CLINICAL STUDIES OF T-3262 IN RESPIRATORY INFECTION
We clinically evaluated T-3262, a pyridone-carboxylic acid derivative, in respiratory infection. The subjects were 12 cases: bronchopneumonia 4, diffuse panbronchiolitis 3, acute bronchitis 2 and 1 each of acute exacerbation of chronic bronchitis, bacterial pyothorax and pharyngitis. Causative organ...
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| Published in | CHEMOTHERAPY Vol. 36; no. Supplement9-Clinical; pp. 413 - 417 |
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| Main Authors | , , |
| Format | Journal Article |
| Language | Japanese |
| Published |
Japanese Society of Chemotherapy
20.12.1988
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| Online Access | Get full text |
| ISSN | 0009-3165 1884-5894 |
| DOI | 10.11250/chemotherapy1953.36.Supplement9-Clinical_413 |
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| Abstract | We clinically evaluated T-3262, a pyridone-carboxylic acid derivative, in respiratory infection. The subjects were 12 cases: bronchopneumonia 4, diffuse panbronchiolitis 3, acute bronchitis 2 and 1 each of acute exacerbation of chronic bronchitis, bacterial pyothorax and pharyngitis. Causative organisms were 3 strains of Pseudomonas aeruginosa, 2 of Haemophilus influenzae, one each of Streptococcus pneumoniae, Streptococcus aureus, Klebsiella sp., Haemophilus parainfluenzae, Acinetobacter and Enterobacter cloacae. Two cases were superinfected and three were found with normal flora. The daily dose was 450-900 mg, and the duration of the trial was 7-42 days (mean, 20.6 days). The total dose was 3.15-21.0g and the mean was 11.7g. The bacteriological results were eradication in 5 cases, colonization in 1, and persistent infection in 2 of diffuse panbronchiolitis due to P. aeruginosa. Clinical efficacy was excellent in 2 cases (16.7%), good in 5 (41.7%), fair in 2 (16.7%) and poor in 3 (25.0%). Vomiting and upper abdominal pain was observed in one case each. For evaluation of drug transfer to sputum, 300 mg of T-3262 was administered to 2 cases of diffuse panbronchiolitis. Maximum sputum concentration was observed at 3 or 6 h at a concentration of 0.25 or 0.16μg/ml, which was 30% or 42% of that in serum. Our data showed that transfer of T-3262 into sputum was relatively good. |
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| AbstractList | We clinically evaluated T-3262, a pyridone-carboxylic acid derivative, in respiratory infection. The subjects were 12 cases: bronchopneumonia 4, diffuse panbronchiolitis 3, acute bronchitis 2 and 1 each of acute exacerbation of chronic bronchitis, bacterial pyothorax and pharyngitis. Causative organisms were 3 strains of Pseudomonas aeruginosa, 2 of Haemophilus influenzae, one each of Streptococcus pneumoniae, Streptococcus aureus, Klebsiella sp., Haemophilus parainfluenzae, Acinetobacter and Enterobacter cloacae. Two cases were superinfected and three were found with normal flora. The daily dose was 450-900 mg, and the duration of the trial was 7-42 days (mean, 20.6 days). The total dose was 3.15-21.0g and the mean was 11.7g. The bacteriological results were eradication in 5 cases, colonization in 1, and persistent infection in 2 of diffuse panbronchiolitis due to P. aeruginosa. Clinical efficacy was excellent in 2 cases (16.7%), good in 5 (41.7%), fair in 2 (16.7%) and poor in 3 (25.0%). Vomiting and upper abdominal pain was observed in one case each. For evaluation of drug transfer to sputum, 300 mg of T-3262 was administered to 2 cases of diffuse panbronchiolitis. Maximum sputum concentration was observed at 3 or 6 h at a concentration of 0.25 or 0.16μg/ml, which was 30% or 42% of that in serum. Our data showed that transfer of T-3262 into sputum was relatively good. |
| Author | KAWAI, TAKESHI TOYODA, TAKEO ONAKA, AKIO |
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| References | 2) 河合健, 尾仲章男, 味澤篤, 加茂隆, 内田博: 呼吸器感染症に対するカルパペネム系抗生剤Imipenem/Cilastatin sodiumの基礎的ならびに臨床的研究. Chemotherapy 33 (S-4): 470-475, 1985 1) 勝正孝, 松岡康夫: 合成抗菌剤. 臨床成人病, 17: 108-115, 1987 3) 第34回日本化学療法学会東日本支部総会, 新薬シンポジウム. T-3262, 東京, 1987 |
| References_xml | – reference: 1) 勝正孝, 松岡康夫: 合成抗菌剤. 臨床成人病, 17: 108-115, 1987 – reference: 2) 河合健, 尾仲章男, 味澤篤, 加茂隆, 内田博: 呼吸器感染症に対するカルパペネム系抗生剤Imipenem/Cilastatin sodiumの基礎的ならびに臨床的研究. Chemotherapy 33 (S-4): 470-475, 1985 – reference: 3) 第34回日本化学療法学会東日本支部総会, 新薬シンポジウム. T-3262, 東京, 1987 |
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| Title | CLINICAL STUDIES OF T-3262 IN RESPIRATORY INFECTION |
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