Disposition of KW-4679(4): Metabolism of KW-4679 in Rats and Dogs
The metabolism of KW-4679 was investigated in rats and dogs after oral administration of 14C-KW-4679 or KW-4679. 1) After oral administration to rats, N-mono-demethyl-KW-4679 (Ml), N-di-demethyl-KW-4679 (M2), KW-4679 N-oxide (M3), C8-hydroxyl-KW-4679 (M5), M5 sulfate (M4) and oxidated M5 (M6) were i...
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| Published in | Drug Metabolism and Pharmacokinetics Vol. 10; no. 5; pp. 689 - 706 |
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| Main Authors | , , , , , |
| Format | Journal Article |
| Language | English |
| Published |
The Japanese Society for the Study of Xenobiotics
1995
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| Subjects | |
| Online Access | Get full text |
| ISSN | 0916-1139 |
| DOI | 10.2133/dmpk.10.689 |
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| Abstract | The metabolism of KW-4679 was investigated in rats and dogs after oral administration of 14C-KW-4679 or KW-4679. 1) After oral administration to rats, N-mono-demethyl-KW-4679 (Ml), N-di-demethyl-KW-4679 (M2), KW-4679 N-oxide (M3), C8-hydroxyl-KW-4679 (M5), M5 sulfate (M4) and oxidated M5 (M6) were identified as the metabolites of KW-4679 in bile in addition to unchanged KW-4679. 2) When 14C-KW-4679 was orally administered to fasting male rats, 66.4% of radioactivity detected in plasma at 0.5 hr after administration, accounted for the unchanged KW-4679. The main metabolite in plasma was M1 (7.7%). In urine, also, radioactivity was present mainly as the unchanged KW-4679, which represented 27.3% of dose. The main metabolite excreted in urine was M1 (6.0%) followed by M6, M5, M2, M3 and then by M4. The main metabolite in bile was M6 followed by M4 and then by the unchanged KW-4679. In feces, 19.4% of administered radioactivity was excreted as the unchanged KW-4679. The main metabolite in feces was M5 (5.1%) followed by M6, M1, M4, M2 and then by M3. 3) After oral administration to fasting female rats, the unchanged KW-4679 was a main component of radioactivity excreted in urine, same as in male rats. 4) When 14C-KW-4679 was orally administered to fasting male dogs, 71.1% of radioactivity detected in plasma at 0.5 hr after administration was the unchanged KW-4679. The main metabolite in plasma was M3 (11.0%). The major component in urine was the unchanged KW-4679 (51.6%) followed by M1 (4.5%), M3, M5, M2, M6 and then by M4. KW-4679 was the major component excreted also in feces, representing 6.0% of dose followed by M5, Ml, M6, M4 and then by M2. 5) The metabolic pathway of KW-4679 in rats and dogs consisted of oxidative N-demethylation of the side chain and hydroxylation of dibenzoxepine ring and its sulfation and further oxidation of N-atom in the side chain. |
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| AbstractList | The metabolism of KW-4679 was investigated in rats and dogs after oral administration of 14C-KW-4679 or KW-4679. 1) After oral administration to rats, N-mono-demethyl-KW-4679 (Ml), N-di-demethyl-KW-4679 (M2), KW-4679 N-oxide (M3), C8-hydroxyl-KW-4679 (M5), M5 sulfate (M4) and oxidated M5 (M6) were identified as the metabolites of KW-4679 in bile in addition to unchanged KW-4679. 2) When 14C-KW-4679 was orally administered to fasting male rats, 66.4% of radioactivity detected in plasma at 0.5 hr after administration, accounted for the unchanged KW-4679. The main metabolite in plasma was M1 (7.7%). In urine, also, radioactivity was present mainly as the unchanged KW-4679, which represented 27.3% of dose. The main metabolite excreted in urine was M1 (6.0%) followed by M6, M5, M2, M3 and then by M4. The main metabolite in bile was M6 followed by M4 and then by the unchanged KW-4679. In feces, 19.4% of administered radioactivity was excreted as the unchanged KW-4679. The main metabolite in feces was M5 (5.1%) followed by M6, M1, M4, M2 and then by M3. 3) After oral administration to fasting female rats, the unchanged KW-4679 was a main component of radioactivity excreted in urine, same as in male rats. 4) When 14C-KW-4679 was orally administered to fasting male dogs, 71.1% of radioactivity detected in plasma at 0.5 hr after administration was the unchanged KW-4679. The main metabolite in plasma was M3 (11.0%). The major component in urine was the unchanged KW-4679 (51.6%) followed by M1 (4.5%), M3, M5, M2, M6 and then by M4. KW-4679 was the major component excreted also in feces, representing 6.0% of dose followed by M5, Ml, M6, M4 and then by M2. 5) The metabolic pathway of KW-4679 in rats and dogs consisted of oxidative N-demethylation of the side chain and hydroxylation of dibenzoxepine ring and its sulfation and further oxidation of N-atom in the side chain. |
| Author | YASUZAWA, Tohru YAMAGUCHI, Kazuo OHISHI, Takayoshi MAGARA, Hiroshi KOBAYASHI, Satoshi KOBAYASHI, Hiroyuki |
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| References | 5) 大石孝義,西家弘佳,小林弘幸,小林 智: 新規抗アレルギー薬 KW-4679 の体内動態(第3報) 14C-KW-4679 のイヌにおける経口投与後の吸収および排泄.薬物動態,10(5): 683-688 (1995 3) Ohmori, K., Ishii, H., Ikemura, T., Shirakura, R. and Kitamura, S.: Inhibitory effect of KW-4679 on antigen-induced late asthmatic responses and airway inflammation in guinea pigs. Eur. Resp. J., 6(Suppl): 17, 318S (1993 1) Ishii, H., Manabe, H., Sasaki, Y., Satoh, H., Tamura, T. and Ohmori, K.: Pharmacological properties of a new antiallergic agent KW-4679. Jpn J. Pharmacol., 46(Suppl.): 284 (1988 6) 乗原隆,大石孝義,池永哲二,西家弘佳,佐藤 隆,小林弘幸,小林 智: 新規抗アレルギー薬 KW-4679 の体内動態(第6報)各種実験動物における血漿中動態.薬物動態,10(5): 722-735 (1995 2) Ohshima, E., Otaki, S., Sato, H., Kumazawa, T., Obase, H., Ishii, A., Ishii, H., Ohmori, K. and Hirayama, N.: Synthesis and antiallergic activity of 11-(aminoalkylidene)-6,11-dihydrodibenz[b,e] oxepin derivatives. J. Med. Chem., 35: 2074-2084 (1992 4) 大石孝義,西家弘佳,小林弘幸,小林 智: 新規抗アレルギー薬 KW-4679 の体内動態(第1報) 14C-KW-4679 のラットにおける単回投与時の吸収,分布および排泄.薬物動態,10(5): 651-668 (1995 |
| References_xml | – reference: 3) Ohmori, K., Ishii, H., Ikemura, T., Shirakura, R. and Kitamura, S.: Inhibitory effect of KW-4679 on antigen-induced late asthmatic responses and airway inflammation in guinea pigs. Eur. Resp. J., 6(Suppl): 17, 318S (1993) – reference: 4) 大石孝義,西家弘佳,小林弘幸,小林 智: 新規抗アレルギー薬 KW-4679 の体内動態(第1報) 14C-KW-4679 のラットにおける単回投与時の吸収,分布および排泄.薬物動態,10(5): 651-668 (1995) – reference: 5) 大石孝義,西家弘佳,小林弘幸,小林 智: 新規抗アレルギー薬 KW-4679 の体内動態(第3報) 14C-KW-4679 のイヌにおける経口投与後の吸収および排泄.薬物動態,10(5): 683-688 (1995) – reference: 6) 乗原隆,大石孝義,池永哲二,西家弘佳,佐藤 隆,小林弘幸,小林 智: 新規抗アレルギー薬 KW-4679 の体内動態(第6報)各種実験動物における血漿中動態.薬物動態,10(5): 722-735 (1995) – reference: 2) Ohshima, E., Otaki, S., Sato, H., Kumazawa, T., Obase, H., Ishii, A., Ishii, H., Ohmori, K. and Hirayama, N.: Synthesis and antiallergic activity of 11-(aminoalkylidene)-6,11-dihydrodibenz[b,e] oxepin derivatives. J. Med. Chem., 35: 2074-2084 (1992) – reference: 1) Ishii, H., Manabe, H., Sasaki, Y., Satoh, H., Tamura, T. and Ohmori, K.: Pharmacological properties of a new antiallergic agent KW-4679. Jpn J. Pharmacol., 46(Suppl.): 284 (1988) |
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| Title | Disposition of KW-4679(4): Metabolism of KW-4679 in Rats and Dogs |
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