 제30권3호
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• pp.128-138
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• 1986

Three newly synthesized alkanol esters of d-2-(6-methoxy-2-naphthyl) propionic acid, NAPROXEN were examined for physicochemical properties and biopharmaceutical characteristics. These esters were very stable in solid state, but more than 90% of these esters were hydrolysed to the parent, naproxen in rabbit's liver hornogenates. They showed higher dissolution rate in the artificial gastric and intestinal juice, and significantly greater partition coefficient in n-octanol, when compared with naproxen. The absorption rate constants of these esters were increased, while the elimination rate constants were decreased, comparing with naproxen. The ulcerogenic doses on gastric and intestinal mucosa were increased remarkably, and the antiinflammatory dose against carrageenininduced edema on rat hind paw was decreased markedly in these esters, and thus the safety indexes of these esters were higher than that of naproxen.

• 대한화학회지
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• 제58권2호
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• pp.179-185
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• 2014

시판되는 (S)-naproxen을 강염기 조건에서 라세미화하였다. 라세미화된 naproxen 시료를 분석하여 (R)- 및 (S)-naproxen의 피이크 위치를 확인한 후, 2013년 국내에서 시판된 19개 naproxen의 광학순도를 키랄 HPLC로 조사하였다. Chiralcel OD-H 칼럼과 ChiralHyun-LE(S)-1 칼럼 및 LUX-Cellulose-1 칼럼을 키랄 정지상으로 사용하였고, hexane:isopropanol:acetic acid가 100:1:0.1로 혼합된 용액을 전개용매로 사용하여 흐름속도 1.0 mL/min에서 분석하였다. 각 시료를 최소 3회 이상 분석하여 얻은 평균값을 각각 계산하여 데이터로 이용하였고, 이들의 상대표준편차도 계산하여 그 값이 아주 작게 나타난 것을 확인하였다. 세 종류의 다른 칼럼에서 각각 측정한 광학순도 값이 서로 아주 유사한 값을 보여주었으며, 측정된 naproxen의 광학순도는 이들의 광학순도 데이터가 처음 보고된 2010년 시료의 광학순도 평균값인 98.17%에 비해 높은 99.32%를 보였다.

• 약학회지
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• 제49권1호
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• pp.1-5
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• 2005

Near-infrared (NIR) spectroscopy has been widely applied in various field, since it is nondestructive and no sample preparation is required. In this paper, NIR spectroscopy was used for the determination of naproxen in a commercial pharmaceutical preparation. NIR spectroscopy was used to determine the content of naproxen in intact naproxen tablets containing 250 mg ($65.8\%$ nominal concentration) by collecting NIR spectra in the range of $1100{\sim}1750nm$. The laboratory-made samples had $46.1{\sim}85.5\%$ nominal naproxen concentration. The measurements were made by reflection using a fiber-optic probe and calibration was carried out by partial least square regression (PLSR). Model validation was performed by randomly splitting the data set into calibration and validation data set (63 samples as a calibration data set and 42 samples as a validation data set). The developed NIR calibration gave results comparable to the known values of tablets in a laboratorial manufacturing process with standard error of calibration (SEC) and standard error of prediction (SEP) of $1.06\%\;and\;1.04\%$, respectively. The NIR method showed good accuracy and repeatability. NIR spectroscopic determination in intact tablets allowed the potential use of real time monitoring for a running production process.

• Journal of Microbiology and Biotechnology
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• 제19권12호
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• pp.1596-1602
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• 2009

A lipase-catalyzed esterification reaction of (S)-naproxen ethyl ester by CALB (Candida antarctica lipase B) enzyme was performed in supercritical carbon dioxide. Experiments were performed in a high-pressure cell for 10 h at a stirring rate of 150 rpm over a temperature range of 313.15 to 333.15 K and a pressure range of 50 to 175 bar. The productivity of (S)-naproxen ethyl ester was compared with the result in ambient condition. The total reaction time and conversion yields of the catalyzed reaction in supercritical carbon dioxide were compared with those at ambient temperature and pressure. The experimental results show that the conversion and reaction rate were significantly improved at critical condition. The maximum conversion yield was 9.9% (216 h) at ambient condition and 68.9% (3 h) in supercritical state. The effects of varying amounts of enzyme and water were also examined and the optimum condition was found (7 g of enzyme and 2% water content).

• Journal of Pharmaceutical Investigation
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• 제29권4호
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• pp.343-348
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• 1999

The purpose of this study is to prepare the controlled release adhesive patch containing naproxen. Pressuresensitive adhesive (PSA)-type patch was fabricated by casting of polyisobutylene (PIE.) and mineral oil in toluene. Membrane-controlled release (MCR)-type patch was prepared by the attachment of the controlled release membrane on the PSAtype patch. The membrane was mainly composed of Eudragit, polyethylene glycol(PEG) and glycerin. The drug release profile and skin permeation test with various patches were evaluated in vitro. The release of naproxen from PIE-based PSAtype patch with various loading doses fitted Higuchi's diffusion equation. However, the permeation of naproxen through hairless mouse skin from PSA-type patch followed zero-order kinetics. In MCR-type patch, thickness of controlled release membrane affected on the drug release rate highly. In the composition of membrane, the release rate was decreased as the ratio of Eudragit increased. The drug release from the MCR-type patch followed zero order kinetics. The permeation of naproxen through hairless mouse skin from MCR-type patch showed lag time for the intial release period and didn't fit the zero-order kinetics

• KSBB Journal
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• 제23권3호
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• pp.257-262
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• 2008

본 연구에서는 lipase를 이용한 라세믹-naproxen 2,2,2-trifluoroethyl thioester의 광학분할 반응을 향상시키기 위하여 반응 용매, 반응 온도, 기질 및 lipase 농도 그리고 교반속도의 변수들을 최적화 하였고, isooctane과 물의 계변을 증가시키기 위한 계면 활성제의 영향을 조사하였다. 조사된 유기용매 중 isooctane이 가장 높은 전환율 (92.19%), $V_s\;(2.340{\times}10^{-2}mM/h)$, E값 (36.12) 그리고 $V_s/(E_t)$ ($7.80{\times}10^{-4}mmol/h{\cdot}g$)를 나타내어 lipase 를 이용한 라세믹-naproxen2,2,2-trifluoroethyl thioester의 광학 분할 반응을 위한 가장 효과적인 유기용매로 판단하였다. 반응 표면 분석법을 이용한 반응조건 최적화에서는 반응 온도 $48.2^{\circ}C$, 기질 농도 3.51 mM, lipase 농도 30.11 mg/ml 그리고 교반속도 180 rpm을 최적 반응 조건으로 도출하였고, 이 최적화된 반응 조건으로 광학분할 반응을 수행한 결과, $V_s$, $V_s/(E_t)$ 그리고 전환 율이 각각 19.54%, 19.12%, 4.05% 증가하였다. 계면활성제로써 첨가된 NP-10은 (S)-naproxen 2,2,2-trifluoroethyl thioester의 가장 높은 전환율 (89.43%)을 나타내었고, 반응속도의 감소를 둔화시켰으며, lipase의 광학선택성 (E=59.24)을 향상시켰다.

• Bulletin of the Korean Chemical Society
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• 제18권10호
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• pp.1085-1089
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• 1997

A new HPLC chiral stationary phase (CSP 3) has been prepared by connecting N-phenyl N-propyl amide of (S)-naproxen to silica gel through the 6-methoxy-2-naphthyl group of (S)-naproxen. The new CSP has been applied in resolving a homologous series of N-(3,5-dinitrobenzoyl)-α-amino acid esters and a homologous series of N-(3,5-dinitrobenzoyl)-α-(4-alkylphenyl)alkylamines. The separation factors, α, for resolving a homologous series of N-(3,5-dinitrobenzoyl)-α-amino esters and a homologous series of N-(3,5-dinitrobenzoyl)-α-(4-alkylphenyl)alkylamines on the new CSP have been found to remain almost constant throughout the wide range of the length of the alkyl substituent of the analytes while those on the previously reported CSPs (CSP 1 and 2) which were prepared by connecting N-phenyl N-propyl amide of (S)-naproxen to silica gel through the N-propyl group increase or decrease continuously. These results are concluded to support the chiral recognition models which utilize the intercalation of the alkyl substituent of the racemic analytes between the adjacent strands of CSP 1 or 2 to rationalize the increasing or decreasing trends of separation factors.

• Bulletin of the Korean Chemical Society
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• 제16권10호
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• pp.977-980
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• 1995

A new chiral stationary phase (CSP 2) derived from cyclohexylamide of (S)-naproxen has been prepared. CSP 2 has shown greater enantioselectivities for the two enantiomers of N-(3,5-dinitrobenzoyl)-a-amino esters and amides than the CSP derived from 3,5-dimethylanilide of (S)-naproxen (CSP 1) as expected from the reciprocity conception of chiral recognition. However, CSP 2 has been found to be worse than CSP 1 in resolving N-(3,5-dinitrobenzoyl)-a-arylalkylamines, supporting the previously proposed chiral recognition mechanism which utilizes the 3,5-dimethylphenyl group of CSP 1 as an alternative π-basic interaction site. In addition, CSP 2 has been found to be reasonably good in resolving the two enantiomers of a variety of other π-acidic racemates.

• Bulletin of the Korean Chemical Society
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• 제16권4호
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• pp.344-348
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• 1995

As an effort to elucidate the chiral recognition mechanisms exerted by the (S)-naproxen-derived CSP bearing both π-acidic and π-basic sites, a homologues series of π-basic N-acyl-α-(1-naphthyl)alkylamines and π-acidic N-(3,5-dinitrobenzoyl)-α-amino esters were prepared and resolved. Based on the chromatographic resolution trends of the homologues series of analytes on the (S)-naproxen-derived chiral stationary phase, we proposed chiral recognition mechanisms which demonstrate that the intercalation of the substituent in the analyte molecule between the strands of bonded phase does significantly influence the enantioselectivity for resolving N-acyl-α-(1-naphthyl)alkylamines but the intercalation process is not involved in resolving N-(3,5-dinitrobenzoyl)-α-amino esters.