• 약학회지
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• 제40권3호
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• pp.343-346
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• 1996

The influence of LB20304a, a new fluoroquinolone antibiotic agent, on microflora of caecum in mice was compared with those of ciprofloxacin and piperacillin after administration of drugs for 5 days. Selective medium (CCFMA) was used for the isolation of Clostridium difficile from the specimens of mouse caecum. The emergence of C. difficile in mouse caecum induced by LB20304a was lower than that by ciprofloxacin or piperacillin at day 1 and day 7 after completing administration of drugs.

• Archives of Pharmacal Research
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• 제19권5호
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• pp.359-367
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• 1996

The pharmacokinetics of LB20304 was investigated following intravenous (IV) and oral administration to rats and dogs. Additionally, in vitro metabolism and serum protein binding studies were also conducted. The total body clearance, apparent volume of distribution, terminal half-life, and extent of bioavailability were 21.8 ml/min/kg, 2265 ml/kg, 93.6 min, and 30.8% for rats; and 7.95 ml/min/kg, 4144 ml/kg, 363 min, and 81.1% for dogs, respectively. LB20304 was stable in the liver microsome containing NADPH generating system and its serum protein binding was 58.5-65.8% for rats, 19.1-29.6% for dogs, and 56.9-59.6% for humans. Its tissue concentration levels in lever, stomach, small intestine, and kidney were 9.5 to 26.1 times greater than plasma level, but the concentration in testis was quite low and that in brain was negligible in rats. The 48 hr urinary recovery of the dose was 44% for IV dosing and 14% for oral dosing, shereas the 48 hr biliary recovery of the dose was 6.4% for IV dosing and 4.5% for oral dosing in rats. In summary, the pharmacokinetic properties of LB20304 were characterized by its good oral absorption, long plasma half-life, and good tissue distribution.

• 대한약학회:학술대회논문집
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• 대한약학회 2000년도 춘계총회 및 학술대회
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• pp.64-65
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• 2000

• Archives of Pharmacal Research
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• 제19권6호
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• pp.554-558
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• 1996

High-performance liquid chromatographic method was developed for the determination or LB 20304 (compound 1) in the plasma of rats and dogs. The analyte was deproteinized with 1 volume of methanol and 1/2 volume of 10% zinc sulfate, and the supernatant was injected onto a reversed-phase HPLC column. The mobile phase was a mixture of 24 parts of acetonitrile and 76 parts of 0.1% trifluoroacetic acid. The flow rate was 1 ml/min, and the effluent was monitored by fluorescence detector at an excitation wavelength of 337 nm and an emission wavelength of 460 nm. The retention time of compound 1 was 6.3 min. The assay of compound 1 was linear over the concentration range of 0.2-100.mu.g/ml in the plasma of rats and dogs. The lower limit of quantification was 0.2.mu.g/ml using 100.mu.l of plasma with a 97-99% accuracy and a 12-14% precision. In the 0.5, 5, and 50.mu.g/ml quality control samples, the intra- and inter-day accuracy were 88-95% and 88-97%, whereas intra- and interday precision were 0.5-6.6% and 0.2-9.3%, respectively, in the plasma of rats and dogs. The recoveries were 68-71% independent of concentration and species in the plasma. No interferences from endogenous substances were observed. Taken together, the above HPLC assay method by deproteinization and fluorescence detection was suitable for the determination of compound 1 in the preclinical pharmacokinetics.

• 한국응용약물학회:학술대회논문집
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• 한국응용약물학회 1997년도 춘계학술대회
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• pp.6-11
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• 1997

• 지식경영연구
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• 제2권1호
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• pp.109-132
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• 2001

The purpose of this article is to develop a dynamic model of organizational capabilities and knowledge creation, and at the same time identify the organizational capability factors for effective knowledge creation, by empirically analyzing the history of new Quinolone antibacterial drug compound (LB20304a) discovery process at LG, as a case in point. Major findings of this study are as follows. First, in a science-based area such as drug development, the core of successful knowledge creation lies in creative combination of different bodies of scientific explicit knowledge. Second, the greater the difficulty of learning external knowledge, the more tacit knowledge is needed for the recipient firm to effectively exploit that knowledge. Third, in science-based sector such as pharmaceutical industry, the key for successful knowledge creation lies in the capability of recruiting and retaining star scientists. Finally, for effective knowledge creation, a firm must keep its balance among three dimensions of organizational capabilities: local, process, architectural capabilities.

• Tuberculosis and Respiratory Diseases
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• 제55권1호
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• pp.69-87
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• 2003

배 경 : Gemifloxacin은 그람음성 및 그람양성 균주에 대해서 모두 좋은 활성을 가지고 있는 fluoroquinolone 항균제로서, 임상균주를 이용한 in vitro 시험에서 다른 대조 quinolone에 비하여 S. pneumnoniae의 penicillin 내성 균주에 대해서 활성이 높을 뿐만 아니라, 다른 quinolone 항균제에 내성을 나타내는 S. pneumoniae 임상 균주에 대해서도 좋은 활성을 유지하는 것으로 밝혀져 만성기관지염의 급성악화(AECB)시 사용하기 적절한 치료제로 여겨진다. 목 적 : 한국인에서 AECB를 치료하기 위한 LB20304(gemifloxacin) 160mg 또는 320rng 1일 1회 7일간 투여의 유효성과 안전성을 평가하고자 하였다. 방 법 : Gemifloxacin 100mg과 위약을 1일 1회 7일간 경구 투여한 환자 67명, gemifloxacin 320mg을 1일 1회 7일간 경구 투여한 환자 70명의 환자를 대상으로 무작위 배정, 이중맹검, 병행 치료군, 다기관, 2상 임상시험으로 실시하였다. 결 과 : 두 치료군의 인구통계학적 특징과 임상적 및 흡연 기왕력 등 기저 상태는 대등하였다. Per-protocol(PP) 환자군에서, 추적관찰 시점(days 14-21) 및 치료종료 시점(days 7-10)에서의 임상적 반응은 gemifloxacin 100mg군이 각각 84.2%, 96.5%, 320mg군이 각각88.7%, 96.4%로 두 군간에 유의한 사이가 없었고(각각 p=0.49, p=0.99), 추적관찰 시점 및 치료종료 시점의 미생물학적 반응도 gemifloxacin 160mg군이 각각 78.9%, 81.8%, 320mg군이 각각 84.2%, 86.4%로 두 군간에 유의한 차이가 없었다(각각 p=0.68, p=0.68) 본 임상시험에서 치료 전에 많이 배양된 병원균으로는 S. pneumoniae(12/52), H. influenzae(10/52), K. pneumoniae(6/52), M. catarrhalis(3/52) 로 K. pneumoniae가 비교적 많이 배양된 점을 제외하고는 기존에 알려진 AECB 시 배양되는 병원균의 분포와 큰 차이가 없었다. S. pneumoniae, H. influenzae, K. pneumoniae, M. catarrhalis 등 주요 병원 균에 대한 MIC는 전반적으로 다른 quinolone 항균제보다 gemifloxacin이 더 낮았고, 특히 S. pneumoniae(3 PRSP, 7 ERSP 포함)에 대한 gemifloxacin의 MIC(${\leq}0.03ug/ml$)는 다른 quinolone, beta-lactam, macrolide 항균제보다 월등히 낮아 gemifloxacin 이 AECB의 치료에 매우 유용한 항균제임을 보여주었다. 안전성 결과에서는 gemifloxacin 160mg 및 320mg 투여군 모두 시험약과의 관련성을 배제할 수 없거나 관련이 의심되는 중대한 이상반용은 관찰되지 않았고, 치료 중 및 치료 후 30일 기간동안, 이상반응을 최소한 하나 이상 보고한 환자가 gemifloxacin 160mg군은 26.9%, 320mg군은 31.4%이었다. 가장 흔히 보고된 이상반응은 간효소 수치의 증가로서, 발생 빈도는 160mg군에서 1/67명(1.5%), 320mg군에서 5/70명(7.1%) 이었다. 간효소 수치의 증가로 인해 탈락한 환자는 없었고, 중증도(severity)는 모두 경도(mild)였으며, 별다른 처치 없이 정상으로 회복되었다. 전반적인 이상반응의 profile에서 치료군간 주요한 차이는 없었다. 결 론 : 본 임상시험의 결과, 한국인에서 AECB를 치료하기 위한 gemifloxacin 160mg 또는 320mg 1일 1회 7일간의 투여는 임상적 및 미생물학적으로 매우 유효하고 안전하였다.